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<article article-type="research-article" dtd-version="1.3" xmlns:mml="http://www.w3.org/1998/Math/MathML" xmlns:xlink="http://www.w3.org/1999/xlink" xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance" xml:lang="ru"><front><journal-meta><journal-id journal-id-type="publisher-id">diaendo</journal-id><journal-title-group><journal-title xml:lang="ru">Сахарный диабет</journal-title><trans-title-group xml:lang="en"><trans-title>Diabetes mellitus</trans-title></trans-title-group></journal-title-group><issn pub-type="ppub">2072-0351</issn><issn pub-type="epub">2072-0378</issn><publisher><publisher-name>Endocrinology research centre</publisher-name></publisher></journal-meta><article-meta><article-id pub-id-type="doi">10.14341/DM7920</article-id><article-id custom-type="elpub" pub-id-type="custom">diaendo-7920</article-id><article-categories><subj-group subj-group-type="heading"><subject>Research Article</subject></subj-group><subj-group subj-group-type="section-heading" xml:lang="ru"><subject>Эпидемиология</subject></subj-group><subj-group subj-group-type="section-heading" xml:lang="en"><subject>Epidemiology</subject></subj-group></article-categories><title-group><article-title>MODY в Сибири – молекулярная генетика и клинические проявления</article-title><trans-title-group xml:lang="en"><trans-title>MODY in Siberia – molecular genetics and clinical characteristics</trans-title></trans-title-group></title-group><contrib-group><contrib contrib-type="author" corresp="yes"><name-alternatives><name name-style="eastern" xml:lang="ru"><surname>Овсянникова</surname><given-names>Алла Константиновна</given-names></name><name name-style="western" xml:lang="en"><surname>Ovsyannikova</surname><given-names>Alla Konstantinovna</given-names></name></name-alternatives><bio xml:lang="ru"><p>кандидат медицинских наук, научный сотруник лаборатории клинико-популяционных исследований терапевтических и эндокринных заболеваний</p></bio><bio xml:lang="en"><p>MD, PhD, research associate</p></bio><email xlink:type="simple">aknikolaeva@bk.ru</email><xref ref-type="aff" rid="aff-1"/></contrib><contrib contrib-type="author" corresp="yes"><name-alternatives><name name-style="eastern" xml:lang="ru"><surname>Рымар</surname><given-names>Оксана Дмитриевна</given-names></name><name name-style="western" xml:lang="en"><surname>Rymar</surname><given-names>Oksana Dmitrievna</given-names></name></name-alternatives><bio xml:lang="ru"><p>доктор медицинских наук, заведующая лабораторией клинико-популяционных исследований терапевтических и эндокринных заболеваний </p></bio><bio xml:lang="en"><p>MD, PhD</p></bio><email xlink:type="simple">orymar23@gmail.com</email><xref ref-type="aff" rid="aff-1"/></contrib><contrib contrib-type="author" corresp="yes"><name-alternatives><name name-style="eastern" xml:lang="ru"><surname>Шахтшнейдер</surname><given-names>Елена Владимировна</given-names></name><name name-style="western" xml:lang="en"><surname>Shakhtshneider</surname><given-names>Elena Vladimirovna</given-names></name></name-alternatives><bio xml:lang="ru"><p>кандидат медцинских наук, старший научный сотрудник лаборатории молекулярно-генетических исследований терапевтических заболеваний</p></bio><bio xml:lang="en"><p>MD, PhD, senior research associate</p></bio><email xlink:type="simple">2117409@mail.ru</email><xref ref-type="aff" rid="aff-1"/></contrib><contrib contrib-type="author" corresp="yes"><name-alternatives><name name-style="eastern" xml:lang="ru"><surname>Воропаева</surname><given-names>Елена Николаевна</given-names></name><name name-style="western" xml:lang="en"><surname>Voropaeva</surname><given-names>Elena Nikolaevna</given-names></name></name-alternatives><bio xml:lang="ru"><p>кандидат медицинских наук, научный сотрудник лаборатории молекулярно-генетических исследований терапевтических заболеваний</p></bio><bio xml:lang="en"><p>PhD, research associate</p></bio><email xlink:type="simple">vena.81@mail.ru</email><xref ref-type="aff" rid="aff-1"/></contrib><contrib contrib-type="author" corresp="yes"><name-alternatives><name name-style="eastern" xml:lang="ru"><surname>Иванощук</surname><given-names>Динара Евгеньевна</given-names></name><name name-style="western" xml:lang="en"><surname>Ivanoshchuk</surname><given-names>Dinara Evgenevna</given-names></name></name-alternatives><bio xml:lang="ru"><p>научный сотрудник лаборатории молекулярно-генетических исследований терапевтических заболеваний</p></bio><bio xml:lang="en"><p>MD, research associate</p></bio><email xlink:type="simple">dinara2084@mail.ru</email><xref ref-type="aff" rid="aff-1"/></contrib><contrib contrib-type="author" corresp="yes"><name-alternatives><name name-style="eastern" xml:lang="ru"><surname>Воевода</surname><given-names>Михаил Иванович</given-names></name><name name-style="western" xml:lang="en"><surname>Voevoda</surname><given-names>Mikhail Ivinovich</given-names></name></name-alternatives><bio xml:lang="ru"><p>академик РАН, доктор медицинских наук, профессор, директор  «НИИТПМ»</p></bio><bio xml:lang="en"><p>MD, PhD, Professor</p></bio><email xlink:type="simple">mvoevoda@ya.ru</email><xref ref-type="aff" rid="aff-1"/></contrib></contrib-group><aff-alternatives id="aff-1"><aff xml:lang="ru"><institution>&lt;p&gt;ФГБНУ Научно-исследовательский институт терапии и профилактической медицины&lt;/p&gt;</institution><country>Россия</country></aff><aff xml:lang="en"><institution>&lt;p&gt;Institution of Internal and Preventive Medicine&lt;/p&gt;</institution><country>Russian Federation</country></aff></aff-alternatives><pub-date pub-type="collection"><year>2017</year></pub-date><pub-date pub-type="epub"><day>11</day><month>05</month><year>2017</year></pub-date><volume>20</volume><issue>1</issue><fpage>5</fpage><lpage>12</lpage><permissions><copyright-statement>Copyright &amp;#x00A9; Овсянникова А.К., Рымар О.Д., Шахтшнейдер Е.В., Воропаева Е.Н., Иванощук Д.Е., Воевода М.И., 2017</copyright-statement><copyright-year>2017</copyright-year><copyright-holder xml:lang="ru">Овсянникова А.К., Рымар О.Д., Шахтшнейдер Е.В., Воропаева Е.Н., Иванощук Д.Е., Воевода М.И.</copyright-holder><copyright-holder xml:lang="en">Ovsyannikova A.K., Rymar O.D., Shakhtshneider E.V., Voropaeva E.N., Ivanoshchuk D.E., Voevoda M.I.</copyright-holder><license xml:lang="ru" license-type="creative-commons-attribution" xlink:href="https://creativecommons.org/licenses/by/4.0/" xlink:type="simple"><license-p>Данная работа распространяется под лицензией Creative Commons Attribution 4.0.</license-p></license><license xml:lang="en" license-type="creative-commons-attribution" xlink:href="https://creativecommons.org/licenses/by/4.0/" xlink:type="simple"><license-p>This work is licensed under a Creative Commons Attribution 4.0 License.</license-p></license></permissions><self-uri xlink:href="https://www.dia-endojournals.ru/jour/article/view/7920">https://www.dia-endojournals.ru/jour/article/view/7920</self-uri><abstract><p>Диагностирование MODY имеет высокую клиническую значимость как для пробандов (отсутствует абсолютная потребность в экзогенном инсулине, нормогликемия в большинстве случаев достигается соблюдением диеты или приемом пероральных сахароснижающих препаратов), так и для их родственников (высокая вероятность носительства мутаций у родственников первой степени родства, что требует более тщательного сбора семейного анамнеза и определения показателей углеводного обмена).</p><sec><title>Цель</title><p>Цель. Определить клинические характеристики течения разных подтипов MODY в условиях сибирского региона.</p></sec><sec><title>Материалы и методы</title><p>Материалы и методы. 20 пациентам с клиническим диагнозом MODY проведены осмотр, биохимический и гормональный анализы крови, УЗИ, молекулярно-генетическое исследование.</p></sec><sec><title>Результаты</title><p>Результаты. Было верифицировано четыре подтипа MODY: у 11 пациентов – MODY 2, у двух – MODY 3, у одного – MODY 8 и у двух – MODY 12. При диагностировании MODY у 11 пациентов (69%) отсутствовали клинические проявления нарушений углеводного обмена, у одного пациента выявлялось снижение веса. Среди сопутствующих патологий в анамнезе у пациентов превалировали дислипидемия – у 5 (31%), артериальная гипертония – у 3 (19%). У одного пациента (6%) с MODY диагностирована диабетическая нефропатия, у 2 (13%) – диабетическая ретинопатия, у 3 (19%) – периферическая полинейропатия нижних конечностей. У всех пациентов достигнуты целевые показатели углеводного обмена, уровень С-пептида был в пределах референсных значений.</p></sec><sec><title>Выводы</title><p>Выводы. В представленной исследовательской работе были диагностированы четыре подтипа MODY (2, 3, 8, 12), различающихся по своему течению, наличию осложнений и тактике лечения. С развитием молекулярной генетики наши знания о моногенных формах сахарного диабета пополняются, но до сих пор остается много аспектов, требующих дальнейшего изучения.</p></sec></abstract><trans-abstract xml:lang="en"><p>The diagnosis of maturity onset diabetes of the young (MODY) has high clinical significance in young patients (no absolute need for exogenous insulin; normoglycaemia in most patients achieved by dieting or taking oral hypoglycaemic agents) and their relatives (high probability of first-degree relatives being carriers of mutations, which requires a thorough collection of family history and determination of the parameters of carbohydrate metabolism).</p><sec><title>Aim</title><p>Aim. This study aimed was to determine the clinical characteristics of different subtypes of MODY in a Siberian region.</p></sec><sec><title>Materials and Methods</title><p>Materials and Methods. We performed an examination, biochemical and hormonal blood tests, ultrasound and molecular genetic testing of 20 patients with a clinical diagnosis of MODY.</p></sec><sec><title>Results</title><p>Results. Four subtypes of MODY were verified: MODY2 in 11 patients, MODY3 in two, MODY8 in one and MODY12 in two. Eleven patients (69%) exhibited no clinical manifestations of carbohydrate metabolism disorders, and one patient showed weight loss during early stage of the disease. Comorbidities included dyslipidemia, thyroid gland disorders and arterial hypertension. One patient (6%) exhibited diabetic nephropathy; two (13%), diabetic retinopathy and three (19%), peripheral neuropathy of lower legs. All patients achieved the target carbohydrate metabolism; the level of C-peptide was within the reference range.</p></sec><sec><title>Conclusion</title><p>Conclusion. Four different subtypes of MODY (2, 3, 8, 12) were diagnosed in the present study, which differed in their clinical characteristics, presence of complications and treatment strategies. Our knowledge of monogenic forms of diabetes is expanding with the development in molecular genetics, but several aspects related to them require further study.</p></sec></trans-abstract><kwd-group xml:lang="ru"><kwd>сахарный диабет</kwd><kwd>MODY</kwd><kwd>гены</kwd><kwd>мутации</kwd><kwd>молекулярно-генетическое исследование</kwd></kwd-group><kwd-group xml:lang="en"><kwd>diabetes mellitus</kwd><kwd>MODY</kwd><kwd>genes</kwd><kwd>mutations</kwd><kwd>molecular genetic testing</kwd></kwd-group><funding-group><funding-statement xml:lang="ru">Исследование выполнено при финансовой поддержке РНФ в рамках научного проекта №14-15-00496.</funding-statement><funding-statement xml:lang="en">The reported study was supported by RSCF, research project No. 14-15-00496.</funding-statement></funding-group></article-meta></front><back><ref-list><title>References</title><ref id="cit1"><label>1</label><citation-alternatives><mixed-citation xml:lang="ru">Fajans SS, Bell GI. 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