miR-199a impairs autophagy and induces cardiac hypertrophy through mTOR activation

Li, Z; Song, Yuanxiu; Liu, L; Hou, Ning; An, Xiaomeng; Zhan, Daqian; Li, Y; Zhou, Linkang; Li, P; Yu, Li; Xia, Jiahong; Zhang, Y; Wang, J; Yang, Xiao

doi:10.1038/cdd.2015.95

Cited by 154 publications

(119 citation statements)

References 37 publications

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“…Consistently, the hypertrophic effects of miR-199a could be reversed by overexpression of Atg5 or rapamycin treatment [119]. Similar results have been obtained in studies focusing on miR-30-Ang II [120], miR-34a-Ang II [121], and miR-451-tuberous sclerosis complex 1 [122] autophagy-mediated cardiomyocyte hypertrophy.…”

Section: Therapeutic Potential Of Autophagic Modulation In Chronic Hesupporting

confidence: 84%

Therapeutic targeting of autophagy in myocardial infarction and heart failure

Riquelme

Chávez

Mondaca‐Ruff

et al. 2016

Expert Review of Cardiovascular Therapy

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PubMed searches were performed to discuss the current state of the art regarding the role of autophagy in MI and HF. We review available and potential approaches to modulate autophagy from a pharmacological and genetic perspective. We also discuss the targeting of autophagy in myocardial regeneration. Expert commentary: The targeting of autophagy has potential for the treatment of MI and HF. Autophagy is a process that takes place in virtually all cells of the body and thus, in order to evaluate this therapeutic approach in clinical trials, strategies that specifically target this process in the myocardium is required to avoid unwanted effects in other organs.

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Section: Therapeutic Potential Of Autophagic Modulation In Chronic Hesupporting

confidence: 84%

Therapeutic targeting of autophagy in myocardial infarction and heart failure

Riquelme

Chávez

Mondaca‐Ruff

et al. 2016

Expert Review of Cardiovascular Therapy

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“…In addition, the expression level of miR-199a-5p was significantly increased in gastric cancer tissues compared with paired normal tissues, and higher miR-199a-5p level was associated with increased lymph node metastasis and higher tumor-node-metastasis stage, suggesting that miR-199a-5p may act as an oncogene in gastric cancer (26). Recently, miR-199a-5p has been reported to exhibit inhibitory effects on autophagy (27). For instance, Lee et al observed that protoporphyrin IX, a photocatalyzer, could increase the expression of miR-199a-5p, which further inhibited E2F transcription factor 3 and sensitized mesenchymal tumor cells to chemotherapy drugs (28).…”

Section: Mir-199a-5p Negatively Mediates the Protein Expression Of Bementioning

confidence: 97%

MicroRNA-199a-5p inhibits cisplatin-induced drug resistance via inhibition of autophagy in osteosarcoma cells

Jiang

et al. 2016

Oncology Letters

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Abstract. Osteosarcoma (OS) is the most common cancer of the bone. Chemotherapy is commonly used for the clinical treatment of OS. However, chemoresistance to cisplatin [also known as diamminedichloridoplatinum (II) (DDP)] is a major obstacle for OS therapy, the underlying mechanism of which is not fully understood. The present study aimed to investigate the role of microRNA (miR)-199a-5p in the regulation of chemoresistance to DDP in OS cells. Reverse transcription-quantitative polymerase chain reaction demonstrated that the expression level of miR-199a-5p was significantly reduced in human OS MG63 cells. In addition, DDP treatment also upregulated the protein levels of light chain 3 (LC3)-II and Beclin1 as well as the ratio of LC3-II vs. LC3-I in MG63 cells, indicating that autophagy was activated. Restoration of miR-199a-5p expression promoted DDP-induced inhibition of MG63 cell proliferation and inhibited DDP-induced autophagy, as indicated by the reduced protein levels of LC3-II and Beclin1 and the ratio of LC3-II vs. LC3-I. Finally, luciferase reporter assay data revealed that miR-199a-5p directly targeted Beclin1 and negatively mediated Beclin1 expression at a post-transcriptional level in MG63 cells. In conclusion, our study suggests that miR-199a-5p promotes the cytotoxicity of DDP in OS cells via inhibition of autophagy. Therefore, miR-199a-5p/autophagy signaling is involved in chemoresistance and may become a potential target for the treatment of DDP-resistant OS.

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“…Several miRNAs that induce pathological hypertrophy and heart failure have been identified, such as miR-195, miR-21, miR23a and miR-208a, whereas miR-133 and miR-1 negatively regulate cardiac hypertrophy (Yang et al 2011). Many studies have shown that miRNAs regulate both cardiac hypertrophy and cardiomyocyte autophagy, for example, miR-212/132 and miR-199a; induce cardiac hypertrophy; and attenuate the autophagic response in cardiomyocytes (Ucar et al 2012, Li et al 2015a. Ang II-induced cardiomyocyte hypertrophy in terms of cell area of cardiomyocytes and expression of the cardiomyocyte hypertrophy markers atrial natriuretic peptide (ANP) and β-myosin heavy chain (β-MHC) mRNA; moreover, the level of ATG9A protein and mRNA expression was upregulated.…”

Section: Effects Of Microrna In Ang Ii-induced Autophagymentioning

confidence: 99%

The role of autophagy in angiotensin II-induced pathological cardiac hypertrophy

Zhou

Han

2016

Journal of Molecular Endocrinology

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Pathological cardiac hypertrophy is associated with nearly all forms of heart failure. It develops in response to disorders such as coronary artery disease, hypertension and myocardial infarction. Angiotensin II (Ang II) has direct effects on the myocardium and promotes hypertension. Chronic elevation of Ang II can lead to pathological cardiac hypertrophy and cardiac failure. Autophagy is an important process in the pathogenesis of cardiovascular diseases. Under physiological conditions, autophagy is an essential homeostatic mechanism to maintain the global cardiac structure function by ridding damaged cells or unwanted macromolecules and organelles. Dysregulation of autophagy may play an important role in Ang II-induced cardiac hypertrophy although conflicting reports on the effects of Ang II on autophagy and cardiac hypertrophy exist. Some studies showed that autophagy activation attenuated Ang II-induced cardiac dysfunction. Others suggested that inhibition of the Ang II induced autophagy should be protective. The discrepancies may be due to different model systems and different signaling pathway involved. Ang II-induced cardiac hypertrophy may be alleviated through regulation of autophagy. This review focuses on Ang II to highlight the molecular targets and pathways identified in the prevention and treatment of Ang II-induced pathological cardiac hypertrophy by regulating autophagy.

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miR-199a impairs autophagy and induces cardiac hypertrophy through mTOR activation

Cited by 154 publications

References 37 publications

Therapeutic targeting of autophagy in myocardial infarction and heart failure

Therapeutic targeting of autophagy in myocardial infarction and heart failure

MicroRNA-199a-5p inhibits cisplatin-induced drug resistance via inhibition of autophagy in osteosarcoma cells

The role of autophagy in angiotensin II-induced pathological cardiac hypertrophy

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