Regulatory Action of Plasma from Patients with Obesity and Diabetes towards Muscle Cells Differentiation and Bioenergetics Revealed by the C2C12 Cell Model and MicroRNA Analysis

Obesity and type 2 diabetes mellitus (T2DM) are often combined and pathologically affect many tissues due to changes in circulating bioactive molecules. In this work, we evaluated the effect of blood plasma from obese (OB) patients or from obese patients comorbid with diabetes (OBD) on skeletal musc...

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Veröffentlicht in:BIOMOLECULES 2021-05, Vol.11 (6), p.769
Hauptverfasser: Khromova, Natalya V, Fedorov, Anton V, Ma, Yi, Kondratov, Kirill A, Prikhodko, Stanislava S, Ignatieva, Elena V, Artemyeva, Marina S, Anopova, Anna D, Neimark, Aleksandr E, Kostareva, Anna A, Babenko, Alina Yu, Dmitrieva, Renata I
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Sprache:eng
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Zusammenfassung:Obesity and type 2 diabetes mellitus (T2DM) are often combined and pathologically affect many tissues due to changes in circulating bioactive molecules. In this work, we evaluated the effect of blood plasma from obese (OB) patients or from obese patients comorbid with diabetes (OBD) on skeletal muscle function and metabolic state. We employed the mouse myoblasts C2C12 differentiation model to test the regulatory effect of plasma exposure at several levels: (1) cell morphology; (2) functional activity of mitochondria; (3) expression levels of several mitochondria regulators, i.e., , , and miR-378a-3p. Existing databases were used to computationally predict and analyze mir-378a-3p potential targets. We show that short-term exposure to OB or OBD patients' plasma is sufficient to affect C2C12 properties. In fact, the expression of genes that regulate skeletal muscle differentiation and growth was downregulated in both OB- and OBD-treated cells, maximal mitochondrial respiration rate was downregulated in the OBD group, while in the OB group, a metabolic switch to glycolysis was detected. These alterations correlated with a decrease in and expression in the OB group and with an increase of miR-378a-3p levels in the OBD group.
ISSN:2218-273X
2218-273X
DOI:10.3390/biom11060769