DOCK8-related Immunodeficiency Syndrome (DIDS): Report of Novel Mutations in Iranian Patients

DOCK8-related Immunodeficiency Syndrome (DIDS): Report of Novel Mutations in Iranian Patients


چاپ صفحه		 پژوهان
صفحه نخست سامانه		 چکیده مقاله
چکیده مقاله		 نویسندگان
نویسندگان		 دانلود مقاله
دانلود مقاله		 دانشگاه علوم پزشکی تبریز
دانشگاه علوم پزشکی تبریز

نویسندگان: جواد احمدیان هریس , امیر حسین جعفری روحی , مریم رضازاده

کلمات کلیدی: s DOCK8 · DIDS · Hyper IgE · HIES · Job syndrome · WES

نشریه: 18110 , 12 , 71 , 2021

اطلاعات کلی مقاله
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نویسنده ثبت کننده مقاله مریم رضازاده
مرحله جاری مقاله تایید نهایی
دانشکده/مرکز مربوطه دانشکده پزشکی
کد مقاله 75941
عنوان فارسی مقاله DOCK8-related Immunodeficiency Syndrome (DIDS): Report of Novel Mutations in Iranian Patients
عنوان لاتین مقاله DOCK8-related Immunodeficiency Syndrome (DIDS): Report of Novel Mutations in Iranian Patients
ناشر 8
آیا مقاله از طرح تحقیقاتی و یا منتورشیپ استخراج شده است؟ بلی
عنوان نشریه (خارج از لیست فوق)
نوع مقاله Original Article
نحوه ایندکس شدن مقاله ایندکس شده سطح یک – ISI - Web of Science
آدرس لینک مقاله/ همایش در شبکه اینترنت

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DOCK8 immunodeficiency syndrome (DIDS) is a rare autosomal recessive (AR) disorder characterized by elevated serum IgE levels, eosinophilia, recurrent cutaneous infections, severe eczema, and sinopulmonary and gastrointestinal infections. This syndrome is a multisystem disease that is associated with both immune deficiency and neurological complications. In this study, we describe the clinical characteristics of two Iranian patients with DOCK8 deficiency and propose possible mechanisms for this condition. By using whole exome sequencing (WES), we identified two novel mutations, namely c.3233_3234del AG (p.Q1078fs) in exon 6 and a large deletion with 94 kb (c.405–3231 deletion, p.K135fs), in these two patients. These variations are confirmed with Sanger sequencing and CGH array. Subsequent co-segregation analysis is performed to identify inheritance patterns. Both patients were homozygote and their parents were heterozygote for the variations. For further investigation, prediction tools were applied to identify the pathogenicity of the variations and also for modeling the truncated proteins. The patients did not show neurological abnormalities associated with a deficiency of the N terminal region of DOCK8. The absence of neurological complications in the first patient is justifiable due to the maintenance of the proline-rich region in DOCK8, but for the second patient with expanded deletion which is almost like null DOCK8 protein, it is not presumable, pointing to the fact that the C terminal region of the protein might have functions in the proliferation and migration neurons in the peripheral nervous system. Alternatively, it is possible that neurological abnormalities follow an age-dependent pattern, leading to the appearance of related symptoms later in life. Further multiple functional studies are needed to model different identified variants in animal models to confirm our results and suggest possible mechanisms associated with DOCK8 deficiency in this study.

نویسندگان
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نویسنده نفر چندم مقاله
جواد احمدیان هریسپنجم
امیر حسین جعفری روحیششم
مریم رضازادههشتم

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Yousefnezhad2021_Article_DOCK8-relatedImmunodeficiencyS.pdf1400/09/091340959دانلود