Journal of Biological Chemistry

Journal of Biological Chemistry

Volume 295, Issue 32, 7 August 2020, Pages 11068-11081
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Gene Regulation
Effects of intron conversion in the human CYP11B2 gene on its transcription and blood pressure regulation in transgenic mice

https://doi.org/10.1074/jbc.RA120.013047Get rights and content
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The human cytochrome P450 family 11 subfamily B member 2 (hCYP11B2) gene encodes aldosterone synthase, the rate-limiting enzyme in the biosynthesis of aldosterone. In some humans, hCYP11B2 undergoes a unique intron conversion whose function is largely unclear. The intron conversion is formed by a replacement of the segment of DNA within intron 2 of hCYP11B2 with the corresponding region of the hCYP11B1 gene. We show here that the intron conversion is located in an open chromatin form and binds more strongly to the transcriptional regulators histone acetyltransferase P300 (p300), NFκB, and CCAAT enhancer–binding protein α (CEBPα). Reporter constructs containing the intron conversion had increased promoter activity on transient transfection in H295R cells compared with WT intron 2. We generated humanized transgenic (TG) mice containing all the introns, exons, and 5′- and 3′-flanking regions of the hCYP11B2 gene containing either the intron conversion or WT intron 2. We found that TG mice containing the intron conversion have (a) increased plasma aldosterone levels, (b) increased hCYP11B2 mRNA and protein levels, and (c) increased blood pressure compared with TG mice containing WT intron 2. Results of a ChIP assay showed that chromatin obtained from the adrenals of TG mice containing the intron conversion binds more strongly to p300, NFκB, and CEBPα than to WT intron 2. These results uncover a functional role of intron conversion in hCYP11B2 and suggest a new paradigm in blood pressure regulation.

transgenic mice
aldosterone synthase
single‐nucleotide polymorphism (SNP,)
gene expression
genetics
hypertension
cardiovascular disease
renin-angiotensin system
intron conversion
cytochrome P450 family 11 subfamily B member 2 (CYP11B2)

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This article contains supporting information.

Author contributions—B. M. and A. K. conceptualization; B. M., I. S., S. H., N. R. F., and A. K. data curation; B. M. and I. S. software; B. M., I. S., and A. K. formal analysis; B. M., I. S., S. H., N. R. F., and A. K. validation; B. M., I. S., S. H., N. R. F., and A. K. investigation; B. M., I. S., S. H., N. R. F., and A. K. visualization; B. M., I. S., and A. K. methodology; B. M., I. S., and A. K. writing-original draft; B. M. and A. K. project administration; B. M., I. S., and A. K. writing-review and editing; A. K. resources; A. K. supervision; A. K. funding acquisition.

Funding and additional information—This work was supported by NHLBI, National Institutes of Health Grants RO1 HL 122742 and RO1 HL 130344 (to A. K.). The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health.

Conflict of interest—The authors declare that they have no conflicts of interest with the contents of this article.

Abbreviations—The abbreviations used are:

    Hap

    haplotype

    TG

    transgenic

    IC

    intron conversion

    ES cell

    embryonic stem cell

    qPCR

    quantitative PCR

    BP

    blood pressure

    SBP

    systolic BP

    DBP

    diastolic BP

    MAP

    mean arterial pressure

    HR

    heart rate

    LD

    linkage disequilibrium.

© 2020 Mopidevi et al.