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3. Metabolic and other morbid complications in congenital generalized lipodystrophy type 4

Author

Akinci, Gulcin, primary, Alyaarubi, Saif, additional, Patni, Nivedita, additional, Alhashmi, Nadia, additional, Al‐Shidhani, Azza, additional, Prodam, Flavia, additional, Gagne, Nancy, additional, Babalola, Funmbi, additional, Al Senani, Aisha, additional, Muniraj, Kavitha, additional, Elsayed, Solaf M., additional, Beghini, Marianna, additional, Saydam, Basak Ozgen, additional, Allawati, Moosa, additional, Vaishnav, Madhumati S., additional, Can, Ender, additional, Simsir, Ilgin Y., additional, Sorkina, Ekaterina, additional, Dursun, Fatma, additional, Kamrath, Clemens, additional, Cavdar, Umit, additional, Chakraborty, Partha P., additional, Dogan, Ozlem Akgun, additional, Al Hosin, Aliya, additional, Al Maimani, Ashwaq, additional, Comunoglu, Nil, additional, Hamed, Ahmed, additional, Huseinbegovic, Tea, additional, Scherer, Thomas, additional, Curtis, Jacqueline, additional, Brown, Rebecca J., additional, Topaloglu, Haluk, additional, Simha, Vinaya, additional, Wabitsch, Martin, additional, Tuysuz, Beyhan, additional, Oral, Elif A., additional, Akinci, Baris, additional, and Garg, Abhimanyu, additional

Published
2024
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4. Evaluation of endocrine complications in beta-thalassemia intermedia (β-TI): a cross-sectional multicenter study

Author

Karimi, Mehran, Zarei, Tahereh, Haghpanah, Sezaneh, Azarkeivan, Azita, Kattamis, Christos, Ladis, Vassilis, Kattamis, Antonios, Kilinc, Yurdanur, Daar, Shahina, Alyaarubi, Saif, Khater, Doaa, Wali, Yasser, Elshinawy, Mohamed, Almadhani, Ali, Yassin, Mohamed, Soliman, Ashraf T., Canatan, Duran, Obiedat, Maha, Al-Rimawi, Hala, Mariannis, Demetris, Christodoulides, Constantinos, Christou, Soteroula, Tzoulis, Ploutarchos, Campisi, Saveria, Di Maio, Salvatore, and De Sanctis, Vincenzo

Published
2020
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5. Preliminary Data on COVID-19 in Patients with Hemoglobinopathies: A Multicentre ICET-A Study

Author

de Sanctis, Vincenzo, Canatan, Duran, Corrons, Joan Lluis Vives, Karimi, Mehran, Daar, Shahina, Kattamis, Christos, Soliman, Ashraf T., Wali, Yasser, Alkindi, Salam, Huseynov, Valeh, Nasibova, Afag, Tiryaki, Tarık Onur, Evim, Melike Sezgin, Gunes, Adalet Meral, Karakas, Zeynep, Christou, Soteroula, Campisi, Saveria, Zarei, Tahereh, Khater, Doaa, Oymak, Yesim, Kaleva, Valeriya, Stoyanova, Denka, Banchev, Atanas, Galati, Maria Concetta, Yassin, Mohamed A, Kakar, Shruti, Skafida, Myrto, Kilinc, Yurdanur, Alyaarubi, Saif, Verdiyevas, Narmin, Stoeva, Iva, Raiola, Giuseppe, Mariannis, Demetris, Ruggiero, Leopoldo, and Di Maio, Salvatore

Subjects
Clinical course, Risk factors, SARS-CoV-2, Sickle cell disease, β-thalassemia, COVID-19, Original Article, Patients’ characteristics
Abstract

Objectives This study aims to investigate, retrospectively, the epidemiological and clinical characteristics, laboratory results, radiologic findings, and outcomes of COVID-19 in patients with transfusion-dependent β thalassemia major (TM), β-thalassemia intermedia (TI) and sickle cell disease (SCD). Design A total of 17 Centers, from 10 countries, following 9,499 patients with hemoglobinopathies, participated in the survey. Main outcome data Clinical, laboratory, and radiologic findings and outcomes of patients with COVID-19 were collected from medical records and summarized. Results A total of 13 patients, 7 with TM, 3 with TI, and 3 with SCD, with confirmed COVID-19, were identified in 6 Centers from different countries. The overall mean age of patients was 33.7±12.3 years (range:13–66); 9/13 (69.2%) patients were females. Six patients had pneumonia, and 4 needed oxygen therapy. Increased C-reactive protein (6/10), high serum lactate dehydrogenase (LDH; 6/10), and erythrocyte sedimentation rate (ESR; 6/10) were the most common laboratory findings. 6/10 patients had an exacerbation of anemia (2 with SCD). In the majority of patients, the course of COVID-19 was moderate (6/10) and severe in 3/10 patients. A 30-year-old female with TM, developed a critical SARS-CoV-2 infection, followed by death in an Intensive Care Unit. In one Center (Oman), the majority of suspected cases were observed in patients with SCD between the age of 21 and 40 years. A rapid clinical improvement of tachypnea/dyspnea and oxygen saturation was observed, after red blood cell exchange transfusion, in a young girl with SCD and worsening of anemia (Hb level from 9.2 g/dl to 6.1g/dl). Conclusions The data presented in this survey permit an early assessment of the clinical characteristics of COVID 19 in different countries. 70% of symptomatic patients with COVID- 19 required hospitalization. The presence of associated co-morbidities can aggravate the severity of COVID- 19, leading to a poorer prognosis irrespective of age.

Published
2020

7. Evaluation of Endocrine Complications in Beta-Thalassemia Intermedia Patients: A Cross Sectional Multi-Center Study

Author

Karimi, Mehran Zarei, Tahereh Haghpanah, Sezaneh Azarkeivan, Azita Kattamis, Christos Ladis, Vassilis Kilinc, Yurdanur and Daar, Shahina Alyaarubi, Saif Yasseen, Duaa Yassin, Mohamed A. Soliman, Ashraf Tawfiq Canatan, Duran Obiedat, Maha Remawi, Hala Mariannis, Demetris Christodoulides, Constantinos Christou, Soteroula Tzoulis, Ploutarchos De Sanctis, Vincenzo

Published
2018

8. Evaluation of endocrine complications in beta-thalassemia intermedia (β-TI): a cross-sectional multicenter study

Author

Karimi, Mehran, primary, Zarei, Tahereh, additional, Haghpanah, Sezaneh, additional, Azarkeivan, Azita, additional, Kattamis, Christos, additional, Ladis, Vassilis, additional, Kattamis, Antonios, additional, Kilinc, Yurdanur, additional, Daar, Shahina, additional, Alyaarubi, Saif, additional, Khater, Doaa, additional, Wali, Yasser, additional, Elshinawy, Mohamed, additional, Almadhani, Ali, additional, Yassin, Mohamed, additional, Soliman, Ashraf T., additional, Canatan, Duran, additional, Obiedat, Maha, additional, Al-Rimawi, Hala, additional, Mariannis, Demetris, additional, Christodoulides, Constantinos, additional, Christou, Soteroula, additional, Tzoulis, Ploutarchos, additional, Campisi, Saveria, additional, Di Maio, Salvatore, additional, and De Sanctis, Vincenzo, additional

Published
2019
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9. Evaluation of Endocrine Complications in Beta-Thalassemia Intermedia Patients: A Cross Sectional Multi-Center Study

Author

Karimi, Mehran, primary, Zarei, Tahereh, additional, Haghpanah, Sezaneh, additional, Azarkeivan, Azita, additional, Kattamis, Christos, additional, Ladis, Vassilis, additional, Kilinc, Yurdanur, additional, Daar, Shahina, additional, Alyaarubi, Saif, additional, Yasseen, Duaa, additional, Yassin, Mohamed A, additional, Soliman, Ashraf Tawfiq, additional, Canatan, Duran, additional, Obiedat, Maha, additional, Remawi, Hala, additional, Mariannis, Demetris, additional, Christodoulides, Constantinos, additional, Christou, Soteroula, additional, Tzoulis, Ploutarchos, additional, and De Sanctis, Vincenzo, additional

Published
2018
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10. Erratum. Recessively Inherited LRBA Mutations Cause Autoimmunity Presenting as Neonatal Diabetes. Diabetes 2017;66:2316–2322

Author

Johnson, Matthew B., primary, De Franco, Elisa, additional, Lango Allen, Hana, additional, Al Senani, Aisha, additional, Elbarbary, Nancy, additional, Siklar, Zeynep, additional, Berberoglu, Merih, additional, Imane, Zineb, additional, Haghighi, Alireza, additional, Razavi, Zahra, additional, Ullah, Irfan, additional, Alyaarubi, Saif, additional, Gardner, Daphne, additional, Ellard, Sian, additional, Hattersley, Andrew T., additional, and Flanagan, Sarah E., additional

Published
2018
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11. Comprehensive Screening of Eight Known Causative Genes in Congenital Hypothyroidism With Gland-in-Situ

Author

Nicholas, Adeline K, Serra, Eva G, Cangul, Hakan, Alyaarubi, Saif, Ullah, Irfan, Schoenmakers, Erik, Deeb, Asma, Habeb, Abdelhadi M, Almaghamsi, Mohammad, Peters, Catherine, Nathwani, Nisha, Aycan, Zehra, Saglam, Halil, Bober, Ece, Dattani, Mehul, Shenoy, Savitha, Murray, Philip G, Babiker, Amir, Willemsen, Ruben, Thankamony, Ajay, Lyons, Greta, Irwin, Rachael, Padidela, Raja, Tharian, Kavitha, Davies, Justin H, Puthi, Vijith, Park, Soo-Mi, Massoud, Ahmed F, Gregory, John W, Albanese, Assunta, Pease-Gevers, Evelien, Martin, Howard, Brugger, Kim, Maher, Eamonn R, Chatterjee, V Krishna K, Anderson, Carl A, Schoenmakers, Nadia, Schoenmakers, Erik [0000-0003-0674-8282], Maher, Eamonn [0000-0002-6226-6918], Chatterjee, Krishna [0000-0002-2654-8854], Schoenmakers, Nadia [0000-0002-0847-2884], and Apollo - University of Cambridge Repository

Subjects
Congenital Hypothyroidism/genetics, endocrine system, Genetic Screening, Iron-Binding Proteins/genetics, Receptors, Thyrotropin/genetics, Receptors, Thyrotropin, Original Articles, Autoantigens/genetics, Gene, R1, Iodide Peroxidase/genetics, Autoantigens, Iodide Peroxidase, Thyroglobulin, Pedigree, Phenotype, Thyroglobulin/genetics, Iron-Binding Proteins, Mutation, Congenital Hypothyroidism, Humans
Abstract

Context: Lower TSH screening cutoffs have doubled the ascertainment of congenital hypothyroidism (CH), particularly cases with a eutopically located gland-in-situ (GIS). Although mutations in known dyshormonogenesis genes or TSHR underlie some cases of CH with GIS, systematic screening of these eight genes has not previously been undertaken. Objective: Our objective was to evaluate the contribution and molecular spectrum of mutations in eight known causative genes (TG, TPO, DUOX2, DUOXA2, SLC5A5, SLC26A4, IYD, and TSHR) in CH cases with GIS. Patients, Design, and Setting: We screened 49 CH cases with GIS from 34 ethnically diverse families, using next-generation sequencing. Pathogenicity of novel mutations was assessed in silico. Results: Twenty-nine cases harbored likely disease-causing mutations. Monogenic defects (19 cases) most commonly involved TG (12), TPO (four), DUOX2 (two), and TSHR (one). Ten cases harbored triallelic (digenic) mutations: TG and TPO (one); SLC26A4 and TPO (three), and DUOX2 and TG (six cases). Novel variants overall included 15 TG, six TPO, and three DUOX2 mutations. Genetic basis was not ascertained in 20 patients, including 14 familial cases. Conclusions: The etiology of CH with GIS remains elusive, with only 59% attributable to mutations in TSHR or known dyshormonogenesis-associated genes in a cohort enriched for familial cases. Biallelic TG or TPO mutations most commonly underlie severe CH. Triallelic defects are frequent, mandating future segregation studies in larger kindreds to assess their contribution to variable phenotype. A high proportion (∼41%) of unsolved or ambiguous cases suggests novel genetic etiologies that remain to be elucidated., TG, TPO, DUOX2, DUOXA2, SLC5A5, SLC26A4, IYD and TSHR genes were screened in 49 cases of congenital hypothyroidism with eutopic gland-in-situ. 59% were solved including cases with triallelic mutations.

Published
2016
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12. Comprehensive screening of eight known causative genes in congenital hypothyroidism with gland-in-situ

Author

Nicholas, Adeline K., Serra, Eva G., Cangül, Hakan, Alyaarubi, Saif, Ullah, Irfan, Schoenmakers, Erik, Deeb, Asma, Habeb, Abdelhadi M., Almaghamsi, Mohammad, Peters, Catherine, Nathwani, Nisha, Aycan, Zehra, Bober, Ece, Dattani, Mehul, Shenoy, Savitha, Murray, Philip G., Babiker, Amir, Willemsen, Ruben, Thankamony, Ajay, Lyons, Greta, Irwin, Rachael, Padidela, Raja, Tharian, Kavitha, Davies, Justin H., Puthi, Vijith, Park, Soo-Mi, Massoud, Ahmed F., Gregory, John W., Albanese, Assunta, Pease-Gevers, Evelien, Martin, Howard, Brugger, Kim, Maher, Eamonn R., Chatterjee, V. Krishna K., Anderson, Carl A., Schoenmakers, Nadia, Uludağ Üniversitesi/Tıp Fakültesi/Çocuk Sağlığı ve Hastalıkları Anabilim Dalı., Sağlam, Halil, and C-7392-2019

Subjects
TPO protein, TG gene, Iodide peroxidase, Dual Oxidases, Congenital Hypothyroidism, Oxidoreductases, IYD gene, Autoantigens, Gene, Receptor gene, Thyroglobulin gene, Computer model, Phenomics, DUOX2 gene, Endocrinology & metabolism, Priority journal, Allele, Iodide organification defects, Goiter, Sequence analysis, TSHR gene, Pedigree, Phenotype, Iron-binding proteins, Cohort analysis, Human, TPO gene, Clinical article, Population, DNA sequence, Thyrotropin receptor, Guidelines, Thyroglobulin, Article, Autoantigen, Next generation sequencing, Genetic screening, Genetics, Humans, Pathogenicity, Genetic variation, Iron binding protein, Gene mutation, Receptors, thyrotropin, SLC5A5 gene, Congenital hypothyroidism, Japanese patients, DUOX2 mutations, Mutation, Genetic association, SLC26A4 gene, DUOXA2 gene, Dyshormonogenesis
Abstract

Context: Lower TSH screening cutoffs have doubled the ascertainment of congenital hypothyroidism (CH), particularly cases with a eutopically located gland-in-situ (GIS). Although mutations in known dyshormonogenesis genes or TSHR underlie some cases of CH with GIS, systematic screening of these eight genes has not previously been undertaken. Objective: Our objective was to evaluate the contribution and molecular spectrum of mutations in eight known causative genes (TG, TPO, DUOX2, DUOXA2, SLC5A5, SLC26A4, IYD, and TSHR) in CH cases with GIS. Patients, Design, and Setting:We screened 49 CH cases with GIS from 34 ethnically diverse families, using next-generation sequencing. Pathogenicity of novel mutations was assessed in silica. Results: Twenty-nine cases harbored likely disease-causing mutations. Monogenic defects (19 cases) most commonly involved TG (12), TPO (four), DUOX2 (two), and TSHR (one). Ten cases harbored triallelic (digenic) mutations: TG and TPO (one); SLC26A4 and TPO (three), and DUOX2 and TG (six cases). Novel variants overall included 15 TG, six TPO, and three DUOX2 mutations. Genetic basis was not ascertained in 20 patients, including 14 familial cases. Conclusions: The etiology of CH with GIS remains elusive, with only 59% attributable to mutations in TSHR or known dyshormonogenesis-associated genes in a cohort enriched for familial cases. Biallelic TG or TPO mutations most commonly underlie severe CH. Triallelic defects are frequent, mandating future segregation studies in larger kindreds to assess their contribution to variable phenotype. A high proportion (-41%) of unsolved or ambiguous cases suggests novel genetic etiologies that remain to be elucidated. Wellcome Trust European Commission - 100585/Z/12/Z - 095564/Z/11/Z - 098051 - WT091310 UK Research & Innovation (UKRI) Medical Research Council UK (MRC) - MC_UU_12012/5/B European Commission National Institute for Health Research (NIHR) - (NF-SI-0514-10176) NIHR (CL-2012-06-005)

Published
2016

13. Recessively Inherited LRBA Mutations Cause Autoimmunity Presenting as Neonatal Diabetes

Author

Johnson, Matthew B., primary, De Franco, Elisa, additional, Lango Allen, Hana, additional, Al Senani, Aisha, additional, Elbarbary, Nancy, additional, Siklar, Zeynep, additional, Berberoglu, Merih, additional, Imane, Zineb, additional, Haghighi, Alireza, additional, Razavi, Zahra, additional, Ullah, Irfan, additional, Alyaarubi, Saif, additional, Gardner, Daphne, additional, Güven, Ayla, additional, Ellard, Sian, additional, Hattersley, Andrew T., additional, and Flanagan, Sarah E., additional

Published
2017
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14. Primary hyperparathyroidism mimicking vaso-occlusive crises in sickle cell disease

Author

Krishnamoorthy, Preetha, Alyaarubi, Saif, Abish, Sharon, Gale, Marie, Albuquerque, Pedro, and Jabado, Nada

Subjects
Hyperparathyroidism -- Diagnosis, Hyperparathyroidism -- Case studies, Sickle cell anemia -- Diagnosis, Sickle cell anemia -- Case studies
Abstract

We report a case of bone pain associated with primary hyperparathyroidism in a patient with sickle cell disease. A 17-year-old girl with sickle cell disease (SS phenotype) was seen for bilateral knee and back pain. She had had recurrent severe vaso-occlusive crises and acute chest syndrome in the course of her disease. In the last 2 years, she had frequent visits to the emergency department for severe bone pain. She complained of long-standing fatigue and lethargy. Her physical examination was normal. Hydroxyurea treatment, as well as and long- and short-acting narcotics were given, with little improvement in symptoms. Poor compliance with medication, family dysfunction, and potential narcotic addiction were felt to be significant contributors to the patient's symptoms. She was incidentally found to have an extremely elevated total calcium level of 3.19 mmol/L (range: 2.25-2.76) with an ionized calcium level of 1.9 mmol/L (range: 1.15-1.35). Phosphorus level was 0.82 mmol/L (range: 0.90-1.50), alkaline phosphatase level was elevated at 519 U/L (range: 10-170), and parathyroid hormone level was extremely high at 1645 pg/mL (range: 10-60). Her renal function was normal. Ultrasonography of the neck and a Sestamibi scan revealed a single left inferior parathyroid adenoma adjacent to the thyroid lobe. There was no evidence of an underlying multiple endocrine neoplasia. The patient was diagnosed with primary hyperparathyroidism. Fluid hydration, hydrocortisone, calcitonin, and bisphosphonates were initiated for acute hypercalcemia management before surgical excision of the left parathyroid adenoma. On review of previous blood work, a borderline calcium level of 2.72 was present 18 months before this admission. Two years postsurgery, she has normal renal function, calcium, and parathyroid hormone levels. The weekly visits to the emergency department for pain episodes decreased to 1 every 2 months within the first few months after her surgery. The decrease in pain episodes, even if it coincided with the treatment of primary hyperparathyroidism, may still reflect the natural evolution of sickle cell disease in this patient. However, the high morbidity associated with primary hyperparathyroidism was successfully prevented in this patient. Primary hyperparathyroidism is rare in childhood. In a recent study, it occurred more commonly in female adolescents and was because of a single adenoma, as in our patient. Significant morbidity, mainly secondary to renal dysfunction, was because of the delay in diagnosis after the onset of symptoms (2.0-4.2 years), emphasizing the need for a rapid diagnosis. Sickle cell disease affects ~1 of every 600 blacks in North America. Acute episodes of severe vaso-occlusive crisis account for >90% of sickle cell-related hospitalizations and are a significant cause of morbidity in patients. There is no known association between sickle cell disease and primary hyperparathyroidism, and this case is most probably a random occurrence. However, as emphasized by this case report, pain may also be a harbinger of other disease processes in sickle cell disease. Because management may vary, we suggest that care providers consider the diagnosis of vaso-occlusive crisis as the diagnosis of exclusion and that other etiologies for pain be envisaged in this patient population, especially in the presence of prolonged pain or unusual clinical, radiologic, or biological findings. KEY WORDS. primary hyperparathyroidism, sickle cell, vaso-occlusive crisis, hypercalcemia., URL: www.pediatrics.org/cgi/doi/10.1542/peds.2006-0337 Preetha Krishnamoorthy, MD, Saif Alyaarubi MD, Sharon Abish, MD, Marie Gale, BSc, Pedro Albuquerque, MD, Nada Jabado, MD, [...]

Published
2006

15. Recessively Inherited Mutations Cause Autoimmunity Presenting as Neonatal Diabetes.

Author

Johnson, Matthew B., De Franco, Elisa, Lango Allen, Hana, Al Senani, Aisha, Elbarbary, Nancy, Siklar, Zeynep, Berberoglu, Merih, Imane, Zineb, Haghighi, Alireza, Razavi, Zahra, Ullah, Irfan, Alyaarubi, Saif, Gardner, Daphne, Ellard, Sian, Hattersley, Andrew T., and Flanagan, Sarah E.

Subjects
AUTOIMMUNE diseases, DIABETES, AUTOIMMUNITY, MONOGENIC & polygenic inheritance (Genetics), EXOMES, LYMPHOPROLIFERATIVE disorders, CARRIER proteins, CONSANGUINITY, DISEASE susceptibility, GENEALOGY, GENES, GENETIC techniques, IMMUNITY, TYPE 1 diabetes, GENETIC mutation, RESEARCH funding
Abstract

Young-onset autoimmune diabetes associated with additional autoimmunity usually reflects a polygenic predisposition, but rare cases result from monogenic autoimmunity. Diagnosing monogenic autoimmunity is crucial for patients' prognosis and clinical management. We sought to identify novel genetic causes of autoimmunity presenting with neonatal diabetes (NDM) (diagnosis <6 months). We performed exome sequencing in a patient with NDM and autoimmune lymphoproliferative syndrome and his unrelated, unaffected parents and identified compound heterozygous null mutations in LRBA Biallelic LRBA mutations cause common variable immunodeficiency-8; however, NDM has not been confirmed in this disorder. We sequenced LRBA in 169 additional patients with diabetes diagnosed <1 year without mutations in the 24 known NDM genes. We identified recessive null mutations in 8 additional probands, of which, 3 had NDM (<6 months). Diabetes was the presenting feature in 6 of 9 probands. Six of 17 (35%) patients born to consanguineous parents and with additional early-onset autoimmunity had recessive LRBA mutations. LRBA testing should be considered in patients with diabetes diagnosed <12 months, particularly if they have additional autoimmunity or are born to consanguineous parents. A genetic diagnosis is important as it can enable personalized therapy with abatacept, a CTLA-4 mimetic, and inform genetic counseling. [ABSTRACT FROM AUTHOR]

Published
2017
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18. A novel CASRmutation associated with neonatal severe hyperparathyroidism transmitted as an autosomal recessive disorder

Author

Diaz-Thomas, Alicia, Cannon, John, Iyer, Pallavi, Al-Maawali, Almundher, Fazalullah, Mohammed, Diamond, Frank, Mueller, O. Thomas, Root, Allen W., and Alyaarubi, Saif

Abstract

AbstractBackground:Neonatal severe primary hyperparathyroidism (NSHPT, MIM 239200) is most often an isolated disorder that is due to biallelic inactivating mutations in the CASR, the gene encoding the calcium sensing receptor; NSHPT is inherited from parents with familial hypocalciuric hypercalcemia, each of whom has one mutated CASRallele.Objectives:To report clinical and genetic findings in a brother and sister with NSHPT due to a novel mutation in the CASRtransmitted as an autosomal recessive trait and to examine the functional effect of the mutation.Subjects and methods:A brother and sister with marked hypercalcemia due to NSHPT were identified; the boy also had craniosynostosis requiring surgical repair. The genotyping of the CASRin both children and their parents who were eucalcemic and normophosphatemic was undertaken. In order to examine the significance of the variant CASRidentified, the CASRvariant was expressed in vitro and examined by three computer computational programs [PolyPhen2, MutationTaster, Sorting Intolerant From Tolerant (SIFT)] designed to evaluate the effect of a nucleotide variant on the structure and likely functional consequence upon the protein product.Results:A sequence variant in the CASRwas identified [G>T point mutation at nucleotide c.2303 in exon 7 (c.2303G>T) resulting in the replacement of glycine by valine at codon 768 (p.Gly768Val)]. Two copies of this CASRvariant were present in the genome of the siblings while a single copy of the CASRvariant was present in both of the clinically and biochemically normal parents, a pattern of transmission consistent with autosomal recessive inheritance of NSHPT in this family. When expressed in HEK293 cells in vitro, the novel Gly768Val variant did not interfere with protein generation or migration to the cell membrane in vitro. The analysis of the functional effect of the Gly768Val CASRvariant by the PolyPhen2, MutationTaster, and Sorting Intolerant From Tolerant computer programs revealed that this mutation was very likely to be deleterious.Conclusion:The NSHPT associated with biallelic Gly768Val mutations of the CASRin two siblings with severe hypercalcemia and hyperparathyroidism and their clinically and biochemically normal heterozygous parents was transmitted as an autosomal recessive disorder in this family.

Published
2014
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19. Comprehensive Screening of Eight Known Causative Genes in Congenital Hypothyroidism With Gland-in-Situ

Author

Nicholas, Adeline K, Serra, Eva G, Cangul, Hakan, Alyaarubi, Saif, Ullah, Irfan, Schoenmakers, Erik, Deeb, Asma, Habeb, Abdelhadi M, Almaghamsi, Mohammad, Peters, Catherine, Nathwani, Nisha, Aycan, Zehra, Saglam, Halil, Bober, Ece, Dattani, Mehul, Shenoy, Savitha, Murray, Philip G, Babiker, Amir, Willemsen, Ruben, Thankamony, Ajay, Lyons, Greta, Irwin, Rachael, Padidela, Raja, Tharian, Kavitha, Davies, Justin H, Puthi, Vijith, Park, Soo-Mi, Massoud, Ahmed F, Gregory, John W, Albanese, Assunta, Pease-Gevers, Evelien, Martin, Howard, Brugger, Kim, Maher, Eamonn R, Chatterjee, V Krishna K, Anderson, Carl A, and Schoenmakers, Nadia

Subjects
Phenotype, Iron-Binding Proteins, Mutation, Congenital Hypothyroidism, Humans, Receptors, Thyrotropin, Autoantigens, Iodide Peroxidase, Thyroglobulin, 3. Good health, Pedigree
Abstract

CONTEXT: Lower TSH screening cutoffs have doubled the ascertainment of congenital hypothyroidism (CH), particularly cases with a eutopically located gland-in-situ (GIS). Although mutations in known dyshormonogenesis genes or TSHR underlie some cases of CH with GIS, systematic screening of these eight genes has not previously been undertaken. OBJECTIVE: Our objective was to evaluate the contribution and molecular spectrum of mutations in eight known causative genes (TG, TPO, DUOX2, DUOXA2, SLC5A5, SLC26A4, IYD, and TSHR) in CH cases with GIS. Patients, Design, and Setting: We screened 49 CH cases with GIS from 34 ethnically diverse families, using next-generation sequencing. Pathogenicity of novel mutations was assessed in silico. PATIENTS, DESIGN, AND SETTING: We screened 49 CH cases with GIS from 34 ethnically diverse families, using next-generation sequencing. Pathogenicity of novel mutations was assessed in silico. RESULTS: Twenty-nine cases harbored likely disease-causing mutations. Monogenic defects (19 cases) most commonly involved TG (12), TPO (four), DUOX2 (two), and TSHR (one). Ten cases harbored triallelic (digenic) mutations: TG and TPO (one); SLC26A4 and TPO (three), and DUOX2 and TG (six cases). Novel variants overall included 15 TG, six TPO, and three DUOX2 mutations. Genetic basis was not ascertained in 20 patients, including 14 familial cases. CONCLUSIONS: The etiology of CH with GIS remains elusive, with only 59% attributable to mutations in TSHR or known dyshormonogenesis-associated genes in a cohort enriched for familial cases. Biallelic TG or TPO mutations most commonly underlie severe CH. Triallelic defects are frequent, mandating future segregation studies in larger kindreds to assess their contribution to variable phenotype. A high proportion (∼41%) of unsolved or ambiguous cases suggests novel genetic etiologies that remain to be elucidated.

22. An ICET-A survey on occult and emerging endocrine complications in patients with β-thalassemia major: Conclusions and recommendations.

Author

De Sanctis V, Soliman AT, Canatan D, Tzoulis P, Daar S, Di Maio S, Elsedfy H, Yassin MA, Filosa A, Soliman N, Mehran K, Saki F, Sobti P, Kakkar S, Christou S, Albu A, Christodoulides C, Kilinc Y, Al Jaouni S, Khater D, Alyaarubi SA, Lum SH, Campisi S, Anastasi S, Galati MC, Raiola G, Wali Y, Elhakim IZ, Mariannis D, Ladis V, and Kattamis C

Subjects
Adolescent, Adult, Age Factors, Child, Endocrine System Diseases diagnosis, Endocrine System Diseases therapy, Female, Humans, Male, Middle Aged, Prevalence, Surveys and Questionnaires, Young Adult, beta-Thalassemia diagnosis, beta-Thalassemia therapy, Endocrine System Diseases epidemiology, beta-Thalassemia complications
Abstract

In adult thalassemia major (TM) patients, a number of occult and emerging endocrine complications, such as: central hypothyroidism (CH), thyroid cancer, latent hypocortisolism, and growth hormone deficiency (GHD) have emerged and been reported. As the early detection of these complications is essential for appropriate treatment and follow-up, the International Network of Clinicians for Endocrinopathies in Thalassemia and Adolescent Medicine (ICET-A) promoted a survey on these complications in adult TM patients, among physicians (pediatricians, hematologists and endocrinologists) caring for TM patients in different countries. The data reported by 15 countries are presented.The commonest endocrine complications registered in 3.114 TM adults are CH and GHD (4.6 % and 3.0 %, respectively), followed by latent hypocortisolism (1.2%). In 13 patients (0.41%) a cytological papillary or follicular thyroid carcinoma was diagnosed in 11 and 2 patients, respectively, and a lobectomy or thyroidectomy was carried out. Of 202 TM patients below the age of 18 years, the  reported endocrine complications were: GHD in 4.5%, latent hypocortisolism in 4.4% and central hypothyrodisim in 0.5%. Transition phase was an area of interest for many clinicians, especially as patients with complex chronic health conditions are responding to new treatments extending their lifespan beyond imagination.. In conclusion, our survey provides a better understanding of  physicians' current clinical practices and beliefs in the detection, prevention and treatment of some endocrine complications prevailing in adult TM patients. Regular surveillance, early diagnosis, treatment and follow-up in a multi-disciplinary specialized setting are recommended.

Published
2019
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23. An ICET- A survey on Hypoparathyroidism in Patients with Thalassaemia Major and Intermedia: A preliminary report.

Author

De Sanctis V, Soliman AT, Canatan D, Elsedfy H, Karimi M, Daar S, Rimawi H, Christou S, Skordis N, Tzoulis P, Sobti P, Kakkar S, Kilinc Y, Khater D, Alyaarubi SA, Kaleva V, Lum SH, Yassin MA, Saki F, Obiedat M, Anastasi S, Galati MC, Raiola G, Campisi S, Soliman N, Elshinawy M, Jaouni SA, Di Maio S, Wali Y, Elhakim IZ, and Kattamis C

Subjects
Adolescent, Adult, Child, Female, Ferritins blood, Humans, Male, Middle Aged, Young Adult, beta-Thalassemia blood, Hypoparathyroidism epidemiology, beta-Thalassemia complications
Abstract

Hypoparathyroidism (HPT) is a rare disease with leading symptoms of hypocalcemia, associated with high serum phosphorus levels and absent or inappropriately low levels of parathyroid hormone (PTH). In patients with thalassemias it is mainly attributed to transfusional iron overload, and suboptimal iron chelation therapy. The main objectives of this survey were to provide data on the prevalence, demographic and clinical features of HPT in thalassemia major (TM) and intermedia (TI) patients living in different countries, and to assess its impact in clinical medical practice. A questionnaire was sent to all Thalassemia Centres participating to the International Network of Clinicians for Endocrinopathies in Thalassemia and Adolescence Medicine (ICET-A) Network.Seventeen centers, treating a total of 3023 TM and 739 TI patients, participated to the study. HPT was reported in 206 (6.8%) TM patients and 33 (4.4%) TI patients. In general, ages ranged from 10.5 to 57 years for the TM group and from 20 to 54 years for the TI group. Of the 206 TM patients and 33 TI patients with HPT, 117 (48.9%) had a serum ferritin level >2.500 ng/ml (54.3% TM and 15.1% TI patients) at the last observation. Hypocalcemia varied in its clinical presentation from an asymptomatic biochemical abnormality to a life-threatening condition, requiring hospitalization. Calcium and vitamin D metabolites are currently the cornerstone of therapy in HPT. In TM patients, HPT was preceded or followed by other endocrine and non-endocrine complications. Growth retardation and hypogonadism were the most common complications (53.3% and 67.4%, respectively). Although endocrine complications were more common in patients with TM, non-transfused or infrequently transfused patients with TI suffered a similar spectrum of complications but at a lower rate than their regularly transfused counterparts.In conclusion, although a large international registry would help to better define the prevalence, comorbidities and best treatment of HPT, through the result of this survey we hope to give a clearer understanding of the burden of this disease and its unmet needs. HPT requires lifelong therapy with vitamin D or metabolites and is often associated with complications and comorbidities.Therefore, it is important for endocrinologists and other physicians, who care for these patients, to be aware of recent advances of this disorder.

Published
2018
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24. Diabetes Care in Oman: Obstacles and solutions.

Author

Alyaarubi S

Abstract

Diabetes has become one of the most challenging chronic diseases with its prevalence increasing in most countries worldwide. The Arabian Gulf countries face a similar increasing prevalence of diabetes. Diabetes care requires not only the support of the health authorities, but the contribution of all the sectors of the community and requires good financial support. In Oman, there are many factors which affect the care of diabetes. In this article, these factors are addressed and recommended solutions discussed.

Published
2011

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