Your search keyword '"Severe phenotype"' showing total 270 results

1. Li-Fraumeni syndrome presenting with de novo TP53 mutation, severe phenotype and advanced paternal age: a case report

Author

Juan Pablo Arango-Ibañez, Luis Gabriel Parra-Lara, Ángela R. Zambrano, and Lisa Ximena Rodríguez-Rojas

Subjects

Li Fraumeni syndrome, TP53, P53, De novo mutation, Advanced paternal age, Severe phenotype, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Genetics, QH426-470

Abstract

Abstract Background Li-Fraumeni syndrome (LFS) is an autosomal dominant hereditary cancer syndrome caused by pathogenic variants in the gene TP53. This gene codes for the P53 protein, a crucial player in genomic stability, which functions as a tumor suppressor gene. Individuals with LFS frequently develop multiple primary tumors at a young age, such as soft tissue sarcomas, breast cancer, and brain tumors. Case presentation A 38 years-old female with a history of femur osteosarcoma, ductal carcinoma of the breast, high-grade breast sarcoma, pleomorphic sarcoma of the left upper limb, infiltrating lobular carcinoma of the breast, gastric adenocarcinoma, leiomyosarcoma of the right upper limb, and high-grade pleomorphic renal sarcoma. Complete molecular sequencing of the TP53 gene showed c.586 C > T (p.R196X) in exon 6, which is a nonsense mutation that produces a shorter and malfunctioning P53. Family history includes advanced father’s age at the time of conception (75 years), which has been associated with an increased risk of de novo germline mutations. The patient had seven paternal half-siblings with no cancer history. The patient received multiple treatments including surgery, systemic therapy, and radiotherapy, but died at the age of 38. Conclusions Advanced paternal age is a risk factor to consider when hereditary cancer syndrome is suspected. Early detection of hereditary cancer syndromes and their multi-disciplinary surveillance and treatment is important to improve clinical outcomes for these patients. Further investigation of the relationship between the pathogenic variant of TP53 and its phenotype may guide the stratification of surveillance and treatment.

Published

2024

2. Li-Fraumeni syndrome presenting with de novo TP53 mutation, severe phenotype and advanced paternal age: a case report

Author

Arango-Ibañez, Juan Pablo, Parra-Lara, Luis Gabriel, Zambrano, Ángela R., and Rodríguez-Rojas, Lisa Ximena

Published

2024

3. Heterozygous variant in FGFR3 underlying severe phenotypes in the second trimester: a case report

Author

Shujun Chen, Hongmei Dong, Yong Luo, Yingpin Zhang, and Pan Li

Subjects

Achondroplasia, FGFR3 gene, Heterozygous, Rare variant, Severe phenotype, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Achondroplasia is a congenital skeletal system malformation caused by missense variant of FGFR3 gene with an incidence of 1 per 20,000–30,000 newborns, which is an autosomal dominant inheritance disease. Despite similar imaging features, the homozygous achondroplasia is absolutely lethal due to thoracic stenosis, whereas heterozygous achondroplasia does not lead to fetal death. Case presentation A fetus with progressive rhizomelic short limbs and overt narrow chest was detected by prenatal ultrasound in the second trimester. Gene sequencing results of amniotic fluid sample indicated a rare missense variant NM_000142.4: c.1123G > T(p.Gly375Cys), leading to a glycine to cysteine substitution. Re-sequencing confirmed that it was a heterozygous variant, and thoracic stenosis was then confirmed in the corpse by radiological examination. Conclusions We identified a heterozygous variant of the FGFR3 gene as the rare pathogenic variant of severe achondroplasia in a fetus. Heterozygous variants of p.Gly375Cys may have a severe phenotype similar to homozygote. It’s crucial to combine prenatal ultrasound with genetic examination to differentiate heterozygous from homozygous achondroplasia. The p.Gly375Cys variant of FGFR3 gene may serve as a vital target for the diagnosis of severe achondroplasia.

Published

2023

4. Heterozygous variant in FGFR3 underlying severe phenotypes in the second trimester: a case report.

Author

Chen, Shujun, Dong, Hongmei, Luo, Yong, Zhang, Yingpin, and Li, Pan

Subjects

*GENETIC variation, *FETUS, *MISSENSE mutation, *PHENOTYPES, *FETAL death, *AMNIOTIC liquid, *ACHONDROPLASIA

Abstract

Background: Achondroplasia is a congenital skeletal system malformation caused by missense variant of FGFR3 gene with an incidence of 1 per 20,000–30,000 newborns, which is an autosomal dominant inheritance disease. Despite similar imaging features, the homozygous achondroplasia is absolutely lethal due to thoracic stenosis, whereas heterozygous achondroplasia does not lead to fetal death. Case presentation: A fetus with progressive rhizomelic short limbs and overt narrow chest was detected by prenatal ultrasound in the second trimester. Gene sequencing results of amniotic fluid sample indicated a rare missense variant NM_000142.4: c.1123G > T(p.Gly375Cys), leading to a glycine to cysteine substitution. Re-sequencing confirmed that it was a heterozygous variant, and thoracic stenosis was then confirmed in the corpse by radiological examination. Conclusions: We identified a heterozygous variant of the FGFR3 gene as the rare pathogenic variant of severe achondroplasia in a fetus. Heterozygous variants of p.Gly375Cys may have a severe phenotype similar to homozygote. It's crucial to combine prenatal ultrasound with genetic examination to differentiate heterozygous from homozygous achondroplasia. The p.Gly375Cys variant of FGFR3 gene may serve as a vital target for the diagnosis of severe achondroplasia. [ABSTRACT FROM AUTHOR]

Published

2023

5. Transcriptomics reveals a distinct metabolic profile in T cells from severe allergic asthmatic patients

Author

Carmela Pablo-Torres, Carlota Garcia-Escribano, Martina Romeo, Cristina Gomez-Casado, Ricardo Arroyo Solera, José Luis Bueno-Cabrera, M. del Mar Reaño Martos, Alfredo Iglesias-Cadarso, Carlos Tarín, Ioana Agache, Tomás Chivato, Domingo Barber, María M. Escribese, and Elena Izquierdo

Subjects

t cells, CD3+cells, allergy, transcriptomics, metabolism, severe phenotype, Immunologic diseases. Allergy, RC581-607

Abstract

The reasons behind the onset and continuation of chronic inflammation in individuals with severe allergies are still not understood. Earlier findings indicated that there is a connection between severe allergic inflammation, systemic metabolic alterations and impairment of regulatory functions. Here, we aimed to identify transcriptomic alterations in T cells associated with the degree of severity in allergic asthmatic patients. T cells were isolated from severe (n = 7) and mild (n = 9) allergic asthmatic patients, and control (non-allergic, non-asthmatic healthy) subjects (n = 8) to perform RNA analysis by Affymetrix gene expression. Compromised biological pathways in the severe phenotype were identified using significant transcripts. T cells' transcriptome of severe allergic asthmatic patients was distinct from that of mild and control subjects. A higher count of differentially expressed genes (DEGs) was observed in the group of individuals with severe allergic asthma vs. control (4,924 genes) and vs. mild (4,232 genes) groups. Mild group also had 1,102 DEGs vs. controls. Pathway analysis revealed alterations in metabolism and immune response in the severe phenotype. Severe allergic asthmatic patients presented downregulation in genes related to oxidative phosphorylation, fatty acid oxidation and glycolysis together with increased expression of genes coding inflammatory cytokines (e.g. IL-19, IL-23A and IL-31). Moreover, the downregulation of genes involved in TGFβ pathway together with a decreased tendency on the percentage of T regulatory cell (CD4 + CD25+), suggest a compromised regulatory function in severe allergic asthmatic patients. This study demonstrates a transcriptional downregulation of metabolic and cell signalling pathways in T cells of severe allergic asthmatic patients associated with diminished regulatory T cell function. These findings support a link between energy metabolism of T cells and allergic asthmatic inflammation.

Published

2023

6. Late onset Pompe Disease in India – Beyond the Caucasian phenotype.

Author

Puri, Ratna Dua, Setia, Nitika, N, Vinu, Jagadeesh, Sujatha, Nampoothiri, Sheela, Gupta, Neerja, Muranjan, Mamta, Bhat, Meenakshi, Girisha, Katta M, Kabra, Madhulika, Verma, Jyotsna, Thomas, Divya C., Biji, Ishpreet, Raja, Jayarekha, Makkar, Ravinder, Verma, Ishwar C, and Kishnani, Priya S.

Subjects

*GLYCOGEN storage disease type II, *LEFT ventricular hypertrophy, *PHENOTYPES, *CAUCASIAN race, *AORTIC valve insufficiency, *MUSCLE weakness

Abstract

• We report 20 LOPD patients from India. • The common c.−32–13T>G (IVS1) Caucasian mutation is absent. • Increased severity of disease phenotype with earlier age at disease onset. • Significant cardiac involvement than previously reported in Caucasian population. • GAA variant spectrum and novel variants. We evaluated the clinical histories, motor and pulmonary functions, cardiac phenotypes and GAA genotypes of an Indian cohort of twenty patients with late onset Pompe disease (LOPD) in this multi-centre study. A mean age at onset of symptoms and diagnosis of 9.9 ± 9.7 years and 15.8 ± 12.1 years respectively was identified. All patients had lower extremity limb-girdle muscle weakness. Seven required ventilatory support and seven used mobility assists. Of the four who used both assists, two received ventilatory support prior to wheelchair use. Cardiac involvement was seen in eight patients with various combinations of left ventricular hypertrophy, tricuspid regurgitation, cardiomyopathy, dilated ventricles with biventricular dysfunction and aortic regurgitation. Amongst 20 biochemically diagnosed patients (low residual GAA enzyme activity) GAA genotypes of 19 patients identified homozygous variants in eight and compound heterozygous in 11: 27 missense, 3 nonsense, 2 initiator codon, 3 splice site and one deletion. Nine variants in 7 patients were novel. The leaky Caucasian, splice site LOPD variant, c.−32−13T>G mutation was absent. This first study from India provides an insight into a more severe LOPD phenotype with earlier disease onset at 9.9 years compared to 33.3 years in Caucasian patients, and cardiac involvement more than previously reported. The need for improvement in awareness and diagnosis of LOPD in India is highlighted. [ABSTRACT FROM AUTHOR]

Published

2021

7. The role of enzyme replacement therapy in severe Hunter syndrome—an expert panel consensus

Author

Muenzer, Joseph, Bodamer, Olaf, Burton, Barbara, Clarke, Lorne, Frenking, Gudrun Schulze, Giugliani, Roberto, Jones, Simon, Rojas, Maria Verónica Muñoz, Scarpa, Maurizio, Beck, Michael, and Harmatz, Paul

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Rare Diseases, Clinical Research, Disease Progression, Enzyme Replacement Therapy, Humans, Iduronate Sulfatase, Mucopolysaccharidosis II, Phenotype, Practice Guidelines as Topic, Treatment Outcome, Hunter syndrome, Enzyme replacement therapy, Idursulfase, Cognitive impairment, Severe phenotype, Paediatrics and Reproductive Medicine, Public Health and Health Services, Pediatrics, Paediatrics

Abstract

UnlabelledIntravenous enzyme replacement therapy (ERT) with idursulfase for Hunter syndrome has not been demonstrated to and is not predicted to cross the blood-brain barrier. Nearly all published experience with ERT with idursulfase has therefore been in patients without cognitive impairment (attenuated phenotype). Little formal guidance is available on the issues surrounding ERT in cognitively impaired patients with the severe phenotype. An expert panel was therefore convened to provide guidance on these issues. The clinical experience of the panel with 66 patients suggests that somatic improvements (e.g., reduction in liver volume, increased mobility, and reduction in frequency of respiratory infections) may occur in most severe patients. Cognitive benefits have not been seen. It was agreed that, in general, severe patients are candidates for at least a 6-12-month trial of ERT, excluding patients who are severely neurologically impaired, those in a vegetative state, or those who have a condition that may lead to near-term death. It is imperative that the treating physician discuss the goals of treatment, methods of assessment of response, and criteria for discontinuation of treatment with the family before ERT is initiated.ConclusionThe decision to initiate ERT in severe Hunter syndrome should be made by the physician and parents and must be based on realistic expectations of benefits and risks, with the understanding that ERT may be withdrawn in the absence of demonstrable benefits.

Published

2012

8. Clinical spectrum of severe chronic central serous chorioretinopathy and outcome of photodynamic therapy

Author

Mohabati D, van Dijk EHC, van Rijssen TJ, de Jong EK, Breukink MB, Martinez-Ciriano JP, Dijkman G, Hoyng CB, Fauser S, Yzer S, and Boon CJF

Subjects

Chronic central serous chorioretinopathy, photodynamic therapy, posterior cystoid retinal degeneration, severe phenotype, therapeutic outcome, Ophthalmology, RE1-994

Abstract

Danial Mohabati,1,2 Elon HC van Dijk,1 Thomas J van Rijssen,1 Eiko K de Jong,3 Myrte B Breukink,3 Jose P Martinez-Ciriano,4 Greet Dijkman,1 Carel B Hoyng,3 Sascha Fauser,5 Suzanne Yzer,4 Camiel JF Boon1,6 1Department of Ophthalmology, Leiden University Medical Center, Leiden, the Netherlands; 2Department of Ophthalmology, Rotterdam Ophthalmic Institute, Rotterdam, the Netherlands; 3Department of Ophthalmology, Donders Institute for Brain, Cognition and Behaviour, Radboud University Medical Center, Nijmegen, the Netherlands; 4Department of Ophthalmology, The Rotterdam Eye Hospital, Rotterdam, the Netherlands; 5Department of Ophthalmology, University Hospital of Cologne, Cologne, Germany; 6Department of Ophthalmology, Academic Medical Center, University of Amsterdam, Amsterdam, the Netherlands Purpose: To describe a spectrum of severe chronic central serous chorioretinopathy (cCSC) cases and their response to photodynamic therapy (PDT).Patients and methods: A total of 66 patients (81 eyes) with active severe cCSC were studied, and their response to PDT was compared with a control group consisting of 35 active cCSCs (37 eyes) that did not display characteristics of severity. Best-corrected visual acuity (BCVA) and complete resolution of subretinal fluid (SRF) were considered as main outcome measures.Results: In severe cCSC cases, we found cumulative areas of diffuse atrophic retinal pigment epithelium alterations in 48 eyes (59%), multiple “hot spots” of leakage in 36 eyes (44%), posterior cystoid retinal degeneration in 25 eyes (31%), and 13 eyes (16%) had a diffuse leakage on fluorescein angiography. After PDT treatment, BCVA increased in both groups, from 66 to 72 Early Treatment of Diabetic Retinopathy Study (ETDRS) letters in the case group (P

Published

2018

9. A DM1 family with interruptions associated with atypical symptoms and late onset but not with a milder phenotype.

Author

Ballester‐Lopez, Alfonsina, Koehorst, Emma, Almendrote, Miriam, Martínez‐Piñeiro, Alicia, Lucente, Giuseppe, Linares‐Pardo, Ian, Núñez‐Manchón, Judit, Guanyabens, Nicolau, Cano, Antoni, Lucia, Alejandro, Overend, Gayle, Cumming, Sarah A., Monckton, Darren G., Casadevall, Teresa, Isern, Irina, Sánchez‐Ojanguren, Josep, Planas, Albert, Rodríguez‐Palmero, Agustí, Monlleó‐Neila, Laura, and Pintos‐Morell, Guillem

Abstract

Carriage of interruptions in CTG repeats of the myotonic dystrophy protein kinase gene has been associated with a broad spectrum of myotonic dystrophy type 1 (DM1) phenotypes, mostly mild. However, the data available on interrupted DM1 patients and their phenotype are scarce. We studied 49 Spanish DM1 patients, whose clinical phenotype was evaluated in depth. Blood DNA was obtained and analyzed through triplet‐primed polymerase chain reaction (PCR), long PCR‐Southern blot, small pool PCR, AciI digestion, and sequencing. Five patients of our registry (10%), belonging to the same family, carried CCG interruptions at the 3′‐end of the CTG expansion. Some of them presented atypical traits such as very late onset of symptoms (> 50 years) and a severe axial and proximal weakness requiring walking assistance. They also showed classic DM1 symptoms including cardiac and respiratory dysfunction, which were severe in some of them. Sizes and interrupted allele patterns were determined, and we found a contraction and an expansion in two intergenerational transmissions. Our study contributes to the observation that DM1 patients carrying interruptions present with atypical clinical features that can make DM1 diagnosis difficult, with a later than expected age of onset and a previously unreported aging‐related severe disease manifestation. [ABSTRACT FROM AUTHOR]

Published

2020

10. Case report: An infantile lethal form of Albright hereditary osteodystrophy due to a GNAS mutation.

Author

Leclercq, Valérie, Benoit, Valérie, Lederer, Damien, Delaunoy, Melanie, Ruiz, Marcela, Halleux, Claire, Robaux, Olivier, Wanty, Catherine, and Maystadt, Isabelle

Subjects

*PSEUDO-pseudohypoparathyroidism, *GENETIC mutation, *PHENOTYPES, *SELF-expression, *JUVENILE diseases

Abstract

Key Clinical Message: Germline loss‐of‐function GNAS mutations are associated with multiple phenotypes, depending on the parental origin of the mutant allele. Here, we describe an infantile lethal form of atypical pseudohypoparathyroidism type 1a or 1c with severe Albright's hereditary osteodystrophy phenotype, underlying the extremely variable expressivity of this syndrome. Germline loss‐of‐function GNAS mutations are associated with multiple phenotypes, depending on the parental origin of the mutant allele. Here, we describe an infantile lethal form of atypical pseudohypoparathyroidism type 1a or 1c with severe Albright's hereditary osteodystrophy phenotype, underlying the extremely variable expressivity of this syndrome. [ABSTRACT FROM AUTHOR]

Published

2018

11. Reducing body myopathy – A new pathogenic FHL1 variant and literature review

Author

Isabella Araújo Mota, Pedro Nogueira Fontana, Alzira Alves de Siqueira Carvalho, and Carolina da Cunha Correia

Subjects

Adult, Male, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Adolescent, Biopsy, Mutation, Missense, Muscle Proteins, Reducing body myopathy, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Muscular Diseases, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Child, Muscle, Skeletal, Genetics (clinical), Muscle biopsy, medicine.diagnostic_test, biology, business.industry, Intracellular Signaling Peptides and Proteins, Genetic Diseases, X-Linked, Progressive muscle weakness, LIM Domain Proteins, Middle Aged, FHL1, Pedigree, Phenotype, 030104 developmental biology, Neurology, Severe phenotype, Child, Preschool, Mutation, Pediatrics, Perinatology and Child Health, biology.protein, Female, Creatine kinase, Neurology (clinical), business, 030217 neurology & neurosurgery, Progressive muscular weakness, Rare disease

Abstract

Reducing body myopathy (RBM) is a rare disease marked by progressive muscle weakness caused by a mutation in FHL1 gene. We describe a new pathogenic variant and contrasted it with 44 other cases identified in the literature. A male child presented at age 3 suffering frequent falls and progressive muscular weakness. At age 8, he was wheelchair-bound and required ventilatory support. His mother and sister died due to the same problem. Creatine kinase was 428 IU/L (190). Muscle biopsy showed typical reducing bodies, and genetic analysis identified a novel pathogenic hemizygous variant, c.370_375del. We identified 44 previous reported cases separated in two groups: 28 cases with mean age onset 7.6 ± 5 years and 16 with 26.7 ± 4.2 years. The time for the diagnosis was shorter to younger group. The initial symptoms, rigid spine, contractures, scoliosis and axial and neck weaknesses, dysphagia, cardiac involvement, were predominant in younger group. The variant c.369C G predominated in younger group and c.448T C in older one. Pathogenic variants positions seemed related to severe phenotype. Most wheelchair patients belonged to younger group. The data from this compilation and our case provided a general characterization spectrum and prognosis between two groups of age onset with RBM.

Published

2021

12. Discriminating minor and major forms of drug reaction with eosinophilia and systemic symptoms: Facial edema aligns to the severe phenotype

Author

Sarah Walsh, Daniel Creamer, Salvador J. Diaz-Cano, and Sophie Momen

Subjects

medicine.medical_specialty, Drug allergy, Dermatology, Single Center, Drug reaction with eosinophilia and systemic symptoms, 030207 dermatology & venereal diseases, 03 medical and health sciences, Basal (phylogenetics), 0302 clinical medicine, Eosinophilia, medicine, Edema, Humans, Angioedema, Facial edema, Hyperplasia, integumentary system, business.industry, equipment and supplies, medicine.disease, Phenotype, Pharmaceutical Preparations, Severe phenotype, 030220 oncology & carcinogenesis, Latency stage, Drug Hypersensitivity Syndrome, Histopathology, business, human activities

Abstract

Background Drug reaction with eosinophilia and systemic symptoms (DRESS) is a cutaneous and systemic drug allergy disorder. Patients exist on a severity spectrum, with some experiencing a mild form of the disorder that fails to meet the Registry of Severe Cutaneous Adverse Reactions (SCAR) to Drugs diagnostic criteria for DRESS. Objective We sought to determine whether there were any cutaneous or dermatopathologic features that discriminate between the mild form of DRESS (DRESS minor) and the severe phenotype (DRESS major). Methods Hospitalized patients from a single center with a diagnosis of DRESS were prospectively recruited over a 7-year period. Clinical and dermatopathologic features were analyzed to discriminate between DRESS minor and DRESS major. Results Forty-five patients were included, of whom 19 had a Registry of Severe Cutaneous Adverse Reactions (SCAR) to Drugs score of ≤3 (DRESS minor) and 26 had a score of ≥4 (DRESS major). The mean latency period (P = .001), fever >38.5 °C (P = .001), and a reaction lasting >15 days (P = .010) discriminated DRESS major from DRESS minor. Facial edema was the sole discerning cutaneous feature (P = .025). Discriminating histopathologic features included basal squamatization (P = .005), dermal red blood cell extravasation (P = .009), and interface inflammation (P = .005). Conclusion We propose a new classification system—DRESS minor—to distinguish the milder illness from the severe form, DRESS major. Facial edema and certain histopathologic features can help discriminate between major and minor versions.

Published

2021

13. The emerging role of inorganic elements as potential antigens in sarcoidosis

Author

Marcel Veltkamp and Els Beijer

Subjects

Pulmonary and Respiratory Medicine, Sarcoidosis, business.industry, Environmental Exposure, Disease, Silicon Dioxide, medicine.disease, Lymphocyte proliferation test, Pathogenesis, Berylliosis, Immunological Sensitization, Antigen, Severe phenotype, Occupational Exposure, Pulmonary fibrosis, Immunology, medicine, Humans, business

Abstract

Purpose of review Previous studies mainly described a role for organic agents as possible triggers for sarcoidosis. In this review, we address recent studies suggesting a possible role for inorganic elements, such as metals or silica in sarcoidosis pathogenesis. Recent findings Several epidemiological papers suggest that inorganic agents, either by environmental exposures or occupational activities, could trigger sarcoidosis. Association between inorganics and sarcoidosis is also described in several recently published case reports and studies demonstrating immunological sensitization to inorganic agents in sarcoidosis patients.Studies comparing chronic beryllium disease (CBD) and sarcoidosis suggest that although antigenic triggers may differ, underlying processes may be comparable.Besides the fact that a growing number of studies show a possible role for inorganic triggers, it is also suggested that inorganic triggered sarcoidosis may result in a more severe phenotype, including pulmonary fibrosis. Summary We can use the knowledge already gained on CBD pathogenesis to conduct further research into role of inorganics, such as metals and silica as antigens in sarcoidosis. Given the importance of a lymphocyte proliferation test (LPT) in diagnosing CBD, it seems obvious to also implement this test in the diagnostic work-up of sarcoidosis to identify patients with an inorganic antigenic trigger of their disease.

Published

2021

14. Gastrointestinal Symptoms Predict the Outcomes From COVID-19 Infection

Author

Darbaz Adnan, Faraz Bishehsari, Mahboobeh Mahdavinia, Shahab R. Khan, Ameya A. Deshmukh, Trevor Rempert, and Klodian Dhana

Subjects

medicine.medical_specialty, 2019-20 coronavirus outbreak, Gi symptoms, Demographics, Coronavirus disease 2019 (COVID-19), Gastrointestinal Diseases, SARS-CoV-2, business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Gastroenterology, COVID-19, Comorbidity, Article, medicine.anatomical_structure, Severe phenotype, Internal medicine, medicine, Humans, business, Respiratory tract

Abstract

Coronavirus disease 2019 (COVID-19) has taken hundreds of thousands of lives globally. Besides the respiratory tract, the virus can affect the gastrointestinal (GI) tract. Data regarding the significance of GI symptoms in the COVID-19 course are limited. In this largest US study to date, the authors reviewed electronic encounters of 1003 consecutive patients who were tested positive for the virus between March 12 and April 3, 2020. Initial GI symptoms were present in up to 22.4% of patients and were associated with worse outcomes after adjustment for demographics, comorbidities, and other clinical symptoms. COVID-19 with GI involvement may define a more severe phenotype.

Published

2021

15. Searching for Genotype-Phenotype Correlations in X-Linked Juvenile Retinoschisis

Author

Hiriyanna, Kelaginamane T., Singh-Parikshak, Rita, Bingham, Eve L., Kemp, Jennifer A., Ayyagari, Radha, Yashar, Beverly M., Sieving, Paul A., Anderson, Robert E., editor, LaVail, Matthew M., editor, and Hollyfield, Joe G., editor

Published

2001

16. Congenital disorders of glycosylation: The Saudi experience.

Author

Alsubhi, Sarah, Alhashem, Amal, Faqeih, Eissa, Alfadhel, Majid, Alfaifi, Abdullah, Altuwaijri, Waleed, Alsahli, Saud, Aldhalaan, Hesham, Alkuraya, Fowzan S., Hundallah, Khalid, Mahmoud, Adel, Alasmari, Ali, Mutairi, Fuad Al, Abduraouf, Hanem, AlRasheed, Layan, Alshahwan, Saad, and Tabarki, Brahim

Abstract

We retrospectively reviewed Saudi patients who had a congenital disorder of glycosylation (CDG). Twenty-seven Saudi patients (14 males, 13 females) from 13 unrelated families were identified. Based on molecular studies, the 27 CDG patients were classified into different subtypes: ALG9-CDG (8 patients, 29.5%), ALG3-CDG (7 patients, 26%), COG6-CDG (7 patients, 26%), MGAT2-CDG (3 patients, 11%), SLC35A2-CDG (1 patient), and PMM2-CDG (1 patient). All the patients had homozygous gene mutations. The combined carrier frequency of CDG for the encountered founder mutations in the Saudi population is 11.5 per 10,000, which translates to a minimum disease burden of 14 patients per 1,000,000. Our study provides comprehensive epidemiologic information and prevalence figures for each of these CDG in a large cohort of congenital disorder of glycosylation patients. [ABSTRACT FROM AUTHOR]

Published

2017

17. Two cases of Nicolaides-Baraitser syndrome, one with a novel SMARCA2 variant

Author

Kadri Karaer

Subjects

Male, Microcephaly, medicine.medical_specialty, Foot Deformities, Congenital, Hypotrichosis, Pathology and Forensic Medicine, 03 medical and health sciences, Intellectual Disability, Intellectual disability, medicine, Humans, Coarse facies, Abnormalities, Multiple, Genetic Predisposition to Disease, Genetic Testing, Genetic Association Studies, Genetics (clinical), 030304 developmental biology, 0303 health sciences, business.industry, 030305 genetics & heredity, Facies, Genetic Variation, High-Throughput Nucleotide Sequencing, Sparse scalp hair, General Medicine, Phalanx, medicine.disease, Dermatology, Phenotype, Nicolaides–Baraitser syndrome, Severe phenotype, Child, Preschool, Mutation, Pediatrics, Perinatology and Child Health, Female, Anatomy, Interphalangeal Joint, business, Transcription Factors

Abstract

Nicolaides-Baraitser syndrome (NCBRS) (OMIM 601358) is an uncommon but well-recognized autosomal dominant entity that is characterized by sparse scalp hair, characteristic coarse facies, microcephaly, seizures, developmental delay, intellectual disability (ID) and prominence of the interphalangeal joints and distal phalanges. Seizures are also common finding besides developmental delay and ID, which is severe approximately in half, moderate in one third and mild in the remainder. Here, we report two Turkish patients with NCBRS. One has a novel variant [NM_003070.5:c.3389G>T p.(Gly1130Val)] and a mild-moderate phenotype, and the other has a known variant [NM_003070.5:c.2554G>A p.(Glu852Lys)] correlated with severe phenotype.

Published

2020

18. Repeated evolution of eye loss in Mexican cavefish: Evidence of similar developmental mechanisms in independently evolved populations

Author

Michael Solomon, Courtney L. Smith, Johanna E. Kowalko, Alex C. Keene, Lauren A. Laboissonniere, Estephany Ferrufino, Jeffrey M. Trimarchi, Sunishka Thakur, and Itzel Sifuentes-Romero

Subjects

0106 biological sciences, 0301 basic medicine, Evolution of the eye, genetic structures, Population, Cavefish, Eye, 010603 evolutionary biology, 01 natural sciences, 03 medical and health sciences, Genetics, Animals, 14. Life underwater, education, In Situ Hybridization, Ecology, Evolution, Behavior and Systematics, education.field_of_study, biology, Characidae, Anophthalmos, biology.organism_classification, Biological Evolution, eye diseases, Caves, 030104 developmental biology, Evolutionary biology, Severe phenotype, Freshwater fish, Eye development, Molecular Medicine, %22">Fish , Animal Science and Zoology, sense organs, Developmental Biology

Abstract

Evolution in similar environments often leads to convergence of behavioral and anatomical traits. A classic example of convergent trait evolution is the reduced traits that characterize many cave animals: reduction or loss of pigmentation and eyes. While these traits have evolved many times, relatively little is known about whether these traits repeatedly evolve through the same or different molecular and developmental mechanisms. The small freshwater fish, Astyanax mexicanus, provides an opportunity to investigate the repeated evolution of cave traits. A. mexicanus exists as two forms, a sighted, surface-dwelling form and at least 29 populations of a blind, cave-dwelling form that initially develops eyes that subsequently degenerate. We compared eye morphology and the expression of eye regulatory genes in developing surface fish and two independently evolved cavefish populations, Pachón and Molino. We found that many of the previously described molecular and morphological alterations that occur during eye development in Pachón cavefish are also found in Molino cavefish. However, for many of these traits, the Molino cavefish have a less severe phenotype than Pachón cavefish. Further, cave-cave hybrid fish have larger eyes and lenses during early development compared with fish from either parental population, suggesting that some different changes underlie eye loss in these two populations. Together, these data support the hypothesis that these two cavefish populations evolved eye loss independently, yet through some of the same developmental and molecular mechanisms.

Published

2020

19. Disentangling the Social Context of Nonmedical Use of Prescription Stimulants in College Students

Author

Timothy E. Wilens, Sean Esteban McCabe, MaryKate Martelon, Amy Yule, Tamar A. Kaminski, Colin W. Burke, and Ty S. Schepis

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Universities, Substance-Related Disorders, Medicine (miscellaneous), Intervention protocols, Social Environment, Article, Young Adult, 03 medical and health sciences, 0302 clinical medicine, mental disorders, medicine, Humans, 0501 psychology and cognitive sciences, 030212 general & internal medicine, Medical prescription, General hospital, Students, Psychiatry, Prescription Drug Misuse, business.industry, 05 social sciences, Social environment, Test (assessment), Psychiatry and Mental health, Clinical Psychology, Cross-Sectional Studies, Severe phenotype, Case-Control Studies, Central Nervous System Stimulants, Female, Self Report, Substance use, business, 050104 developmental & child psychology

Abstract

BACKGROUND AND OBJECTIVES The aim of this study was to investigate the social context of nonmedical use of prescription stimulants (NMUPS) among college students who endorsed NMUPS with co-occurring substance use disorders (SUD) compared with those without co-occurring SUDs. METHODS Presented here are new analyses based on data previously collected from college students aged 18 to 28 years derived from the Boston metropolitan area who endorsed NMUPS (N = 100) at least once in their lifetime. Differences between those with lifetime history of SUD (N = 46) and without a history of SUD (N = 54) on the Massachusetts General Hospital ADHD Medication Misuse and Diversion Assessment were analyzed using the Student t test, the Pearson χ2 test, and the Wilcoxon rank-sum test. RESULTS College students who endorsed NMUPS with co-occurring SUD were more likely than those without SUD to have bought or traded stimulants, bought or traded in their car, used at parties with drugs/alcohol, or used intranasally (all P

Published

2020

20. Loss of a conserved MAPK causes catastrophic failure in assembly of a specialized cilium-like structure inToxoplasma gondii

Author

Xiaoyu Hu, William J. O’Shaughnessy, Michael L. Reese, Matthew B. McDougal, and Tsebaot Beraki

Subjects

MAPK/ERK pathway, biology, Kinase, Severe phenotype, Cilium, Ciliogenesis, Toxoplasma gondii, Cell Biology, Conoid, biology.organism_classification, Molecular Biology, Biogenesis, Cell biology

Abstract

Primary cilia are important organizing centers that control diverse cellular processes. Apicomplexan parasites like Toxoplasma gondii have a specialized cilium-like structure called the conoid that organizes the secretory and invasion machinery critical for the parasites' lifestyle. The proteins that initiate the biogenesis of this structure are largely unknown. We identified the Toxoplasma orthologue of the conserved kinase ERK7 as essential to conoid assembly. Parasites in which ERK7 has been depleted lose their conoids late during maturation and are immotile and thus unable to invade new host cells. This is the most severe phenotype to conoid biogenesis yet reported, and is made more striking by the fact that ERK7 is not a conoid protein, as it localizes just basal to the structure. ERK7 has been recently implicated in ciliogenesis in metazoan cells, and our data suggest that this kinase has an ancient and central role in regulating ciliogenesis throughout Eukaryota.

Published

2020

21. Stevens-Johnson syndrome/toxic epidermal necrolysis with severe ocular complications

Author

Mayumi Ueta

Subjects

0301 basic medicine, medicine.medical_specialty, Eye Diseases, Genotype, Immunology, Disease, 03 medical and health sciences, 0302 clinical medicine, HLA Antigens, Genetic predisposition, Humans, Immunology and Allergy, Medicine, Genetic Predisposition to Disease, Medicine use, Vision, Ocular, 030203 arthritis & rheumatology, Chronic stage, business.industry, Cold medications, Anti-Inflammatory Agents, Non-Steroidal, Stevens johnson, Allergens, medicine.disease, Dermatology, Toxic epidermal necrolysis, stomatognathic diseases, 030104 developmental biology, Severe phenotype, Stevens-Johnson Syndrome, sense organs, business

Abstract

Introduction: Stevens-Johnson syndrome (SJS) and its severe phenotype, toxic epidermal necrolysis (TEN), are acute inflammatory vesiculobullous reactions of the skin and mucosa. Approximately 50% of SJS/TEN patients diagnosed by dermatologists and in burn units suffer from severe ocular complications (SOC) in the acute stage.Areas covered: Earlier studies on patients with SJS/TEN with SOC identified cold medicines including multi-ingredient cold medications and non-steroidal anti-inflammatory drugs as the main eliciting drugs. HLA analyzes showed that genetic predisposition might play a role in the response to these drugs. Our analysis of the association between HLA genotypes and cold medicine-related SJS/TEN (CM-SJS/TEN) with SOC revealed that certain HLA genotypes play a role in the development of SJS/TEN with SOC. Genetic predisposition and other factors contributing to the elicitation of CM-SJS/TEN with SOC and the management of patients in the acute and chronic stage of the disease are discussed.Expert opinion: The main sequelae of SJS/TEN are ocular sequelae with visual disturbance. SJS/TEN with SOC needs ophthalmic treatment in addition to systemic treatment from the onset time to reduce the ophthalmic sequelae. In addition, HLA examination and public awareness of SJS/TEN with SOC due to cold medicine use might contribute to preventing visual disturbance due to SJS/TEN.Abbreviations: SJS: Stevens-Johnson syndrome; TEN: toxic epidermal necrolysis; SOC: severe ocular complications.

Published

2020

22. The RabGAPs EPI64A and EPI64B regulate the apical structure of epithelial cells †

Author

Anthony Bretscher, Matthew R Miller, Riasat Zaman, Andrew J Lombardo, David J. McDermitt, and Cécile Sauvanet

Subjects

Scaffold protein, Cell, Biology, Basal (phylogenetics), Ezrin, Cell Line, Tumor, medicine, Humans, CRISPR, Phosphorylation, Molecular Biology, Adaptor Proteins, Signal Transducing, Binding Sites, Microvilli, GTPase-Activating Proteins, Cell Polarity, Epithelial Cells, Cell Biology, Phosphoproteins, Epithelium, Cell biology, Cytoskeletal Proteins, medicine.anatomical_structure, Severe phenotype, Caco-2 Cells, Function (biology), Protein Binding

Abstract

Here we report on the related TBC/RabGAPs EPI64A and EPI64B and show that they function to organize the apical aspect of epithelial cells. EPI64A binds the scaffolding protein EBP50/NHERF1, which itself binds active ezrin in epithelial cell microvilli. Epithelial cells additionally express EPI64B that also localizes to microvilli. However, EPI64B does not bind EBP50 and both proteins are shown to have a microvillar localization domain that spans the RabGAP domains. CRISPR/Cas9 was used to inactivate expression of each protein individually or both in Jeg-3 and Caco2 cells. In Jeg-3 cells, loss of EPI64B resulted in a reduction of apical microvilli, and a further reduction was seen in the double knockout, mostly likely due to misregulation of Rab8 and Rab35. In addition, apical junctions were partially disrupted in cells lacking EPI64A, and accentuated in the double knock out. In Caco2 loss of EPI64B resulted in wavy junctions, whereas loss of both EPI64A and EPI64B had a severe phenotype often resulting in cells with a stellate apical morphology. In the knockout cells, the basal region of the cell remained unchanged, so EPI64A and EPI64B specifically localize to and regulate the morphology of the apical domain of polarized epithelial cells.

Published

2022

23. Integrating newborn screening for spinal muscular atrophy into health care systems: an Australian pilot programme

Author

Veronica Wiley, Arlene D’Silva, Didu S T Kariyawasam, Michelle A. Farrar, and Stephanie Best

Subjects

Protocol (science), Pediatrics, medicine.medical_specialty, Newborn screening, business.industry, Australia, Infant, Newborn, Pilot Projects, Spinal muscular atrophy, medicine.disease, SMA, Predictive value, Muscular Atrophy, Spinal, Neonatal Screening, Developmental Neuroscience, Severe phenotype, Pediatrics, Perinatology and Child Health, Health care, medicine, Humans, Pilot test, Neurology (clinical), business, Delivery of Health Care

Abstract

Aim This study dynamically designed, evaluated, and implemented the components of an Australian newborn bloodspot screening (NBS) pilot programme for spinal muscular atrophy (SMA). Method We used an implementation-effectiveness study design and continuous interdisciplinary review to measure SMA NBS test protocol performance, identify and overcome laboratory and clinical barriers to implementation, and describe progress during the 2-year pilot study. Results The NBS programme screened 252 081 newborn infants from 1st August 2018 to 31st January 2021. Using an NBS pilot test protocol, 21 infants were diagnostically confirmed with SMA. The NBS pilot test protocol had a sensitivity of 100%, specificity greater than 99.9%, false-positive rate less than 0.001%, a false-negative rate of 0%, and positive predictive value of 95.5%. A severe phenotype was predicted on the basis of two copies of SMN2 in 57.2% of newborn infants screening positive for SMA. Clinical signs consistent with SMA were evident in 6 out of 21 screen-positive newborn infants within the first 4 weeks of life. A multidisciplinary team establishing strong partnerships across clinical and laboratory staff was key to implementation. Interpretation This pilot programme suggests that NBS is essential for early identification of newborn infants at risk of SMA and can be effectively translated into clinical practice.

Published

2021

24. Transcriptomics reveals a distinct metabolic profile in T cells from severe allergic asthmatic patients.

Author

Pablo-Torres C, Garcia-Escribano C, Romeo M, Gomez-Casado C, Arroyo Solera R, Bueno-Cabrera JL, Del Mar Reaño Martos M, Iglesias-Cadarso A, Tarín C, Agache I, Chivato T, Barber D, Escribese MM, and Izquierdo E

Abstract

The reasons behind the onset and continuation of chronic inflammation in individuals with severe allergies are still not understood. Earlier findings indicated that there is a connection between severe allergic inflammation, systemic metabolic alterations and impairment of regulatory functions. Here, we aimed to identify transcriptomic alterations in T cells associated with the degree of severity in allergic asthmatic patients. T cells were isolated from severe ( n  = 7) and mild ( n  = 9) allergic asthmatic patients, and control (non-allergic, non-asthmatic healthy) subjects ( n  = 8) to perform RNA analysis by Affymetrix gene expression. Compromised biological pathways in the severe phenotype were identified using significant transcripts. T cells' transcriptome of severe allergic asthmatic patients was distinct from that of mild and control subjects. A higher count of differentially expressed genes (DEGs) was observed in the group of individuals with severe allergic asthma vs. control (4,924 genes) and vs. mild (4,232 genes) groups. Mild group also had 1,102 DEGs vs. controls. Pathway analysis revealed alterations in metabolism and immune response in the severe phenotype. Severe allergic asthmatic patients presented downregulation in genes related to oxidative phosphorylation, fatty acid oxidation and glycolysis together with increased expression of genes coding inflammatory cytokines (e.g. IL-19, IL-23A and IL-31). Moreover, the downregulation of genes involved in TGF β pathway together with a decreased tendency on the percentage of T regulatory cell (CD4 + CD25+), suggest a compromised regulatory function in severe allergic asthmatic patients. This study demonstrates a transcriptional downregulation of metabolic and cell signalling pathways in T cells of severe allergic asthmatic patients associated with diminished regulatory T cell function. These findings support a link between energy metabolism of T cells and allergic asthmatic inflammation., Competing Interests: MME reports payment or honoraria for lectures, presentations, speakers, bureaus, manuscript writing or educational events from Stallergenes and Diater. DB reports consulting fees from ALK A/S and lecture fees from Diater. IA reports consulting fees from Pfizer and Sanofi. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (© 2023 Pablo-Torres, Garcia-Escribano, Romeo, Gomez-Casado, Arroyo Solera, Bueno-Cabrera, Reaño Martos, Iglesias-Cadarso, Tarín, Agache, Chivato, Barber, Escribese and Izquierdo.)

Published

2023

25. Severe phenotype of an Iranian patient with methemoglobinemia type II due to a novel mutation in the CYB5R3 gene

Author

Jamal Manoochehri, Seyed Mohammad Bagher Tabei, Hamed Reza Goodarzi, Mojtaba Jafarinia, and Hossein Jafari Khamirani

Subjects

medicine.medical_specialty, Hematology, business.industry, CYB5R3, Methemoglobinemia, medicine.disease, Oncology, Severe phenotype, hemic and lymphatic diseases, Internal medicine, Pediatrics, Perinatology and Child Health, Immunology, medicine, business, Gene, Novel mutation

Abstract

Methemoglobinemia is a rare autosomal recessive genetic disease caused by disruptive mutations in the CYB5R3 gene (MIM: 250800). Herein, a novel mutation is reported in an Iranian patient affected with methemoglobinemia type II. In this case study, the patient is precisely described according to the thoroughly carried-out examinations and workups. In so doing, the peripheral blood sample was collected to evaluate the methemoglobin level and NADH-CYB5R3 activity test. Moreover, whole-exome sequencing (WES) was recruited to identify the mutation leading to this disorder. Subsequently, Sanger sequencing was employed to confirm the detected mutation. Magnetic Resonance Imaging was also performed to explore the structure of the brain. As identified by the blood test, the methemoglobin level increased up to 25%, and the NADH-CYB5R3 enzyme activity showed to be 13.8 IU/g of Hb. A novel homozygous mutation in CYB5R3 (NM_001171661: g.23435C>T, c.181C>T, p.R61X, rs1210302322) was identified as the cause of the Methemoglobinemia type II in the proband. This nonsense mutation alters arginine to the stop codon at position 61 of protein in the FAD-binding domain that results in a truncated protein. The MRI revealed brain atrophy and corpus calusom hypoplasticity. It was established that this variation can lead to Methemoglobinemia. The proband demonstrates Methemoglobinemia type II phenotype such as cyanosis, severe mental retardation, microcephaly, as well as developmental delay. The brain MRI revealed brain atrophy and corpus calusom hypoplasticity. The cyanosis symptom is managed by daily ascorbic acid uptake.

Published

2021

26. Investigating Optimal Autologous Cellular Platforms for Prenatal or Perinatal Factor VIII Delivery to Treat Hemophilia A

Author

Sunil George, Graça Almeida-Porada, Christopher B. Doering, Christopher Stem, Andrew M. Farland, Anthony Atala, Diane Meares, Ritu M Ramamurthy, Christopher Rodman, H. Trent Spencer, and Christopher D. Porada

Subjects

FVIII, Factor replacement, QH301-705.5, business.industry, Genetic enhancement, Transgene, mesenchymal stromal (stem) cell therapy, Cell Biology, Postnatal treatment, Bioinformatics, gene therapy, Viral vector, Cell and Developmental Biology, Immune system, endothelial progenitor cell, Severe phenotype, Perinatal factor, Medicine, hemophilia A, Biology (General), business, Developmental Biology, Original Research

Abstract

Patients with the severe form of hemophilia A (HA) present with a severe phenotype, and can suffer from life-threatening, spontaneous hemorrhaging. While prophylactic FVIII infusions have revolutionized the clinical management of HA, this treatment is short-lived, expensive, and it is not available to many A patients worldwide. In the present study, we evaluated a panel of readily available cell types for their suitability as cellular vehicles to deliver long-lasting FVIII replacement following transduction with a retroviral vector encoding a B domain-deleted human F8 transgene. Given the immune hurdles that currently plague factor replacement therapy, we focused our investigation on cell types that we deemed to be most relevant to either prenatal or very early postnatal treatment and that could, ideally, be autologously derived. Our findings identify several promising candidates for use as cell-based FVIII delivery vehicles and lay the groundwork for future mechanistic studies to delineate bottlenecks to efficient production and secretion of FVIII following genetic-modification.

Published

2021

27. NOTCH3 variant position is associated with NOTCH3 aggregation load in CADASIL vasculature

Author

Julie W. Rutten, Aat A. Mulder, Gido Gravesteijn, Ingrid M Hegeman, Remco J. Hack, Carolina R. Jost, Saskia A J Lesnik Oberstein, Remco van Doorn, and Minne N Cerfontaine

Subjects

Pathology, medicine.medical_specialty, Histology, Brain vasculature, NOTCH3 variant position, Neuroimaging, CADASIL, Brain tissue, Protein aggregation, NOTCH3 score, Pathology and Forensic Medicine, Disease severity, Modified Rankin Scale, Physiology (medical), GOM deposit, medicine, Humans, Receptor, Notch3, NOTCH3 aggregation, Receptors, Notch, business.industry, Brain, medicine.disease, Magnetic Resonance Imaging, Phenotype, Neurology, Severe phenotype, Mutation, Immunohistochemistry, Neurology (clinical), business

Abstract

Aims CADASIL, the most prevalent hereditary cerebral small vessel disease, is caused by cysteine-altering NOTCH3 variants (NOTCH3(cys)) leading to vascular NOTCH3 protein aggregation. It has recently been shown that variants located in one of NOTCH3 protein epidermal growth-factor like repeat (EGFr) domains 1-6, are associated with a more severe phenotype than variants located in one of the EGFr domains 7-34. The underlying mechanism for this genotype-phenotype correlation is unknown. The aim of this study was to analyse whether NOTCH3(cys) variant position is associated with NOTCH3 protein aggregation load. Methods We quantified vascular NOTCH3 aggregation in skin biopsies (n = 25) and brain tissue (n = 7) of CADASIL patients with a NOTCH3(cys) EGFr 1-6 variant or a EGFr 7-34 variant, using NOTCH3 immunohistochemistry (NOTCH3 score) and ultrastructural analysis of granular osmiophilic material (GOM count). Disease severity was assessed by neuroimaging (lacune count and white matter hyperintensity volume) and disability (modified Rankin scale). Results Patients with NOTCH3(cys) EGFr 7-34 variants had lower NOTCH3 scores (P = 1.3 center dot 10(-5)) and lower GOM counts (P = 8.2 center dot 10(-5)) than patients with NOTCH3(cys) EGFr 1-6 variants in skin vessels. A similar trend was observed in brain vasculature. In the EGFr 7-34 group, NOTCH3 aggregation levels were associated with lacune count (P = 0.03) and white matter hyperintensity volume (P = 0.02), but not with disability. Conclusions CADASIL patients with an EGFr 7-34 variant have significantly less vascular NOTCH3 aggregation than patients with an EGFr 1-6 variant. This may be one of the factors underlying the difference in disease severity between NOTCH3(cys) EGFr 7-34 and EGFr 1-6 variants.

Published

2021

28. Severe limb-girdle muscular dystrophy 2A in two young siblings from Guinea-Bissau associated with a novel null homozygous mutation in CAPN3 gene.

Author

Oliveira Santos, Miguel, Ninitas, Pedro, and Conceição, Isabel

Subjects

*LIMB-girdle muscular dystrophy, *SIBLINGS, *MUSCLE weakness, *GENES, *NONINVASIVE ventilation

Abstract

Highlights • Calpainopathy is the most common type of LGMD worldwide. • First description of calpainopathy in sub-Saharan African region. • A novel null homozygous c.1702dup mutation was found in the CAPN3 gene. • Our two young siblings exhibited a particularly severe phenotype. Abstract Limb-girdle muscular dystrophy 2A (LGMD2A) or calpainopathy is the most common type of LGMD worldwide, representing about 30–40% of all described cases. Nevertheless, its prevalence in sub-Saharan African countries is unknown. We report two young siblings from Guinea-Bissau with recessive calpainopathy due to novel null homozygous c.1702Gdup mutation in CAPN3 gene. Their phenotype was quite aggressive concerning limb-girdle atrophy and muscle weakness as well as respiratory involvement. The proband needed nocturnal non-invasive ventilation at the age of 32, and his 33-year-old affected sister succumbed to an acute respiratory arrest after an intercurrent infection. This is the first description of calpainopathy in the sub-Saharian African region. Although there is no consistent genotype–phenotype correlation in calpainopathy, the new null homozygous mutation found in the CAPN3 gene may be associated with the particularly severe phenotype observed in our patients. [ABSTRACT FROM AUTHOR]

Published

2018

29. Posterior segment optical coherence tomography findings in a case of nephropathic cystinosis

Author

Omar Al Abdulsalam

Subjects

Pathology, medicine.medical_specialty, genetic structures, Cystinosis, Cystine, Case Report, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Optical coherence tomography, Nephropathic Cystinosis, medicine, 030212 general & internal medicine, optical coherence tomography, medicine.diagnostic_test, business.industry, Infantile nephropathic cystinosis, medicine.disease, eye diseases, Posterior segment of eyeball, Ophthalmology, chemistry, Severe phenotype, 030221 ophthalmology & optometry, nephropathic cystinosis, sense organs, business

Abstract

Cystinosis is a rare autosomal recessive lysosomal storage disorder characterized by abnormal accumulation of intracellular cystine in various tissues including the brain, kidneys, bones, and eyes. Infantile nephropathic cystinosis is the most severe phenotype of cystinosis that has been associated with a wide spectrum of ocular features. In this report, the author describes a posterior segment spectral-domain optical coherence tomography (SD-OCT) finding that has not been previously reported in a case of nephropathic cystinosis.

Published

2020

30. The spectrum of staphylococcal scalded skin syndrome: a case series in children

Author

Daniel R. Mazori, J. B. Alexander, Sharon A. Glick, and A. Leonard

Subjects

Male, medicine.medical_specialty, Dermatology, Disease, medicine.disease_cause, 030207 dermatology & venereal diseases, 03 medical and health sciences, 0302 clinical medicine, Humans, Medicine, Child, Skin pathology, Skin, business.industry, Patient Acuity, Infant, Staphylococcal scalded skin syndrome, medicine.disease, Phenotype, Staphylococcus aureus, Severe phenotype, 030220 oncology & carcinogenesis, Female, Staphylococcal Scalded Skin Syndrome, business

Abstract

Staphylococcal scalded skin syndrome (SSSS) is a disease caused by certain toxigenic strains of Staphylococcus aureus. While the classic severe phenotype is widely recognized in children, SSSS in fact exists on a spectrum with mild and moderate variants. Misunderstanding the phenotypic spectrum of SSSS may result in misdiagnosis of an otherwise treatable condition. To increase awareness of the heterogeneity of SSSS, we report four cases that together represent a range of clinical presentations.

Published

2019

31. Monozygotic dichorionic diamniotic twins with large interstitial deletion of chromosome 1p

Author

Brian L Shaffer, Cori Feist, Leah Yieh, Amanda Kim, and Christina Ramo

Subjects

Genetics, lcsh:R5-920, medicine.diagnostic_test, business.industry, lcsh:R, lcsh:Medicine, Case Report, General Medicine, Case Reports, 030204 cardiovascular system & hematology, 03 medical and health sciences, chromosome 1p, 0302 clinical medicine, monozygotic twins, Chromosome (genetic algorithm), Severe phenotype, 030220 oncology & carcinogenesis, medicine, business, lcsh:Medicine (General), interstitial deletion, Genetic testing

Abstract

We describe twins with an interstitial deletion of chromosome 1 with a severe phenotype compared to previously described cases. As genetic testing is more frequently performed, it is important for clinicians to understand the spectrum of clinical findings that can occur with this particular deletion.

Published

2019

32. Dual diagnosis causing severe phenotype in a patient with Angelman syndrome

Author

Michael Parker, Ddd Study, Meena Balasubramanian, Santosh R. Mordekar, and Farah Kanani

Subjects

Male, business.industry, MEDLINE, General Medicine, medicine.disease, Bioinformatics, Phenotype, Pathology and Forensic Medicine, Text mining, Diagnosis, Dual (Psychiatry), ras GTPase-Activating Proteins, Severe phenotype, Intellectual Disability, Angelman syndrome, Pediatrics, Perinatology and Child Health, Humans, Dual diagnosis, Medicine, Angelman Syndrome, Anatomy, Child, business, Genetics (clinical)

Published

2019

33. Red Blood Cell Stiffness Driving Patient Symptoms: A Study of Red Blood Cell Population Rigidity in Sickle Cell Patient Genotype SC Relation to Overlooked Clinical Symptoms

Author

Mark Shamoun, Omolola Eniola-Adefeso, and Mario Gutierrez

Subjects

Hemoglobin SS, medicine.medical_specialty, Red blood cell population, business.industry, Cell, Disease, Gastroenterology, Hemoglobin sc, Red blood cell, medicine.anatomical_structure, Severe phenotype, hemic and lymphatic diseases, Internal medicine, Genotype, medicine, business

Abstract

Sickle cell disease (SCD) is a systemic hematological disease. Various genotypes of the disease exist; however, the two most common include hemoglobin SS (Hgb SS) and hemoglobin SC (Hgb SC) disease. Hgb SC is typically considered a less severe genotype; however, some patients with SC disease still have significant complications. Ektacytometry is utilized to measure red blood cell deformability in sickle cell patients and may help identify patients at risk for severe disease. We described a patient with genotype hemoglobin SC with a more severe phenotype, who we show to have very rigid red blood cells via ektacytometry.

Published

2021

34. Ocular adnexal phenotype and management of a patient with mosaic expression of a mutation in TWIST2

Author

Matthew A. De Niear, Louise A. Mawn, Ty W. Abel, and James J. Law

Subjects

Pathology, medicine.medical_specialty, Mutation, Surgical approach, Macrostomia, business.industry, Twist-Related Protein 1, medicine.disease_cause, Phenotype, Repressor Proteins, 03 medical and health sciences, Ophthalmology, 0302 clinical medicine, medicine.anatomical_structure, Severe phenotype, 030221 ophthalmology & optometry, medicine, Humans, Eyelid, 030223 otorhinolaryngology, business, Eyelid coloboma

Abstract

Ablepharon-macrostomia syndrome (AMS) and Barber-Say syndrome (BSS) are congenital ectodermal dysplasias associated with mutations in the TWIST2 gene. Among the ophthalmic anomalies that occur in these syndromes, underdevelopment of the anterior lamella of the eyelid is a defining feature. Reports of mosaic expression of TWIST2 mutations are extremely rare, with only five confirmed or suspected cases described to date. Mosaic expression of TWIST2 variants is correlated with a less severe phenotype than that reported for the typical expression of TWIST2 variants associated with BSS or AMS. Abnormal development of the anterior lamella appears to be a common feature in all cases of AMS with mosaic expression. Here, we describe the phenotype of a patient with mosaic expression of a TWIST2 mutation that is typically associated with AMS. We additionally describe the surgical approach employed in the treatment of this patient.

Published

2021

35. Nos défauts génétiques cachés

Author

Bertrand Jordan, Anthropologie bio-culturelle, Droit, Ethique et Santé (ADES), and Aix Marseille Université (AMU)-EFS ALPES MEDITERRANEE-Centre National de la Recherche Scientifique (CNRS)

Subjects

Genetics, 0303 health sciences, education.field_of_study, [SDV]Life Sciences [q-bio], 030305 genetics & heredity, Population, Population genetics, Heterozygote advantage, General Medicine, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Severe phenotype, Carrier screening, education, Deleterious mutation, Exome sequencing, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology

Abstract

A systematic study analysing the exomes of several thousand individuals indicates that each of them carries at least one strongly deleterious mutation that is innocuous in a heterozygote but results in a severe phenotype in the homozygous state. Most of these mutations are very rare, while a few are present in 1 or 2% of the population. The frequency of at-risk couples is approximately 1.5%, but increases dramatically to 25% if the partners of the couple are first cousins. This work has important implications for carrier screening and population genetics in general.

Published

2021

36. Expanding the phenotypic and genotypic spectrum of Bietti crystalline dystrophy

Author

Ricardo P. Casaroli-Marano, André V Gomes, Fabiana Louise Motta, Caio Henrique Marques Texeira, Juliana Maria Ferraz Sallum, Mariana Matioli da Palma, and Mariana Vallim Salles

Subjects

0301 basic medicine, medicine.medical_specialty, CYP4V2 protein, Case Report, Cristal·lí, QH426-470, genetic testing, 03 medical and health sciences, 0302 clinical medicine, BIETTI CRYSTALLINE DYSTROPHY, Ophthalmology, Genotype, Genetics, Malalties hereditàries, Medicine, Missense mutation, Crystalline lens, Macular hole, Genetics (clinical), Retina, insertion-deletion mutation, business.industry, missense mutation, Retinal detachment, medicine.disease, Phenotype, eye diseases, 030104 developmental biology, medicine.anatomical_structure, bietti crystalline dystrophy, Severe phenotype, 030221 ophthalmology & optometry, sense organs, business, Genetic diseases

Abstract

The rare form of retinal dystrophy, Bietti crystalline dystrophy, is associated with variations in CYP4V2, a member of the cytochrome P450 family. This study reports patients affected by typical and atypical Bietti crystalline dystrophy, expanding the spectrum of this disease. This is an observational case series of patients with a clinical and molecular diagnosis of Bietti crystalline dystrophy that underwent multimodal imaging. Four unrelated patients are described with two known variants, c.802‐8_810del17insGC and c.518T > G (p.Leu173Trp), and one novel missense variant, c.1169G > T (p.Arg390Leu). The patient with the novel homozygous variant had the most severe phenotype resulting in macular hole formation and retinal detachment in both eyes. To the best of our knowledge, there is no association of these features with Bietti crystalline dystrophy. Patient 1 was the youngest patient and had the mildest phenotype with crystals in the retina without chorioretinal atrophy and visual complaints. Patients 2 and 3 presented with fewer crystals and chorioretinal atrophy. These three patients presented a classic phenotype. The fourth patient presented with an atypical and severe phenotype. This study reveals a new genotype and new phenotype associated with this disorder. Keywords: bietti crystalline dystrophy; CYP4V2 protein; genetic testing; missense mutation; insertion‐deletion mutation

Published

2021

37. Deep intronic deletion in intron 3 of PLP1 is associated with a severe phenotype of Pelizaeus-Merzbacher disease

Author

Nobuhiko Okamoto, Keiko Yamamoto-Shimojima, Toshiyuki Yamamoto, Tadashi Kaname, Kumiko Yanagi, and Hiroyuki Akagawa

Subjects

Genetics, Gene amplification, lcsh:QH426-470, lcsh:Life, Intron, Pelizaeus–Merzbacher disease, Disease, Biology, medicine.disease, Biochemistry, lcsh:Genetics, lcsh:QH501-531, Severe phenotype, RNA splicing, Genetics research, medicine, Data Report, Molecular Biology, Minigene

Abstract

Recently, altered PLP1 splicing was confirmed as a genetic cause of hypomyelination of early myelinating structures (HEMS). A novel deep intronic deletion in intron 3 of PLP1 (NM_000533.5: c.453+59_+259del) was identified, and an in vitro minigene assay detected abnormal splicing patterns. However, the clinical and radiological findings of the patient were compatible with a severe phenotype of Pelizaeus-Merzbacher disease rather than HEMS, which may be due to undetected abnormal PLP1 splicing.

Published

2021

38. A nationwide survey of PMM2-CDG in Italy: high frequency of a mild neurological variant associated with the L32R mutation.

Author

Barone, Rita, Carrozzi, M., Parini, R., Battini, R., Martinelli, D., Elia, M., Spada, M., Lilliu, F., Ciana, G., Burlina, A., Leuzzi, V., Leoni, M., Sturiale, L., Matthijs, G., Jaeken, J., Rocco, M., Garozzo, D., and Fiumara, A.

Subjects

*GENETIC mutation, *GLYCOSYLATION, *CONGENITAL disorders, *GENOTYPES, *TRANSFERRIN, *DISEASE progression

Abstract

PMM2-CDG ( PMM2 gene mutations) is the most common congenital disorder of N-glycosylation. We conducted a nationwide survey to characterize the frequency, clinical features, glycosylation and genetic correlates in Italian patients with PMM2-CDG. Clinical information was obtained through a questionnaire filled in by the referral physicians including demographics, neurological and systemic features, neuroimaging data and genotype. Glycosylation analyses of serum transferrin were complemented by MALDI-Mass Spectrometry (MALDI-MS). Between 1996 and 2012, data on 37 Italian patients with PMM2-CDG were collected. All the patients with a severe phenotype were unable to walk unaided, 84 % had severe intellectual disability and 81 % microcephaly. Conversely, among 17 mildly affected patients 82 % had independent ambulation, 64 % had borderline to mild intellectual disability and 35 % microcephaly. Epilepsy and stroke-like events did not occur among patients with the mild phenotype. The rate and extent of systemic involvement were more pronounced in severely affected patients. The L32R misfolding mutation of the PMM2 gene occurred in 70 % of the patients with the mild phenotype and was associated with a less severe underglycosylation of serum Tf at MALDI-MS analyses. Despite their different disease severity, all patients had progressive (olivo)ponto-cerebellar atrophy that was the hallmark clinical feature for the diagnosis. A mild neurological phenotype of PMM2-CDG marked by preserved ambulatory ability and autonomy and associated with L32R mutation is particularly frequent in Italy. PMM2-CDG should be considered in patients with even mild developmental disability and/or unexplained progressive cerebellar atrophy. [ABSTRACT FROM AUTHOR]

Published

2015

39. Hip pathologies in mucopolysaccharidosis type III

Author

Sandra Breyer, Eik Vettorazzi, Katharina von Cossel, Alexander S Spiro, Leonie Schmitz, Ralf Stuecker, Amit Gulati, Martin Rupprecht, and Nicole Muschol

Subjects

Male, lcsh:Diseases of the musculoskeletal system, MPS, Radiography, Sanfilippo syndrome, Hip dysplasia (canine), 0302 clinical medicine, lcsh:Orthopedic surgery, Femur Head Necrosis, Hip Dislocation, Orthopedics and Sports Medicine, Child, 030222 orthopedics, Osteonecrosis, Hip dysplasia, medicine.anatomical_structure, Severe phenotype, Child, Preschool, Skeletal dysplasia, Female, Dysostosis multiplex, Research Article, Adult, medicine.medical_specialty, Adolescent, Pain, Mucopolysaccharidosis type III, Young Adult, 03 medical and health sciences, Femoral head, Skeletal disease, Chart review, Internal medicine, medicine, Humans, Retrospective Studies, Hip, business.industry, Mucopolysaccharidoses, medicine.disease, lcsh:RD701-811, Orthopedic surgery, Surgery, lcsh:RC925-935, business, 030217 neurology & neurosurgery

Abstract

Background Mucopolysaccharidosis type III (MPS III) comprises a group of rare lysosomal storage diseases. Although musculoskeletal symptoms are less pronounced than in other MPS subtypes, pathologies of hip and spine have been reported in MPS III patients. The purpose of this study was to describe hip pathologies and influencing parameters in MPS III patients. Methods A retrospective chart review was performed for 101 MPS III patients. Thirty-two patients met the inclusion criteria of enzymatically or genetically confirmed diagnosis and anteroposterior radiograph of the hips. Modified Ficat classification, Wiberg’s center-edge angle, and Reimer’s migration percentage were measured. Results The mean age at data assessment was 11.0 years (SD 5.7). Osteonecrosis of the femoral head was observed in 17/32 patients. No statistically significant association was found between these changes and age, sex, or MPS III subtype. Patients with a severe phenotype showed significantly higher rates of osteonecrosis (14/17) than patients with an intermediate phenotype. Hip dysplasia was present in 9/32 patients and was significantly associated with osteonecrosis of the femoral head (p = 0.04). Conclusions The present study demonstrates a high rate of hip pathologies in MPS III patients. Hip dysplasia and severe phenotype were significantly correlated with osteonecrosis of the femoral head. Therefore, radiographs of the hips are highly recommended in baseline and follow-up assessments of MPS III patients. Trial registration Retrospectively registered.

Published

2021

40. Clinical Phenotype in an Early-Onset French Pediatric Population: Charcot-Marie-Tooth's Disease Type 2A

Author

C. Majorel-Beraud, Caroline Espil-Taris, E. Baudou, Claude Cances, P. Beze-Beyrie, Ulrike Walther-Louvier, François Rivier, P. Cintas, Physiologie & médecine expérimentale du Cœur et des Muscles [U 1046] (PhyMedExp), Université de Montpellier (UM)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), and Centre Hospitalier Régional Universitaire [Montpellier] (CHRU Montpellier)

Subjects

0301 basic medicine, Pediatrics, medicine.medical_specialty, [SDV]Life Sciences [q-bio], Disease, medicine.disease_cause, GTP Phosphohydrolases, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, Charcot-Marie-Tooth Disease, Medicine, Humans, Clinical phenotype, Child, ComputingMilieux_MISCELLANEOUS, Early onset, Retrospective Studies, Mutation, business.industry, Retrospective cohort study, General Medicine, Phenotype, 3. Good health, 030104 developmental biology, Severe phenotype, Pediatrics, Perinatology and Child Health, Neurology (clinical), business, 030217 neurology & neurosurgery, Pediatric population

Abstract

Charcot–Marie–Tooth's disease type 2A (MCT2A), induced by mutation of the mitofusin 2 (MFN2) gene represents the main cause of MCT2. The aim of this study is to provide details of the clinical and electromyographic phenotype of MCT2A in a pediatric population. We conducted a French multicenter retrospective study, including all children with a genetic diagnosis of MCT2A. Thirteen MCT2A children were included with a beginning of symptoms before the age of 10 years (“early-onset group”). We report two new mutations: c.1070 A → T (p.Lys357.Met) and c.280 C → G (p.Arg94Gly). The evolution of the disease is marked by a fast worsening for three patients with loss of motor autonomy, while the evolution is relatively stable for eight patients. The group of early-onset MCT2A seems more heterogeneous than previously described, with a nonconstant severe phenotype.

Published

2021

41. A rare case of patient with neurofibromatosis type 1 in a genotype-phenotype correlation revealing a submicroscopic deletion on the long arm of chromosome 17

Author

Elmira Mainazarova, Cholpon Dzhumakova, Tugolbai Tagaev, Asel Namazbekova, and Vityala Yethindra

Subjects

Genetics, Chromosome 17 (human), Correlation, Microarray, Severe phenotype, Rare case, medicine, macromolecular substances, Neurofibromatosis, Biology, medicine.disease, Long arm, Genotype phenotype

Abstract

We are reporting a case of neurofibromatosis type 1 in a genotype-phenotype correlation and chromosomal microarray test revealed a submicroscopic deletion on the long arm of chromosome 17, which is associated with a more severe phenotype. The presence of a more severe phenotype warrants precise monitoring of complications.

Published

2021

42. Parkinson's disease-dementia in trans LRP10 and GBA variants: Response to deep brain stimulation

Author

Barbara Garavaglia, Arianna Braccia, Mariachiara Sensi, Alessandra Ferlini, Alba Scerrati, Francesca Gualandi, Marcella Neri, Celeste Panteghini, and Michele Alessandro Cavallo

Subjects

Oncology, medicine.medical_specialty, Deep brain stimulation, Parkinson's disease, LRP10, medicine.medical_treatment, Parkinson's disease and dementia, Disease, NO, Familial Parkinson's disease, Internal medicine, Genotype, Medicine, Dementia, business.industry, medicine.disease, nervous system diseases, nervous system, Neurology, Severe phenotype, GBA, Neurology (clinical), Trans-acting, Geriatrics and Gerontology, business

Abstract

We report on a patient with Parkinson's disease and dementia who underwent DBS with excellent response in motor features; the genotype is heterozygous for a novel LRP10 variant in trans with a GBA variant. He had a more severe phenotype compared to the father who only carries the LRP10 variant.

Published

2021

43. Systemic lupus erythematosus in children

Author

Laura B Lewandowski and Laura E. Schanberg

Subjects

Clinical trial, Pediatrics, medicine.medical_specialty, Severe phenotype, business.industry, Medicine, Limited evidence, Disease, Adult care, Age of onset, business, Disease damage

Abstract

An estimated 15%–20% of all systemic lupus erythematosus (SLE) is diagnosed during childhood (childhood-onset systemic lupus erythematosus [cSLE]). This chapter focuses on the unique features of cSLE, including clinical presentation and manifestations, treatment, and outcomes, highlighting differences from adult-onset disease. Perhaps the most striking difference is the more severe phenotype that occurs with earlier age of onset. Monogenic causes of SLE are rare in adult-onset disease but are increasingly recognized as mechanistic drivers of disease in the youngest patients. Treatment considerations unique to pediatric patients include the effects of medicine on growth and development, as well as a more limited evidence base to guide treatment, as clinical trials rarely focus on cSLE patients. Clinicians, patients, and families also face challenges in medical decision-making trying to balance the long-term effects of medication with projected disease damage based on limited data, due to the difficulty of studying long-term outcomes after patients transition to adult care.

Published

2021

44. Unusually severe hypophosphatemic rickets caused by a novel and complex re-arrangement of the PHEX gene.

Author

Pekkarinen, Tuula, Lorenz‐Depiereux, Bettina, Lohman, Martina, and Mäkitie, Outi

Abstract

X-linked hypophosphatemia (XLH) is caused by mutations in PHEX. Several other genetic forms of hypophosphatemia have also been described. These disorders share variable clinical presentation ranging from mild hypophosphatemia to severe lower extremity bowing. We report on a 43-year-old woman with short stature, painful leg deformities, and poor dentation. Her biochemical profile showed hypophosphatemia with renal phosphate wasting. Due to unusually severe clinical presentation and absence of mutations in Sanger sequencing of the PHEX gene, quantitative multiplex ligation-dependent probe amplification was performed. A large deletion within the PHEX gene encompassing exons 8 to 11 was identified. We generated a specific junction fragment using long-range PCR and sequenced the junction fragment to determine the exact deletion breakpoints. We found a heterozygous novel complex re-arrangement involving gross deletions, insertions, and inversion of PHEX (hg19:g.22,115,003_22,141,395del;g:22,145,536_22,150,789delinsCins22,114,640_22,114,698invinsA). Thus, the complex re-arrangement including a deletion of coding exons 8 to 11 of the PHEX can be regarded as the cause of XLH in the patient reported here. Phosphate and active vitamin D treatment was initiated with subsequent relief in bone pain and physical improvement. This report expands the spectrum of clinical severity underlying genetic defects in XLH and highlights the importance of conventional medical therapy even at adult age. Furthermore, our findings underscore the importance of search for gene deletions in patients with suspected XLH. © 2014 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2014

45. Severe phenotype in an apparent homozygosity caused by a large deletion in the CFTR gene: a case report.

Author

da Silva Martins, Raisa, Proença Fonseca, Ana Carolina, Samudio Acosta, Franklyn Enrique, Folescu, Tania Wrobel, Shinzato Higa, Laurinda Yoko, Sad, Izabela Rocha, de Miranda Chaves, Célia Regina Moutinho, Cabello, Pedro Hernan, and Kalil Cabello, Giselda Maria

Abstract

Background: Over 1900 mutations have been identified in the cystic fibrosis conductance transmembrane regulator gene, including single nucleotide substitutions, insertions, and deletions. Unidentified mutations may still lie in introns or in regulatory regions, which are not routinely investigated, or in large genomic deletions, which are not revealed by conventional molecular analysis. The apparent homozygosity for a rare, cystic fibrosis conductance transmembrane regulator mutation screened by standard molecular analysis should be further investigated to confirm if the mutation is in fact homozygous. We describe a patient presenting with an apparent homozygous S4X mutation. Case presentation: A 13-year-old female patient of African descent with clinical symptoms of classic cystic fibrosis and a positive sweat test (97 mEq/L, diagnosed at age 3 years) presented with pancreatic insufficiency and severe pulmonary symptoms (initial lung colonization with Pseudomonas aeruginosa at age 4 years; forced vital capacity: 69%; forced expiratory volume: 51%; 2011). Furthermore, she developed severe acute lung disease and recurrent episodes of dehydration requiring hospitalization. The girl carried the CFTR mutation S4X in apparent homozygosity. However, further analysis revealed a large deletion in the second allele that included the region of the mutation. The deletion that we describe includes nucleotides 120–142, which correspond to a loss of 23 nucleotides that abolishes the normal translation initiation codon. Conclusion: This study reiterates the view that large, cystic fibrosis conductance transmembrane regulator deletions are an important cause of severe cystic fibrosis and emphasizes the importance of including large deletions/duplications in cystic fibrosis conductance transmembrane regulator diagnostic tests. [ABSTRACT FROM AUTHOR]

Published

2014

46. Characterization of the severe phenotype of pyruvate kinase deficiency

Author

Rachael F. Grace, Janet L. Kwiatkowski, Wilma Barcellini, Bertil Glader, Nina Kollmar, Susanne Holzhauer, Hasan Al-Sayegh, Vicky R. Breakey, Wendy B. London, Sujit Sheth, Kevin H.M. Kuo, Jennifer A. Rothman, Marcin W. Wlodarski, Jenny M. Despotovic, Melissa J. Rose, Stefan W. Eber, Hassan M. Yaish, Hanny Al-Samkari, Yves D. Pastore, Kathryn Addonizio, Christine M. Knoll, Alexis A. Thompson, Dagmar Pospisilova, Satheesh Chonat, Mukta Sharma, Melissa N. McNaull, Yaddanapudi Ravindranath, Eduard J. van Beers, D. Holmes Morton, Heather A. Bradeen, Joachim B. Kunz, Madeleine Verhovsek, and Heng Wang

Subjects

medicine.medical_specialty, business.industry, Ethics committee, Disease Association, Hematology, Laboratory results, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Disease severity, Severe phenotype, 030220 oncology & carcinogenesis, Family medicine, medicine, Data monitoring committee, business, health care economics and organizations, Natural history study, 030215 immunology

Abstract

Background: Pyruvate kinase deficiency (PKD) is the most common cause of chronic hereditary non-spherocytic hemolytic anemia. The spectrum of disease in PKD is broad, ranging from an incidentally discovered mild anemia to a severe transfusion-dependent anemia. Splenectomy partially ameliorates the anemia and reduces the transfusion burden in the majority of patients. Because hemoglobin poorly correlates with symptoms in PKD, transfusion requirements are typically used clinically to classify disease severity with those who are regularly transfused despite splenectomy recognized as the most severely affected subgroup. Aim: To compare demographics, complications, and laboratory results between the most severely-affected PKD patients (those that are splenectomized and regularly transfused) with non-regularly transfused splenectomized PKD patients. Methods: After ethics committee approval, patients were enrolled on the PKD Natural History Study, a prospective 30 site international study. All patients had molecularly confirmed PKD. Only splenectomized patients were included in the analysis. Transfusion frequency was observed over a 3-year period. Patients were divided into two groups based on transfusion frequency: the severe phenotype group was defined as those who receive regular transfusions (≥6 discrete red cell transfusion episodes per year) and the control group did not receive regular transfusions. Phenotype stability over the 3-year period was also assessed. Results: 154 splenectomized patients with PKD were included: 30 patients in the severe PKD phenotype group and 124 patients in the comparison PKD group. Results of the analysis comparing the two groups are described in the Table. Severely affected patients were more likely to be female (77% versus 51%, p=0.013), older at the time of splenectomy (median age: 5 versus 3.6, p=0.011), have iron overload (93% vs. 51%, p Conclusions: Patients with PKD who are regularly transfused despite splenectomy appeared to have similar rates of PKD-associated complications (except for iron overload) and similar relevant laboratory values and genotypes when compared to those who are not regularly transfused after splenectomy. The similarity observed between severe phenotype patients and comparison patients with PKD may result from a protective effect of transfusion (e.g. reduction of bone fractures and extramedullary hematopoiesis) or could suggest transfusion-dependence is an artificial signifier of disease severity, reflective of provider practices and patient symptoms rather than an actual distinct phenotype. Transfusion requirements in severe PKD appear to fluctuate significantly over time. Download : Download high-res image (830KB) Download : Download full-size image Disclosures Al-Samkari: Dova: Consultancy, Research Funding; Agios: Consultancy, Research Funding; Moderna: Consultancy. van Beers: RR Mechatronics: Research Funding; Agios Pharmaceuticals, Inc.: Membership on an entity's Board of Directors or advisory committees, Research Funding; Novartis: Consultancy, Research Funding; Pfizer: Research Funding. Barcellini: Agios: Consultancy, Other: Advisory board; Apellis: Consultancy; Incyte: Consultancy, Other: Advisory board; Bioverativ: Consultancy, Other: Advisory board; Novartis: Research Funding, Speakers Bureau; Alexion: Consultancy, Research Funding, Speakers Bureau. Eber: Agios Pharmaceuticals, Inc.: Consultancy. Glader: Agios Pharmaceuticals, Inc: Consultancy, Membership on an entity's Board of Directors or advisory committees, Research Funding. Chonat: Alexion: Other: advisory board; Agios Pharmaceuticals, Inc.: Other: advisory board. Kuo: Pfizer: Consultancy; Novartis: Consultancy, Honoraria; Celgene: Consultancy; Agios: Consultancy; Alexion: Consultancy, Honoraria; Apellis: Consultancy; Bioverativ: Other: Data Safety Monitoring Board; Bluebird Bio: Consultancy. Despotovic: Dova: Honoraria; Novartis: Research Funding; Amgen: Research Funding. Kwiatkowski: Celgene: Consultancy; Terumo: Research Funding; Apopharma: Research Funding; bluebird bio, Inc.: Consultancy, Research Funding; Agios: Consultancy; Imara: Consultancy; Novartis: Research Funding. Thompson: Baxalta: Research Funding; Novartis: Consultancy, Research Funding; bluebird bio, Inc.: Consultancy, Research Funding; Celgene: Consultancy, Research Funding. Ravindranath: Agios Pharmaceuticals, Inc.: Other: I am site PI on several Agios-sponsored studies, Research Funding. Rothman: Pfizer: Consultancy, Honoraria, Research Funding; Novartis: Honoraria, Research Funding; Agios: Honoraria, Research Funding. Verhovsek: Sickle Cell Awareness Group of Ontario: Membership on an entity's Board of Directors or advisory committees; Sickle Cell Disease Association of Canada: Membership on an entity's Board of Directors or advisory committees, Research Funding; Canadian Haemoglobinopathy Association: Membership on an entity's Board of Directors or advisory committees; Vertex: Consultancy. Kunz: Novartis: Membership on an entity's Board of Directors or advisory committees. Sheth: CRSPR/Vertex: Other: Clinical Trial Steering committee; Apopharma: Other: Clinical trial DSMB; Celgene: Consultancy. London: United Therapeutics: Consultancy; ArQule, Inc: Consultancy. Grace: Novartis: Research Funding; Agios Pharmaceuticals, Inc: Consultancy, Membership on an entity's Board of Directors or advisory committees, Research Funding.

Published

2020

47. Peripheral microangiopathy in Eisenmenger syndrome: A nailfold video capillaroscopy study

Author

Haralambos Karvounis, Afroditi K. Boutou, Eva Triantafyllidou, Gerhard-Paul Diller, George Giannakoulas, Michael A. Gatzoulis, Alexandros Garyfallos, Alexandra Arvanitaki, Christos Feloukidis, and Theodoros Dimitroulas

Subjects

Adult, medicine.medical_specialty, 030204 cardiovascular system & hematology, Scleroderma, Angiopathy, Microscopic Angioscopy, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, In patient, 030212 general & internal medicine, Lung, Scleroderma, Systemic, business.industry, Microangiopathy, Eisenmenger Complex, medicine.disease, Peripheral, Capillaries, medicine.anatomical_structure, Cross-Sectional Studies, Nails, Severe phenotype, Eisenmenger syndrome, Cardiology, Female, Cardiology and Cardiovascular Medicine, business

Abstract

Eisenmenger syndrome (ES) comprises a severe phenotype of pulmonary arterial hypertension characterized by angiopathy of the lung circulation. The aim of the present study was to demonstrate the presence of systemic microvascular abnormalities in patients with ES using nailfold video-capillaroscopy (NVC) and to identify potential correlations of nailfold capillaroscopic characteristics with non-invasive markers of systemic organ function.Α cross-sectional NVC study was performed in 17 consecutive patients with ES and 17 healthy controls matched for age and sex. NVC quantitative (capillary density, capillary dimensions, haemorrhages, thrombi, shape abnormalities) and qualitative (normal, non-specific or scleroderma pattern) parameters were evaluated.Patients with ES [median age 40 (18-65) years, 11 women] presented reduced capillary density [8.8 (7.2-10.2) loops/mm vs. 9.9 (8.3-10.9) loops/mm, p = .004] and increased loop width [15.9 (10.3-21.7) μm vs. 12.3 (7.6-15.2) μm, p.001], while they had significantly more abnormal capillaries than healthy controls [2.5 (0.9-5.4) abnormal loops/mm vs. 1.0 (0.0-1.7) abnormal loops/mm, p.001]. NVC shape abnormalities in ES were positively correlated with NT-proBNP (r = 0.52, p = .03) and were negatively associated with estimated glomerular filtration rate (r = -0.60, p = .02). Additionally, capillary loop diameter was positively correlated with increased haemoglobin levels (r = 0.55, p = .03) and negatively correlated with reduced peripheral oxygen saturation (r = - 0.56, p = .02).This study supports the hypothesis of peripheral microvascular involvement in ES parallel to pulmonary microangiopathy detected by NVC. Further longitudinal studies are needed to confirm our preliminary results.

Published

2020

48. Review of clinical and molecular variability in autosomal recessive cutis laxa 2A

Author

Grazia Nardella, Marco Castori, Stefano Castellana, Silvia Morlino, Lucia Micale, Carmela Fusco, and Massimiliano Copetti

Subjects

Adult, Mutation, Missense, Genes, Recessive, Biology, Cutis Laxa, Genetic Heterogeneity, Life Expectancy, Loss of Function Mutation, Intellectual disability, Genetics, medicine, Missense mutation, Humans, splice, Global developmental delay, Frameshift Mutation, Genetics (clinical), Alleles, Genetic Association Studies, Skin, Base Sequence, Age Factors, High-Throughput Nucleotide Sequencing, Exons, medicine.disease, Phenotype, Null allele, Pedigree, Proton-Translocating ATPases, Severe phenotype, Codon, Nonsense, Female, RNA Splice Sites, Cutis laxa

Abstract

ATP6V0A2-related cutis laxa, also known as autosomal recessive cutis laxa type 2A (ARCL2A), is a subtype of hereditary cutis laxa originally characterized by skin, skeletal, and neurological involvement, and a combined defect of N-glycosylation and O-glycosylation. The associated clinical spectrum subsequently expanded to a less severe phenotype dominated by cutaneous involvement. At the moment, ARCL2A was described in a few case reports and series only. An Italian adult woman ARCL2A with a phenotype restricted to skin and the two novel c.3G>C and c.1101dup ATP6V0A2 variants has been reported. A systematic literature review allowed us to identify 69 additional individuals from 64 families. Available data were scrutinized in order to describe the clinical and molecular variability of ARCL2A. About 78.3% of known variants were predicted null alleles, while 11 were missense and 2 affected noncanonical splice sites. Age at ascertainment appeared as the unique phenotypic discriminator with earlier age more commonly associated with facial dysmorphism (p .02), high/cleft palate (p .005), intellectual disability/global developmental delay (p .013), and seizures (p .024). No specific genotype-phenotype correlations were identified. This work confirmed the existence of an attenuated phenotype associated with ATP6V0A2 biallelic variants and offers an updated critique to the clinical and molecular variability of ARCL2A.

Published

2020

49. P0057ADPKD: COMPLEX GENOTYPES MAY EXPLAIN SEVERE PHENOTYPE AND INTRAFAMILIAL PHENOTYPIC VARIABILITY

Author

Elisa Delbarba, Gianfranco Savoldi, Claudia Izzi, Nadia Dallera, Chiara Dordoni, Francesco Scolari, Cinzia Mazza, and Laura Econimo

Subjects

Genetics, Cystic kidney, Transplantation, Non-Mendelian inheritance, urogenital system, business.industry, urologic and male genital diseases, Phenotype, female genital diseases and pregnancy complications, Nephrology, Severe phenotype, Genotype, Medicine, Allele, business, Paternal Inheritance, Gene

Abstract

Background and Aims Discordant affected relative-pairs are seen in ∼10% of families with Autosomal Dominant Polycystic Kidney Disease (ADPKD); Method Among our single-center ADPKD cohort (186 index patients), we selected pedigrees (P) in which marked familial phenotypic variability or severe and early onset disease was investigated by NGS and MLPA analysis of PKD1 and PKD2 genes and NGS analysis of other cystogenes. Segregation analysis by Sanger sequencing of PKD variants was performed in available affected and unaffected family members. Results In P1 and P2, the index cases (IC), presented with very early onset (VEO) disease characterized by prenatal/neonatal enlarged and hyperechogenic kidneys mimicking autosomal recessive polycystic kidney disease (ARPKD). In P1, with neonatal onset, the ADPKD affected father transmitted a PKD1 PT variant p.Gln4231*, whereas the mother, without renal cystic phenotype, transmitted a PKD1 hypomorphic variant p.Asp1332Asn. In P2, the ADPKD-PKD2 mother’s pregnancy was complicated by Potter sequence. Parent’s PKHD1 gene analysis was negative. Two missense NT variants in PKD1/PKD2 genes were detected in the healthy father, respectively p.Gly1944Arg and p.Thr203Ile. Therefore, a complex PKD inheritance was supposed in the fetus. Fetus DNA was not available. In P3 early onset (EO) ADPKD in two monozygous twins was underpinned by a PKD1 NT variant (p.Arg1951Gln) inherited by the ADPKD mild affected father and worsened by a de novo PKD1 truncating variant p.Arg2402*. In P4 and P5 a digenic ADPKD (PKD1 +PKD2 and PKD1 +PKHD1) was diagnosed in severe ADPKD IC. In P4 the two most severely affected siblings carried a PKD2 T variant (p.Ala365fs) and a PKD1 NT variant p-Cys259Tyr. In P5 the IC presented with EO ADPKD, a de novo splicing variant c.2097 + 5_+6insT in PKD1 gene was discovered but the phenotype was probably worsened by the presence of biallelic variant in a second cystogene PKHD1: one paternally inherited: p.Gly1712Arg and one maternally inherited: p.Asp3088Asn . Elderly parents in P6 had mild ADPKD with bilateral few kidney cysts and preserved eGFR, whereas IC showed moderate/severe CKD due to ADPKD biallelic variants. The IC carried a homozygous PKD1 NT variant (p.Arg4154Cys): each mutant allele inherited from the mild ADPKD affected parents. Conclusion Our study illustrates the genetic complexity in an otherwise “simple” Mendelian disorder, providing insights into the genetic basis of severity of ADPKD cases and into ADPKD intrafamilial disease variability. In our pedigree all cases with more severe clinical picture in the family presented at least two PKD variants. In P5 we found for the first time an EO ADPKD due to both PKD1 and PKHD1 variants. PKD1 and PKD2 sequence analysis together with cystic kidney disease gene panel analysis is recommended in those patients with discordant phenotype compared to family members. Molecular study of PKD patients is expected to be a good prognostic tool together with clinical and renal imaging data to better manage disease therapy, follow-up and reproductive issues.

Published

2020

50. Non-deletional alpha thalassaemia: a review

Author

Mei I Lai, Ibrahim Kalle Kwaifa, and Sabariah Md Noor

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Genotype-phenotype correlation, Alpha (ethology), lcsh:Medicine, Gene Expression, Review, Biology, Asymptomatic, 03 medical and health sciences, 0302 clinical medicine, α-Thalassaemia, alpha-Globins, alpha-Thalassemia, Pregnancy, hemic and lymphatic diseases, medicine, Molecular basis, Humans, Pharmacology (medical), Gene, Genetics (clinical), Genetics, Alpha Gene, lcsh:R, General Medicine, Phenotype, Human genetics, Globin gene expression, 030104 developmental biology, Severe phenotype, 030220 oncology & carcinogenesis, Non-deletional mutations, Mutation, Female, medicine.symptom

Abstract

Background Defective synthesis of the α-globin chain due to mutations in the alpha-globin genes and/or its regulatory elements leads to alpha thalassaemia syndrome. Complete deletion of the 4 alpha-globin genes results in the most severe phenotype known as haemoglobin Bart’s, which leads to intrauterine death. The presence of one functional alpha gene is associated with haemoglobin H disease, characterised by non-transfusion-dependent thalassaemia phenotype, while silent and carrier traits are mostly asymptomatic. Main body Clinical manifestations of non-deletional in alpha thalassaemia are varied and have more severe phenotype compared to deletional forms of alpha thalassaemia. Literature for the molecular mechanisms of common non-deletional alpha thalassaemia including therapeutic measures that are necessarily needed for the understanding of these disorders is still in demand. This manuscript would contribute to the better knowledge of how defective production of the α-globin chains due to mutations on the alpha-globin genes and/or the regulatory elements leads to alpha thalassaemia syndrome. Conclusion Since many molecular markers are associated with the globin gene expression and switching over during the developmental stages, there is a need for increased awareness, new-born and prenatal screening program, especially for countries with high migration impact, and for improving the monitoring of patients with α-thalassaemia.

Published

2020