Interstitial microRNA miR-214 attenuates inflammation and polycystic kidney disease progression
Ronak Lakhia, Matanel Yheskel, Andrea Flaten, Harini Ramalingam, Karam Aboudehen, Silvia Ferrè, Laurence Biggers, Abheepsa Mishra, Christopher Chaney, Darren P. Wallace, Thomas Carroll, Peter Igarashi, Vishal Patel
Ronak Lakhia, Matanel Yheskel, Andrea Flaten, Harini Ramalingam, Karam Aboudehen, Silvia Ferrè, Laurence Biggers, Abheepsa Mishra, Christopher Chaney, Darren P. Wallace, Thomas Carroll, Peter Igarashi, Vishal Patel
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Research Article Nephrology

Interstitial microRNA miR-214 attenuates inflammation and polycystic kidney disease progression

Abstract

Renal cysts are the defining feature of autosomal dominant polycystic kidney disease (ADPKD); however, the substantial interstitial inflammation is an often-overlooked aspect of this disorder. Recent studies suggest that immune cells in the cyst microenvironment affect ADPKD progression. Here we report that microRNAs (miRNAs) are new molecular signals in this crosstalk. We found that miR-214 and its host long noncoding RNA Dnm3os are upregulated in orthologous ADPKD mouse models and cystic kidneys from humans with ADPKD. In situ hybridization revealed that interstitial cells in the cyst microenvironment are the primary source of miR-214. While genetic deletion of miR-214 does not affect kidney development or homeostasis, surprisingly, its inhibition in Pkd2- and Pkd1-mutant mice aggravates cyst growth. Mechanistically, the proinflammatory TLR4/IFN-γ/STAT1 pathways transactivate the miR-214 host gene. miR-214, in turn as a negative feedback loop, directly inhibits Tlr4. Accordingly, miR-214 deletion is associated with increased Tlr4 expression and enhanced pericystic macrophage accumulation. Thus, miR-214 upregulation is a compensatory protective response in the cyst microenvironment that restrains inflammation and cyst growth.

Authors

Ronak Lakhia, Matanel Yheskel, Andrea Flaten, Harini Ramalingam, Karam Aboudehen, Silvia Ferrè, Laurence Biggers, Abheepsa Mishra, Christopher Chaney, Darren P. Wallace, Thomas Carroll, Peter Igarashi, Vishal Patel

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Figure 3

miR-214 deletion augments cyst-associated inflammation.

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miR-214 deletion augments cyst-associated inflammation. (A) Volcano plot...
(A) Volcano plot showing 972 differentially expressed genes between Pkd2-KO miR-214–/– and Pkd2-KO kidneys (n = 3/group). (B) Unbiased pathway analysis revealed that inflammation-associated pathways are among the top dysregulated pathways in Pkd2-KO miR-214–/– kidneys compared with Pkd2-KO kidneys. (C) Q-PCR analysis showed that the expression of M2-like macrophage markers Mrc1, Ccl2, Arg1, and Ym1 is increased in Pkd2-KO miR-214–/– kidneys (n = 8) compared with Pkd2-KO kidneys (n = 8). Western blot (D) and quantification (E) demonstrated increased MRC1 expression in Pkd2-KO miR-214–/– kidneys (n = 9) compared with Pkd2-KO kidneys (n = 9). (F) Immunofluorescence staining revealed enhanced accumulation of MRC1+ macrophages (red) surrounding cyst epithelial cells in Pkd2-KO miR-214–/– kidneys (n = 5). The sections are costained with DAPI (blue). *P < 0.05; Student’s unpaired t test (C and E); error bars indicate SEM.