Type 2 diabetes and metabolic syndrome: identification of the molecular mechanisms, key signaling pathways and transcription factors aimed to reveal new therapeutical targets
Ivan I. Dedov,
Vsevolod A. Tkachuk,
Nikolai B. Gusev,
Vladimir P. Shirinsky,
Aleksandr V. Vorotnikov,
Tatiana N. Kochegura,
Aleksander Y. Mayorov,
Marina V. Shestakova 
Abstract
Type 2 diabetes mellitus (T2DM) is a socially important disease with only symptomatic therapy developed due to lack of knowledge about its pathogenesis and underlying mechanism. Insulin resistance (IR) is the first link of T2DM pathogenesis and results in decrease of ability of insulin to stimulate glucose uptake by target cells. Development of IR involves genetic predisposition, excessive nutrition, stress, obesity or chronic inflammation due to disruption of insulin signaling within cells. Molecular mechanisms and markers of IR are characterized rather poorly, which prevents early diagnosis and creation of preventive therapy. Euglycemic clamp test is still a golden standard for IR diagnosis in clinic. Hyperglycemia is a distant consequence of IR in which damaging effect of oxidative and carbonyl stress is realized and diagnosis of T2DM is stipulated. Molecular chaperones and small heat-shock proteins have a protective effect at the early stages of T2DM pathogenesis, preventing development of reticulum stress and apoptosis. Endothelial dysfunction is related to T2DM and its cardiovascular complications, however, it is unknown on which stage of pathogenesis these changes occur and what are their molecular inductors. Finally, transcriptional activity and adipogenic differentiation play an important role in formation of new fat depots from predecessor cells and activation of brown and “beige” fat demonstrating hypolipidemic and hypoglycemic properties. The aim of this study was investigation of pathophysiological mechanisms of development of IR and endothelial dysfunction, role of transcription factor Prep1 and small heat shock proteins, evaluation of novel methods of diagnostics of IR and therapeutic potential of brown and “beige” fat, determination of biotargets for new antidiabetic drugs.
Keywords
insulin resistance,
diabetes mellitus,
hyperglycaemia,
metabolic syndrome,
brown fat,
"beige" adipocytes,
insulin,
oxidative stress,
molecular mechanisms,
PKB/Akt,
Prep1,
PPARγ, small heat shock proteins,
endothelial dysfunction
Supporting agencies: Благодарности.
Авторы приносят благодарность за участие в исследовании:
сотрудникам ФГБУ "Национальный медицинский исследовательский центр эндокринологииʺ Минздрава России - д.м.н., профессору Тюльпакову А.Н., д.м.н., профессору Кураевой Т.Л., к.м.н. Соркиной Е.Л., к.м.н. Шестаковой Е.А., Филлипову Ю.И., аспиранту Кокшаровой Е.О., аспиранту Склянику И.А., аспиранту Мишиной Е.Е., Горелышеву А.С.;
сотрудникам Московского государственного университета имени М.В.Ломоносова -
к.м.н. Акопян Ж.А., к.б.н. Егорову А.Д., к.б.н. Кулебякину К.Ю., Степановой А.В., к.б.н. Судницыной М.В., к.б.н. Дацкевич П.Н., к.б.н. Нефедовой В.В., Рыжавской А.С., аспиранту Мурановой Л.К., Герасимович Е.С.;
сотрудникам ФГБУ "Национальный медицинский исследовательский центр кардиологииʺ Министерства здравоохранения Российской Федерации - к.ф-м.н. Пенькову Д.Н., к.б.н. Хапчаеву А.Ю.
Авторы выражают искреннюю благодарность д.м.н. Плехановой О.С. за помощь в подготовке рукописи.
About the Authors
Ivan I. DedovEndocrinology Research Centre
Russian Federation
MD, PhD, Professor
Vsevolod A. Tkachuk
Lomonosov Moscow State University; Russian Cardiology Research and Production Complex
Russian Federation
PhD, Professor
Nikolai B. Gusev
Lomonosov Moscow State University
Russian Federation
PhD, Professor
Vladimir P. Shirinsky
Lomonosov Moscow State University; Russian Cardiology Research and Production Complex
Russian Federation
PhD, Professor
Aleksandr V. Vorotnikov
Lomonosov Moscow State University; Russian Cardiology Research and Production Complex
Russian Federation
PhD in Biology, leader research associate
Tatiana N. Kochegura
Lomonosov Moscow State University
Russian Federation
MD, PhD, senior research associate
Aleksander Y. Mayorov
Lomonosov Moscow State University; Russian Cardiology Research and Production Complex
Russian Federation
MD, PhD
Marina V. Shestakova
Endocrinology Research Centre; Lomonosov Moscow State University
Russian Federation
MD, PhD, Professor
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Supplementary files
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1. Fig. 1. Determination of molecular markers of IL in linear adipocytes 3T3L1. (A) Preadipocyte culture and (B) mature 3T3L1 adipocytes with lipid droplets stained with OilRedO. The scale segment is 100 nm. (B) Diagram of the transfer of insulin signal in fat and muscle cells from the receptor to the insulin-dependent glucose transporter Glut4. Red and blue are the activating and inhibiting effects and the phosphorylated residues, respectively. (D) The ability of insulin to stimulate the phosphorylation of cascade components falls under the conditions of experimental IR caused by dyslipidemia (treatment of cells with palmitic acid during the day). Representative results of Western blotting of cell lysates that were stimulated or not stimulated with 100 nM insulin for 20 minutes are shown; To control the load, we used stain on glyceraldehyde phosphate dehydrogenase (GAPD). | |
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2. Fig. 2. General scheme of pathogenesis of diabetes mellitus type 2 and associated cardiovascular complications. | |
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Dedov I.I., Tkachuk V.A., Gusev N.B., Shirinsky V.P., Vorotnikov A.V., Kochegura T.N., Mayorov A.Y., Shestakova M.V. Type 2 diabetes and metabolic syndrome: identification of the molecular mechanisms, key signaling pathways and transcription factors aimed to reveal new therapeutical targets. Diabetes mellitus. 2018;21(5):364-375. (In Russ.)
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