Genetic variation in APOL1 associates with younger age at hemodialysis initiation

Zahra Kanji; Camille E. Powe; Julia B. Wenger; Chunmei Huang; Elizabeth Ankers; Dorothy A. Sullivan; Gina Collerone; Neil R. Powe; Marcello Tonelli; Ishir Bhan; Andrea J. Bernhardy; Salvatore DiBartolo; David Friedman; Giulio Genovese; Martin R. Pollak; Ravi Thadhani

doi:10.1681/ASN.2010121234

Genetic variation in APOL1 associates with younger age at hemodialysis initiation

Zahra Kanji, Camille E. Powe, Julia B. Wenger, Chunmei Huang, Elizabeth Ankers, Dorothy A. Sullivan, Gina Collerone, Neil R. Powe, Marcello Tonelli, Ishir Bhan, Andrea J. Bernhardy, Salvatore DiBartolo, David Friedman, Giulio Genovese, Martin R. Pollak, Ravi Thadhani

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Abstract

African Americans have a markedly higher incidence of ESRD compared with other racial groups. Two variants in the APOL1 gene, to date observed only among individuals of recent African ancestry, associate with increased risk for renal disease among African Americans. Here, we investigated whether these risk alleles also associate with age at initiation of chronic hemodialysis. We performed a crosssectional study of 407 nondiabetic African Americans with ESRD who participated in the Accelerated Mortality on Renal Replacement (ArMORR) study, a prospective cohort of incident chronic hemodialysis patients. African Americans carrying two copies of the G1 risk allele initiated chronic hemodialysis at a mean age of 49.0 ± 14.9 years, which was significantly younger than both subjects with one copy of the G1 allele (55.9 ± 16.7 years; P = 0.014) and subjects without either risk allele (61.8 ± 17.1 years; P =6.2 × 10 ^-7). The association between the presence of the G1 allele and age at initiation of hemodialysis remained statistically significant after adjusting for sociodemographic and other potential confounders. We did not detect an association between the G2 risk allele and age at initiation of hemodialysis, but the sample size was limited. In conclusion, genetic variations in APOL1 identify African Americans that initiate chronic hemodialysis at a younger age. Early interventions to prevent progression of kidney disease may benefit this high-risk population.

Original language	English (US)
Pages (from-to)	2091-2097
Number of pages	7
Journal	Journal of the American Society of Nephrology
Volume	22
Issue number	11
DOIs	https://doi.org/10.1681/ASN.2010121234
State	Published - Nov 2011
Externally published	Yes

ASJC Scopus subject areas

Nephrology

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Kanji, Z., Powe, C. E., Wenger, J. B., Huang, C., Ankers, E., Sullivan, D. A., Collerone, G., Powe, N. R., Tonelli, M., Bhan, I., Bernhardy, A. J., DiBartolo, S., Friedman, D., Genovese, G., Pollak, M. R., & Thadhani, R. (2011). Genetic variation in APOL1 associates with younger age at hemodialysis initiation. Journal of the American Society of Nephrology, 22(11), 2091-2097. https://doi.org/10.1681/ASN.2010121234

Kanji, Z, Powe, CE, Wenger, JB, Huang, C, Ankers, E, Sullivan, DA, Collerone, G, Powe, NR, Tonelli, M, Bhan, I, Bernhardy, AJ, DiBartolo, S, Friedman, D, Genovese, G, Pollak, MR & Thadhani, R 2011, 'Genetic variation in APOL1 associates with younger age at hemodialysis initiation', Journal of the American Society of Nephrology, vol. 22, no. 11, pp. 2091-2097. https://doi.org/10.1681/ASN.2010121234

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title = "Genetic variation in APOL1 associates with younger age at hemodialysis initiation",

abstract = "African Americans have a markedly higher incidence of ESRD compared with other racial groups. Two variants in the APOL1 gene, to date observed only among individuals of recent African ancestry, associate with increased risk for renal disease among African Americans. Here, we investigated whether these risk alleles also associate with age at initiation of chronic hemodialysis. We performed a crosssectional study of 407 nondiabetic African Americans with ESRD who participated in the Accelerated Mortality on Renal Replacement (ArMORR) study, a prospective cohort of incident chronic hemodialysis patients. African Americans carrying two copies of the G1 risk allele initiated chronic hemodialysis at a mean age of 49.0 ± 14.9 years, which was significantly younger than both subjects with one copy of the G1 allele (55.9 ± 16.7 years; P = 0.014) and subjects without either risk allele (61.8 ± 17.1 years; P =6.2 × 10 -7). The association between the presence of the G1 allele and age at initiation of hemodialysis remained statistically significant after adjusting for sociodemographic and other potential confounders. We did not detect an association between the G2 risk allele and age at initiation of hemodialysis, but the sample size was limited. In conclusion, genetic variations in APOL1 identify African Americans that initiate chronic hemodialysis at a younger age. Early interventions to prevent progression of kidney disease may benefit this high-risk population.",

author = "Zahra Kanji and Powe, {Camille E.} and Wenger, {Julia B.} and Chunmei Huang and Elizabeth Ankers and Sullivan, {Dorothy A.} and Gina Collerone and Powe, {Neil R.} and Marcello Tonelli and Ishir Bhan and Bernhardy, {Andrea J.} and Salvatore DiBartolo and David Friedman and Giulio Genovese and Pollak, {Martin R.} and Ravi Thadhani",

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doi = "10.1681/ASN.2010121234",

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AU - Kanji, Zahra

AU - Powe, Camille E.

AU - Wenger, Julia B.

AU - Huang, Chunmei

AU - Ankers, Elizabeth

AU - Sullivan, Dorothy A.

AU - Collerone, Gina

AU - Powe, Neil R.

AU - Tonelli, Marcello

AU - Bhan, Ishir

AU - Bernhardy, Andrea J.

AU - DiBartolo, Salvatore

AU - Friedman, David

AU - Genovese, Giulio

AU - Pollak, Martin R.

AU - Thadhani, Ravi

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AB - African Americans have a markedly higher incidence of ESRD compared with other racial groups. Two variants in the APOL1 gene, to date observed only among individuals of recent African ancestry, associate with increased risk for renal disease among African Americans. Here, we investigated whether these risk alleles also associate with age at initiation of chronic hemodialysis. We performed a crosssectional study of 407 nondiabetic African Americans with ESRD who participated in the Accelerated Mortality on Renal Replacement (ArMORR) study, a prospective cohort of incident chronic hemodialysis patients. African Americans carrying two copies of the G1 risk allele initiated chronic hemodialysis at a mean age of 49.0 ± 14.9 years, which was significantly younger than both subjects with one copy of the G1 allele (55.9 ± 16.7 years; P = 0.014) and subjects without either risk allele (61.8 ± 17.1 years; P =6.2 × 10 -7). The association between the presence of the G1 allele and age at initiation of hemodialysis remained statistically significant after adjusting for sociodemographic and other potential confounders. We did not detect an association between the G2 risk allele and age at initiation of hemodialysis, but the sample size was limited. In conclusion, genetic variations in APOL1 identify African Americans that initiate chronic hemodialysis at a younger age. Early interventions to prevent progression of kidney disease may benefit this high-risk population.

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Genetic variation in APOL1 associates with younger age at hemodialysis initiation

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