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Therapeutics for APOL1 nephropathies: putting out the fire in the podocyte

  1. Author:
    Heymann, Jurgen
    Winkler, Cheryl
    Hoek, Maarten
    Susztak, Katalin
    Kopp, Jeffrey B.

  2. Author Address

    NIDDK, Kidney Dis Sect, NIH, Bethesda, MD 20892 USA.NCI, Mol Genet Epidemiol Sect, Basic Res Lab,NIH, Basic Sci Program,Leidos Biomed Res,Frederick Nat, Frederick, MD 21701 USA.Merck & Co Inc, Merck Res Labs, Kenilworth, NJ USA.Univ Penn, Sch Med, Dept Med, Renal Electrolyte & Hypertens Div,Perelman Sch Me, Philadelphia, PA 19104 USA.
    1. Year: 2017
    2. Date: Jan 01
  2. Journal: NEPHROLOGY DIALYSIS TRANSPLANTATION
  3. OXFORD UNIV PRESS,
    1. 32
    2. Supplement: 1
    3. Pages: i65-i70
  5. Type of Article: Article
  6. Article Number: i65-i70
  7. ISSN: 0931-0509
  1. Abstract:

    APOL1 nephropathies comprise a range of clinical and pathologic syndromes, which can be summarized as focal segmental glomerulosclerosis, in various guises, and arterionephrosclerosis, otherwise known as hypertensive kidney diseases. Current therapies for these conditions may achieve therapeutic targets, reduction in proteinuria and control of blood pressure, respectively, but often fail to halt the progressive decline in kidney function. It appears that current therapies fail to address certain underlying critical pathologic processes that are driven, particularly in podocytes and microvascular cells, by the APOL1 renal risk genetic variants. Mechanisms hypothesized to be responsible for APOL1 variant-associated cell injury can be summarized in five domains: increased APOL1 gene expression, activation of inflammasomes, activation of protein kinase R, electrolyte flux across plasma or intracellular membranes, and altered endolysosomal trafficking associated with endoplasmic reticulum stress. We briefly review the available evidence for these five mechanisms and suggest possible novel therapeutic approaches.

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External Sources

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  2. DOI: 10.1093/ndt/gfw402
  3. PMID: 28391347
  4. View record in Web of ScienceĀ®
  5. WOS: 000397027100009

Library Notes

  1. Fiscal Year: FY2016-2017
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