Your search keyword '"Norberto Guelbert"' showing total 70 results

1. Corrigendum to 'Classic and atypical late infantile neuronal ceroid lipofuscinosis in Latin America: Clinical and genetic aspects, and treatment outcome with cerliponase alfa.' [Molecular Genetics and Metabolism ReportsVolume 38 (2024) 101060]

Author

Norberto Guelbert, Oscar Mauricio Espitia Segura, Carolina Amoretti, Angélica Arteaga Arteaga, Nora Graciela Atanacio, Natacha Sabrina Bazan, Ellaine Doris Fernandes Carvalho, Maria Denise Fernandes Carvalho de Andrade, Inés María Denzler, Consuelo Durand, Erlane Ribeiro, Juan Carlos Giugni, Gabriel González, Dolores González Moron, Guillermo Guelbert, Zulma Janneth Hernández Rodriguez, Katiane Embiruçu Emilia, Marcelo Andrés Kauffman, Nury Isabel Mancilla, Laureano Marcon, Alessandra Marques Pereira, Carolina Fischinger Moura de Souza, Victor Adrián Muñoz, Ricardo Andrés Naranjo Flórez, André Luiz Pessoa, María Victoria Ruiz, Martha Luz Solano Villareal, Norma Spécola, Lina Marcela Tavera, Javiera Tello, Mónica Troncoso Schifferli, Sonia Ugrina, María Magdalena Vaccarezza, Diane Vergara, and María Mercedes Villanueva

Subjects

Medicine (General), R5-920, Biology (General), QH301-705.5

Published

2024

2. Classic and Atypical Late Infantile Neuronal Ceroid Lipofuscinosis in Latin America: Clinical and Genetic Aspects, and Treatment Outcome with Cerliponase Alfa

Author

Norberto Guelbert, Oscar Mauricio Espitia Segura, Carolina Amoretti, Angélica Arteaga Arteaga, Nora Graciela Atanacio, Sabrina Bazan Natacha, Ellaine Doris Fernandes Carvalho, Maria Denise Fernandes Carvalho de Andrade, Inés María Denzler, Consuelo Durand, Erlane Ribeiro, Juan Carlos Giugni, Gabriel González, Dolores González Moron, Guillermo Guelbert, Zulma Janneth Hernández Rodriguez, Katiane Embiruçu Emilia, Marcelo Andrés Kauffman, Nury Isabel Mancilla, Laureano Marcon, Alessandra Marques Pereira, Carolina Fischinger Moura de Souza, Victor Adrián Muñoz, Ricardo Andrés Naranjo Flórez, André Luiz Pessoa, María Victoria Ruiz, Martha Luz Solano Villareal, Norma Spécola, Lina Marcela Tavera, Javiera Tello, Mónica Troncoso Schifferli, Sonia Ugrina, María Magdalena Vaccarezza, Diane Vergara, and María Mercedes Villanueva

Subjects

Batten disease, Enzyme replacement therapy, Epilepsy, Language delay, Ataxia, Cerliponase alfa, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Introduction: Late infantile neuronal ceroid lipofuscinosis type 2 (CLN2), is a neurodegenerative autosomal recessive disease caused by TPP1 gene variants, with a spectrum of classic and atypical phenotypes. The aim of treatment is to slow functional decline as early as possible in an attempt to improve quality of life and survival. This study describes the clinical characteristics as well as the response to treatment with cerliponase alfa. Materials and methods: A retrospective study was conducted in five Latin-American countries, using clinical records from patients with CLN2. Clinical follow-up and treatment variables are described. A descriptive and bivariate statistical analysis was performed. Results: A total of 36 patients were observed (range of follow-up of 61–110 weeks post-treatment). At presentation, patients with the classic phenotype (n = 16) exhibited regression in language (90%), while seizures were the predominant symptom (87%) in patients with the atypical phenotype (n = 20). Median age of symptom onset and time to first specialized consultation was 3 (classical) and 7 (atypical) years, while the median time interval between onset of symptoms and treatment initiation was 4 years (classical) and 7.5 (atypical). The most frequent variant was c.827 A > T in 17/72 alleles, followed by c.622C > T in 6/72 alleles. All patients were treated with cerliponase alfa, and either remained functionally stable or had a loss of 1 point on the CLN2 scale, or up to 2 points on the Wells Cornel and Hamburg scales, when compared to pretreatment values. Discussion and conclusion: This study reports the largest number of patients with CLN2 currently on treatment with cerliponase alfa in the world. Data show a higher frequency of patients with atypical phenotypes and a high allelic proportion of intron variants in our region. There was evidence of long intervals until first specialized consultation, diagnosis, and enzyme replacement therapy. Follow-up after the initiation of cerliponase alfa showed slower progression or stabilization of the disease, associated with adequate clinical outcomes and stable functional scores. These improvements were consistent in both clinical phenotypes.

Published

2024

3. Neuronal ceroid lipofuscinosis in the South American-Caribbean region: An epidemiological overview

Author

Guillermo Guelbert, Ana Clara Venier, Ines Adriana Cismondi, Adriana Becerra, Juan Carlos Vazquez, Elmer Andrés Fernández, Ana Lucía De Paul, Norberto Guelbert, Ines Noher, and Favio Pesaola

Subjects

neuronal ceroid lipofuscinoses (NCL), South America-Caribbean, epidemiology, genotype, phenotype, Neurology. Diseases of the nervous system, RC346-429

Abstract

Neuronal ceroid lipofuscinoses (NCLs) comprise 13 hereditary neurodegenerative pathologies of very low frequency that affect individuals of all ages around the world. All NCLs share a set of symptoms that are similar to other diseases. The exhaustive collection of data from diverse sources (clinical, genetic, neurology, ophthalmology, etc.) would allow being able in the future to define this group with greater precision for a more efficient diagnostic and therapeutic approach. Despite the large amount of information worldwide, a detailed study of the characteristics of the NCLs in South America and the Caribbean region (SA&C) has not yet been done. Here, we aim to present and analyse the multidisciplinary evidence from all the SA&C with qualitative weighting and biostatistical evaluation of the casuistry. Seventy-one publications from seven countries were reviewed, and data from 261 individuals (including 44 individuals from the Cordoba cohort) were collected. Each NCL disease, as well as phenotypical and genetic data were described and discussed in the whole group. The CLN2, CLN6, and CLN3 disorders are the most frequent in the region. Eighty-seven percent of the individuals were 10 years old or less at the onset of symptoms. Seizures were the most common symptom, both at onset (51%) and throughout the disease course, followed by language (16%), motor (15%), and visual impairments (11%). Although symptoms were similar in all NCLs, some chronological differences could be observed. Sixty DNA variants were described, ranging from single nucleotide variants to large chromosomal deletions. The diagnostic odyssey was probably substantially decreased after medical education activities promoted by the pharmaceutical industry and parent organizations in some SA&C countries. There is a statistical deviation in the data probably due to the approval of the enzyme replacement therapy for CLN2 disease, which has led to a greater interest among the medical community for the early description of this pathology. As a general conclusion, it became clear in this work that the combined bibliographical/retrospective evaluation approach allowed a general overview of the multidisciplinary components and the epidemiological tendencies of NCLs in the SA&C region.

Published

2022

4. Guidelines on the diagnosis, clinical assessments, treatment and management for CLN2 disease patients

Author

Sara E. Mole, Angela Schulz, Eben Badoe, Samuel F. Berkovic, Emily C. de Los Reyes, Simon Dulz, Paul Gissen, Norberto Guelbert, Charles M. Lourenco, Heather L. Mason, Jonathan W. Mink, Noreen Murphy, Miriam Nickel, Joffre E. Olaya, Maurizio Scarpa, Ingrid E. Scheffer, Alessandro Simonati, Nicola Specchio, Ina Von Löbbecke, Raymond Y. Wang, and Ruth E. Williams

Subjects

Expert mapping, Guideline development program, CLN2, Batten, Neurodegenerative disorder, Key Opinion Leader, Medicine

Abstract

Abstract Background CLN2 disease (Neuronal Ceroid Lipofuscinosis Type 2) is an ultra-rare, neurodegenerative lysosomal storage disease, caused by an enzyme deficiency of tripeptidyl peptidase 1 (TPP1). Lack of disease awareness and the non-specificity of presenting symptoms often leads to delayed diagnosis. These guidelines provide robust evidence-based, expert-agreed recommendations on the risks/benefits of disease-modifying treatments and the medical interventions used to manage this condition. Methods An expert mapping tool process was developed ranking multidisciplinary professionals, with knowledge of CLN2 disease, diagnostic or management experience of CLN2 disease, or family support professionals. Individuals were sequentially approached to identify two chairs, ensuring that the process was transparent and unbiased. A systematic literature review of published evidence using Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidance was independently and simultaneously conducted to develop key statements based upon the strength of the publications. Clinical care statements formed the basis of an international modified Delphi consensus determination process using the virtual meeting (Within3) online platform which requested experts to agree or disagree with any changes. Statements reaching the consensus mark became the guiding statements within this manuscript, which were subsequently assessed against the Appraisal of Guidelines for Research and Evaluation (AGREEII) criteria. Results Twenty-one international experts from 7 different specialities, including a patient advocate, were identified. Fifty-three guideline statements were developed covering 13 domains: General Description and Statements, Diagnostics, Clinical Recommendations and Management, Assessments, Interventions and Treatment, Additional Care Considerations, Social Care Considerations, Pain Management, Epilepsy / Seizures, Nutritional Care Interventions, Respiratory Health, Sleep and Rest, and End of Life Care. Consensus was reached after a single round of voting, with one exception which was revised, and agreed by 100% of the SC and achieved 80% consensus in the second voting round. The overall AGREE II assessment score obtained for the development of the guidelines was 5.7 (where 1 represents the lowest quality, and 7 represents the highest quality). Conclusion This program provides robust evidence- and consensus-driven guidelines that can be used by all healthcare professionals involved in the management of patients with CLN2 disease and other neurodegenerative disorders. This addresses the clinical need to complement other information available.

Published

2021

5. Enzyme replacement therapy interruption in mucopolysaccharidosis type IVA patients and its impact in different clinical outcomes

Author

Juan Politei, Gloria Liliana Porras‐Hurtado, Norberto Guelbert, Alejandro Fainboim, Dafne Dain Gandelman Horovitz, and José María Satizábal

Subjects

case series, enzyme replacement therapy, interruption, Morquio, MPS IVA, mucopolysaccharidosis IVA, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract Mucopolysaccharidosis type IVA (MPS IVA) is an autosomal recessive lysosomal storage disorder caused by mutations in the GALNS gene, which leads to deficient activity of N‐acetylglucosamine‐6‐sulfate sulfatase. MPS IVA patients usually present skeletal dysplasia, coarse features, short stature, airway obstruction, cervical spinal cord compression, dental abnormalities, and cardiac valvular alterations. Enzyme replacement therapy (ERT) with elosulfase alfa is the only disease‐specific treatment available for MPS IVA patients and has been shown to improve important clinical and biochemical parameters; however, little is known about the effects of ERT interruption on these patients. In this article, we report the impact of different periods of treatment interruption on clinical outcomes of 18 MPS IVA patients. All MPS IVA patients included in this case series were treated and followed up in Latin American centers and had been receiving elosulfase alfa intravenously for at least 8 months before ERT was interrupted. Different clinical parameters and assessments were evaluated at variable timepoints following therapy interruption. Altogether, our report indicates that some beneficial ERT effects in MPS IVA patients may last after different periods of treatment interruption, as cardiac and respiratory function improvements. However, worsening of important disease parameters after ERT interruption, such as the increase in uGAGs, pain, joint and skeletal aspects, and surgery indications suggests that treatment discontinuation should be avoided in order to maintain the disease as stable as possible, aiming to optimize these patients' life expectancy and quality of life.

Published

2021

6. Neuronal Ceroid Lipofuscinosis Type 2: A Case Series from Argentina

Author

Guillermo Guelbert and Norberto Guelbert

Subjects

Neuronal ceroid lipofuscinosis, CLN, cerliponase alfa, Medicine (General), R5-920

Abstract

Abstract Neuronal ceroid lipofuscinosis type 2 (CLN2) disease is a rare autosomal recessive neurodegenerative disorder caused by mutations in the CLN2/TPP1 gene, leading to a deficiency in tripeptidyl peptidase 1 activity. Enzyme replacement therapy with cerliponase alfa (recombinant human TPP1 [rhTPP1]; Brineura®) was approved in the United States and Europe for the treatment of CLN2 disease in 2017. We retrospectively report a cohort of 19 patients with CLN2 assisted in a specialized center in Argentina, including 8 newly diagnosed cases. Speech disorders and white matter changes/ventricular system enlargement were the most frequent clinical and imaging findings at CLN2 disease onset, respectively. Patients treated with cerliponase alfa presented a stable or improved course of the disease in this Latin American real world setting, as described in clinical trials.

Published

2022

7. Urea cycle disorders in Argentine patients: clinical presentation, biochemical and genetic findings

Author

Silene M. Silvera-Ruiz, José A. Arranz, Johannes Häberle, Celia J. Angaroni, Miriam Bezard, Norberto Guelbert, Adriana Becerra, Fernanda Peralta, Raquel Dodelson de Kremer, and Laura E. Laróvere

Subjects

Urea cycle defects, Hyperammonemia, Ornithine transcarbamylase deficiency, Argininosuccinate synthetase deficiency, Argininosuccinate lyase deficiency, Medicine

Abstract

Abstract Background The incidence, prevalence, and molecular epidemiology of urea cycle disorders (UCDs) in Argentina remain underexplored. The present study is the first to thoroughly assess the clinical and molecular profiles of UCD patients examined at a single reference center in Argentina. Results Forty-nine UCD cases were collected. About half (26/49, 53%) manifested neonatally with classical presentation and had a high mortality (25/26, 96%). Ornithine transcarbamylase deficiency (OTCD) was the most common UCD (26 patients). Argininosuccinate synthetase deficiency (ASSD) was detected in 19 cases, while argininosuccinate lyase deficiency (ASLD) was diagnosed in 4 cases. Molecular genetic analysis revealed 8 private OTC mutations and two large deletion/duplication events in the OTC gene. Most mutations in the ASS1 and ASL genes were recurrent missense changes, and four alterations were novel. The clinical outcome of our UCD cohort was poor, with an overall mortality of 57% (28/49 cases), and a 28% (6/21) disability rate among the survivors. Conclusions Most patients in our case series showed severe neonatal onset, with high morbidity/mortality. We detected in total 19 mutations, most of them recurrent and of high frequency worldwide. Noteworthy, we highlight the presence of a geographic cluster with high prevalence of a point mutation in the ASS1 gene. This study suggests that these disorders may be more frequent than commonly assumed, and stresses the need for increased awareness amongst health professionals and greater availability of diagnostic tools for accurate identification, early diagnosis, and timely treatment.

Published

2019

8. 'Atypical' Phenotypes of Neuronal Ceroid Lipofuscinosis: The Argentine Experience in the Genomic Era

Author

Favio Pesaola, Guillermo Guelbert, Ana Clara Venier, Inés Adriana Cismondi, Adriana Becerra, Juan Carlos G. Vazquez, Elmer Fernandez, Ana Lucia De Paul, Norberto Guelbert, and Inés Noher

Subjects

Neuronal CeroidLipofuscinosis, Genomics, CLN1, CLN2, CLN8, Atypical Phenotypes, Medicine (General), R5-920

Abstract

ABSTRACT Neuronal Ceroid Lipofuscinosis (NCL) refers to a group of inherited lysosomal storage disorders characterized by the intracellular accumulation of ceroid-lipofuscin compounds and neurodegeneration. Fourteen genes are currently recognized with disease-causing DNA variants: PPT1/CLN1, TPP1/CLN2, CLN3, DNAJC5/CLN4, CLN5, CLN6, MFSD8/CLN7, CLN8, CTSD/CN10, GRN/CLN11, ATP13A2/CLN12, CTSF/CLN13, KCTD7/CLN14, TBCK/CLN15. In the frame of the Cordoba cohort, we studied N=51 cases. The aim of this paper is the observational and retrospective analysis of the “atypical” phenotypes. PCR-Sanger sequencing and/or massive exome sequencing were used as a screening methodology. One CLN1 subject showed an atypical prolonged (P) phenotype with null PPT1 activity and a heterozygous compound genotype: E5 c.451C>T, p.Arg151*/g.6302T>G (I3 c.363-3T>G). Other 11 CLN2 individuals (except one girl) showed TPP1 activity decreased to around 10% of the minimum value of the reference interval in leukocytes and saliva. The DNA variants E7 c.827A>T, p.Asp276Val and I7 c.887-10A>G were the most prevalent. One CLN8 individual showed an atypical congenital phenotype with a heterozygous combination of DNA variants: E2 c.1A>G, p.?/E3 c.792C>G, p.Asn264Lys. Massive sequencing was installed as a screening methodology for the precision diagnosis of atypical CLN1, CLN2, and CLN8 phenotypes. A genetic/phenotypic local registry is under construction.

Published

2021

9. Position of Experts Regarding Follow-Up of Patients with Neuronal Ceroid Lipofuscinosis-2 Disease in Latin America

Author

Norberto Guelbert, Nora Atanacio, Inés Denzler, Emília Katiane Embiruçu, Nury Mancilla, Ricardo Naranjo, André Pessoa, Norma Spécola, Lina Tavera, Mónica Troncoso, and Diane Vergara

Subjects

CLN2 disease, neuronal ceroid lipofuscinosis type 2, follow-up, lipofuscin storage diseases, neuronal ceroid lipofuscinosis., Medicine (General), R5-920

Abstract

Abstract Given the lack of standardized guidance for follow-up of patients with neuronal ceroid lipofucsinosis-2 disease in Latin-American countries and the heterogeneity of the region, an expert panel was created with the participation of 11 pediatric neurologists from Colombia, Argentina, Brazil and Chile. The aim of the expert panel was to describe a framework for standardized follow-up in patients with neuronal ceroid lipofucsinosis-2 disease, on or off therapy, that could benefit patients and treating physicians alike. Experts made recommendations in the following areas: seizures, abnormal movements and ataxia, sleep disorders and pain, cognitive function, visual function, hearing and speech, cardiac function, quality of life, and motor function. Recommendations include the most appropriate tools for use in the Latin-American context and health care systems, and provide feasible follow-up guidance, applicable in public and private healthcare facilities. They take into consideration the availability of clinical assessment resources, tools (scales, questionnaires, paraclinical tests) and access to these tools in Latin-American countries, as well as other regional and local needs defined by the participating experts.

Published

2020

10. Proceedings of the 23rd Paediatric Rheumatology European Society Congress: part two

Author

Olga Lomakina, Ekaterina Alekseeva, Sania Valieva, Tatiana Bzarova, Irina Nikishina, Elena Zholobova, Svetlana Rodionovskaya, Maria Kaleda, Yasuo Nakagishi, Masaki Shimizu, Mao Mizuta, Akihiro Yachie, Yuko Sugita, Nami Okamoto, Kousuke Shabana, Takuji Murata, Hiroshi Tamai, Eve M. Smith, Peng Yin, Andrea L. Jorgensen, Michael W. Beresford, on behalf of On behalf of the UK JSLE Cohort Study, Antonio Eleuteri, Beatrice Goilav, Laura Lewandowski, Angel Phuti, Dawn Wahezi, Tamar Rubinstein, Caroline Jones, Paul Newland, Stephen Marks, Rachel Corkhill, Diana Ekdawy, Clarissa Pilkington, Kjell Tullus, Chaim Putterman, Chris Scott, Antony C. Fisher, Andrea Jorgensen, Ezgi Deniz Batu, Can Kosukcu, Ekim Taskiran, Sema Akman, Kubra Ozturk, Betul Sozeri, Erbil Unsal, Zelal Ekinci, Yelda Bilginer, Mehmet Alikasifoglu, Seza Ozen, Hanna Lythgoe, Hermine I. Brunner, Gaurav Gulati, Jordan T. Jones, Mekibib Altaye, Jamie Eaton, Mark Difrancesco, Joo Guan Yeo, Jingyao Leong, Loshinidevi D/O Thana Bathi, Thaschawee Arkachaisri, Salvatore Albani, Nagla Abdelrahman, Michael W Beresford, Valentina Leone, UK JSLE study group supported by the National Institute of Health Research Clinical Research Network, Noortje Groot, D. Shaikhani, I. E. M. Bultink, M. Bijl, R. J. E. M. Dolhain, Y. K. O. Teng, E. Zirkzee, K. de Leeuw, R. Fritsch-Stork, S. S. M. Kamphuis, Rachael D. Wright, Reem Abdawani, Laila Al Shaqshi, Ibrahim Al Zakwani, Natali W. Gormezano, David Kern, Oriany L. Pereira, Gladys C. C. Esteves, Adriana M. Sallum, Nadia E. Aikawa, Rosa M. Pereira, Clovis A. Silva, Eloisa Bonfa, Jessica Beckmann, Nora Bartholomä, Nils Venhoff, Philipp Henneke, Ulrich Salzer, Ales Janda, Alina Lucica Boteanu, Sandra Garrote Corral, Alberto Sifuentes Giraldo, Mariluz Gámir Gámir, Antonio Zea Mendoza, Amra Adrovic, Reyhan Dedeoglu, Sezgin Sahin, Kenan Barut, Aida Koka, Funda Oztunc, Ozgur Kasapcopur, Ana Luisa Rodriguez-Lozano, Francisco Rivas-Larrauri, Silvestre García de la Puente, Andressa G. F. Alves, Maria F. D. A. Giacomin, Juliana Farhat, Alfésio L. F. Braga, Adriana M. E. Sallum, Lúcia M. D. A. Campos, Luiz A. A. Pereira, Ana J. D. F. C. Lichtenfels, Clóvis A. Silva, Sylvia C. L. Farhat, Banu Acar, Z. Birsin Ozcakar, Nilgün Çakar, Nermin Uncu, Gökçe Gür, Semanur Özdel, Fatoş Yalçınkaya, Christiaan Scott, Nicky Brice, Peter Nourse, Christine Arango, Angela C. Mosquera, Clara Malagon, Ana P. Sakamoto, Marco F. C. D. Silva, Ananadreia S. Lopes, Gleice C. S. Russo, Adriana E. M. Sallum, Katia Kozu, Eloisa Bonfá, Claudia Saad-Magalhães, Rosa M. R. Pereira, Claudio A. Len, Maria T. Terreri, Deepti Suri, Siyaram Didel, Amit Rawat, Surjit Singh, Despoina Maritsi, MArgarita Onoufriou, Olga Vougiouka, Maria Tsolia, Edi Paleka Bosak, Mandica Vidović, Mirta Lamot, Lovro Lamot, Miroslav Harjaček, Erika Van Nieuwenhove, Adrian Liston, Carine Wouters, Fatemeh Tahghighi, Vahid Ziaee, Seid-Reza Raeeskarami, Francisca Aguiar, Sandra Pereira, Mariana Rodrigues, Cláudia Moura, Gustavo Rocha, Hercília Guimarães, Iva Brito, Rita Fonseca, Gerd Horneff, Ariane Klein, Kirsten Minden, Hans-Iko Huppertz, Frank Weller-Heinemann, Jasmin Kuemmerle-Deschner, J-Peter Haas, Anton Hospach, BIKER collaborative group, Ricardo Menendez-Castro, Boris Huegle, Johannes-Peter Haas, Joost Swart, Gabriella Giancane, Francesca Bovis, Elio Castagnola, Andreas Groll, Daniel J. Lovell, Tom Wolfs, Michael Hofer, Violeta Panaviene, Susan Nielsen, Jordi Anton, Florence Uettwiller, Valda Stanevicha, Maria Trachana, Denise Pires Marafon, Constantin Ailioaie, Elena Tsitsami, Sylvia Kamphuis, Troels Herlin, Pavla Doležalová, Gordana Susic, Berit Flatø, Flavio Sztajnbok, Angela Pistorio, Alberto Martini, Nico Wulffraat, Nicolino Ruperto, Marco Gattorno, Antonio Brucato, Martina Finetti, George Lazaros, Silvia Maestroni, Mara Carraro, Davide Cumetti, Alessandra Carobbio, Monia Lorini, Alessandro Rimini, Renzo Marcolongo, Anna Valenti, Gian Luca Erre, Riccardo Belli, Fiorenzo Gaita, Maria Pia Sormani, Massimo Imazio, Mario Abinun, Nicola Smith, Tim Rapley, Flora McErlane, Lianne Kearsley-Fleet, Kimme L. Hyrich, Helen Foster, Nikolay Tzaribachev, Andrew Zeft, Rolando Cimaz, John Bohnsack, Thomas Griffin, Ruy Carrasco, Jason Dare, Ivan Foeldvari, Richard Vehe, Teresa Simon, Hermine Brunner, S. Verazza, S. Davì, A. Consolaro, A. Insalaco, V. Gerloni, R. Cimaz, F. Zulian, S. Pastore, F. Corona, G. Conti, P. Barone, M. Cattalini, E. Cortis, L. Breda, A. N. Olivieri, A. Civino, R. Podda, D. Rigante, F. La Torre, G. D’Angelo, M. Jorini, R. Gallizzi, M. C. Maggio, R. Consolini, A. De Fanti, M. G. Alpigiani, A. Martini, A. Ravelli, on behalf of Italian Pediatric Rheumatology Study Group, Aysenur Pac Kısaarslan, Zubeyde Gunduz, Ruhan Dusunsel, Ismail Dursun, Hakan Poyrazoglu, Ekaterina Kuchinskaya, Farida Abduragimova, Mikhail Kostik, Erik Sundberg, Soley Omarsdottir, Lena Klevenvall, Helena Erlandsson-Harris, Gokalp Basbozkurt, Ozge Erdemli, Dogan Simsek, Fatih Yazici, Yildirim Karsioglu, Aysen Tezcaner, Dilek Keskin, Huseyin Ozkan, Cengizhan Acikel, Erkan Demirkaya, Ilonka Orbán, Krisztina Sevcic, Valentin Brodszky, Emese Kiss, Ismaiel A. Tekko, Madeleine Rooney, James McElnay, Cliff Taggart, Helen McCarthy, Ryan F. Donnelly, Drug Delivery Group, Mary Slatter, Zohreh Nademi, Mark Friswell, Sharmila Jandial, Terence Flood, Sophie Hambleton, Andrew Gennery, Andrew Cant, Phoi-Ngoc Duong, Isabelle Koné-Paut, Giovanni Filocamo, María Luz Gamir, Helga Sanner, Laura Carenini, Mesut Topdemir, Yildirim Karslioglu, Faysal Gok, Nadezhda Tsurikova, Elena Ligostaeva, Navdha R. Ramchurn, O. Kostareva, I. Nikishina, S. Arsenyeva, S. Rodionovskaya, M. Kaleda, D. Alexeev, Ismail Dursun Dursun, Sara Murias, Estefania Barral, Rosa Alcobendas, Eugenia Enriquez, Agustin Remesal, Jaime de Inocencio, Tania M. Castro, Simone A. Lotufo, Tatjana Freye, Raffaella Carlomagno, Thomas Zumbrunn, Jan Bonhoeffer, Elvira Cannizzaro Schneider, Daniela Kaiser, Michaël Hofer, Véronique Hentgen, Andreas Woerner, Juvenile Inflammatory Rheumatism (JIR) Cohort, Tobias Schwarz, Jens Klotsche, Martina Niewerth, Gerd Ganser, ICON study group, Jerold Jeyaratnam, Nienke ter Haar, Donato Rigante, Fatma Dedeoglu, Ezgi Baris, Sebastiaan Vastert, Joost Frenkel, Jonathan S. Hausmann, Kathleen G. Lomax, Ari Shapiro, Karen L. Durrant, P. A. Brogan, M. Hofer, J. B. Kuemmerle-Deschner, B. Lauwerys, A. Speziale, K. Leon, X. Wei, R. M. Laxer, Sara Signa, Marta Rusmini, Elena Campione, Sabrina Chiesa, Alice Grossi, Alessia Omenetti, Roberta Caorsi, Gianmaria Viglizzo, Isabella Ceccherini, Silvia Federici, Helen Lachmann, Nicola Ruperto, on behalf of PRINTO and Eurofever Registry, Federica Vanoni, on behalf of PRINTO and Eurofever Project, Sonia Melo Gomes, Ebun Omoyinmi, Juan I. Arostegui, Eva Gonzalez-Roca, Despina Eleftheriou, Nigel Klein, Paul Brogan, Stefano Volpi, Elettra Santori, Paolo Picco, Claudia Pastorino, Gillian Rice, Alessandra Tesser, Yanick Crow, Fabio Candotti, Ada B. Sinoplu, Gozde Yucel, Gizem Pamuk, Laura O. Damian, Cecilia Lazea, Mihaela Sparchez, Paulina Vele, Laura Muntean, Adriana Albu, Simona Rednic, Calin Lazar, Leonardo O. Mendonça, Alessandra Pontillo, Jorge Kalil, Fabio M. Castro, Myrthes T. Barros, Manuela Pardeo, Virginia Messia, Fabrizio De Benedetti, Antonella Insalaco, Giorgia Malighetti, Chiara Gorio, Francesca Ricci, Ilaria Parissenti, Paola Montesano, Barbara Bonafini, Veronica Medeghini, Marco Cattalini, Lucio Giordano, Giulia Zani, Rosalba Ferraro, Donatella Vairo, Silvia Giliani, Maria Cristina Maggio, Girolamo Luppino, Giovanni Corsello, Maria Isabel Gonzalez Fernandez, Berta Lopez Montesinos, Adriana Rodriguez Vidal, Juan I. Arostegui Gorospe, Inmaculada Calvo Penades, Nadia K. Rafiq, Karen Wynne, Khalid Hussain, Paul A. Brogan, Elizabeth Ang, Nicholas Ng, Ayla Kacar, Ozge Altug Gucenmez, Balahan Makay, Sevket Erbil Unsal, Yasin Sahin, Tufan Kutlu, Fugen Cullu-Cokugras, Hasret Ayyildiz-Civan, Tulay Erkan, Sana Al Zuhbi, Eiman Abdalla, Ricardo A. Russo, María M. Katsicas, Francesca Minoia, Angelo Ravelli, Sagar Bhattad, Anju Gupta, Vignesh Pandiarajan, Ritambhra Nada, Kaara Tiewsoh, Philip Hawkins, Dorota Rowczenio, Sarka Fingerhutova, Jana Franova, Leona Prochazkova, Eva Hlavackova, Pavla Dolezalova, Havva Evrengül, Selçuk Yüksel, Mustafa Doğan, Dolunay Gürses, Harun Evrengül, Silvia De Pauli, Serena Pastore, Anna Monica Bianco, Giovanni Maria Severini, Andrea Taddio, Alberto Tommasini, Svetlana O. Salugina, Evgeny Fedorov, Elena Kamenets, Ekaterina Zaharova, Tatiana Sleptsova, Ekaterina Alexeeva, Kirill Savostyanov, Alexander Pushkov, Tatyana Bzarova, Saniya Valieva, Rina Denisova, Kseniya Isayeva, Evgeniya Chistyakova, Margarita Soloshenko, Elena Kaschenko, Utako Kaneko, Chihaya Imai, Akihiko Saitoh, Vitor A. Teixeira, Filipa O. Ramos, Manuela Costa, Yonatan Butbul Aviel, Shafe Fahoum, Riva Brik, Zeynep Birsin Özçakar, Banu Acar Celikel, Fatos Yalcinkaya, Benedetta Schiappapietra, Sergio Davi’, Federica Mongini, Luisa Giannone, Cecilia Bava, Maria Giannina Alpigiani, Alessandro Consolaro, Dragana S. Lazarevic, Jelena Vojinovic, Jelena Basic, Valentina Muratore, Valentina Marzetti, Neus Quilis, Belen Serrano Benavente, Alessandra Alongi, Adele Civino, Lorenzo Quartulli, Giedre Januskeviciute, Pieter van Dijkhuizen, N. Groot, W. van Dijk, A. Kardolus, Raul Gutiérrez Suárez, Ellen B. Nordal, Veronika G. Rypdal, Lillemor Berntson, Maria Ekelund, Kristiina Aalto, Suvi Peltoniemi, Marek Zak, Mia Glerup, Ellen D. Arnstad, Anders Fasth, Marite Rygg, the Nordic Study Group of Pediatric Rheumatology (NoSPeR), Ana Catarina Duarte, Sandra Sousa, Lídia Teixeira, Ana Cordeiro, Mª José Santos, Ana Filipa Mourão, Maria José Santos, Mónica Eusébio, Ana Lopes, Filipa Oliveira-Ramos, Manuel Salgado, Paula Estanqueiro, José Melo-Gomes, Fernando Martins, José Costa, Carolina Furtado, Ricardo Figueira, Jaime C. Branco, João E. Fonseca, Helena Canhão, Ana F. Mourão, Maria Jose Santos, Andrea Coda, Samuel Cassidy, Kerry West, Gordon Hendry, Debra Grech, Julie Jones, Fiona Hawke, Davinder Singh Grewal, Charlene Foley, Orla Killeen, Emma MacDermott, Douglas Veale, Ursula Fearon, Dilek Konukbay, Ela Tarakci, Nilay Arman, Sezgin Şahin, Jane Munro, Esi Morgan, Meredith Riebschleger, Jennifer Horonjeff, Vibeke Strand, Clifton Bingham, Ma. Theresa M. Collante, Margarita Ganeva, Stefan Stefanov, Albena Telcharova, Dimitrina Mihaylova, Radoslava Saraeva, Reni Tzveova, Radka Kaneva, Adelina Tsakova, Katya Temelkova, GRANT Medical University, Sofia 68/, Maria Mercedes C. Picarelli, Luiz C. Danzmann, Florencia Barbé-Tuana, Lucas K. Grun, Marcus H. Jones, Marijan Frković, Karla Ištuk, Ika Birkić, Saša Sršen, Marija Jelušić, Alan Easton, Rachael Quarmby, Raju Khubchandani, Mercedes Chan, Radoslav Srp, Katerina Kobrova, Dana Nemcova, Jozef Hoza, Michal Uher, Melania Saifridova, Lenka Linkova, Sirirat Charuvanij, Isree Leelayuwattanakul, Thita Pacharapakornpong, Sakda A.-O. Vallipakorn, Butsabong Lerkvaleekul, Soamarat Vilaiyuk, Stefano Lanni, Sergio Davì, Randy Q. Cron, Chiara Passarelli, Elisa Pisaneschi, Antonio Novelli, Claudia Bracaglia, Ivan Caiello, Kathy de Graaf, Florence Guilhot, Walter Ferlin, Grant Schulert, Alexi A. Grom, Robert Nelson, Cristina de Min, Dirk Holzinger, Christoph Kessel, Ndate Fall, Alexei Grom, Wilco de Jager, Raffaele Strippoli, Anna Horne, Stephan Ehl, Sandra Ammann, Kai Lehmberg, Karin Beutel, Dirk Foell, AnnaCarin Horne, Laura Pagani, Graciela Espada, Yi-jin Gao, Susan Shenoi, Sheila Weitzman, Giusi Prencipe, Antonia Pascarella, Walter G. Ferlin, Laurence Chatel, Philippe Jacqmin, Kathy De Graaf, Maria Ballabio, Zoë Johnson, Geneviève Lapeyre, Fabrizio de Benedetti, de Min Cristina, Hiroyuki Wakiguchi, Shunji Hasegawa, Reiji Hirano, Fumiko Okazaki, Tamaki Nakamura, Hidenobu Kaneyasu, Shouichi Ohga, Kazuko Yamazaki, Tomo Nozawa, Taichi Kanetaka, Shuichi Ito, Shumpei Yokota, Kirsty McLellan, Ishbel MacGregor, Neil Martin, Joyce Davidson, Sandra Hansmann, Andreas Eikelberg, Iris Haug, Sabrina Schuller, Susanne M. Benseler, Single Hub and Access point for paediatric Rheumatology in Europe (SHARE), Liliia S. Nazarova, Kseniia V. Danilko, Viktor A. Malievsky, Tatiana V. Viktorova, Angela Mauro, Angela Barnicoat, Jane Hurst, Nathalie Canham, Sandrine Lacassagne, Anastasia Wiener, Boris Hügle, Bernd Denecke, Ivan Costa-Filho, Johannes Peter Haas, Klaus Tenbrock, David Popp, Arjan Boltjes, Frank Rühle, Stefanie Herresthal, Femke van Wijk, Joachim Schultze, Monika Stoll, Luisa Klotz, Thomas Vogl, Johannes Roth, Estefania Quesada-Masachs, Daniel Álvarez de la Sierra, Marina Garcia Prat, Ana M. Marín Sánchez, Ricardo Pujol Borrell, Sara Marsal Barril, Mónica Martínez Gallo, Consuelo Modesto Caballero, Iryna Chyzheuskaya, Lyudmyla M. Byelyaeva, Rostislav M. Filonovich, Helena K. Khrustaleva, Larisa I. Zajtseva, Tamara M. Yuraga, Thomas Giner, Lukas Hackl, Julia Albrecht, Reinhard Würzner, Juergen Brunner, Marta Minute, Fulvio Parentin, Agostino Nocerino, Mette Nørgaard, Mikel Alberdi-Saugstrup, Marek S. Zak, Susan M. Nielsen, Ellen Nordal, Klaus G. Müller, Nordic Study Group of Pediatric Rheumatology (NoSPeR), Mojca Zajc Avramovič, Vita Dolžan, Nataša Toplak, Tadej Avčin, N. Ruperto, D. J. Lovell, C. Wallace, M. Toth, I. Foeldvari, J. Bohnsack, D. Milojevic, C. Rabinovich, D. Kingsbury, K. Marzan, P. Quartier, K. Minden, E. Chalom, G. Horneff, R. M. Kuester, J. Dare, M. Heinrich, H. Kupper, J. Kalabic, H. I. Brunner, on behalf of PRINTO and PRCSG, Ruben Burgos-Vargas, Tamas Constantin, Joke Dehoorne, Valda Stanevica, Katarzyna Kobusinska, Zbigniew Zuber, Richard Mouy, Ingrida Rumba-Rozenfelde, Chantal Job-Deslandre, Ronald Pederson, Jack Bukowski, Tina Hinnershitz, Bonnie Vlahos, Paula Keskitalo, Salla Kangas, Paula Vähäsalo, Raul A. Chavez Valencia, David Martino, Anne-Louise Ponsonby, Rachel Chiaroni-Clarke, Braydon Meyer, Roger C. Allen, Jonathan D. Akikusa, Jeffrey M. Craig, Richard Saffrey, Justine A. Ellis, Carol Wallace, Yosef Uziel, Gary Sterba, Rayfel Schneider, Ricardo Russo, Athimalaipet V. Ramanan, Jana Pachlopnik Schmid, Kim E Nichols, Paivi Miettunen, Toshiyuki Kitoh, Norman T. Ilowite, Jan-Inge Henter, Alexei A Grom, Edward M. Behrens, Tadej Avcin, Maurizio Aricò, Sriharsha Grevich, Peggy Lee, Sarah Ringold, Brian Leroux, Hannah Leahey, Megan Yuasa, Jessica Foster, Jeremy Sokolove, Lauren Lahey, William Robinson, Joshua Newson, Anne Stevens, Stephanie J. W. Shoop, Suzanne M. M. Verstappen, Wendy Thomson, Janet E. McDonagh, CAPS, Timothy Beukelman, Yuki Kimura, Marc Natter, Norm Ilowite, Kelly Mieszkalski, Grendel Burrell, Brian Best, Helen Bristow, Shannon Carr, Anne Dennos, Rachel Kaufmann, Laura Schanberg, for the CARRA Registry Investigators, Gabriele Simonini, Francesca Lancini, Margaux Gerbaux, Phu-Quoc Lê, Laurence Goffin, Valérie Badot, Céline La, Laure Caspers, François Willermain, Alina Ferster, Maria Ceci, Francesco Licciardi, Marco Turco, Francesca Santarelli, Davide Montin, Claudia Toppino, Clotilde Alizzi, Bruno Papia, Beatrice Vergara, Umberto Corpora, Luca Messina, Maria Tsinti, Vasiliko Dermentzoglou, Panagiotis Tziavas, Marija Perica, Lana Tambić Bukovac, Mustafa Çakan, Nuray Aktay Ayaz, Gonca Keskindemirci, Michael Lang, Catherine Laing, Susanne Benseler, Tommy Gerschman, Nadia Luca, Heinrike Schmeling, Anastasia Dropol, Jaymi Taiani, Nicole Johnson, Brian Rusted, Panagiota Nalbanti, Polyxeni Pratsidou, Grigoris Pardalos, Vasiliki Tzimouli, Anna Taparkou, Maria Stavrakidou, Fotios Papachristou, Florence Kanakoudi-Tsakalidou, Peter Bale, Emily Robinson, Jason Palman, Elizabeth Ralph, Kimberly Gilmour, Clare Heard, Lucy R. Wedderburn, Yara Barrense-Dias, Antonarakis Gregory, Dhouib Amira, Scolozzi Paolo, Hanquinet Sylviane, Hofer Michaël, Nataliya Panko, Salah Shokry, Liudmila Rakovska, Sally Pino, Adriana Diaz-Maldonado, Pilar Guarnizo, Sofia Torreggiani, Paolo Cressoni, Umberto Garagiola, Giancarla Di Landro, Giampietro Farronato, Fabrizia Corona, Samantha Bell, Parveen Bhatti, Lee Nelson, Beth A. Mueller, T. A. Simon, A. Baheti, N. Ray, Z. Guo, Anasuya Hazra, Thomas Stock, Ronnie Wang, Charles Mebus, Christine Alvey, Manisha Lamba, Sriram Krishnaswami, Umberto Conte, Min Wang, Daniel Kingsbury, Elena Koskova, Elzbieta Smolewska, Richard K. Vehe, Daniel Lovell, Tomohiro Kubota, Junko Yasumura, Toshitaka Kizawa, Masato Yashiro, Tsuyoshi Yamatou, Yuichi Yamasaki, Syuji Takei, Yoshifumi Kawano, Ulrika Järpemo Nykvist, Bo Magnusson, Rikard Wicksell, Karin Palmblad, Gunnar L. Olsson, Mohammadreza Modaressi, Mohammad-Hassan Moradinejad, Valentina Seraya, Alisa Vitebskaya, Veronica Moshe, Gil Amarilyo, Liora Harel, Phillip J Hashkes, Amir Mendelson, Noa Rabinowicz, Yonit Reis, Zane Dāvidsone, Arina Lazareva, Ruta Šantere, Dace Bērziņa, Valda Staņēviča, Giulia Camilla Varnier, Susan Maillard, Cristina Ferrari, Silvia Zaffarano, Juvenile Dermatomyositis Research Group and European Federation of Immunological Societies, Judith Wienke, Felicitas Bellutti Enders, Lucas L. van den Hoogen, Jorre S. Mertens, Timothy R. Radstake, Henny G. Hotten, Ruth Fritsch, Lucy Wedderburn, Kiran Nistala, Berent Prakken, Annet van Royen-Kerkhof, Mohammad Alhemairi, Mohammed Muzaffer, Pieter Van Dijkhuizen, Claire T. Deakin, Stefania Simou, Maria De Iorio, Qiong Wu, Tania Amin, Lee Dossetter, Juvenile Dermatomyositis Research Group (JDRG), Raquel Campanilho-Marques, Claire Deakin, Clarissa A. Pilkington, on behalf of Juvenile Dermatomyositis Research Group (JDRG), Silvia Rosina, Sirisucha Soponkanaporn, on behalf of the UK Juvenile Dermatomyositis Research Group (JDRG), Zehra S. Arıcı, Gökçen D. Tuğcu, Ezgi D. Batu, Hafize E. Sönmez, Deniz Doğru-Ersöz, Beril Talim, Nural Kiper, Seza Özen, Alexander Solyom, Ezgi Batu, John Mitchell, Ariana Kariminejad, Fatemeh Hadipour, Zahra Hadipour, Marta Torcoletti, Carlo Agostoni, Maja Di Rocco, Pranoot Tanpaiboon, Andrea Superti-Furga, Luisa Bonafé, Nur Arslan, Norberto Guelbert, Karoline Ehlert, Giedre Grigelioniene, Ratna Puri, Edward Schuchman, Pilar Gomez, Tatiana Gonzalez, Ricardo Yepez, Camilo Vargas, GRIP study group, Falcini Fernanda, Gemma Lepri, Alessandra Ferrari, Marco Matucci-Cerinic, Antonella Meini, Gian Marco Moneta, Emiliano Marasco, Rebecca Nicolai, Luisa Bracci-Laudiero, Olga Kopchak, Alexander Mushkin, Alexey Maletin, Catalina Mosquera, Rita A. Amorim, Juliana Molina, Gustavo Moreira, Flávia H. Santos, Melissa Fraga, Livia Keppeke, Vanessa M. Silva, Camila Hirotsu, Sergio Tufik, Maria Teresa Terreri, Vinícius L. Braga, Maria Beatriz Fonseca, Vania Schinzel, Maria Teresa R. Terreri, Liliana Jorge, Liana Guerra, Edson Amaro Junior, Maria Cristina Castiglione, Alessandra Tricarico, Emily Boulter, Andre Schultz, Kevin Murray, Fernanda Falcini, Stefano Stagi, Eleonora Bellucci, Ingrid H. R. Grein, Gecilmara Pileggi, Natália B. F. Pinto, Aline L. de Oliveira, Lyudmila Belyaeva, Rostislav Filonovich, Helena Khrustaleva, Larisa Zajtseva, Jaanika Ilisson, Chris Pruunsild, Olivier Gilliaux, Francis Corazza, Christophe Lelubre, on behalf of PANLAR Pediatric Rheumatology Study Group, Zoilo Morel, Claudia Saad-Magalhães C, Luis Lira, Mabel Ladino, Ruth Eraso, Ivonne Arroyo, Clovis Silva, Carlos Rose, and PANLAR Pediatric Rheumatology Study Group

Subjects

Pediatrics, RJ1-570, Diseases of the musculoskeletal system, RC925-935

Published

2017

11. Guidelines for diagnosis and treatment of Hunter Syndrome for clinicians in Latin America

Author

Roberto Giugliani, Martha Luz Solano Villarreal, C. Araceli Arellano Valdez, Antonieta Mahfoud Hawilou, Norberto Guelbert, Luz Norela Correa Garzón, Ana Maria Martins, Angelina Acosta, Juan Francisco Cabello, Aída Lemes, Mara Lucia Schmitz Ferreira Santos, and Hernán Amartino

Subjects

Hunter syndrome, lysosomal disease, iduronate-2-sulfatase, enzyme replacement therapy, treatment guidelines, Genetics, QH426-470

Abstract

This review aims to provide clinicians in Latin America with the most current information on the clinical aspects, diagnosis, and management of Hunter syndrome, a serious and progressive disease for which specific treatment is available. Hunter syndrome is a genetic disorder where iduronate-2-sulfatase (I2S), an enzyme that degrades glycosaminoglycans, is absent or deficient. Clinical manifestations vary widely in severity and involve multiple organs and tissues. An attenuated and a severe phenotype are recognized depending on the degree of cognitive impairment. Early diagnosis is vital for disease management. Clinical signs common to children with Hunter syndrome include inguinal hernia, frequent ear and respiratory infections, facial dysmorphisms, macrocephaly, bone dysplasia, short stature, sleep apnea, and behavior problems. Diagnosis is based on screening urinary glycosaminoglycans and confirmation by measuring I2S activity and analyzing I2S gene mutations. Idursulfase (recombinant I2S) (Elaprase®, Shire) enzyme replacement therapy (ERT), designed to address the underlying enzyme deficiency, is approved treatment and improves walking capacity and respiratory function, and reduces spleen and liver size and urinary glycosaminoglycan levels. Additional measures, responding to the multi-organ manifestations, such as abdominal/inguinal hernia repair, carpal tunnel surgery, and cardiac valve replacement, should also be considered. Investigational treatment options such as intrathecal ERT are active areas of research, and bone marrow transplantation is in clinical practice. Communication among care providers, social workers, patients and families is essential to inform and guide their decisions, establish realistic expectations, and assess patients' responses.

Published

2014

12. Cerliponase alfa in the treatment of patients with classic and atypical late infantile neuronal ceroid lipofuscinosis in Latin America

Author

Norberto Guelbert, Oscar M Espitia Segura, Carolina Amoretti, Angélica Arteaga Arteaga, Nora G Atanacio, Natacha S Bazan, Ellaine D.F Carvalho, María D. F Carvalho de Andrade, Inés M Denzler, Consuelo Durand, Erlane M Ribeiro, Juan C Giugni, Gabriel González, Dolores González Moron, Guillermo Guelbert, Zulma J Hernández Rodriguez, Emilia K Embiruçu, Marcelo A Kauffman, Nury I Mancilla, Laureano Marcon, Alessandra Marques Pereira, Carolina F Fischinger Moura de Souza, Victor A Muñoz, Ricardo A Naranjo Florez, André L Pessoa, Maria V Ruiz, Martha M Solano Villareal, Norma Spécola, Lina M Tavera, Javiera Tello, Mónica Troncoso Schifferli, Sonia Urgrina, María M Vaccarezza, Diane Vergara, and María M Villanueva

Abstract

Introduction: Late infantile neuronal ceroid lipofuscinosis type 2 (CLN2), is a neurodegenerative autosomal recessive disease caused by TPP1 gene variants, with a spectrum of classic and atypical phenotypes. The aim of treatment is to slow functional decline as early as possible, improving quality of life and survival. This study describes the clinical characteristics as well as response to treatment with cerliponase alfa. Materials and Methods: A retrospective study was conducted in five Latin-American countries, based on clinical records from patients with CLN2. Clinical follow-up and treatment variables are described. A descriptive and bivariate statistical analysis was performed. Results: A total of 36 patients are reported with a mean age of symptom onset and time to first specialized consultation of 4.7±2.3 and 6±3.1 years, respectively. Seizures were the predominant symptom (80.6%). In a subgroup analysis, most patients with the classic phenotype exhibited regression in language (90%), while the patients with the atypical phenotype had seizures as the predominant symptom (87%). The mean age of symptom onset and time to first specialized consultation was 3.5±2.0 and 4.9±3.2 years, respectively, in patients with the classic phenotype and 6.2±1.8 and 7.5±2.4 in patients with the atypical phenotype. The mean time interval between onset of symptoms and treatment initiation was 3.8 years in patients with classic phenotype and 7.4 in patients with atypical phenotype. All patients were treated with cerliponase alfa, maintaining overall functional stability as compared to pretreatment values. Discussion and conclusion: This study reports at this time the largest number of patients with CLN2 in treatment with cerliponase alfa in the world. Data show a higher frequency of patients with atypical phenotype and a high allelic proportion of intron variants in our region. There was evidence of long intervals until first specialized consultation, diagnosis, and enzyme replacement therapy. Follow-up after the initiation of cerliponase alfa showed slower-to-no-progression of the disease, associated with adequate clinical outcomes and stable functional scores. These improvements were consistent in both clinical phenotypes.

Published

2022

13. Initial management of acute hyperammonemia in pediatrics

Author

Hernán, Eiroa, Consuelo, Durand, Marina, Szlago, Marcela, Pereyra, Mariana, Nuñez, Norberto, Guelbert, Gabriela, Pacheco, and Soledad, Kleppe

Abstract

Hyperammonemia is a medical emergency. There are no publications regarding the availability of resources, supplies, and knowledge necessary for the initial management of hyperammonemia by pediatricians in Argentina; however, according to the authors' experience, the necessary resources are not available all year round in a large portion of our territory. Based on such state of affairs, an international bibliographic review on this topic and the authors' experience, we developed a series of ecommendations for the initial pediatric management of this emergency, with the objective of reducing deficiencies, allowing adequate clinical suspicion leading to a timely diagnosis and emergency management and a rational use of pharmacological resources (some of which are costly) to reduce the morbidity and mortality associated with hyperammonemia.La hiperamonemia constituye una emergencia médica. No existen publicaciones que hagan referencia a la disponibilidad de recursos, insumos y conocimientos necesarios para el manejo inicial de esta por parte del pediatra en nuestro país, pero, según la experiencia de los autores, los recursos necesarios no se encuentran disponibles los 365 días del año en una gran porción de nuestro territorio. Sobre la base de este estado de situación, de una revisión bibliográfica internacional sobre el tema y de la experiencia de los autores, se elaboraron una serie de recomendaciones para el manejo pediátrico inicial de esta emergencia, que tienen como objetivo poder reducir las deficiencias, permitir una sospecha clínica adecuada que lleve a un diagnóstico y tratamiento de emergencia oportunos, con utilización racional de recursos farmacológicos (algunos de ellos de alto costo), para reducir la morbimortalidad que asocia la patología.

Published

2022

14. Revealing the clinical phenotype of atypical neuronal ceroid lipofuscinosis type 2 disease: Insights from the largest cohort in the world

Author

Carmen Mendes, André Luiz Santos Pessoa, Luis A Lizcano, Charles Marques Lourenço, Nury Mancilla, Francisca Mallorens, Mónica Troncoso, Carolina Rivera-Nieto, Nora Atanacio, Norberto Guelbert, N. Specola, Emily Gardner, Diane Vergara, Sara E. Mole, Lina Tavera, and Carolina Fischinger Moura de Souza

Subjects

Batten disease, Pediatrics, medicine.medical_specialty, seizure, TPP1 deficiency, Late onset, Disease, 03 medical and health sciences, 0302 clinical medicine, Neuronal Ceroid-Lipofuscinoses, 030225 pediatrics, Humans, Medicine, 030212 general & internal medicine, late onset, Child, Clinical phenotype, Aged, Retrospective Studies, Tripeptidyl-Peptidase 1, business.industry, Medical record, Original Articles, medicine.disease, Neuronal Ceroid Lipofuscinosis Type 2, Phenotype, Child, Preschool, Pediatrics, Perinatology and Child Health, Cohort, Original Article, mutation, Differential diagnosis, business, Brazil

Abstract

Aim Neuronal ceroid lipofuscinosis type 2 (CLN2) disease is an autosomal recessive inherited neurodegenerative lysosomal storage disorder caused by deficient tripeptidyl peptidase 1 (TPP1) enzyme, leading to progressive deterioration of neurological functions commonly occurring in children aged 2-4 years and culminating in early death. Atypical cases associated with earlier or later symptom onset, or even protracted course, have already been reported. Such variable manifestations may constitute an additional challenge to early diagnosis and initiation of appropriate treatment. The present work aimed to analyse clinical data from a cohort of Latin American CLN2 patients with atypical phenotypes. Methods Experts in inborn errors of metabolism from Latin America selected patients from their centres who were deemed by the clinicians to have atypical forms of CLN2, according to the current literature on this topic and their practical experience. Clinical and genetic data from the medical records were retrospectively revised. All cases were presented and analysed by these experts at an Advisory Board Meeting in Sao Paulo, Brazil, in October 2018. Results Seizures, language abnormalities and behavioural disorders were found as the first manifestations, appearing at the median age of 6 years, an older age than classically described for the late infantile form. Three novel mutations were also identified. Conclusion Our findings reinforce the inclusion of CLN2 in the differential diagnosis of children presenting with seizures, behavioural disorders and language abnormalities. Early diagnosis will allow early initiation of specific therapy.

Published

2020

15. Cerliponase Alfa for the Treatment of Atypical Phenotypes of CLN2 Disease: A Retrospective Case Series

Author

Marina Trivisano, Lenora Lehwald, Paul Gissen, Jessica Cohen-Pfeffer, Nicola Specchio, Angela Schulz, Christoph Schwering, Laura Lee, Raymond Y. Wang, Renée Shediac, Eva Wibbeler, Norberto Guelbert, Emily de los Reyes, Fernanda Leal-Pardinas, Miriam Nickel, and Gianni Amato

Subjects

Male, 0301 basic medicine, Aging, Pathology, Internationality, Endocrinology, Diabetes and Metabolism, Cerliponase alfa, Disease, Neurodegenerative, Biochemistry, Epilepsy, Endocrinology, 0302 clinical medicine, cerliponase alfa, Child, late infantile neuronal ceroid lipofuscinosis, Clinical course, Phenotype, Recombinant Proteins, Neuronal Ceroid Lipofuscinosis Type 2, Natural history, Treatment Outcome, natural history, Child, Preschool, Neurological, Cognitive Sciences, Female, medicine.medical_specialty, Clinical Sciences, CLN2 disease, 03 medical and health sciences, Rare Diseases, Neuronal Ceroid-Lipofuscinoses, Genetics, medicine, Humans, Preschool, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Molecular Biology, Retrospective Studies, Neurology & Neurosurgery, business.industry, Neurosciences, Original Articles, medicine.disease, neuronal ceroid lipofuscinosis type 2, Brain Disorders, Orphan Drug, 030104 developmental biology, atypical, Pediatrics, Perinatology and Child Health, Neurology (clinical), Late infantile neuronal ceroid lipofuscinosis, business, 030217 neurology & neurosurgery, Follow-Up Studies

Abstract

Background: The classic phenotype of CLN2 disease (neuronal ceroid lipofuscinosis type 2) typically manifests between ages 2 and 4 years with a predictable clinical course marked by epilepsy, language developmental delay, and rapid psychomotor decline. Atypical phenotypes exhibit variable time of onset, symptomatology, and/or progression. Intracerebroventricular-administered cerliponase alfa (rhTPP1 enzyme) has been shown to stabilize motor and language function loss in patients with classic CLN2 disease, but its impact on individuals with atypical phenotypes has not been described. Methods: A chart review was conducted of 14 patients (8 male, 6 female) with atypical CLN2 phenotypes who received cerliponase alfa. Pre- and posttreatment CLN2 Clinical Rating Scale Motor and Language (ML) domain scores were compared. Results: Median age at first presenting symptom was 5.9 years. First reported symptoms were language abnormalities (6 [43%] patients), seizures (4 [29%]), ataxia/language abnormalities (3 [21%]), and ataxia alone (1 [7%]). Median age at diagnosis was 10.8 years. ML score declined before treatment in 13 (93%) patients. Median age at treatment initiation was 11.7 years; treatment duration ranged from 11 to 58 months. From treatment start, ML score remained stable in 11 patients (treatment duration 11-43 months), improved 1 point in 1 patient after 13 months, and declined 1 point in 2 patients after 15 and 58 months, respectively. There were 13 device-related infections in 8 patients (57%) and 10 hypersensitivity reactions in 6 (43%). Conclusions: Cerliponase alfa is well tolerated and has the potential to stabilize motor and language function in patients with atypical phenotypes of CLN2 disease.

Published

2020

16. ASAH1 pathogenic variants associated with acid ceramidase deficiency: Farber disease and spinal muscular atrophy with progressive myoclonic epilepsy

Author

Ratna Dua Puri, Alexander Solyom, Christina Grant, Sarah H. Elsea, Bo Magnusson, Maja DiRocco, Nur Arslan, Karoline Ehlert, Norberto Guelbert, John J. Mitchell, Laila Selim, Christina Lampe, Seza Ozen, Andreas Hahn, Marta Torcoletti, Carlos Ferreira, Kirt Martin, Iman G. Mahmoud, Seema Kapoor, Erik Sundberg, Maha S. Zaki, Neslihan Oneli Mungan, Paul Harmatz, and Gülden Gökçay

Subjects

Adult, Acid Ceramidase, Adolescent, medicine.medical_treatment, Hematopoietic stem cell transplantation, Biology, Bioinformatics, Muscular Atrophy, Spinal, Young Adult, 03 medical and health sciences, Genetics, medicine, Animals, Humans, Child, Genetics (clinical), 030304 developmental biology, Genetic testing, Mice, Knockout, 0303 health sciences, Farber disease, medicine.diagnostic_test, 030305 genetics & heredity, Infant, Myoclonic Epilepsies, Progressive, medicine.disease, Natural history, Farber Lipogranulomatosis, Child, Preschool, Spinal muscular atrophy with progressive myoclonic epilepsy, Mutation, ASAH1, Cohort study

Abstract

Farber disease and spinal muscular atrophy with progressive myoclonic epilepsy are a spectrum of rare lysosomal storage disorders characterized by acid ceramidase deficiency (ACD), resulting from pathogenic variants in N-acylsphingosine amidohydrolase 1 (ASAH1). Other than simple listings provided in literature reviews, a curated, comprehensive list of ASAH1 mutations associated with ACD clinical phenotypes has not yet been published. This publication includes mutations in ASAH1 collected through the Observational and Cross-Sectional Cohort Study of the Natural History and Phenotypic Spectrum of Farber Disease (NHS), ClinicalTrials.gov identifier NCT03233841, in combination with an up-to-date curated list of published mutations. The NHS is the first to collect retrospective and prospective data on living and deceased patients with ACD presenting as Farber disease, who had or had not undergone hematopoietic stem cell transplantation. Forty-five patients representing the known clinical spectrum of Farber disease (living patients aged 1-28 years) were enrolled. The curation of known ASAH1 pathogenic variants using a single reference transcript includes 10 previously unpublished from the NHS and 63 that were previously reported. The publication of ASAH1 variants will be greatly beneficial to patients undergoing genetic testing in the future by providing a significantly expanded reference list of disease-causing variants.

Published

2020

17. Consequences of late diagnosis and treatment in patients with Gaucher disease type 1: Experience of the Argentine group

Author

Barbara C. Soberon, Guillermo I. Drelichman, Nicolas Fernandez Escobar, Nora Basack, Gabriel Aguilar, Maria Silvia Larroude, Adriana E. Rocaspana, Analia G. Carvani, Adriana D.V. Arizó, Sandra R. Borchichi, Maria A. Cedola, Maria F. Cuello, Vanesa Avalos, Blanca Diez, Marta Dragosky, Gustavo L. Kantor, Elsa M. Nucifora, Graciela Pujal, Paola L. Reichel, Adriana N. Degano, Nora Watman, Graciela O. Elena, Norberto Guelbert, Juan J. Chain, and Marcela A. Aznar

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2023

18. eP280: Continued improvement in adults with acid sphingomyelinase deficiency after 2 years of olipudase alfa in the ASCEND placebo-controlled trial

Author

Melissa Wasserstein, Antonio Barbato, Renata Gallagher, Roberto Giugliani, Norberto Guelbert, Julia Hennermann, Carla Hollak, Takayuki Ikezoe, Robin Lachmann, Olivier Lidove, Paulina Mabe, Eugen Mengel, Maurizio Scarpa, Ebubekir Senates, Michel Tchan, Jesus Villarrubia, Beth Thurberg, Abhimanyu Yarramaneni, Andreea Rawlings, Yong Kim, and Monica Kumar

Subjects

Genetics (clinical)

Published

2022

19. Farber disease clinical impact: Patient reported outcomes as a measure of disease burden

Author

John Mitchell, Paul Harmatz, Laila Selim, Iman Gamal El Din, Neslihan Mungan, Fatma Bulut, Christina Lampe, Christina L. Grant, Carlos R. Ferreira, Ratna D. Puri, Sunita Bijarnia-Mahay, Nur Arslan, Norberto Guelbert, Maha S. Zaki, Seema Kapoor, Andreas Hahn, Bo Magnusson, Erik Sundberg, Seza Ozen, Ezgi D. Batu, Maja Di Rocco, Gulden Gokcay, Kathleen Crosby, and Alexander Solyom

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2022

20. Lesch-Nyhan Disease and Its Variants: Phenotypic and Mutation Spectrum of Hypoxanthine-Guanine Phosphoribosyltransferase Deficiency in Argentine Patients

Author

Adriana Becerra, Lynette D. Fairbanks, Norberto Guelbert, Emilia Escuredo, Hyder A. Jinnah, Raquel Dodelson de Kremer, and Laura E. Laróvere

Subjects

Oncology, HPRT1 mutation, medicine.medical_specialty, Medicine (General), Endocrinology, Diabetes and Metabolism, Pedigree chart, Disease, Hyperuricemia, hyperuricemia, Single Center, purl.org/becyt/ford/3.3 [https], R5-920, Internal medicine, Genotype, medicine, Genetics (clinical), biology, business.industry, nutritional and metabolic diseases, Lesch-Nyhan disease, Hypoxanthine-guanine phosphoribosyltransferase deficiency, medicine.disease, Hypoxanthine-guanine phosphoribosyltransferase, Pediatrics, Perinatology and Child Health, Cohort, biology.protein, Phosphoribosyltransferase, purl.org/becyt/ford/3 [https], business, Lesch-Nyhan variant

Abstract

Hypoxanthine-guanine phosphoribosyltransferase (HPRT) deficiency is a disorder of purine metabolism responsible for Lesch-Nyhan Disease (LND) and its variants, HPRT-related hyperuricemia with neurologic dysfunction (HND) and HPRT-related hyperuricemia (HRH). The objective of this study was to characterize a cohort of Argentine patients with HPRT deficiency diagnosed in a single center. Results: Twenty nine patients were studied, including 12 LND, 15 HND and 2 HRH. The average onset age was 0.64 years for LND with motor delay as the main manifestation, 8.84 years for HND and 2.5 years for HRH; nephrological manifestations predominated as presenting features in these variants. The average diagnosis age was 3.58 years for LND, 17.21 years for HND and 2.5 years for HRH. Clinical heterogeneity was more evident in HND, even in members of the same family. All patients presented hyperuricemia and no detectable HPRT activity in erythrocyte lysate. The molecular study allowed to identify 9 different mutations in HPRT1 gene from 24 patients (11 independent pedigrees) and to establish genotype-phenotype correlation. In conclusion, this study describes the genotypic/phenotypic spectrum of HPRT deficiency in Argentine patients and highlights the need to increase awareness about the suspicion of these diseases, especially the LND variants with high clinical heterogeneity. Fil: Laróvere, Laura Elena. Universidad Nacional de Córdoba. Facultad de Medicina. Centro de Estudios de las Metabolopatías Congénitas; Argentina. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina Fil: Fairbanks, Lynette D.. Purine Research Laboratory, St. Thomass Hosp; Reino Unido Fil: Jinnah, H. A.. University of Emory; Estados Unidos Fil: Guelbert, Norberto Bernardo. Hospital de Niños de la Santísima Trinidad, Córdoba; Argentina Fil: Escuredo, Emilia. Purine Research Laboratory, St. Thomass Hosp; Reino Unido Fil: Becerra, Adriana Berónica. Hospital de Niños de la Santísima Trinidad, Córdoba; Argentina Fil: Dodelson de Kremer, Raquel. Universidad Nacional de Córdoba. Facultad de Medicina. Centro de Estudios de las Metabolopatías Congénitas; Argentina

Published

2021

21. 'Atypical' Phenotypes of Neuronal Ceroid Lipofuscinosis: The Argentine Experience in the Genomic Era

Author

Guillermo Guelbert, Adriana Becerra, Favio Pesaola, Ana Clara Venier, Ana Lucía De Paul, Inés Adriana Cismondi, Ines Noher, Juan Carlos G. Vazquez, Norberto Guelbert, and Elmer Andrés Fernández

Subjects

Genetics, Atypical Phenotypes, Medicine (General), KCTD7, CLN1, Endocrinology, Diabetes and Metabolism, CLN2, PPT1, Neuronal Ceroid Lipofuscinosis, Genomics, Biology, medicine.disease, Phenotype, CLN8, R5-920, Neuronal CeroidLipofuscinosis, Pediatrics, Perinatology and Child Health, Genotype, medicine, Neuronal ceroid lipofuscinosis, Gene, Genetics (clinical), Exome sequencing

Abstract

Neuronal Ceroid Lipofuscinosis (NCL) refers to a group of inherited lysosomal storage disorders characterized by the intracellular accumulation of ceroid-lipofuscin compounds and neurodegeneration. Fourteen genes are currently recognized with disease-causing DNA variants: PPT1/CLN1, TPP1/CLN2, CLN3, DNAJC5/CLN4, CLN5, CLN6, MFSD8/CLN7, CLN8, CTSD/CN10, GRN/CLN11, ATP13A2/CLN12, CTSF/CLN13, KCTD7/CLN14, TBCK/CLN15. In the frame of the Cordoba cohort, we studied N=51 cases. The aim of this paper is the observational and retrospective analysis of the “atypical” phenotypes. PCR-Sanger sequencing and/or massive exome sequencing were used as a screening methodology. One CLN1 subject showed an atypical prolonged (P) phenotype with null PPT1 activity and a heterozygous compound genotype: E5 c.451C>T, p.Arg151*/g.6302T>G (I3 c.363-3T>G). Other 11 CLN2 individuals (except one girl) showed TPP1 activity decreased to around 10% of the minimum value of the reference interval in leukocytes and saliva. The DNA variants E7 c.827A>T, p.Asp276Val and I7 c.887-10A>G were the most prevalent. One CLN8 individual showed an atypical congenital phenotype with a heterozygous combination of DNA variants: E2 c.1A>G, p.?/E3 c.792C>G, p.Asn264Lys. Massive sequencing was installed as a screening methodology for the precision diagnosis of atypical CLN1, CLN2, and CLN8 phenotypes. A genetic/phenotypic local registry is under construction. publishedVersion Fil: Pesaola, Favio. Consejo Nacional de Investigaciones Científicas y Técnicas. Instituto de Investigación en Ciencias de la Salud; Argentina. Fil: Pesaola, Favio. Universidad Nacional de Córdoba. Facultad de Ciencias Médicas; Argentina. Fil: Pesaola, Favio. Hospital de Niños de la Provincia de Córdoba. Programa de Investigación Traslacional de Lipofuscinosis Ceroideas Neuronales; Argentina. Fil: Guelbert, Guillermo. Universidad Nacional de Córdoba. Facultad de Ciencias Médicas; Argentina. Fil: Guelbert, Guillermo. Hospital de Niños de la Provincia de Córdoba. Programa de Investigación Traslacional de Lipofuscinosis Ceroideas Neuronales; Argentina. Fil: Guelbert, Guillermo. Hospital de Niños de la Provincia de Córdoba. Sección de Enfermedades Metabólicas Hereditarias; Argentina. Fil: Venier, Ana Clara. Universidad Nacional de Córdoba. Facultad de Ciencias Exactas, Físicas y Naturales; Argentina. Fil: Venier, Ana Clara. Hospital de Niños de la Provincia de Córdoba. Programa de Investigación Traslacional de Lipofuscinosis Ceroideas Neuronales; Argentina. Fil: Venier, Ana Clara. Consejo Nacional de Investigaciones Científicas y Técnicas. Instituto de Investigación en Ciencias de la Salud; Argentina. Fil: Cismondi, Inés Adriana. Universidad Nacional de Córdoba. Facultad de Odontología; Argentina. Fil: Cismondi, Inés Adriana. Hospital de Niños de la Provincia de Córdoba. Programa de Investigación Traslacional de Lipofuscinosis Ceroideas Neuronales; Argentina. Fil: Becerra, Adriana. Universidad Nacional de Córdoba. Facultad de Ciencias Médicas; Argentina. Fil: Beccera, Adriana. Hospital de Niños de la Provincia de Córdoba. Programa de Investigación Traslacional de Lipofuscinosis Ceroideas Neuronales; Argentina. Fil: Becerra, Adriana. Hospital de Niños de la Provincia de Córdoba. Sección de Enfermedades Metabólicas Hereditarias; Argentina. Fil: Vazquez, Juan Carlos G. Universidad Católica de Córdoba; Argentina. Fil: Vazquez, Juan Carlos G. Consejo Nacional de Investigaciones Científicas y Técnicas, Centro de Investigación y Desarrollo en Inmunología y Enfermedades Infecciosas; Argentina. Fil: Fernández, Elmer. Universidad Católica de Córdoba; Argentina. Fil: Fernández, Elmer. Consejo Nacional de Investigaciones Científicas y Técnicas, Centro de Investigación y Desarrollo en Inmunología y Enfermedades Infecciosas; Argentina. Fil: De Paul, Ana Lucia. Universidad Nacional de Córdoba. Facultad de Ciencias Médicas. Centro de Microscopía Electrónica; Argentina. Fil: De Paul, Ana Lucia. Consejo Nacional de Investigaciones Científicas y Técnicas. Instituto de Investigación en Ciencias de la Salud; Argentina. Fil: Guelbert, Norberto. Universidad Nacional de Córdoba. Facultad de Ciencias Médicas; Argentina. Fil: Guelbert, Norberto. Hospital de Niños de la Provincia de Córdoba. Programa de Investigación Traslacional de Lipofuscinosis Ceroideas Neuronales; Argentina. Fil: Guelbert, Norberto. Clínica Universitaria Reina Fabiola; Argentina. Fil: Noher, Inés. Fil: Venier, Universidad Nacional de Córdoba. Facultad de Ciencias Exactas, Físicas y Naturales; Argentina. Fil: Noher, Inés. Hospital de Niños de la Provincia de Córdoba. Programa de Investigación Traslacional de Lipofuscinosis Ceroideas Neuronales; Argentina.

Published

2021

22. Guidelines on the diagnosis, clinical assessments, treatment and management for CLN2 disease patients

Author

Ruth Williams, Norberto Guelbert, Maurizio Scarpa, Samuel F. Berkovic, Raymond Y. Wang, Noreen Murphy, Nicola Specchio, Simon Dulz, Paul Gissen, Joffre E Olaya, Emily de los Reyes, Jonathan W. Mink, Ingrid E. Scheffer, Alessandro Simonati, Sara E. Mole, Angela Schulz, Miriam Nickel, Eben Badoe, Ina von Löbbecke, Heather L Mason, and Charles Marques Lourenço

Subjects

medicine.medical_specialty, Consensus, Family support, media_common.quotation_subject, education, Psychological intervention, Disease, Neurodegenerative, 7.3 Management and decision making, 03 medical and health sciences, 0302 clinical medicine, Multidisciplinary approach, Neuronal Ceroid-Lipofuscinoses, Clinical Research, Batten, Medicine, Humans, Pharmacology (medical), Quality (business), 030212 general & internal medicine, Genetics (clinical), Guideline development program, media_common, Genetics & Heredity, Other Medical and Health Sciences, Tripeptidyl-Peptidase 1, business.industry, Research, Neurosciences, CLN2, General Medicine, Guideline, Neurodegenerative disorder, Brain Disorders, Systematic review, Good Health and Well Being, Key Opinion Leader, Family medicine, Expert mapping, Modified-Delphi, Management of diseases and conditions, business, End-of-life care, 030217 neurology & neurosurgery

Abstract

Background CLN2 disease (Neuronal Ceroid Lipofuscinosis Type 2) is an ultra-rare, neurodegenerative lysosomal storage disease, caused by an enzyme deficiency of tripeptidyl peptidase 1 (TPP1). Lack of disease awareness and the non-specificity of presenting symptoms often leads to delayed diagnosis. These guidelines provide robust evidence-based, expert-agreed recommendations on the risks/benefits of disease-modifying treatments and the medical interventions used to manage this condition. Methods An expert mapping tool process was developed ranking multidisciplinary professionals, with knowledge of CLN2 disease, diagnostic or management experience of CLN2 disease, or family support professionals. Individuals were sequentially approached to identify two chairs, ensuring that the process was transparent and unbiased. A systematic literature review of published evidence using Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidance was independently and simultaneously conducted to develop key statements based upon the strength of the publications. Clinical care statements formed the basis of an international modified Delphi consensus determination process using the virtual meeting (Within3) online platform which requested experts to agree or disagree with any changes. Statements reaching the consensus mark became the guiding statements within this manuscript, which were subsequently assessed against the Appraisal of Guidelines for Research and Evaluation (AGREEII) criteria. Results Twenty-one international experts from 7 different specialities, including a patient advocate, were identified. Fifty-three guideline statements were developed covering 13 domains: General Description and Statements, Diagnostics, Clinical Recommendations and Management, Assessments, Interventions and Treatment, Additional Care Considerations, Social Care Considerations, Pain Management, Epilepsy / Seizures, Nutritional Care Interventions, Respiratory Health, Sleep and Rest, and End of Life Care. Consensus was reached after a single round of voting, with one exception which was revised, and agreed by 100% of the SC and achieved 80% consensus in the second voting round. The overall AGREE II assessment score obtained for the development of the guidelines was 5.7 (where 1 represents the lowest quality, and 7 represents the highest quality). Conclusion This program provides robust evidence- and consensus-driven guidelines that can be used by all healthcare professionals involved in the management of patients with CLN2 disease and other neurodegenerative disorders. This addresses the clinical need to complement other information available.

Published

2021

23. Management of CLN1 Disease: International Clinical Consensus

Author

Joni A. Turunen, Ruth Williams, Margie Frazier, Emily de los Reyes, Kristen Drago, Minna Laine, Sharon King, Elaine C. Wirrell, Tanya Levin, Heather R. Adams, Angela Schulz, Alessandro Simonati, Jonathan W. Mink, Norberto Guelbert, Danielle Peifer, Meral Topçu, Erika F. Augustine, Miriam Nickel, HUS Children and Adolescents, Lastenneurologian yksikkö, University of Helsinki, Clinicum, HUS Head and Neck Center, and Silmäklinikka

Subjects

Movement disorders, Palliative care, Clinical care, Drug-resistant epilepsy, Lysosomal storage disease, CHILDREN, Disease, FORMS, 3124 Neurology and psychiatry, 0302 clinical medicine, Multidisciplinary approach, 3123 Gynaecology and paediatrics, BRAIN, Child, Palliative Care, 3. Good health, Phenotype, Neurology, Caregivers, Child, Preschool, Practice Guidelines as Topic, Disease Progression, medicine.symptom, Palmitoyl-protein thioesterase 1, SLEEP DISORDERS, medicine.medical_specialty, Consensus, Adolescent, Visual impairment, Infantile neuronal ceroid lipofuscinosis, 03 medical and health sciences, PPT1, Quality of life (healthcare), Rare Diseases, Developmental Neuroscience, Neuronal Ceroid-Lipofuscinoses, Stakeholder Participation, 030225 pediatrics, medicine, Humans, business.industry, MUTATIONS, 3112 Neurosciences, Infant, Membrane Proteins, STEM-CELL TRANSPLANTATION, INFANTILE TYPE, NEURONAL CEROID-LIPOFUSCINOSIS, PROTEIN THIOESTERASE DEFICIENCY, medicine.disease, GENE, Family medicine, Pediatrics, Perinatology and Child Health, Neurology (clinical), Thiolester Hydrolases, business, Rare disease, 030217 neurology & neurosurgery

Abstract

Background: CLN1 disease (neuronal ceroid lipofuscinosis type 1) is a rare, genetic, neurodegenerative lysosomal storage disorder caused by palmitoyl-protein thioesterase 1 (PPT1) enzyme deficiency. Clinical features include developmental delay, psychomotor regression, seizures, ataxia, movement disorders, visual impairment, and early death. In general, the later the age at symptom onset, the more protracted & nbsp;Pediatric Neurology 120 (2021) 38e51 the disease course. We sought to evaluate current evidence and to develop expert practice consensus to support clinicians who have not previously encountered patients with this rare disease. Methods: We searched the literature for guidelines and evidence to support clinical practice recommendations. We surveyed CLN1 disease experts and caregivers regarding their experiences and recommendations, and a meeting of experts was conducted to ascertain points of consensus and clinical practice differences. Results: We found a limited evidence base for treatment and no clinical management guidelines specific to CLN1 disease. Fifteen CLN1 disease experts and 39 caregivers responded to the surveys, and 14 experts met to develop consensus-based recommendations. The resulting management recommendations are uniquely informed by family perspectives, due to the inclusion of caregiver and advocate perspectives. A family-centered approach is supported, and individualized, multidisciplinary care is emphasized in the recommendations. Ascertainment of the specific CLN1 disease phenotype (infantile-, late infantile-, juvenile-, or adult-onset) is of key importance in informing the anticipated clinical course, prognosis, and care needs. Goals and strategies should be periodically reevaluated and adapted to patients' current needs, with a primary aim of optimizing patient and family quality of life. (c) 2021 The Authors. Published by Elsevier Inc. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).

Published

2020

24. Ten years of screening for congenital disorders of glycosylation in Argentina: case studies and pitfalls

Author

C. G. Asteggiano, María Fernanda Peralta, Nydia Beatriz Azar, Niels Suldrup Suldrup, María Beatriz Bistué Millón, Raquel Dodelson de Kremer, Norberto Guelbert, Marcela Pereyra, N. Specola, and Magali Papazoglu

Subjects

Male, 0301 basic medicine, Pathology, Glycosylation, chemistry.chemical_compound, Congenital Disorders of Glycosylation, 0302 clinical medicine, Mass Screening, Medicine, Exome, Child, Exome sequencing, chemistry.chemical_classification, medicine.diagnostic_test, Homozygote, Galactosemia, Transferrin, Phenotype, Child, Preschool, Female, medicine.symptom, Adult, Galactosemias, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Argentina, Collagen Type VI, 03 medical and health sciences, Neonatal Screening, Humans, Genetic Predisposition to Disease, Genetic Testing, Myopathy, Glycoproteins, Genetic testing, Isoelectric focusing, business.industry, Infant, Newborn, Genetic Variation, Infant, Sequence Analysis, DNA, medicine.disease, 030104 developmental biology, chemistry, Pediatrics, Perinatology and Child Health, Glycolipids, Isoelectric Focusing, business, Glycoprotein, 030217 neurology & neurosurgery

Abstract

Congenital Disorders of Glycosylation (CDG) are genetic diseases caused by hypoglycosylation of glycoproteins and glycolipids. Most CDG are multisystem disorders with mild to severe involvement. We studied 554 patients (2007–2017) with a clinical phenotype compatible with a CDG. Screening was performed by serum transferrin isoelectric focusing. The diagnosis was confirmed by genetic testing (Sanger or exome sequencing). A confirmed abnormal pattern was found in nine patients. Seven patients showed a type 1 pattern: four with PMM2-CDG, two with ALG2-CDG, and one with classical galactosemia. A type 2 pattern was found in two patients: one with a CDG-IIx and one with a transferrin protein variant. Abnormal transferrin pattern were observed in a patient with a myopathy due to a COL6A2 gene variant. CDG screening in Argentina from 2007 to 2017 revealed 4 PMM2-CDG patients, 2 ALG2-CDG patients with a novel homozygous gene variant and 1 CDG-IIx.

Published

2018

25. Management Strategies for CLN2 Disease

Author

Charlie Fairhurst, Norberto Guelbert, Renée Shediac, Szilard Kiss, Lenora Lehwald, Ruth Williams, Martin Blohm, Andrea West, Jessica L. Cohen-Pfeffer, Angela Schulz, John A. Lawson, Meral Topçu, Annamaria Kofler, Margie Frazier, Svetlana Mikhaylova, Emily de los Reyes, Jonathan W. Mink, Nicola Specchio, Kristen Drago, Miriam Nickel, Boris Zernikow, Heather R. Adams, Jonas Denecke, Mary Anne Leung, Katherine B. Sims, and Ina von Löbbecke

Subjects

medicine.medical_specialty, Palliative care, Language delay, Clinical Neurology, Cerliponase alfa, Disease, 03 medical and health sciences, 0302 clinical medicine, Quality of life (healthcare), Developmental Neuroscience, Neuronal Ceroid-Lipofuscinoses, 030225 pediatrics, Neurodisability, Humans, Medicine, Pediatrics, Perinatology, and Child Health, Disease management (health), Psychiatry, Tripeptidyl-Peptidase 1, business.industry, Disease Management, Neuronal Ceroid Lipofuscinosis Type 2, Neurology, Pediatrics, Perinatology and Child Health, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

CLN2 disease (neuronal ceroid lipofuscinosis type 2) is a rare, autosomal recessive, pediatric-onset, rapidly progressive neurodegenerative lysosomal storage disorder caused by tripeptidyl peptidase 1 (TPP1) enzyme deficiency, and is characterized by language delay, seizures, rapid cognitive and motor decline, blindness, and early death. No management guidelines exist and there is a paucity of published disease-specific evidence to inform clinical practice, which currently draws upon experience from the field of childhood neurodisability. Twenty-four disease experts were surveyed on CLN2 disease management and a subset met to discuss current practice. Management goals and strategies are consistent among experts globally and are guided by the principles of pediatric palliative care. Goals and interventions evolve as the disease progresses, with a shift in focus from maintenance of function early in the disease to maintenance of quality of life. A multidisciplinary approach is critical for optimal patient care. This work represents an initial step toward the development of consensus-based management guidelines for CLN2 disease.

Published

2017

26. Acid Ceramidase Deficiency is characterized by a unique plasma cytokine and ceramide profile that is altered by therapy

Author

Aneal Khan, Charles Marques Lorenco, Alexander Solyom, Janet Gardner-Medwin, Makoto Yoshimitsu, Edward H. Schuchman, John D. Mitchell, Maja Di Rocco, Thierry Levade, Bo Magnusson, Maria Teresa Terreri, Rawane Dagher, Karoline Ehlert, Rossella Parini, Xingxuan He, Shaalee Dworski, Balahan Makay, Bruno Maranda, Nur Arslan, Lilianna Barillas-Arias, Boris Hügle, Norberto Guelbert, Ping Lu, Andrea Jarisch, Pranoot Tanpaiboon, James S. Norris, and Jeffrey A. Medin

Subjects

Male, 0301 basic medicine, Ceramide, Lymphocytosis, medicine.medical_treatment, Arthritis, Hematopoietic stem cell transplantation, Ceramides, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, medicine, Animals, Humans, Molecular Biology, Bone Marrow Transplantation, Farber disease, medicine.disease, Arthritis, Juvenile, Pathophysiology, Farber Lipogranulomatosis, Hexosaminidases, 030104 developmental biology, Cytokine, chemistry, Immunology, Cytokines, Molecular Medicine, Female, lipids (amino acids, peptides, and proteins), Tumor necrosis factor alpha, medicine.symptom

Abstract

Acid Ceramidase Deficiency (Farber disease, FD) is an ultra-rare Lysosomal Storage Disorder that is poorly understood and often misdiagnosed as Juvenile Idiopathic Arthritis (JIA). Hallmarks of FD are accumulation of ceramides, widespread macrophage infiltration, splenomegaly, and lymphocytosis. The cytokines involved in this abnormal hematopoietic state are unknown. There are dozens of ceramide species and derivatives, but the specific ones that accumulate in FD have not been investigated. We used a multiplex assay to analyze cytokines and mass spectrometry to analyze ceramides in plasma from patients and mice with FD, controls, Farber patients treated by hematopoietic stem cell transplantation (HSCT), JIA patients, and patients with Gaucher disease. KC, MIP-1 alpha, and MCP-1 were sequentially upregulated in plasma from FD mice. MCP-1, IL-10, IL-6, IL-12, and VEGF levels were elevated in plasma from Farber patients but not in control or JIA patients. C16-Ceramide (C16-Cer) and dhC16-Cer were upregulated in plasma from FD mice. a-OH-C18-Cer, dhC12-Cer, dhC24:1-Cer, and C22:1-Cer-1P accumulated in plasma from patients with FD. Most cytokines and only a-OH-C18-Cer returned to baseline levels in HSCT-treated Farber patients. Sphingosines were not altered. Chitotriosidase activity was also relatively low. A unique cytokine and ceramide profile was seen in the plasma of Farber patients that was not observed in plasma from HSCT-treated Farber patients, JIA patients, or Gaucher patients. The cytokine profile can potentially be used to prevent misdiagnosis of Farber as JIA and to monitor the response to treatment. Further understanding of why these signaling molecules and lipids are elevated can lead to better understanding of the etiology and pathophysiology of FD and inform development of future treatments. (C) 2016 Elsevier B.V. All rights reserved.

Published

2017

27. Enfermedad CLN8 congénita de lipofuscinosis neuronal ceroidea: un nuevo fenotipo

Author

Romina Kohan, Norberto Guelbert, F Pesaola, A M Oller-Ramirez, Inés Adriana Cismondi, I Noher de Halac, and Patricia Pons

Subjects

Fatal outcome, CIENCIAS MÉDICAS Y DE LA SALUD, business.industry, CONGENITAL PHENOTYPE, NEURONAL CEROID LIPOFUSCINOSIS, CLN8 DISEASE, COMPOUND HETEROZYGOUS MUTATION, purl.org/becyt/ford/3.1 [https], General Medicine, Bioquímica y Biología Molecular, LATIN AMERICA, 03 medical and health sciences, Medicina Básica, 0302 clinical medicine, INDEX CASE, Medicine, purl.org/becyt/ford/3 [https], Neurology (clinical), business, Humanities, 030217 neurology & neurosurgery

Abstract

La enfermedad CLN8 es uno de los 13 tipos genéticos reconocidos de lipofuscinosis neuronal ceroidea, un grupo de trastornos neurodegenerativos de acumulación lisosómica, los más frecuentes en la infancia. La causan mutaciones en la proteína transmembrana CLN8 de 286 aminoácidos, cuya función se desconoce. Las variantes patológicas en el gen CLN8 se asociaron con dos fenotipos diferentes: la variante infantil tardía en individuos de diversos países alrededor del mundo, y la epilepsia progresiva con retraso mental, que aparece en pacientes finlandeses y turcos. Caso clínico. Niña que mostró retraso psicomotor y demencia desde el nacimiento, convulsiones tonicoclónicas, mioclonía, ataxia con atrofia cerebelosa y muerte temprana a los 12 años. La microscopia electrónica de la piel mostró una mezcla de citosomas con patrones de depósitos osmiofílicos granulares, curvilíneos y de huella digital, y mitocondrias hipertrofiadas. Se encontraron dos variantes patológicas de ADN en el gen CLN8 (exón 2 c.1A>G; p./ exón 3 c.792C>G; p.Asn264Lys), lo que confirmó un genotipo heterocigoto compuesto. Éste es el caso índice en América Latina para el nuevo fenotipo congénito de la enfermedad CLN8. La sospecha de esta patología debería sustentarse genéticamente en casos de síndrome neurodegenerativo con retraso psicomotor desde el nacimiento, dificultad del habla y convulsiones. El curso clínico incluye ataxia, atrofia cerebelosa y muerte temprana. CLN8 disease is one of the thirteen recognized genetic types of neuronal ceroid lipofuscinosis, a group of neurodegenerative lysosomal storage disorders, most frequent in childhood. A putative 286 amino acids transmembrane CLN8 protein with unknown function is affected. Pathological variants in the CLN8 gene were associated with two different phenotypes: variant late-infantile in individuals from many countries worldwide, and epilepsy progressive with mental retardation, appearing in Finnish and Turkish subjects. Case report. The girl showed psychomotor delay and dementia since birth, tonic-clonic seizures, myoclonus, ataxia with cerebellar atrophy, and early death at 12 years old. Electron microscopy of the skin showed mixed GROD, curvilinear, fingerprint cytosomes and mitochondrial hypertrophy. Two pathological DNA variants in the CLN8 gene (exon 2 c.1A>G; p.?/ exon 3 c.792C>G; p.Asn264Lys) were found confirming a compound heterozygous genotype. This case is the Latin American index for a new congenital phenotype of the CLN8 disease. The congenital phenotype has to be added to the clinical spectrum of the CLN8 disease. The suspicion of CLN8 disease should be genetically sustained in challenging cases of a neurodegenerative syndrome with psychomotor delay since birth, speech difficulty and seizures. The course includes ataxia, cerebellar atrophy, and early death. Fil: Pesaola, Favio Nicolas. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Universidad Nacional de Córdoba. Facultad de Medicina. Centro de Estudios de las Metabolopatías Congénitas; Argentina Fil: Kohan, Romina. Universidad Nacional de Córdoba. Facultad de Odontología; Argentina Fil: Cismondi, Inés Adriana. Universidad Nacional de Córdoba. Facultad de Odontología; Argentina Fil: Guelbert, Norberto Bernardo. Sec de Enferm Metabólicas Hereditarias, Hospital Niños; Argentina Fil: Pons, Patricia. Centro de Microscopía Electrónica; Argentina Fil: Oller, Ana María del Valle. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Universidad Nacional de Córdoba. Facultad de Medicina. Centro de Estudios de las Metabolopatías Congénitas; Argentina Fil: Noher de Halac, Inés. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Universidad Nacional de Córdoba. Facultad de Medicina. Centro de Estudios de las Metabolopatías Congénitas; Argentina

Published

2019

28. Adults with chronic acid sphingomyelinase deficiency show significant visceral, pulmonary, and hematologic improvements after enzyme replacement therapy with olipudase-alfa: 1-year results of the ASCEND placebo-controlled trial

Author

Ebubekir Senates, Robin H. Lachmann, Jesús Villarrubia, Melissa P. Wasserstein, Takayuki Ikezoe, Carla E. M. Hollak, Oliver Lidove, Norberto Guelbert, Michel Tchan, Renata C. Gallagher, Yixin Chen, Beth L. Thurberg, Patricia A. Fraser, Laila Arash-Kaps, Atef Zaher, Eugen Mengel, Roberto Giugliani, Monica Kumar, Maurizio Scarpa, Paulina Mabe, and Antonio Barbato

Subjects

medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, Placebo-controlled study, Olipudase alfa, Enzyme replacement therapy, Biochemistry, Gastroenterology, Endocrinology, Internal medicine, Genetics, medicine, Acid sphingomyelinase, business, Molecular Biology, medicine.drug

Published

2021

29. Skeletal involvement in Gaucher disease: An observational multicenter study of prognostic factors in the Argentine Gaucher disease patients

Author

Gabriel Fernández, José Ferro, María Veloso, Marta Dragosky, Nazario Boido, Ramiro Fernández, Liliana Franco, Sandra Zirone, Roberto Albina, Victoria Lanza, Susana S. Meschengieser, Hugo Medici, Nicolás Fernández Escobar, Lucia Barazzutti, Graciela Elena, Andrea Schenone, José Luis Saavedra, Analía Carvani, Greogorio Buchovsky, Luis Aversa, Alejandra Cedola, David Verón, Katja Muller, Nora Watman, Beatriz Girardi, Marcela Corrales, Graciela Galván, Marcelo Contte, Angie Barbieri María, Gabriela Nuñez, Luis Quiroga, Gabriela Aguilar, Alba Ruiz, Julieta Bietti, Marisa Marquez, Lucía Richard, Hugo Robledo, Paola Reichel, Graciela Zárate, Leonardo Feldman, María Fernanda Cuello, Sergio Gómez, Victoria Welsh, Francis Del Río, Mario Savarino, María Á Lvarez Bollea, María Silvia Larroude, Andrés Marino, Marcela Aznar, Moira Bolesina, Cristina Cabral Castella, S Ernesto Veber, Gustavo Kantor, Patricia De Ambrosio, Daniel Bar, Adriana Degano, Alba Sanabria, Viviana Bacciedoni, Norberto Guelbert, Rubén Colimodio, María Nucifora, Marcelo Pujol, Adriana Arizo, Alcyra Fynn, Germán Damiani, Nora Basack, Juan José Chain, Bárbara Soberón, Graciela Pujal, María Brun, Sandra Borchichi, Gisela Nisnovich, Rossana Jaureguiberry, Gustavo Carro, Marina Szlago, Hugo Donato, Alejandra Maro, Ccecilia Baduel, Blanca Diez, María Cristina Rapetti, Isabel Pacheco, Maura Papucci, Guillermo Drelichman, Maya Schweri, and Ignacio Fernández

Subjects

0301 basic medicine, medicine.medical_specialty, Bone disease, business.industry, medicine.medical_treatment, Splenectomy, nutritional and metabolic diseases, Hematology, Disease, Enzyme replacement therapy, medicine.disease, Gastroenterology, Surgery, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Multicenter study, 030220 oncology & carcinogenesis, Internal medicine, medicine, Observational study, Young adult, medicine.symptom, business, Bone pain

Abstract

Patients with Gaucher type 1 (GD1) throughout Argentina were enrolled in the Argentine bone project to evaluate bone disease and its determinants. We focused on presence and predictors of bone lesions (BL) and their relationship to therapeutic goals (TG) with timing and dose of enzyme replacement therapy (ERT). A total of 124 patients on ERT were enrolled in a multi-center study. All six TG were achieved by 82% of patients: 70.1% for bone pain and 91.1% for bone crisis. However, despite the fact that bone TGs were achieved, residual bone disease was present in 108 patients on ERT (87%) at time 0. 16% of patients showed new irreversible BL (bone infarcts and avascular osteonecrosis) despite ERT, suggesting that they appeared during ERT or were not detected at the moment of diagnosis. We observed 5 prognostic factors that predicted a higher probability of being free of bone disease: optimal ERT compliance; early diagnosis; timely initiation of therapy; ERT initiation dose ≥45 UI/kg/EOW; and the absence of history of splenectomy. Skeletal involvement was classified into 4 major phenotypic groups according to BL: group 1 (12.9%) without BL; group 2 (28.2%) with reversible BL; group 3 (41.9%) with reversible BL and irreversible chronic BL; and group 4 (16.9%) with acute irreversible BL. Our study identifies prognostic factors for achieving best therapeutic outcomes, introduces new risk stratification for patients and suggests the need for a redefinition of bone TG. Am. J. Hematol. 91:E448-E453, 2016. © 2016 Wiley Periodicals, Inc.

Published

2016

30. Farber disease (acid ceramidase deficiency) natural history study: Prospective and retrospective clinical data

Author

Bo Magnusson, Maja DiRocco, Alexander Solyom, Seema Kapoor, Iman Gamal el Din, Ratna Dua Puri, John J. Mitchell, Nur Arslan, Maha S. Zaki, Neslihan Önenli Mungan, Norberto Guelbert, Erik Sundberg, Christina Grant, Laila Selim, Carlos Ferreira, Balahan Makay, Seza Ozen, Andreas Hahn, Paul Harmatz, Christina Lampe, Fatma Derya Bulut, Sunita Bijarnia-Mahay, Marta Torcoletti, Ezgi Deniz Batu, and Gülden Gökçay

Subjects

Oncology, medicine.medical_specialty, Farber disease, business.industry, Endocrinology, Diabetes and Metabolism, medicine.disease, Biochemistry, Acid Ceramidase Deficiency, Endocrinology, Internal medicine, Genetics, medicine, business, Molecular Biology, Natural history study

Published

2020

31. Farber disease (acid ceramidase deficiency): Data from an ongoing natural history study

Author

Iman Gamal el Din, Alan Kimura, Christina Lampe, Erik Sundberg, Laila Selim, Alexander Solyom, Fatma Derya Bulut, Marta Torcoletti, Balahan Makay, Seza Ozen, Ezgi Deniz Batu, Carlos Ferreira, Paul Harmatz, Bo Magnusson, Maja Di Rocco, Sunita Bijarnia-Mahay, Neslihan Önenli Mungan, Norberto Guelbert, Seema Kapoor, Gülden Gökçay, Nur Arslan, John J. Mitchell, Ratna Dua Puri, and Çukurova Üniversitesi

Subjects

Farber disease, Endocrinology, business.industry, Endocrinology, Diabetes and Metabolism, Immunology, Genetics, medicine, medicine.disease, business, Molecular Biology, Biochemistry, Natural history study, Acid Ceramidase Deficiency

Abstract

15th Annual Research Meeting of the WORLDSymposium(TM) -- FEB 04-07, 2019 -- Orlando, FL WOS: 000457351700338 … WORLDSymposium

Published

2019

32. Evaluación de las neuroimágenes y descripción del compromiso multisistémico en una familia con enfermedad de Fabry

Author

Juan Politei, Celia J. Angaroni, Sebastian Lescano, Hugo Robledo, Norberto Guelbert, Marina Szlago, and Alicia Giner de Ayala

Subjects

Gynecology, medicine.medical_specialty, Neurology, business.industry, medicine, Neurology (clinical), business, AGALSIDASE BETA

Abstract

Resumen La enfermedad de Fabry es el resultado de la deficiencia de alfa-galactosidasa A lisosomal, lo que resulta en deposito progresivo y patologico de glicoesfingolipidos en varias estirpes celulares. El dolor neuropatico suele ser la primera manifestacion en las variantes fenotipicas clasicas. Asociada a la insuficiencia renal y cardiaca, los accidentes cerebrovasculares pueden derivar en la muerte de los pacientes. Se describen los hallazgos de la evaluacion clinica completa y de las neuroimagenes en 9 pacientes pertenecientes a una misma familia. Todos los pacientes presentaron acroparestesias y el 33% de los casos mostro lesiones isquemicas periventriculares silentes, asi como en otro paciente se evidenciaron lesiones compatibles con un proceso inflamatorio. La enfermedad de Fabry debe ser incluida por los neurologos dentro de las posibilidades diagnosticas en pacientes jovenes con dolor neuropatico (neuropatia de fibras finas) y en pacientes con stroke criptogenico debido a la posibilidad de un tratamiento especifico que ha demostrado ser mas eficaz cuanto mas temprano sea indicado.

Published

2015

33. Recommendations for Evaluation and Management of Pain in Patients With Mucopolysaccharidosis in Latin America

Author

Norberto Guelbert, Ana Maria Martins, Gisel Gordillo-González, Juan Politei, Martha Solano, Carolina Fischinger Moura de Souza, Charles Marques Lourenço, Mariana M. Junqueira, and Tatiana Sá Pacheco Carneiro Magalhães

Subjects

myalgia, medicine.medical_specialty, Adolescent, Mucopolysaccharidosis, Pain, 03 medical and health sciences, Young Adult, 0302 clinical medicine, 030202 anesthesiology, Pain assessment, medicine, Humans, Pain Management, Carpal tunnel, Brief Pain Inventory, Bone pain, Child, General Nursing, Pain Measurement, business.industry, Chronic pain, Mucopolysaccharidoses, medicine.disease, Anesthesiology and Pain Medicine, medicine.anatomical_structure, Latin America, Child, Preschool, FLACC scale, Physical therapy, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

The mucopolysaccharidosis (MPS) constitutes a heterogeneous group of rare genetic disorders caused by enzymatic deficiencies that lead to the accumulation of glycosaminoglycans. Several types of MPS are described, historically numbered from I to IX. Clinical observations strongly suggest the presence of chronic pain in patients with all types of MPS. There are few data in the literature on the evaluation and management of pain in these patients, a fact that can compromise the quality of life even more. Professionals with extensive experience in the care for patients with MPS held a meeting in April 2017 to discuss and propose recommendations for the evaluation and management of pain in patients with MPS in Latin America. This article summarizes the content of the discussions and presents the recommendations produced at the meeting. Patients with MPS present joint, bone, and muscle pain, as well as entrapment syndromes (spinal, optic nerve, carpal tunnel). The panel suggests the use of the following instruments for pain assessment: Face, Legs, Activity, Cry and Consolability Scale for children of up to four years of age and patients unable to communicate their pain; Child Health Assessment Questionnaire Scale; Facial Pain Scale and Numerical Pain Scale for patients of five to18 years of age; Brief Pain Inventory and Short Form Health Survey 36 scales for patients aged 18 years or older. Based on the scores verified in these scales, the panel proposes pharmacological interventions for pain relief in this population of patients.

Published

2018

34. Impact of long-term elosulfase alfa on activities of daily living in patients with Morquio A syndrome in an open-label, multi-center, phase 3 extension study

Author

Celeste Decker, Norberto Guelbert, Julian Raiman, Derralynn Hughes, Fiona Stewart, John J. Mitchell, Moeenaldeen Al-Sayed, Paul Harmatz, Christian J. Hendriksz, Rossella Parini, Sara M. Hawley, Barbara K. Burton, Roberto Giugliani, and Robert Matousek

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Activities of daily living, Adolescent, Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, Population, 030105 genetics & heredity, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, Endocrinology, Elosulfase alfa, Double-Blind Method, Internal medicine, Activities of Daily Living, Genetics, medicine, Humans, Respiratory function, Enzyme Replacement Therapy, education, Child, Molecular Biology, Aged, Retrospective Studies, education.field_of_study, business.industry, Mucopolysaccharidosis IV, Retrospective cohort study, Middle Aged, medicine.disease, Chondroitinsulfatases, Treatment Outcome, chemistry, Child, Preschool, Cohort, Female, business, Natural history study

Abstract

Background Long-term safety and efficacy of elosulfase alfa enzyme replacement therapy (ERT) were assessed in 173 patients with Morquio A syndrome (mucopolysaccharidosis IVA) in a 96-week, open-label, multi-center, phase 3 extension study (MOR-005) of the pivotal 24-week, placebo-controlled study (MOR-004). Changes in efficacy endpoints were evaluated over 120 weeks, from MOR-004 baseline to MOR-005 week 96. We report the impact of ERT on activities of daily living (ADL) across three domains (mobility, self-care, and caregiver-assistance), as assessed by the Mucopolysaccharidosis Health Assessment Questionnaire (MPS-HAQ) after 72 and 120 weeks or approximately 1 and 2 years. Results Mean baseline MPS-HAQ domain scores showed impairments in mobility, self-care, and independence. The MOR-005 intent-to-treat population (ITT; N = 169, including 158 with 2 years follow-up) showed sustained significant reductions (representing improvements) in mobility and self-care domain least square (LS) mean scores vs. baseline at 1 and 2 years and a non-significant decrease in the caregiver-assistance domain at 2 years. At week 120, LS mean (SE) changes from baseline were − 0.5 (0.1) for mobility (P = 0.002), − 0.4 (0.1) for self-care (P = 0.001), and − 1.0 (0.5) for caregiver-assistance (P = 0.06) (ITT population). Improvements in MPS-HAQ domain scores vs. baseline at 1 and 2 years were greater in patients continuously treated with the weekly dosing regimen than in the total MOR-005 population and statistically significant across domains. A comparable untreated cohort of patients from the Morquio A Clinical Assessment Program (MorCAP) natural history study (ITT population, N = 94, including 37 with 2 years follow-up) showed no improvement over 2 years, with two of the three domains worsening (LS mean (SE) changes from baseline: 0.3 (0.3) for mobility, 0.4 (0.2) for self-care, − 0.5 (0.8) for caregiver-assistance). Changes in LS mean scores vs. baseline were statistically significantly different between MOR-005 and MorCAP for the mobility domain (− 0.7 (SE 0.4), P = 0.0490) and the self-care domain (− 0.7 (SE 0.3), P = 0.0146) at 2 years. Conclusions Together, these findings suggest that long-term elosulfase alfa ERT is associated with partial recovery of functional abilities, improving Morquio A patients' abilities to perform ADL. Trial registration: ClinicalTrials.gov NCT01415427 . Registered 8 August 2011, retrospectively registered.

Published

2017

35. Guidelines for diagnosis and treatment of Hunter Syndrome for clinicians in Latin America

Author

Mara Lucia Schmitz Ferreira Santos, Roberto Giugliani, Luz Norela Correa Garzón, Ana Maria Martins, C. Araceli Arellano Valdez, Hernan Amartino, Norberto Guelbert, Juan Francisco Cabello, Aída Lemes, Martha Solano Villarreal, Angelina Xavier Acosta, and Antonieta Mahfoud Hawilou

Subjects

Pediatrics, medicine.medical_specialty, Lysosomal disease, lcsh:QH426-470, Idursulfase, iduronate-2-sulfatase, Terapia de reposição de enzimas, Review Article, treatment guidelines, Biology, Iduronato sulfase, Mucopolissacaridose II, Treatment guidelines, Genetics, medicine, Hernia, Respiratory function, Molecular Biology, lysosomal disease, Genetic disorder, Macrocephaly, Iduronate-2-sulfatase, Hunter syndrome, Enzyme replacement therapy, medicine.disease, lcsh:Genetics, medicine.symptom, medicine.drug, enzyme replacement therapy

Abstract

This review aims to provide clinicians in Latin America with the most current information on the clinical aspects, diagnosis, and management of Hunter syndrome, a serious and progressive disease for which specific treatment is available. Hunter syndrome is a genetic disorder where iduronate-2-sulfatase (I2S), an enzyme that degrades glycosaminoglycans, is absent or deficient. Clinical manifestations vary widely in severity and involve multiple organs and tissues. An attenuated and a severe phenotype are recognized depending on the degree of cognitive impairment. Early diagnosis is vital for disease management. Clinical signs common to children with Hunter syndrome include inguinal hernia, frequent ear and respiratory infections, facial dysmorphisms, macrocephaly, bone dysplasia, short stature, sleep apnea, and behavior problems. Diagnosis is based on screening urinary glycosaminoglycans and confirmation by measuring I2S activity and analyzing I2S gene mutations. Idursulfase (recombinant I2S) (Elaprase(®), Shire) enzyme replacement therapy (ERT), designed to address the underlying enzyme deficiency, is approved treatment and improves walking capacity and respiratory function, and reduces spleen and liver size and urinary glycosaminoglycan levels. Additional measures, responding to the multi-organ manifestations, such as abdominal/inguinal hernia repair, carpal tunnel surgery, and cardiac valve replacement, should also be considered. Investigational treatment options such as intrathecal ERT are active areas of research, and bone marrow transplantation is in clinical practice. Communication among care providers, social workers, patients and families is essential to inform and guide their decisions, establish realistic expectations, and assess patients' responses.

Published

2014

36. Guía para el diagnóstico, seguimiento y tratamiento de la enfermedad de Fabry

Author

Pablo Neumann, Norberto Antongiovanni, Alejandro Fainboim, Isaac Kisinovsky, Hernán Amartino, Gustavo Cabrera, Sergio Carmona, Romina Ceci, Alberto Cicerán, Martín Choua, Griselda Doxastakis, Sonia De Maio, Roberto Ebner, Ana María Escobar, Gustavo Ferrari, Mariano Forrester, Norberto Guelbert, Paula Luna, Cinthia Marchesoni, Francisca Masllorens, Juan Politei, Ricardo Reisin, Diego Ripeau, Paula Rozenfeld, Graciela Serebrinsky, Ana Lía Tarabuso, and Juan Trípoli

Subjects

lcsh:Immunologic diseases. Allergy, Enfermedad de Fabry, Diagnóstico, lcsh:R, lcsh:Medicine, lcsh:RC109-216, lcsh:RC581-607, Seguimiento, Terapia de reemplazo enzimático, Guía, lcsh:Infectious and parasitic diseases

Abstract

La enfermedad de Fabry es un trastorno de almacenamiento lisosomal hereditario ligado al cromosoma X, ocasionado por el déficit de la enzima alfa galactosidasa A. El conocimiento sobre esta patología, y en particular su manejo médico, ha progresado notablemente en la última década, incluyendo el desarrollo de su tratamiento específico. La presente guía fue desarrollada por profesionales médicos de diversas especialidades involucrados en la atención de pacientes con enfermedad de Fabry. La discusión y análisis de las evidencias científicas disponibles, sumado a la experiencia de cada uno de los participantes, ha permitido desarrollar los conceptos vertidos en esta guía con el objetivo de brindar una herramienta útil para todos los profesionales que asisten a pacientes con enfermedad de Fabry.

Published

2013

37. The Morquio A Clinical Assessment Program: Baseline results illustrating progressive, multisystemic clinical impairments in Morquio A subjects

Author

Carla E. M. Hollak, Ana Maria Martins, Rossella Parini, Karl Eugen Mengel, Barbara K. Burton, Norberto Guelbert, Shuan-Pei Lin, Celeste Decker, Ashok Vellodi, Simon Jones, Paul Harmatz, Christian J. Hendriksz, Nathalie Guffon, Roberto Giugliani, Peter Slasor, Vassili Valayannopoulos, John J. Mitchell, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Endocrinology

Subjects

Adult, Male, Vital capacity, medicine.medical_specialty, Adolescent, Cross-sectional study, Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, Motor Activity, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, Elosulfase alfa, Quality of life, Surveys and Questionnaires, Internal medicine, Activities of Daily Living, Genetics, medicine, Humans, Medical history, Respiratory function, Child, Exercise, Molecular Biology, Glycosaminoglycans, 030304 developmental biology, 0303 health sciences, business.industry, Infant, Newborn, Infant, Mucopolysaccharidosis IV, medicine.disease, United States, Respiratory Function Tests, Cross-Sectional Studies, chemistry, Keratan Sulfate, Child, Preschool, Physical Endurance, Quality of Life, Physical therapy, Female, business, 030217 neurology & neurosurgery

Abstract

Objectives The objectives of this study are to quantify endurance and respiratory function and better characterize spectrum of symptoms and biochemical abnormalities in mucopolysaccharidosis IVA subjects. Methods MorCAP was a multicenter, multinational, cross sectional study amended to be longitudinal in 2011. Each study visit required collection of medical history, clinical assessments, and keratan sulfate (KS) levels. Results Data from the first visit of 325 subjects (53% female) were available. Mean age was 14.5 years. Mean ± SD height z-scores were − 5.6 ± 3.1 as determined by the CDC growth charts. Mean ± SD from the 6-minute-walk-test was 212.6 ± 152.2 m, revealing limitations in functional endurance testing, and 30.0 ± 24.0 stairs/min for the 3-minute-stair-climb test. Respiratory function showed limitations comparable to MPS VI patients; mean ± SD was 1.2 ± 0.9 l based on forced vital capacity and 34.8 ± 25.5 l/min based on maximum voluntary ventilation. Mean urinary keratan sulfate (uKS) was elevated for all ages, and negatively correlated with age. Higher uKS correlated with greater clinical impairment based on height z-scores, endurance and respiratory function tests. The MPS Health Assessment Questionnaire reveals impairments in mobility and activities of daily living in comparison to an age-matched control population. Conclusions MPS IVA is a multisystem disorder with a continuum of clinical presentation. All affected individuals experience significant functional limitations and reduced quality of life. Older patients have more severe exercise and respiratory capacity limitations, and more frequent cardiac pathology illustrating the progressive nature of disease.

Published

2013

38. Neuronal ceroid lipofuscinosis type CLN2: A new rationale for the construction of phenotypic subgroups based on a survey of 25 cases in South America

Author

Patricia Pons, Mónica Troncoso, Raquel Dodelson de Kremer, Graciela Alonso, Ana María Oller-Ramírez, Katherine B. Sims, Winnie Xin, Norberto Guelbert, Scarlet Witting, Romina Kohan, Inés Adriana Cismondi, Inés Noher de Halac, David A. Pearce, and María Noelia Carabelos

Subjects

Adult, Male, Adolescent, media_common.quotation_subject, Nonsense, Argentina, Biology, medicine.disease_cause, Aminopeptidases, Article, Young Adult, Microscopy, Electron, Transmission, Neuronal Ceroid-Lipofuscinoses, Genetics, medicine, Humans, Missense mutation, Prospective Studies, Allele, Child, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Alleles, Retrospective Studies, media_common, Mutation, Tripeptidyl-Peptidase 1, Alternative splicing, Intron, Computational Biology, Reproducibility of Results, General Medicine, South America, medicine.disease, Phenotype, Introns, Pedigree, Alternative Splicing, Child, Preschool, Female, Neuronal ceroid lipofuscinosis, Serine Proteases

Abstract

Tripeptidyl-peptidase 1 (TPP1) null or residual activity occurs in neuronal ceroid lipofuscinosis (NCL) with underlying TPP1/CLN2 mutations. A survey of 25 South American CLN2 affected individuals enabled the differentiation of two phenotypes: classical late-infantile and variant juvenile, each in approximately 50% of patients, with residual TPP1 activity occurring in approximately 32%. Each individual was assigned to one of three subgroups: (I) n = 11, null TPP1 activity in leukocytes; (II) n = 8, residual TPP1 activity of 0.60–15.85 nmol/h/mg (nr 110–476); (III) n = 6, activity not measured in leukocytes. Curvilinear bodies (CB) appeared in almost all studied CLN2 subjects; the only exceptions occurred in cases of subgroup II: two individuals had combined CBs/fingerprints (FPs), and one case had pure FPs. There were 15 mutations (4 first published in this paper, 3 previously observed in South America by our group, and 8 previously observed by others). In subgroup I, mutations were either missense or nonsense; in subgroups II and III, mutations prevailed at the non-conserved intronic site, c.887 − 10A>G (intron 7), and to a lesser extent at c.89 + 5G>C (intron 2), in heterozygous combinations. Grouping phenotypically and genetically known individuals on the basis of TPP1 activity supported the concept that residual enzyme activity underlies a protracted disease course. The prevalence of intronic mutations at non-conserved sites in subgroup II individuals indicates that some alternative splicing might allow some residual TPP1 activity.

Published

2013

39. Impact of long-term elosulfase alfa treatment on respiratory function in patients with Morquio A syndrome

Author

Julian Raiman, Robert Matousek, Paul Harmatz, Elaina Jurecki, John J. Mitchell, Moeenaldeen Al-Sayed, Roberto Giugliani, Celeste Decker, Fiona Stewart, Kenneth I. Berger, Norberto Guelbert, Derralynn Hughes, Christian J. Hendriksz, Barbara K. Burton, and Rossella Parini

Subjects

0301 basic medicine, Adult, Male, Pediatrics, medicine.medical_specialty, Adolescent, Clinical Sciences, Morquio A syndrome, 030105 genetics & heredity, law.invention, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Elosulfase alfa, Randomized controlled trial, Double-Blind Method, law, Forced Expiratory Volume, Genetics, medicine, Humans, Genetics(clinical), Respiratory function, In patient, Enzyme Replacement Therapy, Child, Preschool, Genetics (clinical), Aged, Genetics & Heredity, business.industry, Respiration, Mucopolysaccharidosis IV, Enzyme replacement therapy, Middle Aged, Long-Term Care, Chondroitinsulfatases, 3. Good health, Surgery, Respiratory Function Tests, Clinical trial, chemistry, Child, Preschool, Original Article, Female, business, 030217 neurology & neurosurgery

Abstract

Objective To present long-term respiratory function outcomes from an open-label, multi-center, phase 3 extension study (MOR-005) of elosulfase alfa enzyme replacement therapy (ERT) in patients with Morquio A syndrome. Methods In part 1 of MOR-005, patients initially randomized to ERT in the 24-week pivotal study (MOR-004) remained on their regimen (2.0 mg/kg/week or every other week); placebo patients were re-randomized to one of the two regimens. During part 2, all patients received elosulfase alfa 2.0 mg/kg/week. Respiratory function was one of the efficacy endpoints evaluated in MOR-005. Change from MOR-004 baseline to 120 weeks of treatment for the combined population was determined and compared with results from untreated patients from a Morquio A natural history study (MorCAP). Results Maximum voluntary ventilation (MVV) improved up to week 72 and then stabilized; forced vital capacity (FVC) and forced expiratory volume in 1 s (FEV1) increased continuously over 120 weeks. Mean increases in the modified per-protocol population was 9.2 % for FVC, 8.8 % for FEV1, and 6.1 % for MVV after 120 weeks. All patients ≤14 years showed respiratory improvements, presumably in part related to growth; however, these were greater in treated patients. For those >14 years, treated patients showed improvements, while deterioration occurred in untreated. Altogether, the improvements were significantly greater (P

Published

2016

40. Evaluation of Bone Mineral Density in Patients with Type 1 Gaucher Disease in Argentina

Author

M. Rapetti, Maria Silvia Larroude, M. Alvarez Bollea, Adriana Arizo, K. Muller, G. Pujal, Marta Dragosky, Norberto Guelbert, A. Degano, Gabriel Aguilar, Leonardo Feldman, Hugo Robledo, Sandra Zirone, Graciela Elena, A. Albina, R. Jaureguiberry, Alba A Ruiz, M. Slago, Andrea Schenone, Juan Jose Chain, G. Galvan, Nora Watman, Gustavo L. Kantor, Alcira Fynn, Julieta Bietti, P. Reichel, N. Fernandez Escobar, Guillermo Drelichman, R. Fernandez, F. Del Rio, M. Marquez, Alejandra Maro, Marcela A Aznar, G. Zarate, Ignacio Rossi, M.A. Barbieri, V. Bacciedoni, M. Bolesina, H. Arrocena, I. Fernandez, Nora Basack, G. Fernandez, G. Buchovsky, V. Lanza, María Fernanda Cuello, and S. E. Veber

Subjects

musculoskeletal diseases, 0301 basic medicine, Adult, Male, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, Osteoporosis, Argentina, 030209 endocrinology & metabolism, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Absorptiometry, Photon, Bone Density, medicine, Humans, Radiology, Nuclear Medicine and imaging, Orthopedics and Sports Medicine, In patient, Child, Femoral neck, Aged, Bone mineral, Gaucher Disease, Lumbar Vertebrae, business.industry, Femur Neck, Type 1 Gaucher Disease, Enzyme replacement therapy, Middle Aged, medicine.disease, Surgery, Osteopenia, Bone Diseases, Metabolic, medicine.anatomical_structure, Female, 030101 anatomy & morphology, Densitometry, Nuclear medicine, business

Abstract

The purpose of this study was to evaluate the frequency of osteoporosis (OP) in patients with Gaucher disease (GD) in Argentina. GD patients from 28 centers were consecutively included from April 2012 to 2014. Bone mineral density (BMD) was determined by dual X-ray absorptiometry in the lumbar spine and the femoral neck or the total proximal femur for patients ≥20 yr of age, and by whole-body scan in the lumbar spine in patients20 yr of age. In children, mineral density was calculated using the chronological age and Z height. OP diagnosis was determined following adult and pediatric official position of the International Society for Clinical Densitometry. A total of 116 patients were included, of which 62 (53.5%) were women. The median age was 25.8 yr. All patients received enzyme replacement therapy, with a median time of 9.4 yr. Normal BMD was found in 89 patients (76.7%), whereas low bone mass (LBM) or osteopenia was found in 15 patients (13%) and OP in 12 patients (10.3%). The analysis of the pediatric population revealed that 4 patients (9.3%) had LBM and 3 (7%) had OP (Z-score ≤ -2 + fractures height-adjusted by Z), whereas in the adult population (n = 73), 11 patients (15%) had LBM or osteopenia and 9 (12.3%) had OP. Bone marrow infiltration and the presence of fractures were significantly correlated with the presence of OP (p = 0.04 and0.001, respectively). This is the first study in Argentina and in the region describing the frequency of OP or LBM in GD patients treated with imiglucerase using the official position of the International Society for Clinical Densitometry.

Published

2016

41. Long-term endurance and safety of elosulfase alfa enzyme replacement therapy in patients with Morquio A syndrome

Author

Kenneth I. Berger, Elaina Jurecki, Julian Raiman, John J. Mitchell, Rossella Parini, Peter Slasor, Fiona Stewart, Moeenaldeen Al-Sayed, Christian J. Hendriksz, Roberto Giugliani, Derralynn Hughes, Martha Solano Villarreal, Barbara K. Burton, Paul Harmatz, Norberto Guelbert, Robert Matousek, and Adam J. Shaywitz

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, Population, Context (language use), Placebo, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Endocrinology, Elosulfase alfa, Double-Blind Method, Internal medicine, Genetics, medicine, Humans, Enzyme Replacement Therapy, Dosing, education, Adverse effect, Child, Molecular Biology, Aged, education.field_of_study, Intention-to-treat analysis, business.industry, Mucopolysaccharidosis IV, Middle Aged, Chondroitinsulfatases, 3. Good health, Surgery, 030104 developmental biology, chemistry, Keratan Sulfate, Child, Preschool, Cohort, Physical Endurance, Female, business, 030217 neurology & neurosurgery

Abstract

Long-term efficacy and safety of elosulfase alfa enzyme replacement therapy were evaluated in Morquio A patients over 96weeks (reaching 120weeks in total from pre-treatment baseline) in an open-label, multi-center, phase III extension study. During this extension of a 24-week placebo-controlled phase III study, all patients initially received 2.0mg/kg elosulfase alfa either weekly or every other week, prior to establishment of 2.0mg/kg/week as the recommended dose, at which point all patients received weekly treatment. Efficacy measures were compared to baseline of the initial 24-week study, enabling analyses of changes over 120weeks. In addition to performing analyses for the entire intent-to-treat (ITT) population (N=173), analyses were also performed for a modified per-protocol (MPP) population (N=124), which excluded patients who had orthopedic surgery during the extension study or were non-compliant with the study protocol (as determined by ≥20% missed infusions). Six-minute walk test (6MWT) was the primary efficacy measure; three-minute stair climb test (3MSCT) and normalized urine keratan sulfate (uKS) were secondary efficacy measures. Mean (SE) change from baseline to Week 120 in 6MWT distance was 32.0 (11.3)m and 39.9 (10.1)m for patients receiving elosulfase alfa at 2.0mg/kg/week throughout the study (N=56) and 15.1 (7.1)m and 31.7 (6.8)m in all patients combined, regardless of dosing regimen, for the ITT and MPP populations, respectively. Further analyses revealed that durability of 6MWT improvements was not impacted by baseline 6MWT distance, use of a walking aid, or age. Mean (SE) change at Week 120 in the 3MSCT was 5.5 (1.9) and 6.7 (2.0)stairs/min for patients receiving elosulfase alfa at 2.0mg/kg/week throughout the study and 4.3 (1.2) and 6.8 (1.3)stairs/min in all patients combined, regardless of dosing regimen, for the ITT and MPP populations, respectively Across all patients, mean (SE) change at Week 120 in normalized uKS was -59.4 (1.8)% and -62.3 (1.8)% in the ITT and MPP populations, respectively. In the absence of a placebo group, significance of the sustained improvements could not be evaluated directly. However, to provide context for interpretation of results, comparisons were performed with untreated patients from a Morquio A natural history study. In contrast to the results of the extension study, the untreated patients experienced constant uKS levels and a gradual decline in endurance test results over a similar period of time. Differences from the untreated natural history study patients were significant for 6MWT, 3MSCT, and uKS outcomes for the cohort of patients receiving optimal dosing throughout the study and for all cohorts pooled together, for both ITT and MPP populations (P

Published

2016

42. Therapeutic Approaches to the Challenge of Neuronal Ceroid Lipofuscinoses

Author

R. Kohan, Graciela Alonso, V. Tapia Anzolini, Ana María Oller-Ramírez, Inés Adriana Cismondi, Norberto Guelbert, Sara E. Mole, I. Noher de Halac, and R. Dodelson de Kremer

Subjects

Pharmaceutical Science, Biology, Article, Mucopolysaccharidosis type I, Neuronal Ceroid-Lipofuscinoses, medicine, Animals, Humans, Dementia, Enzyme Replacement Therapy, Polymorphism, Genetic, Clinical Trials, Phase I as Topic, Tripeptidyl-Peptidase 1, Neurodegeneration, PPT1, Genetic Therapy, Enzyme replacement therapy, medicine.disease, Phenotype, CLN3, CLN8, Mutation, Immunology, Stem cell, Neuroscience, Biotechnology

Abstract

The Neuronal Ceroid Lipofuscinoses (NCLs) are lysosomal storage diseases (LSDs) affecting the central nervous system (CNS), with generally with recessive inheritance. They are characterized by pathological lipofuscin-like material accumulating in cells. The clinical phenotypes at all onset ages show progressive loss of vision, decreasing cognitive and motor skills, epileptic seizures and premature death, with dementia without visual loss prominent in the rarer adult forms. Eight causal genes, CLN10/CTSD, CLN1/PPT1, CLN2/TPP1, CLN3, CLN5, CLN6, CLN7/MFSD8, CLN8, with more than 269 mutations and 49 polymorphisms (http://www.ucl.ac.uk/ncl) have been described. Other NCL genes are hypothesized, including CLN4 and CLN9; CLCN6, CLCN7 and possibly SGSH are under study. Some therapeutic strategies applied to other LSDs with significant systemic involvement would not be effective in NCLs due to the necessity of passing the blood brain barrier to prevent the neurodegeneration, repair or restore the CNS functionality. There are therapies for the NCLs currently at preclinical stages and under phase 1 trials to establish safety in affected children. These approaches involve enzyme replacement, gene therapy, neural stem cell replacement, immune therapy and other pharmacological approaches. In the next decade, progress in the understanding of the natural history and the biochemical and molecular cascade of events relevant to the pathogenesis of these diseases in humans and animal models will be required to achieve significant therapeutic advances.

Published

2011

43. Recommendations for evaluation and management of pain in patients with mucopolysaccharidosis in Latin America

Author

Carolina Fischinger Moura de Souza, Martha Solano, Norberto Guelbert, Gisel Gordillo Gonzalez, Charles Marques Lourenço, Mariana M. Junqueira, and Juan Politei

Subjects

Pediatrics, medicine.medical_specialty, Latin Americans, business.industry, Endocrinology, Diabetes and Metabolism, Mucopolysaccharidosis, medicine.disease, Biochemistry, Endocrinology, Genetics, medicine, In patient, business, Molecular Biology

Published

2018

44. CLN2 disease (neuronal ceroid lipofuscinosis type 2): Experience in the real world with cerliponase alfa intracerebroventricular enzyme replacement therapy in a public hospital in Cordoba, Argentina

Author

Victor Munoz, Guillermo Guelbert, Francisco Pueyrredon, Guillermo Seratti, Roberto Caraballo, Norberto Guelbert, Raul Jalil, Tatiana Rodrigo, and Daniel Velazquez

Subjects

Pediatrics, medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, Disease, Enzyme replacement therapy, Cerliponase alfa, Biochemistry, Neuronal Ceroid Lipofuscinosis Type 2, Endocrinology, Public hospital, Genetics, Medicine, business, Molecular Biology

Published

2018

45. Enfermedad de Morquio (mucopolisacaridosis IV-A): aspectos clínicos, diagnósticos y nuevo tratamiento con terapia de reemplazo enzimático

Author

Andrea Schenone, Norberto Guelbert, Juan Politei, Alejandro Fainboim, and Marina Szlago

Subjects

medicine.medical_specialty, business.industry, Mucopolysaccharidosis, Mucopolysaccharidosis type IV, Enzyme replacement therapy, medicine.disease, Short stature, chemistry.chemical_compound, Elosulfase alfa, chemistry, Internal medicine, Pediatrics, Perinatology and Child Health, medicine, Lysosomal storage disease, Mucopolysaccharidosis IV, medicine.symptom, business, Rare disease

Abstract

Mucopolysaccharidosis type IV-A (Morquio A disease) is an autosomal recessive lysosomal storage disease caused by mutations in the gene encoding the N-acetylgalactosamine-6-sulfate sulfatase, that results in impaired catabolism of two glycosaminoglycans, chondroitin-6-sulfate and keratan sulfate. Clinical presentations reflect a spectrum of progression from a severe phenotype to an attenuated expression. Accumulation of substrate manifests predominantly as short stature and skeletal dysplasia, including atlantoaxial instability and cervical cord compression. Other abnormalities in the visual, auditory, cardiovascular and respiratory systems can also affect individuals with Morquio disease. Elosulfase alfa showed in clinical trials in children and adults a significant and sustained improvement in endurance and urinary levels of keratan sulfate. Data from the ongoing observational, multinational Morquio A Registry Study will provide valuable information on the long-term efficacy and safety of elosulfase alfa in patients, as well as on the natural history of this very rare disease.

Published

2015

46. Identification of a common mutation in mucopolysaccharidosis IVA: correlation among genotype, phenotype, and keratan sulfate

Author

Piedad Sarmient, Tatiana Dieter, Adriana M. Montaño, Luis A. Barrera, Ida Vanessa Doederlein Schwartz, Raquel Dodelson de Kremer, Tatsuo Nishioka, Olga Peña Serrato, Norberto Guelbert, Seiji Yamaguchi, Roberto Giugliani, Shunji Tomatsu, Akihiko Noguchi, Monica A. Gutierrez, and Gabriela M. Repetto

Subjects

Adult, Male, Adolescent, Genotype, Mucopolysaccharidosis, Mutant, Mutation, Missense, Biology, Gene mutation, medicine.disease_cause, Mucopolysaccharidosis Type IVA, Gene Frequency, Genetics, medicine, Humans, Missense mutation, Genetic Testing, Child, Genetics (clinical), DNA Primers, Mutation, Sequence Analysis, DNA, South America, medicine.disease, Molecular biology, Chondroitinsulfatases, Phenotype, Keratan Sulfate, Child, Preschool, Female, Allelic heterogeneity

Abstract

Mucopolysaccharidosis IVA (MPS IVA) is a lysosomal storage disorder caused by the deficiency of N-acetylgalactosamine-6-sulfate sulfatase (GALNS). Mutation screening of the GALNS was performed by genomic PCR and direct sequence analyses in 20 MPS IVA patients from Latin America. In this study, 12 different gene mutations including nine unreported ones were identified in 16 severe and four attenuated patients and accounted for 90.0% of the unrelated mutant alleles. The gene alterations were missense mutations except one insertion. Six recurrent mutations, p.A75G, p.G116S, p.G139S, p.N164T, p.R380S, and p.R386C, accounted for 5.0, 10.0, 5.0, 7.5, 5.0, and 32.5% of the unrelated mutant alleles, respectively. The p.R386C mutation was identified in all Latin American populations studied. Eleven mutations correlated with a severe form, while one mutation, p.R380S, was associated with an attenuated form. MPS IVA patients had an elevation of urine and plasma keratan sulfate (KS) concentrations compared with those of the age-matched control. KS concentrations in severe patients were higher than those in attenuated patients. These data provide evidence for extensive allelic heterogeneity and presence of a common mutation in Latin American patients. Accumulation of mutations with clinical description and KS concentration will lead us to predict clinical severity of the patient more precisely.

Published

2004

47. Expert opinion on the management of CLN2 disease

Author

Angela Schulz, Svetlana Mikhailova, Lenora Lehwald, Charlie Fairhurst, Renée Shediac, Ruth Williams, Szilard Kiss, Jessica L. Cohen-Pfeffer, Heather R. Adams, Meral Topçu, Jonas Denecke, Martin Blohm, Annamaria Kofler, Ina von Löbbecke, Margie Frazier, Norberto Guelbert, Mary-Anne Leung, Katherine B. Sims, Emily de los Reyes, Jonathan W. Mink, John A. Lawson, Andrea West, Miriam Nickel, Nicola Specchio, and Kristen Drago

Subjects

Medical education, Endocrinology, Endocrinology, Diabetes and Metabolism, Expert opinion, Genetics, Disease, Psychology, Molecular Biology, Biochemistry

Published

2016

48. [Morquio disease (Mucopolysaccharidosis type IV-A): clinical aspects, diagnosis and new treatment with enzyme replacement therapy]

Author

Juan, Politei, Andrea B, Schenone, Norberto, Guelbert, Alejandro, Fainboim, and Marina, Szlago

Subjects

Child, Preschool, Humans, Mucopolysaccharidosis IV, Enzyme Replacement Therapy, Chondroitinsulfatases

Abstract

Mucopolysaccharidosis type IV-A (Morquio A disease) is an autosomal recessive lysosomal storage disease caused by mutations in the gene encoding the N-acetylgalactosamine-6-sulfate sulfatase, that results in impaired catabolism of two glycosaminoglycans, chondroitin-6-sulfate and keratan sulfate. Clinical presentations reflect a spectrum of progression from a severe phenotype to an attenuated expression. Accumulation of substrate manifests predominantly as short stature and skeletal dysplasia, including atlantoaxial instability and cervical cord compression. Other abnormalities in the visual, auditory, cardiovascular and respiratory systems can also affect individuals with Morquio disease. Elosulfase alfa showed in clinical trials in children and adults a significant and sustained improvement in endurance and urinary levels of keratan sulfate. Data from the ongoing observational, multinational Morquio A Registry Study will provide valuable information on the long-term efficacy and safety of elosulfase alfa in patients, as well as on the natural history of this very rare disease.

Published

2015

49. Longitudinal analysis of endurance and respiratory function from a natural history study of Morquio A syndrome

Author

Peter Slasor, Ashok Vellodi, Celeste Decker, Ana Maria Martins, Norberto Guelbert, Frits A. Wijburg, Rossella Parini, Roberto Giugliani, Ke Yang, Nathalie Guffon, John J. Mitchell, Vassili Valayannopoulos, Paul Harmatz, Barbara K. Burton, Christian J. Hendriksz, Simon Jones, Shuan-Pei Lin, Karl Eugen Mengel, Amsterdam Gastroenterology Endocrinology Metabolism, Paediatric Metabolic Diseases, UCSF Benioff Childrens Hosp Oakland, MC Univ Mainz, Dept Genet UFRGS, INAGEMP, Hop Univ Necker Enfants Malad, Mackay Mem Hosp, Mackay Med Coll, San Gerardo Univ Hosp, Hop Femme Mere Enfant, Ann & Robert H Lurie Childrens Hosp, Northwestern Univ, Birmingham Childrens Hosp NHS Fdn Trust, McGill Univ, Universidade Federal de São Paulo (UNIFESP), Univ Manchester, Hosp Ninos Cordoba, Great Ormond St Hosp Children NHS Fdn Trust, Univ Amsterdam, and BioMarin Pharmaceut Inc

Subjects

Adult, Male, Vital capacity, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, Morquio A syndrome, Motor Activity, MPS IVA, Biochemistry, 6 minute walk test, Endurance, Young Adult, FEV1/FVC ratio, chemistry.chemical_compound, Endocrinology, Elosulfase alfa, Morquio A, Forced Expiratory Volume, Internal medicine, Genetics, Humans, Medicine, Respiratory function, Mucopolysaccharidosis IVA, Longitudinal Studies, Child, Molecular Biology, business.industry, Respiration, Longitudinal analysis, Infant, Mucopolysaccharidosis IV, Repeated measures design, Maximal Voluntary Ventilation, Middle Aged, chemistry, Child, Preschool, Ambulatory, Physical Endurance, Cardiology, Physical therapy, Female, business, Natural history study

Abstract

Objectives: Baseline data from the Morquio A Clinical Assessment Program (MorCAP) revealed that individuals with Morquio A syndrome show substantial impairment in multiple domains including endurance and respiratory function (Harmatz et al., Mol Genet Metab, 2013). Here, 1- and 2-year longitudinal endurance and respiratory function data are presented.Methods: Endurance was assessed using the 6-minute walk test (6MWT) and the 3-minute stair climb test (3MSCT). Respiratory function was evaluated by measuring forced vital capacity (PVC) and maximum voluntary ventilation (MW). Data were analyzed using repeated measures ANCOVA models. Annualized estimates of change were determined using model estimates and interpolation.Results: 353, 184, and 78 subjects were assessed at Year 0 (baseline), Year 1, and Year 2, respectively. the overall annualized estimate of change (SE) in 6MWT distance was -4.86 +/- 3.25 m; a larger decline of -6.84 +/- 5.38 m was observed in the subset of subjects meeting the inclusion/exclusion criteria of the Phase 3 clinical trial of elosulfase alfa (>= 5 years of age with baseline 6MWT distance >= 30 and

Published

2015

50. [Untitled]

Author

Gabriel Civallero, Carlos Quiroga Mayor, Catalina Depetris-Boldini, E. Regula Baumgartner, Terttu Suormala, Norberto Guelbert, Ana E. Paschini-Capra, Laura E. Laróvere, Raquel Dodelson de Kremer, and Alexandra Latini

Subjects

medicine.medical_specialty, Leukodystrophy, Biology, 3-Methylcrotonyl-CoA carboxylase deficiency, medicine.disease, Biochemistry, Hypotonia, White matter, Central nervous system disease, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Cerebrospinal fluid, medicine.anatomical_structure, Endocrinology, Biotin, chemistry, Internal medicine, Failure to thrive, medicine, Neurology (clinical), medicine.symptom

Abstract

We report the first case of isolated biotin resistant 3-methylcrotonyl-CoA carboxylase (MCC) deficiency in Argentina. The diagnosis was established at 14 months of age by urinary organic-acid analysis and confirmed by enzyme assay in fibroblasts. The patient suffered from severe psychomotor retardation, hypotonia, areflexia, and failure to thrive, and died unexpectedly at 3 years 4 months of life. Brain MRI at 14 months showed signals of the white matter on cerebral T2-weighted, which were indicative of confluent and multiple foci of leukodystrophy, a pattern not previously described in this entity. In addition, high levels of oxypurines were detected in cerebrospinal fluid. This might be related to energetic consequences of the enzyme deficiency in the brain. This case extends the phenotype of isolated MCC deficiency in infancy and suggests this entity should be considered to be one of the possible causes of “metabolic leukodystrophies.”

Published

2002