Integrative Genomics Identifies Novel Associations with APOL1 Risk Genotypes in Black NEPTUNE Subjects

Sampson, Matthew G.; Robertson, Catherine; Martini, Sebastian; Mariani, Laura; Lemley, Kevin V.; Gillies, Christopher E.; Otto, Edgar A.; Kopp, Jeffrey B.; Randolph, A. G.; Vega-Warner, Virginia; Eichinger, Felix; Nair, Viji; Gipson, Debbie S.; Cattran, Daniel C.; Johnstone, Duncan B.; O’Toole, John F.; Bagnasco, Serena M.; Song, Peter; Barisoni, Laura; Troost, Jonathan P.; Kretzler, Matthias; Sedor, John R.

doi:10.1681/asn.2014111131

Cited by 114 publications

(124 citation statements)

References 39 publications

(42 reference statements)

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“…Another study compared APOL1 transcript levels in glomerular and tubulointerstitial compartments microdissected from human kidney biopsy samples of nephrotic syndrome subjects. Concordant with the immunohistology, APOL1 mRNA in both compartments was similar between nephrotic syndrome subjects with and without APOL1 risk genotypes 34 . These data suggest that APOL1 -associated kidney diseases do not result from differential abundance of variant APOL1 compared to APOL1-G0.…”

Section: Apol 1 Abundance and Kidney Diseasesupporting

confidence: 74%

“…As previously mentioned, APOL1 transcript levels were similar in glomerular or tubulointerstitial compartments of kidney biopsies from proteinuric African Americans with high and low risk APOL1 risk genotypes 34 . In addition, differential expression analysis, comparing transcriptomes from kidney biopsies of subjects with APOL1 high risk and low risk genotypes, identified only five differentially expressed genes (CXCL9, CXCL11, and UBD in glomerulus; SNOR14B and MUC13 in tubulointerstitium).…”

Section: Apol1-activated Signaling Pathwayssupporting

confidence: 67%

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The Cell Biology of APOL1

O’Toole

Bruggeman

Madhavan

et al. 2017

Seminars in Nephrology

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The association of variants in the APOL1 gene, which encodes apolipoprotein L1 (APOL1), with progressive non-diabetic kidney diseases in African Americans has prompted intense investigation into the function(s) of APOL1. APOL1 is an innate immune effector that protects humans from infection by some trypanosomal parasites. We review the data characterizing APOL1 trypanolytic function, which has been a basis for studies of APOL1 function in mammalian cells. Subsequently, we discuss the studies that use animal models, mammalian cell culture models, and kidney biopsy tissue to discover the mechanisms of variant APOL1-associated kidney diseases.

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Section: Apol 1 Abundance and Kidney Diseasesupporting

confidence: 74%

Section: Apol1-activated Signaling Pathwayssupporting

confidence: 67%

The Cell Biology of APOL1

O’Toole

Bruggeman

Madhavan

et al. 2017

Seminars in Nephrology

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“…UBD is a ubiquitin-like protein involved in the targeted degradation of cellular proteins, and UBD transcripts were recently shown to be upregulated in patients with APOL1-associated glomerular disease in the NEPTUNE cohort. 36 The strengths of this study are the high-quality analytical methods used, which enabled the testing of a number of hypotheses regarding APOL1 levels and APOL1-HDL-associated proteins and renal disease, including the association of specific variant proteins with CKD. This study was well powered and was done in a cohort with pre-established association between APOL1 genotype and risk of CKD.…”

Section: Discussionmentioning

confidence: 99%

Plasma Levels of Risk-Variant APOL1 Do Not Associate with Renal Disease in a Population-Based Cohort

Kozlitina

Zhou

Brown

et al. 2016

JASN

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Two common missense variants in APOL1 (G1 and G2) have been definitively linked to CKD in black Americans. However, not all individuals with the renal-risk genotype develop CKD, and little is known about how APOL1 variants drive disease. Given the association of APOL1 with HDL particles, which are cleared by the kidney, differences in the level or quality of mutant APOL1-HDL particles could be causal for disease and might serve as a useful risk stratification marker. We measured plasma levels of G0 (low risk), G1, and G2 APOL1 in 3450 individuals in the Dallas Heart Study using a liquid chromatography-MS method that enabled quantitation of the different variants. Additionally, we characterized native APOL1-HDL from donors with no or two APOL1 risk alleles by size-exclusion chromatography and analysis of immunopurified APOL1-HDL particles. Finally, we identified genetic loci associated with plasma APOL1 levels and tested for APOL1-dependent association with renal function. Although we replicated the previous association between APOL1 variant status and renal function in nondiabetic individuals, levels of circulating APOL1 did not associate with microalbuminuria or GFR. Furthermore, the size or known components of APOL1-HDL did not consistently differ in subjects with the renal-risk genotype. Genetic association studies implicated variants in loci harboring haptoglobin-related protein (HPR), APOL1, and ubiquitin D (UBD) in the regulation of plasma APOL1 levels, but these variants did not associate with renal function. Collectively, these data demonstrate that the risk of renal disease associated with APOL1 is probably not related to circulating levels of the mutant protein.

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“…In epidemiologic studies, Apolipoprotein L1 (APOL1) high-risk genotypes have been associated with poor renal outcomes in individuals of African ancestry (15,16). Because a published subset analysis of 90 NEPTUNE patients of African ancestry found APOL1 to be associated with complete remission and eGFR loss (17), future NEPTUNE studies will benefit from incorporation of complete APOL1 genotyping. IST was not a significant predictor of CRever among patients with MCD.…”

Section: Discussionmentioning

confidence: 99%

Complete Remission in the Nephrotic Syndrome Study Network

Gipson

Troost

Lafayette

et al. 2016

Clinical Journal of the American Society of Nephrology

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Background and objectives This analysis from the Nephrotic Syndrome Study Network (NEPTUNE) assessed the phenotypic and pathology characteristics of proteinuric patients undergoing kidney biopsy and defined the frequency and factors associated with complete proteinuria remission (CRever).Design, setting, participants, & measurements We enrolled adults and children with proteinuria $0.5 g/d at the time of first clinically indicated renal biopsy at 21 sites in North America from April 2010 to June 2014 into a prospective cohort study. NEPTUNE central pathologists assigned participants to minimal-change disease (MCD), FSGS, membranous nephropathy, or other glomerulopathy cohorts. Outcome measures for this analysis were (1) CRever with urine protein-to-creatinine ratio (UPC) ,0.3 g/g with preserved native kidney function and (2) ESRD. Continuous variables are reported as median and interquartile range (IQR; 25th, 75th percentile). Cox proportional hazards modeling was used to assess factors associated with CRever.Results We enrolled 441 patients: 116 (27%) had MCD, 142 (32%) had FSGS, 66 (15%) had membranous nephropathy, and 117 (27%) had other glomerulopathy. The baseline UPC was 4.1 g/g (IQR, 1.9, 7.7) and the eGFR was 81 ml/min per 1.73 m 2 (IQR, 50, 105). Median duration of observation was 19 months (IQR,11, 30). CRever occurred in 46% of patients, and 4.6% progressed to ESRD. Multivariate analysis demonstrated that higher prebiopsy proteinuria (hazard ratio, 0.3; 95% confidence interval, 0.2 to 0.5) and pathology diagnosis (FSGS versus MCD; hazard ratio, 0.2; 95% confidence interval, 0.1 to 0.5) were inversely associated with CRever. The effect of immunosuppressive therapy on remission varied by pathology diagnosis.Conclusions In NEPTUNE, the high frequency of other pathology in proteinuric patients affirms the value of the diagnostic kidney biopsy. Clinical factors, including level of proteinuria before biopsy, pathology diagnosis, and immunosuppression, are associated with complete remission.

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Integrative Genomics Identifies Novel Associations with APOL1 Risk Genotypes in Black NEPTUNE Subjects

Cited by 114 publications

References 39 publications

The Cell Biology of APOL1

The Cell Biology of APOL1

Plasma Levels of Risk-Variant APOL1 Do Not Associate with Renal Disease in a Population-Based Cohort

Complete Remission in the Nephrotic Syndrome Study Network

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