Literature DB >> 25866874

Evidence That Up-Regulation of MicroRNA-29 Contributes to Postnatal Body Growth Deceleration.

Fariha Kamran1, Anenisia C Andrade1, Aikaterini A Nella1, Samuel J Clokie1, Geoffrey Rezvani1, Ola Nilsson1, Jeffrey Baron1, Julian C Lui1.   

Abstract

Body growth is rapid in infancy but subsequently slows and eventually ceases due to a progressive decline in cell proliferation that occurs simultaneously in multiple organs. We previously showed that this decline in proliferation is driven in part by postnatal down-regulation of a large set of growth-promoting genes in multiple organs. We hypothesized that this growth-limiting genetic program is orchestrated by microRNAs (miRNAs). Bioinformatic analysis identified target sequences of the miR-29 family of miRNAs to be overrepresented in age-down-regulated genes. Concomitantly, expression microarray analysis in mouse kidney and lung showed that all members of the miR-29 family, miR-29a, -b, and -c, were strongly up-regulated from 1 to 6 weeks of age. Real-time PCR confirmed that miR-29a, -b, and -c were up-regulated with age in liver, kidney, lung, and heart, and their expression levels were higher in hepatocytes isolated from 5-week-old mice than in hepatocytes from embryonic mouse liver at embryonic day 16.5. We next focused on 3 predicted miR-29 target genes (Igf1, Imp1, and Mest), all of which are growth-promoting. A 3'-untranslated region containing the predicted target sequences from each gene was placed individually in a luciferase reporter construct. Transfection of miR-29 mimics suppressed luciferase gene activity for all 3 genes, and this suppression was diminished by mutating the target sequences, suggesting that these genes are indeed regulated by miR-29. Taken together, the findings suggest that up-regulation of miR-29 during juvenile life drives the down-regulation of multiple growth-promoting genes, thus contributing to physiological slowing and eventual cessation of body growth.

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Year:  2015        PMID: 25866874      PMCID: PMC4447640          DOI: 10.1210/me.2015-1047

Source DB:  PubMed          Journal:  Mol Endocrinol        ISSN: 0888-8809


  30 in total

1.  Coordinated postnatal down-regulation of multiple growth-promoting genes: evidence for a genetic program limiting organ growth.

Authors:  Julian C Lui; Patricia Forcinito; Maria Chang; Weiping Chen; Kevin M Barnes; Jeffrey Baron
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Review 2.  Regulation of mRNA translation and stability by microRNAs.

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3.  An extensive genetic program occurring during postnatal growth in multiple tissues.

Authors:  Gabriela P Finkielstain; Patricia Forcinito; Julian C K Lui; Kevin M Barnes; Rose Marino; Sami Makaroun; Vina Nguyen; Jacob E Lazarus; Ola Nilsson; Jeffrey Baron
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Review 4.  Mechanisms limiting body growth in mammals.

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Review 5.  MicroRNAs in development and disease.

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Journal:  FEBS Lett       Date:  2013-04-12       Impact factor: 4.124

7.  Evidence that Igf2 down-regulation in postnatal tissues and up-regulation in malignancies is driven by transcription factor E2f3.

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Authors:  Julian C Lui
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3.  Pregnancy-driven cardiovascular maternal miR-29 plasticity in obesity.

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4.  Gradual Rarefaction of Hematopoietic Precursors and Atrophy in a Depleted microRNA 29a, b and c Environment.

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6.  miR-29b overexpression induces cochlear hair cell apoptosis through the regulation of SIRT1/PGC-1α signaling: Implications for age-related hearing loss.

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7.  Association of plasma microRNA expression with age, genetic background and functional traits in dairy cattle.

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9.  MiR-29a Increase in Aging May Function as a Compensatory Mechanism Against Cardiac Fibrosis Through SERPINH1 Downregulation.

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10.  Cardiac myocyte miR-29 promotes pathological remodeling of the heart by activating Wnt signaling.

Authors:  Yassine Sassi; Petros Avramopoulos; Deepak Ramanujam; Laurenz Grüter; Stanislas Werfel; Simon Giosele; Andreas-David Brunner; Dena Esfandyari; Aikaterini S Papadopoulou; Bart De Strooper; Norbert Hübner; Regalla Kumarswamy; Thomas Thum; Xiaoke Yin; Manuel Mayr; Bernhard Laggerbauer; Stefan Engelhardt
Journal:  Nat Commun       Date:  2017-11-20       Impact factor: 14.919

  10 in total

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