MicroRNA-7a regulates pancreatic β cell function
Mathieu Latreille, … , Patrik Rorsman, Markus Stoffel
Mathieu Latreille, … , Patrik Rorsman, Markus Stoffel
Published May 1, 2014
Citation Information: J Clin Invest. 2014;124(6):2722-2735. https://doi.org/10.1172/JCI73066.
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Research Article Endocrinology

MicroRNA-7a regulates pancreatic β cell function

Abstract

Dysfunctional microRNA (miRNA) networks contribute to inappropriate responses following pathological stress and are the underlying cause of several disease conditions. In pancreatic β cells, miRNAs have been largely unstudied and little is known about how specific miRNAs regulate glucose-stimulated insulin secretion (GSIS) or impact the adaptation of β cell function to metabolic stress. In this study, we determined that miR-7 is a negative regulator of GSIS in β cells. Using Mir7a2 deficient mice, we revealed that miR-7a2 regulates β cell function by directly regulating genes that control late stages of insulin granule fusion with the plasma membrane and ternary SNARE complex activity. Transgenic mice overexpressing miR-7a in β cells developed diabetes due to impaired insulin secretion and β cell dedifferentiation. Interestingly, perturbation of miR-7a expression in β cells did not affect proliferation and apoptosis, indicating that miR-7 is dispensable for the maintenance of endocrine β cell mass. Furthermore, we found that miR-7a levels are decreased in obese/diabetic mouse models and human islets from obese and moderately diabetic individuals with compensated β cell function. Our results reveal an interconnecting miR-7 genomic circuit that regulates insulin granule exocytosis in pancreatic β cells and support a role for miR-7 in the adaptation of pancreatic β cell function in obesity and type 2 diabetes.

Authors

Mathieu Latreille, Jean Hausser, Ina Stützer, Quan Zhang, Benoit Hastoy, Sofia Gargani, Julie Kerr-Conte, Francois Pattou, Mihaela Zavolan, Jonathan L.S. Esguerra, Lena Eliasson, Thomas Rülicke, Patrik Rorsman, Markus Stoffel

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Figure 5

miR-7a and its targets regulates SNARE oligomerization and insulin secretion in pancreatic β cells.

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miR-7a and its targets regulates SNARE oligomerization and insulin secre...
(A) V5-tagged Snca expression vectors. (B) Dispersed islets from Mir7a2fl/fl and Rip-Cre Mir7a2fl/fl mice were cotransfected with the indicated vectors (V5-tagged Lacz served as internal control for transfection efficiency) and immunoblotted. V5-SNCA levels normalized to V5-LACZ and γ-tubulin are indicated below. (C and D) MIN6 cells were (C) transfected with V5-tagged Snca or control EGFP vectors or (D) infected with Ad–miR-7a2 and cotransfected with V5-tagged Lacz and Snca 3′-UTR WT or Mut120 plasmids, and levels of V5-SNCA in VAMP2 IPs were determined by immunoblotting. Relative V5-SNCA levels in cell lysate (normalized to V5-LACZ) and VAMP2 IP (normalized to IP VAMP2) are indicated below in D. (E) SNARE oligomerization in MIN6 cells cotransfected with VAMP2-, SNAP25-, and SYN1A-encoding vectors and increasing amounts of V5-SNCA. Immunoblotting was performed in native and denaturing conditions. (F) MIN6 cells were transfected with LNA-based miR-7a inhibitor or control, and SNAP25 was measured in VAMP2 IP. Relative levels of indicated proteins normalized to V5-LACZ and tubulin (cell lysate) or VAMP2 (IP VAMP) are indicated below. (G) MIN6 cells were transfected with LNA-based miR-7a inhibitor or control, and SNARE oligomers were detected by immunoblotting. SNCA level (bottom) served as a control. (HJ) Insulin secretion assays in MIN6 cells transfected with control or miR-7a mimics (H), miR-7a inhibitors (I), or Snca siRNAs (J) (n = 6). Data are mean ± SD. *P < 0.05.