Exogenous miR-29a Attenuates Muscle Atrophy and Kidney Fibrosis in Unilateral Ureteral Obstruction Mice

Wang, Bin; Wang, Juan; He, Wei; Zhao, Yajie; Zhang, Aiqing; Yan, Lei; Hassounah, Faten; Ma, Fuying; Klein, Janet D.; Wang, Xiaonan H.; Wang, Haidong

doi:10.1089/hum.2019.287

Cited by 27 publications

(22 citation statements)

References 39 publications

(53 reference statements)

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“…A disintegrin and metalloproteinases (ADAMs) are involved in renal fibrosis and TGF‐β/Smad2/3 signaling upregulates Adam 10, 12, 17, 19 expression in renal cells and in unilateral ureteral obstruction models of renal fibrosis 35 . The increase in Adams12 and 19 expression correlated strongly with a decrease in miR‐29s expression and the overexpression of miR‐29s blocked TGF‐β‐mediated upregulation of Adam12 and Adam19 gene expression and improve renal fibrosis 35,36,176 . These studies strongly suggest ADAMs are involved in renal fibrosis and are regulated by both miR‐29s and TGF‐β making thempotential therapeutic targets for the prevention of renal fibrosis.…”

Section: Role Of Mir‐29 Family In Cardiorenal Syndromementioning

confidence: 92%

The role of miR‐29 family in disease

Horita

Farquharson

Stephen

2021

J of Cellular Biochemistry

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MicroRNAs are small noncoding RNAs that can bind to the target sites in the 3’‐untranslated region of messenger RNA to regulate posttranscriptional gene expression. Increasing evidence has identified the miR‐29 family, consisting of miR‐29a, miR‐29b‐1, miR‐29b‐2, and miR‐29c, as key regulators of a number of biological processes. Moreover, their abnormal expression contributes to the etiology of numerous diseases. In the current review, we aimed to summarize the differential expression patterns and functional roles of the miR‐29 family in the etiology of diseases including osteoarthritis, osteoporosis, cardiorenal, and immune disease. Furthermore, we highlight the therapeutic potential of targeting members of miR‐29 family in these diseases. We present miR‐29s as promoters of osteoblast differentiation and apoptosis but suppressors of chondrogenic and osteoclast differentiation, fibrosis, and T cell differentiation, with clear avenues for therapeutic manipulation. Further research will be crucial to identify the precise mechanism of miR‐29 family in these diseases and their full potential in therapeutics.

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Section: Role Of Mir‐29 Family In Cardiorenal Syndromementioning

confidence: 92%

The role of miR‐29 family in disease

Horita

Farquharson

Stephen

2021

J of Cellular Biochemistry

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“…Several lines of evidence suggest that miR-29a is an important antifibrotic agent in the kidney. Expression of miR-29a was reduced in the kidney in rodent UUO models [ 149 ] and in urinary exosomes from CKD patients [ 150 , 151 , 152 ], while renal fibrosis was suppressed after administration of AAV-miR-29 in mice with UUO or DN [ 153 ]. Muscle satellite cell exosomes engineered to contain enriched levels of miR-29a and to elaborate a surface RVG-moiety that targeted acetylcholine receptors in the kidney were therapeutic after intramuscular injection in the UUO model [ 154 ].…”

Section: Renal Fibrosismentioning

confidence: 99%

“…Levels of vitronectin in urine and urinary EVs [ 161 ] or of miR-21 in plasma EVs [ 162 ] were proposed as biomarkers for post-kidney transplantation patients with a high incidence of tubulointerstitial fibrosis. Finally, miR-29a was elevated in serum EVs from mice with UUO [ 153 ] and plasma-derived exosomal miRs in rats that had undergone 5/6th partial nephrectomy or two-kidney-one-clip were associated with pathways of fibrosis and injury and could be discriminated from free plasma miRs [ 163 ].…”

Section: Renal Fibrosismentioning

confidence: 99%

Extracellular Vesicles in Organ Fibrosis: Mechanisms, Therapies, and Diagnostics

Brigstock

2021

Cells

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Fibrosis is the unrelenting deposition of excessively large amounts of insoluble interstitial collagen due to profound matrigenic activities of wound-associated myofibroblasts during chronic injury in diverse tissues and organs. It is a highly debilitating pathology that affects millions of people globally and leads to decreased function of vital organs and increased risk of cancer and end-stage organ disease. Extracellular vesicles (EVs) produced within the chronic wound environment have emerged as important vehicles for conveying pro-fibrotic signals between many of the cell types involved in driving the fibrotic response. On the other hand, EVs from sources such as stem cells, uninjured parenchymal cells, and circulation have in vitro and in vivo anti-fibrotic activities that have provided novel and much-needed therapeutic options. Finally, EVs in body fluids of fibrotic individuals contain cargo components that may have utility as fibrosis biomarkers, which could circumvent current obstacles to fibrosis measurement in the clinic, allowing fibrosis stage, progression, or regression to be determined in a manner that is accurate, safe, minimally-invasive, and conducive to repetitive testing. This review highlights the rapid and recent progress in our understanding of EV-mediated fibrotic pathogenesis, anti-fibrotic therapy, and fibrosis staging in the lung, kidney, heart, liver, pancreas, and skin.

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“…miR-29 expression was downregulated following myocardial infarction and after treatment of isolated heart fibroblasts with TGF-β [ 112 ]. Overexpression of miR-29 inhibited the pro-fibrotic response in isolated cardiac fibroblasts and in animal models [ 113 , 114 ]. These studies focused on endogenous miR-29 in cardiac fibroblasts; however, recent studies have shown that miR-29 carried by exosomes is able to reduce skeletal muscle atrophy and kidney fibrosis in a unilateral ureteral obstruction-induced model of kidney disease [ 114 ].…”

Section: Role Of Exosomes In Fibrosis and Fibroblast Activationmentioning

confidence: 99%

Roles of Exosomes in Cardiac Fibroblast Activation and Fibrosis

Hohn

Tan

Carver

et al. 2021

Cells

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Alterations in the accumulation and composition of the extracellular matrix are part of the normal tissue repair process. During fibrosis, this process becomes dysregulated and excessive extracellular matrix alters the biomechanical properties and function of tissues involved. Historically fibrosis was thought to be progressive and irreversible; however, studies suggest that fibrosis is a dynamic process whose progression can be stopped and even reversed. This realization has led to an enhanced pursuit of therapeutic agents targeting fibrosis and extracellular matrix-producing cells. In many organs, fibroblasts are the primary cells that produce the extracellular matrix. In response to diverse mechanical and biochemical stimuli, these cells are activated or transdifferentiate into specialized cells termed myofibroblasts that have an enhanced capacity to produce extracellular matrix. It is clear that interactions between diverse cells of the heart are able to modulate fibroblast activation and fibrosis. Exosomes are a form of extracellular vesicle that play an important role in intercellular communication via the cargo that they deliver to target cells. While relatively recently discovered, exosomes have been demonstrated to play important positive and negative roles in the regulation of fibroblast activation and tissue fibrosis. These roles as well as efforts to engineer exosomes as therapeutic tools will be discussed.

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Exogenous miR-29a Attenuates Muscle Atrophy and Kidney Fibrosis in Unilateral Ureteral Obstruction Mice

Cited by 27 publications

References 39 publications

The role of miR‐29 family in disease

The role of miR‐29 family in disease

Extracellular Vesicles in Organ Fibrosis: Mechanisms, Therapies, and Diagnostics

Roles of Exosomes in Cardiac Fibroblast Activation and Fibrosis

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