Transgenic expression of human APOL1 risk variants in podocytes induces kidney disease in mice

Pazit Beckerman; Jing Bi-Karchin; Ae Seo Deok Park; Chengxiang Qiu; Patrick D. Dummer; Irfana Soomro; Carine M. Boustany-Kari; Steven S. Pullen; Jeffrey H. Miner; Chien An A. Hu; Tibor Rohacs; Kazunori Inoue; Shuta Ishibe; Moin A. Saleem; Matthew B. Palmer; Ana Maria Cuervo; Jeffrey B. Kopp; Katalin Susztak

doi:10.1038/nm.4287

Transgenic expression of human APOL1 risk variants in podocytes induces kidney disease in mice

Pazit Beckerman, Jing Bi-Karchin, Ae Seo Deok Park, Chengxiang Qiu, Patrick D. Dummer, Irfana Soomro, Carine M. Boustany-Kari, Steven S. Pullen, Jeffrey H. Miner, Chien An A. Hu, Tibor Rohacs, Kazunori Inoue, Shuta Ishibe, Moin A. Saleem, Matthew B. Palmer, Ana Maria Cuervo, Jeffrey B. Kopp, Katalin Susztak

Developmental & Molecular Biology

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Abstract

African Americans have a heightened risk of developing chronic and end-stage kidney disease, an association that is largely attributed to two common genetic variants, termed G1 and G2, in the APOL1 gene. Direct evidence demonstrating that these APOL1 risk alleles are pathogenic is still lacking because the APOL1 gene is present in only some primates and humans; thus it has been challenging to demonstrate experimental proof of causality of these risk alleles for renal disease. Here we generated mice with podocyte-specific inducible expression of the APOL1 reference allele (termed G0) or each of the risk-conferring alleles (G1 or G2). We show that mice with podocyte-specific expression of either APOL1 risk allele, but not of the G0 allele, develop functional (albuminuria and azotemia), structural (foot-process effacement and glomerulosclerosis) and molecular (gene-expression) changes that closely resemble human kidney disease. Disease development was cell-type specific and likely reversible, and the severity correlated with the level of expression of the risk allele. We further found that expression of the risk-variant APOL1 alleles interferes with endosomal trafficking and blocks autophagic flux, which ultimately leads to inflammatory-mediated podocyte death and glomerular scarring. In summary, this is the first demonstration that the expression of APOL1 risk alleles is causal for altered podocyte function and glomerular disease in vivo.

Original language	English (US)
Pages (from-to)	429-438
Number of pages	10
Journal	Nature Medicine
Volume	23
Issue number	4
DOIs	https://doi.org/10.1038/nm.4287
State	Published - Apr 1 2017

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1038/nm.4287

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Beckerman, P., Bi-Karchin, J., Park, A. S. D., Qiu, C., Dummer, P. D., Soomro, I., Boustany-Kari, C. M., Pullen, S. S., Miner, J. H., Hu, C. A. A., Rohacs, T., Inoue, K., Ishibe, S., Saleem, M. A., Palmer, M. B., Cuervo, A. M., Kopp, J. B., & Susztak, K. (2017). Transgenic expression of human APOL1 risk variants in podocytes induces kidney disease in mice. Nature Medicine, 23(4), 429-438. https://doi.org/10.1038/nm.4287

Beckerman, P, Bi-Karchin, J, Park, ASD, Qiu, C, Dummer, PD, Soomro, I, Boustany-Kari, CM, Pullen, SS, Miner, JH, Hu, CAA, Rohacs, T, Inoue, K, Ishibe, S, Saleem, MA, Palmer, MB, Cuervo, AM, Kopp, JB & Susztak, K 2017, 'Transgenic expression of human APOL1 risk variants in podocytes induces kidney disease in mice', Nature Medicine, vol. 23, no. 4, pp. 429-438. https://doi.org/10.1038/nm.4287

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title = "Transgenic expression of human APOL1 risk variants in podocytes induces kidney disease in mice",

abstract = "African Americans have a heightened risk of developing chronic and end-stage kidney disease, an association that is largely attributed to two common genetic variants, termed G1 and G2, in the APOL1 gene. Direct evidence demonstrating that these APOL1 risk alleles are pathogenic is still lacking because the APOL1 gene is present in only some primates and humans; thus it has been challenging to demonstrate experimental proof of causality of these risk alleles for renal disease. Here we generated mice with podocyte-specific inducible expression of the APOL1 reference allele (termed G0) or each of the risk-conferring alleles (G1 or G2). We show that mice with podocyte-specific expression of either APOL1 risk allele, but not of the G0 allele, develop functional (albuminuria and azotemia), structural (foot-process effacement and glomerulosclerosis) and molecular (gene-expression) changes that closely resemble human kidney disease. Disease development was cell-type specific and likely reversible, and the severity correlated with the level of expression of the risk allele. We further found that expression of the risk-variant APOL1 alleles interferes with endosomal trafficking and blocks autophagic flux, which ultimately leads to inflammatory-mediated podocyte death and glomerular scarring. In summary, this is the first demonstration that the expression of APOL1 risk alleles is causal for altered podocyte function and glomerular disease in vivo.",

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AU - Beckerman, Pazit

AU - Bi-Karchin, Jing

AU - Park, Ae Seo Deok

AU - Qiu, Chengxiang

AU - Dummer, Patrick D.

AU - Soomro, Irfana

AU - Boustany-Kari, Carine M.

AU - Pullen, Steven S.

AU - Miner, Jeffrey H.

AU - Hu, Chien An A.

AU - Rohacs, Tibor

AU - Inoue, Kazunori

AU - Ishibe, Shuta

AU - Saleem, Moin A.

AU - Palmer, Matthew B.

AU - Cuervo, Ana Maria

AU - Kopp, Jeffrey B.

AU - Susztak, Katalin

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N2 - African Americans have a heightened risk of developing chronic and end-stage kidney disease, an association that is largely attributed to two common genetic variants, termed G1 and G2, in the APOL1 gene. Direct evidence demonstrating that these APOL1 risk alleles are pathogenic is still lacking because the APOL1 gene is present in only some primates and humans; thus it has been challenging to demonstrate experimental proof of causality of these risk alleles for renal disease. Here we generated mice with podocyte-specific inducible expression of the APOL1 reference allele (termed G0) or each of the risk-conferring alleles (G1 or G2). We show that mice with podocyte-specific expression of either APOL1 risk allele, but not of the G0 allele, develop functional (albuminuria and azotemia), structural (foot-process effacement and glomerulosclerosis) and molecular (gene-expression) changes that closely resemble human kidney disease. Disease development was cell-type specific and likely reversible, and the severity correlated with the level of expression of the risk allele. We further found that expression of the risk-variant APOL1 alleles interferes with endosomal trafficking and blocks autophagic flux, which ultimately leads to inflammatory-mediated podocyte death and glomerular scarring. In summary, this is the first demonstration that the expression of APOL1 risk alleles is causal for altered podocyte function and glomerular disease in vivo.

AB - African Americans have a heightened risk of developing chronic and end-stage kidney disease, an association that is largely attributed to two common genetic variants, termed G1 and G2, in the APOL1 gene. Direct evidence demonstrating that these APOL1 risk alleles are pathogenic is still lacking because the APOL1 gene is present in only some primates and humans; thus it has been challenging to demonstrate experimental proof of causality of these risk alleles for renal disease. Here we generated mice with podocyte-specific inducible expression of the APOL1 reference allele (termed G0) or each of the risk-conferring alleles (G1 or G2). We show that mice with podocyte-specific expression of either APOL1 risk allele, but not of the G0 allele, develop functional (albuminuria and azotemia), structural (foot-process effacement and glomerulosclerosis) and molecular (gene-expression) changes that closely resemble human kidney disease. Disease development was cell-type specific and likely reversible, and the severity correlated with the level of expression of the risk allele. We further found that expression of the risk-variant APOL1 alleles interferes with endosomal trafficking and blocks autophagic flux, which ultimately leads to inflammatory-mediated podocyte death and glomerular scarring. In summary, this is the first demonstration that the expression of APOL1 risk alleles is causal for altered podocyte function and glomerular disease in vivo.

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Transgenic expression of human APOL1 risk variants in podocytes induces kidney disease in mice

Abstract

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