Your search keyword '"Apol1"' showing total 45 results

1. Safety and Tolerability of the APOL1 Inhibitor, Inaxaplin, following Single- and Multiple-Ascending Doses in Healthy Adults

Author

Ogo Egbuna, Vincent Audard, George Manos, Simon Tian, Fanuel Hagos, and Glenn M. Chertow

Subjects

apol1, apol1-mediated kidney disease, chronic kidney disease, inaxaplin, safety, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Introduction: Toxic gain-of-function Apolipoprotein L1 (APOL1) variants contribute to the development of proteinuric nephropathies collectively referred to as APOL1-mediated kidney disease (AMKD). Despite standard-of-care treatments, patients with AMKD experience accelerated progression to end-stage kidney disease. The identification of two APOL1 variants as the genetic cause of AMKD inspired development of inaxaplin, an inhibitor of APOL1 channel activity that reduces proteinuria in patients with AMKD. Methods: We conducted two phase 1 studies evaluating the safety, tolerability, and pharmacokinetics of single-ascending doses (SAD) and multiple-ascending doses (MAD) of inaxaplin in healthy participants. In the SAD cohorts, participants were randomized to receive inaxaplin as a single dose (range, 7.5 mg to 165 mg) or placebo. In the MAD cohorts, participants were randomized to receive multiple doses of inaxaplin (range, 15 to 120 mg daily) or placebo for 14 days. We assessed safety and tolerability based on adverse events (AEs), clinical laboratory values, electrocardiograms (ECGs), and vital signs. Results: A total of 178 participants were randomized in the SAD/MAD cohorts of both studies (mean age: 36.7 years; 94.9% male). The proportion of participants with any AEs was similar in the inaxaplin (24.6%) and placebo (22.7%) groups. All AEs were mild or moderate in severity; there were no serious AEs. Headache was the most common AE: 10.4% and 2.3% in the inaxaplin and placebo groups, respectively. There were no drug-related treatment discontinuations and no clinically relevant trends in laboratory values, ECGs, or vital signs. Discussion/Conclusion: Inaxaplin is safe and well tolerated at single doses up to 165 mg and multiple doses up to 120 mg daily for 14 days. These results are consistent with the favorable safety profile of inaxaplin in a completed phase 2a proof-of-concept study. Together, these findings support continued evaluation of inaxaplin in an ongoing phase 2/3 pivotal trial as a potential precision medicine for patients with AMKD.

Published

2024

2. Safety and Tolerability of the APOL1 Inhibitor, Inaxaplin, following Single- and Multiple-Ascending Doses in Healthy Adults.

Author

Egbuna, Ogo, Audard, Vincent, Manos, George, Tian, Simon, Hagos, Fanuel, and Chertow, Glenn M.

Subjects

CHRONIC kidney failure, TERMINATION of treatment, ADULTS, KIDNEY diseases, VITAL signs

Abstract

Introduction: Toxic gain-of-function Apolipoprotein L1 (APOL1) variants contribute to the development of proteinuric nephropathies collectively referred to as APOL1-mediated kidney disease (AMKD). Despite standard-of-care treatments, patients with AMKD experience accelerated progression to end-stage kidney disease. The identification of two APOL1 variants as the genetic cause of AMKD inspired development of inaxaplin, an inhibitor of APOL1 channel activity that reduces proteinuria in patients with AMKD. Methods: We conducted two phase 1 studies evaluating the safety, tolerability, and pharmacokinetics of single-ascending doses (SAD) and multiple-ascending doses (MAD) of inaxaplin in healthy participants. In the SAD cohorts, participants were randomized to receive inaxaplin as a single dose (range, 7.5 mg to 165 mg) or placebo. In the MAD cohorts, participants were randomized to receive multiple doses of inaxaplin (range, 15 to 120 mg daily) or placebo for 14 days. We assessed safety and tolerability based on adverse events (AEs), clinical laboratory values, electrocardiograms (ECGs), and vital signs. Results: A total of 178 participants were randomized in the SAD/MAD cohorts of both studies (mean age: 36.7 years; 94.9% male). The proportion of participants with any AEs was similar in the inaxaplin (24.6%) and placebo (22.7%) groups. All AEs were mild or moderate in severity; there were no serious AEs. Headache was the most common AE: 10.4% and 2.3% in the inaxaplin and placebo groups, respectively. There were no drug-related treatment discontinuations and no clinically relevant trends in laboratory values, ECGs, or vital signs. Discussion/Conclusion: Inaxaplin is safe and well tolerated at single doses up to 165 mg and multiple doses up to 120 mg daily for 14 days. These results are consistent with the favorable safety profile of inaxaplin in a completed phase 2a proof-of-concept study. Together, these findings support continued evaluation of inaxaplin in an ongoing phase 2/3 pivotal trial as a potential precision medicine for patients with AMKD. [ABSTRACT FROM AUTHOR]

Published

2024

3. APOL1 Kidney-Risk Variants Induce Mitochondrial Fission

Author

Ma, Lijun, Ainsworth, Hannah C, Snipes, James A, Murea, Mariana, Choi, Young A, Langefeld, Carl D, Parks, John S, Bharadwaj, Manish S, Chou, Jeff W, Hemal, Ashok K, Petrovic, Snezana, Craddock, Ann L, Cheng, Dongmei, Hawkins, Gregory A, Miller, Lance D, Hicks, Pamela J, Saleem, Moin A, Divers, Jasmin, Molina, Anthony JA, and Freedman, Barry I

Subjects

Biomedical and Clinical Sciences, Genetics, Kidney Disease, Biotechnology, Prevention, 2.1 Biological and endogenous factors, Aetiology, Renal and urogenital, African Americans, APOL1, chronic kidney disease, FSGS, mitochondria, Biomedical and clinical sciences, Health sciences

Abstract

IntroductionAPOL1 G1 and G2 nephropathy-risk variants cause mitochondrial dysfunction and contribute to kidney disease. Analyses were performed to determine the genetic regulation of APOL1 and elucidate potential mechanisms in APOL1-nephropathy.MethodsA global gene expression analysis was performed in human primary renal tubule cell lines derived from 50 African American individuals. Follow-up gene knock out, cell-based rescue, and microscopy experiments were performed.ResultsAPOL1 genotypes did not alter APOL1 expression levels in the global gene expression analysis. Expression quantitative trait locus (eQTL) analysis in polyinosinic-polycytidylic acid (poly IC)-stimulated renal tubule cells revealed that single nucleotide polymorphism (SNP) rs513349 adjacent to BAK1 was a trans eQTL for APOL1 and a cis eQTL for BAK1; APOL1 and BAK1 were co-expressed in cells. BAK1 knockout in a human podocyte cell line resulted in diminished APOL1 protein, supporting a pivotal effect for BAK1 on APOL1 expression. Because BAK1 is involved in mitochondrial dynamics, mitochondrial morphology was examined in primary renal tubule cells and HEK293 Tet-on cells of various APOL1 genotypes. Mitochondria in APOL1 wild-type (G0G0) tubule cells maintained elongated morphology when stimulated by low-dose poly IC, whereas those with G1G1, G2G2, and G1G2 genotypes appeared to fragment. HEK293 Tet-on cells overexpressing APOL1 G0, G1, and G2 were created; G0 cells appeared to promote mitochondrial fusion, whereas G1 and G2 induced mitochondrial fission. The mitochondrial dynamic regulator Mdivi-1 significantly preserved cell viability and mitochondrial cristae structure and reversed mitochondrial fission induced by overexpression of G1 and G2.ConclusionResults suggest the mitochondrial fusion/fission pathway may be a therapeutic target in APOL1-nephropathy.

Published

2020

4. APOL1 Long-term Kidney Transplantation Outcomes Network (APOLLO): Design and Rationale

Author

Freedman, Barry I, Moxey-Mims, Marva M, Alexander, Amir A, Astor, Brad C, Birdwell, Kelly A, Bowden, Donald W, Bowen, Gordon, Bromberg, Jonathan, Craven, Timothy E, Dadhania, Darshana M, Divers, Jasmin, Doshi, Mona D, Eidbo, Elling, Fornoni, Alessia, Gautreaux, Michael D, Gbadegesin, Rasheed A, Gee, Patrick O, Guerra, Giselle, Hsu, Chi-yuan, Iltis, Ana S, Jefferson, Nichole, Julian, Bruce A, Klassen, David K, Koty, Patrick P, Langefeld, Carl D, Lentine, Krista L, Ma, Lijun, Mannon, Roslyn B, Menon, Madhav C, Mohan, Sumit, Moore, J Brian, Murphy, Barbara, Newell, Kenneth A, Odim, Jonah, Ortigosa-Goggins, Mariella, Palmer, Nicholette D, Park, Meyeon, Parsa, Afshin, Pastan, Stephen O, Poggio, Emilio D, Rajapakse, Nishadi, Reeves-Daniel, Amber M, Rosas, Sylvia E, Russell, Laurie P, Sawinski, Deirdre, Smith, S Carrie, Spainhour, Mitzie, Stratta, Robert J, Weir, Matthew R, Reboussin, David M, Kimmel, Paul L, and Brennan, Daniel C

Subjects

Clinical Research, Organ Transplantation, Transplantation, Kidney Disease, Renal and urogenital, Good Health and Well Being, African Americans, APOL1, chronic kidney disease, graft failure, kidney transplantation, outcomes

Abstract

IntroductionMuch of the higher risk for end-stage kidney disease (ESKD) in African American individuals relates to ancestry-specific variation in the apolipoprotein L1 gene (APOL1). Relative to kidneys from European American deceased-donors, kidneys from African American deceased-donors have shorter allograft survival and African American living-kidney donors more often develop ESKD. The National Institutes of Health (NIH)-sponsored APOL1 Long-term Kidney Transplantation Outcomes Network (APOLLO) is prospectively assessing kidney allograft survival from donors with recent African ancestry based on donor and recipient APOL1 genotypes.MethodsAPOLLO will evaluate outcomes from 2614 deceased kidney donor-recipient pairs, as well as additional living-kidney donor-recipient pairs and unpaired deceased-donor kidneys.ResultsThe United Network for Organ Sharing (UNOS), Association of Organ Procurement Organizations, American Society of Transplantation, American Society for Histocompatibility and Immunogenetics, and nearly all U.S. kidney transplant programs, organ procurement organizations (OPOs), and histocompatibility laboratories are participating in this observational study. APOLLO employs a central institutional review board (cIRB) and maintains voluntary partnerships with OPOs and histocompatibility laboratories. A Community Advisory Council composed of African American individuals with a personal or family history of kidney disease has advised the NIH Project Office and Steering Committee since inception. UNOS is providing data for outcome analyses.ConclusionThis article describes unique aspects of the protocol, design, and performance of APOLLO. Results will guide use of APOL1 genotypic data to improve the assessment of quality in deceased-donor kidneys and could increase numbers of transplanted kidneys, reduce rates of discard, and improve the safety of living-kidney donation.

Published

2020

5. Molecular Dynamic Simulation Reveals Structure Differences in APOL1 Variants and Implication in Pathogenesis of Chronic Kidney Disease.

Author

Mayanja, Richard, Kintu, Christopher, Diabate, Oudou, Soremekun, Opeyemi, Oluwagbemi, Olugbenga Oluseun, Wele, Mamadou, Kalyesubula, Robert, Jjingo, Daudi, Chikowore, Tinashe, and Fatumo, Segun

Subjects

*CHRONIC kidney failure, *DYNAMIC simulation, *MOLECULAR dynamics, *ALLOSTERIC proteins, *DISEASE risk factors, *OCCLUSION (Chemistry)

Abstract

Background: According to observational studies, two polymorphisms in the apolipoprotein L1 (APOL1) gene have been linked to an increased risk of chronic kidney disease (CKD) in Africans. One polymorphism involves the substitution of two amino-acid residues (S342G and I384M; known as G1), while the other involves the deletion of two amino-acid residues in a row (N388 and Y389; termed G2). Despite the strong link between APOL1 polymorphisms and kidney disease, the molecular mechanisms via which these APOL1 mutations influence the onset and progression of CKD remain unknown. Methods: To predict the active site and allosteric site on the APOL1 protein, we used the Computed Atlas of Surface Topography of Proteins (CASTp) and the Protein Allosteric Sites Server (PASSer). Using an extended molecular dynamics simulation, we investigated the characteristic structural perturbations in the 3D structures of APOL1 variants. Results: According to CASTp's active site characterization, the topmost predicted site had a surface area of 964.892 Å2 and a pocket volume of 900.792 Å3. For the top three allosteric pockets, the allostery probability was 52.44%, 46.30%, and 38.50%, respectively. The systems reached equilibrium in about 125 ns. From 0–100 ns, there was also significant structural instability. When compared to G1 and G2, the wildtype protein (G0) had overall high stability throughout the simulation. The root-mean-square fluctuation (RMSF) of wildtype and variant protein backbone Cα fluctuations revealed that the Cα of the variants had a large structural fluctuation when compared to the wildtype. Conclusion: Using a combination of different computational techniques, we identified binding sites within the APOL1 protein that could be an attractive site for potential inhibitors of APOL1. Furthermore, the G1 and G2 mutations reduced the structural stability of APOL1. [ABSTRACT FROM AUTHOR]

Published

2022

6. Association Between APOL1 Genotype and Kidney Diseases and Annual Kidney Function Change: A Systematic Review and Meta-Analysis of the Prospective Studies

Author

Jagannathan R, Rajagopalan K, Hogan J, Hart A, Newell KA, Pastan SO, and Patzer RE

Subjects

apol1, chronic kidney disease, end-stage renal diseases, disparities, african americans, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Ram Jagannathan,1 Kanya Rajagopalan,2 Julien Hogan,3,4 Allyson Hart,5,6 Kenneth A Newell,4 Stephen O Pastan,7 Rachel E Patzer4,7,8 1Department of Medicine, Division of Hospital Medicine, Emory University School of Medicine, Atlanta, GA, USA; 2Department of Global Health, Rollins School of Public Health, Emory University, Atlanta, GA, USA; 3Pediatric Nephrology Department, Robert Debre University Hospital, Paris, 75019, France; 4Department of Surgery, Division of Transplantation, Emory University School of Medicine, Atlanta, GA, USA; 5Division of Nephrology, Department of Medicine, Hennepin Healthcare, Minneapolis, MN, USA; 6University of Minnesota Medical School, Minneapolis, MN, USA; 7Department of Medicine, Emory University School of Medicine, Atlanta, GA, USA; 8Department of Epidemiology, Rollins School of Public Health, Emory University, Atlanta, GA, USACorrespondence: Ram JagannathanDepartment of Medicine, Division of Hospital Medicine, Emory University School of Medicine, Atlanta, GA, 30322, USAEmail ram.jagannathan@emory.eduBackground: Two coding risk variants in the Apo L1 gene (APOL1) underlie most of the excess risk for kidney diseases in recent African ancestry patients. Strength and consistency of the relationship between APOL1 high-risk genotypes and the risk of chronic kidney diseases (CKD) and end-stage renal disease (ESRD) are not uniform.Objective: To conduct a systematic review and meta-analysis of prospective studies assessing the association of APOL1 genotypes and the risk of developing CKD, ESRD, and CKD to ESRD in adults.Methods: Systematic search of MEDLINE, EMBASE, and Google Scholar was performed for prospective studies assessing the associations between APOL1 genotypes and CKD, ESRD, and progression from CKD to ESRD. Secondary analyses were to evaluate the annual kidney function change by APOL1 gene status. Random effects models were used to estimate pooled risk ratios (RRs) and weighted mean differences for outcomes of interest.Results: The search yield 10 prospective during a follow-up period ranging from 4.4 to 25 years. The high-risk APOL1 genotype was associated with the incidence of CKD (RR:1.41[95% CI: 1.14– 1.75]), the progression from CKD to ESRD (RR: 1.70[95% CI:1.44; 2.01]) compared with the low-risk APOL1 genotype. There was no appreciable association between high-risk APOL1 genotype with the incidence of ESRD. Furthermore, high-risk APOL1 genotype was associated with a marginal decrement in the annual eGFR decline (− 0.55[95% CI: − 0.94 to − 0.16]) mL/min/1.73m2 compared with low-risk APOL1 genotype status.Conclusion: In summary, African Americans carrying APOL1 high-risk genotypes are at increased risk of developing CKD and ESRD. Given that the APOL1 risk alleles are common among individuals with African ancestry, with ∼ 18% of African Americans carrying high-risk alleles, these findings highlight the potential identification of subgroups of patients who may benefit from APOL1 screening and developing culturally-appropriate interventions.Keywords: APOL1, chronic kidney disease, end-stage renal diseases, disparities, African Americans

Published

2021

7. Distinct APOL1 functions in trypanosomes and kidney podocytes.

Author

Pays, Etienne

Subjects

*KIDNEY diseases, *TRYPANOSOMA brucei, *CHRONIC kidney failure

Abstract

The human serum protein apolipoprotein L1 (APOL1) kills Trypanosoma brucei but not the sleeping sickness agent Trypanosoma rhodesiense. APOL1 C-terminal variants can kill T. rhodesiense but they also induce kidney disease. Given topological and functional differences between intracellular and extracellular APOL1 isoforms, I propose that trypanolysis and kidney disease result from distinct APOL1 activities. [ABSTRACT FROM AUTHOR]

Published

2022

8. Assessment of Barriers to Donation for Potential Black Kidney Donors

Author

Jessica Kearney, Priscilla Smith, Rob Elias, and Kate Bramham

Subjects

Chronic Kidney Disease, Transplantation, Hypertension, Ethnicity, APOL1, Genotype, Diseases of the genitourinary system. Urology, RC870-923

Published

2021

9. A focus on the association of Apol1 with kidney disease in children.

Author

Ekulu, Pepe M., Nkoy, Agathe B., Adebayo, Oyindamola C., Kazadi, Orly K., Aloni, Michel N., Arcolino, Fanny O., Ngiyulu, Rene M., Gini, Jean-Lambert E., Lepira, François B., Van den Heuvel, Lamberthus P., and Levtchenko, Elena N.

Subjects

*HYPERTENSION risk factors, *KIDNEY disease risk factors, *CHRONIC kidney failure, *GENETICS, *HEALTH services accessibility, *HEALTH status indicators, *METABOLISM, *RACE, *APOLIPOPROTEINS, *IMMUNITY, *ALBUMINURIA, *DISEASE risk factors, *CHILDREN

Abstract

Individuals of African origin have an increased risk of developing various progressive chronic kidney diseases (CKD). This risk has been attributed to genetic variants (G1, G2) in apolipoprotein-L1 (APOL1) gene. In the pediatric population, especially in children affected by sickle cell disease (SCD), by human immunodeficiency virus (HIV), or with various glomerular diseases, APOL1 risk variants have been associated with the development of hypertension, albuminuria, and more rapid decline of kidney function. The present review focuses on existing APOL1-related epidemiological data in children with CKD. It also includes data from studies addressing racial disparities in CKD, the APOL1-related innate immunity, and the relationship between APOL1 and CKD and pathogenic pathways mediating APOL1-related kidney injury. [ABSTRACT FROM AUTHOR]

Published

2021

10. Race, APOL1 Risk Variants, and Clinical Outcomes among Older Adults: The ARIC Study.

Author

Chen, Teresa K., Coresh, Josef, Daya, Natalie, Ballew, Shoshana H., Tin, Adrienne, Crews, Deidra C., and Grams, Morgan E.

Subjects

*KIDNEY disease risk factors, *ALBUMINURIA, *CHRONIC kidney failure, *CONFIDENCE intervals, *CREATININE, *GLOMERULAR filtration rate, *HOSPITAL care, *KIDNEY diseases, *LONGITUDINAL method, *SCIENTIFIC observation, *RACE, *RISK assessment, *GENOTYPES, *OLD age

Abstract

BACKGROUND/OBJECTIVES: APOL1 high‐risk genotypes confer an increased risk for kidney disease, but their clinical significance among older adults remains unclear. We aimed to determine whether APOL1 genotype status (high risk = 2 risk alleles; low risk = 0–1 risk alleles) and self‐reported race (Black; White) are associated with number of hospitalizations, incident chronic kidney disease (CKD), end‐stage renal disease (ESRD), and mortality among older adults participating in a community‐based cohort study. DESIGN: Observational longitudinal cohort study. SETTING: The Atherosclerosis Risk in Communities (ARIC) study. PARTICIPANTS: Community‐dwelling older adults (mean age = 75.8 years; range = 66–90 years). RESULTS: Among 5,564 ARIC participants (78.2% White, 19.1% APOL1 low‐risk Black, and 2.7% APOL1 high‐risk Black), the proportion with creatinine and cystatin C–based estimated glomerular filtration rate (eGFRCrCys) below 60 mL/min/1.73 m2 at baseline was 40.6%, 34.8%, and 43.2%, respectively. Over a mean follow‐up of 5.1 years, APOL1 high‐risk Blacks had a 2.67‐fold higher risk for ESRD compared with low‐risk Blacks (95% confidence interval [CI] = 1.05–6.79) in models adjusted for age and sex. This association was no longer significant upon further adjustment for baseline eGFRCrCys and albuminuria (hazard ratio [HR] = 1.08; 95% CI =.39–2.96). Rate of hospitalizations and risks of mortality and incident CKD did not differ significantly by APOL1 genotype status. Compared with Whites, Blacks had 1.85‐fold and 3.45‐fold higher risks for incident CKD and ESRD, respectively, in models adjusted for age, sex, eGFRCrCys, and albuminuria. These associations persisted after additional adjustments for clinical/socioeconomic factors and APOL1 genotype (incident CKD: HR = 1.38; 95% CI = 1.06–1.81; ESRD: HR = 3.20; 95% CI = 1.16–8.86). CONCLUSION: Among older Black adults, APOL1 high‐risk genotypes were associated with lower kidney function and therefore higher risk of ESRD. Racial disparities in incident kidney disease persisted in older age and were not fully explained by APOL1. [ABSTRACT FROM AUTHOR]

Published

2021

11. Genome‐wide association study for time to failure of kidney transplants from African American deceased donors.

Author

Divers, Jasmin, Ma, Lijun, Brown, William Mark, Palmer, Nicholette D., Choi, Young, Israni, Ajay K., Pastan, Stephen O., Julian, Bruce A., Gaston, Robert S., Hicks, Pamela J., Reeves‐Daniel, Amber M., and Freedman, Barry I.

Subjects

*KIDNEY transplantation, *KIDNEY failure, *AFRICAN Americans, *SINGLE nucleotide polymorphisms, *DIABETIC nephropathies

Abstract

Two renal‐risk variants in the apolipoprotein L1 gene (APOL1) in African American (AA) deceased donors (DD) are associated with shorter renal allograft survival after transplantation. To identify additional genes contributing to allograft survival, a genome‐wide association study was performed in 532 AA DDs. Phenotypic data were obtained from the Scientific Registry of Transplant Recipients. Association and single‐nucleotide polymorphism (SNP)‐by‐APOL1 interaction tests were conducted using death‐censored renal allograft survival accounting for relevant covariates. Replication and inverse‐variance‐weighted meta‐analysis were performed using data from 250 AA DD in the Genomics of Transplantation study. Accounting for APOL1, multiple SNPs near the Nudix Hydrolase 7 gene (NUDT7) showed strong independent effects (P = 1.6 × 10−8‐2.2 × 10−8). Several SNPs in the Translocation protein SEC63 homolog (SEC63; P = 2 × 10−9‐3.7 × 10−8) and plasmacytoma variant translocation 1 (PVT1) genes (P = 4.0 × 10−8‐7 × 10−8) modified the effect of APOL1 on allograft survival. SEC63 is expressed in human renal tubule cells and glomeruli, and PVT1 is associated with diabetic kidney disease. Overall, associations were detected for 41 SNPs (P = 2 × 10−9‐5 × 10−8) contributing independently or interacting with APOL1 to impact renal allograft survival after transplantation from AA DD. Given the small sample size of the discovery and replication sets, independent validations and functional genomic efforts are needed to validate these results. [ABSTRACT FROM AUTHOR]

Published

2020

12. Kidney disease and electrolytes in COVID-19: more than meets the eye.

Author

Carriazo, Sol, Kanbay, Mehmet, and Ortiz, Alberto

Subjects

*INAPPROPRIATE ADH syndrome, *COVID-19, *COVID-19 pandemic, *KIDNEY diseases, *CHRONIC kidney failure, *ACUTE kidney failure, *MYOCARDIAL reperfusion

Abstract

COVID-19 is a global pandemic fuelled in some countries by government actions. The current issue of Clinical Kidney Journal presents 15 articles on COVID-19 and kidney disease from three continents, providing a global perspective of the impact of severe acute respiratory syndrome coronavirus 2 on electrolytes and different kidney compartments (glomeruli, tubules and vascular compartments) and presenting clinically as a syndrome of inappropriate antidiuretic hormone secretion, acute kidney injury, acute kidney disease, collapsing glomerulopathy and thrombotic microangiopathy, among others, in the context of a brand-new cardiorenal syndrome. Kidney injury may need acute dialysis that may overwhelm haemodialysis (HD) and haemofiltration capabilities. In this regard, acute peritoneal dialysis (PD) may be lifesaving. Additionally, pre-existent chronic kidney disease increases the risk of more severe COVID-19 complications. The impact of COVID-19 on PD and HD patients is also discussed, with emphasis on preventive measures. Finally, current therapeutic approaches and potential future therapeutic approaches undergoing clinical trials, such as complement targeting by eculizumab, are also presented. [ABSTRACT FROM AUTHOR]

Published

2020

13. APOL1 Renal-Risk Variants Do Not Associate With Incident Cardiovascular Disease or Mortality in the Systolic Blood Pressure Intervention Trial

Author

Barry I. Freedman, Michael V. Rocco, Jeffrey T. Bates, Michel Chonchol, Amret T. Hawfield, James P. Lash, Vasilios Papademetriou, John R. Sedor, Karen Servilla, Paul L. Kimmel, Barry M. Wall, and Nicholas M. Pajewski

Subjects

African Americans, albuminuria, APOL1, cardiovascular disease, chronic kidney disease, SPRINT, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Relationships between apolipoprotein L1 gene (APOL1) renal-risk variants (RRVs) and cardiovascular disease (CVD) remain controversial. To clarify associations between APOL1 and CVD, a total of 2568 African American Systolic Blood Pressure Intervention Trial (SPRINT) participants were assessed for the incidence of CVD events (primary composite including nonfatal myocardial infarction, acute coronary syndrome not resulting in myocardial infarction, nonfatal stroke, nonfatal acute decompensated heart failure, and CVD death), renal outcomes, and all-cause mortality. Methods: Cox proportional hazards regression models were used, adjusting for age, sex, African ancestry proportion, and treatment group (systolic blood pressure target of

Published

2017

14. JC polyoma viruria associates with protection from chronic kidney disease independently from apolipoprotein L1 genotype in African Americans.

Author

Freedman, Barry I, Kistler, Amy L, Skewes-Cox, Peter, Ganem, Don, Spainhour, Mitzie, Turner, Jolyn, Divers, Jasmin, Langefeld, Carl D, Murea, Mariana, and Hicks, Pamela J

Subjects

*CHRONIC kidney failure, *POLYOMAVIRUSES, *DISEASE risk factors, *DISEASES in African Americans, *VIRUS diseases, *POLYMERASE chain reaction, *MESSENGER RNA

Abstract

Background Viral infections can trigger chronic kidney disease (CKD) and the urine virome may inform risk. The Natural History of APOL1 -Associated Nephropathy Study (NHAANS) reported that urine JC polyomavirus (JCPyV) associated with a lower risk of APOL1 -associated nephropathy in African Americans. Herein, association was assessed between urine JCPyV with CKD in African Americans independent from the APOL1 genotype. Methods Quantitative polymerase chain reaction was performed for urinary detection of JCPyV and BK polyoma virus (BKPyV) in 200 newly recruited nondiabetic African Americans. A combined analysis was performed in these individuals plus 300 NHAANS participants. Results In the 200 new participants, urine JCPyV was present in 8.8% of CKD cases and 45.8% of nonnephropathy controls (P = 3.0 × 10−8). In those with APOL1 renal-risk genotypes, JCPyV was detected in 5.1% of cases and 40.0% of controls (P = 0.0002). In those lacking APOL1 renal-risk genotypes, JCPyV was detected in 12.2% of cases and 48.8% of controls (P = 8.5 × 10−5). BKPyV was detected in 1.3% of cases and 0.8% of controls (P  =  0.77). In a combined analysis with 300 NHAANS participants (n = 500), individuals with urine JCPyV had a 63% lower risk of CKD compared with those without urine JCPyV (odds ratio 0.37; P = 4.6 × 10−6). RNA fluorescence in situ hybridization confirmed the presence of JCPyV genomic DNA and JCPyV messenger RNA (mRNA) in nondiseased kidney. Conclusions Inverse relationships exist between JCPyV viruria and non-diabetic CKD. Future studies should determine whether renal inflammation associated with CKD is less permissive for JCPyV reactivation/replication or whether JCPyV is a marker of reduced host immune responsiveness that diminishes immune pathologic contributions to CKD. [ABSTRACT FROM AUTHOR]

Published

2018

15. Apolipoprotein L1 and Chronic Kidney Disease Risk in Young Potential Living Kidney Donors.

Author

Locke, Jayme E., Sawinski, Deirdre, Reed, Rhiannon D., Shelton, Brittany, MacLennan, Paul A., Kumar, Vineeta, Mehta, Shikha, Mannon, Roslyn B., Gaston, Robert, Julian, Bruce A., Carr, John J., Terry, James G., Kilgore, Meredith, Massie, Allan B., Segev, Dorry L., and Lewis, Cora E.

Abstract

Objective: The aim of this study was to develop a novel chronic kidney disease (CKD) risk prediction tool for young potential living kidney donors. Summary of Background Data: Living kidney donor selection practices have evolved from examining individual risk factors to a risk calculator incorporating multiple characteristics. Owing to limited long-term data and lack of genetic information, current risk tools lack precision among young potential living kidney donors, particularly African Americans (AAs). Methods: We identified a cohort of young adults (18–30 years) with no absolute contraindication to kidney donation from the longitudinal cohort study Coronary Artery Risk Development in Young Adults. Risk associations for CKD (estimated glomerular filtration rate <60 mL/min/1.73 m2) were identified and assigned weighted points to calculate risk scores. Results: A total of 3438 healthy adults were identified [mean age 24.8 years; 48.3% AA; median follow-up 24.9 years (interquartile range: 24.5–25.2)]. For 18-year olds, 25-year projected CKD risk varied by ethnicity and sex even without baseline clinical and genetic abnormalities; risk was 0.30% for European American (EA) women, 0.52% for EA men, 0.52% for AA women, 0.90% for AA men. Among 18-year-old AAs with apolipoprotein L1 gene (APOL1) renal-risk variants without baseline abnormalities, 25-year risk significantly increased: 1.46% for women and 2.53% for men; among those with 2 APOL1 renal-risk variants and baseline abnormalities, 25-year risk was higher: 2.53% to 6.23% for women and 4.35% to 10.58% for men. Conclusions: Young AAs were at highest risk for CKD, and APOL1 renal-risk variants drove some of this risk. Understanding the genetic profile of young AA potential living kidney donors in the context of baseline health characteristics may help to inform candidate selection and counseling. [ABSTRACT FROM AUTHOR]

Published

2018

16. A null variant in the apolipoprotein L3 gene is associated with non-diabetic nephropathy.

Author

Skorecki, Karl L., Lee, Jessica H., Langefeld, Carl D., Rosset, Saharon, Tzur, Shay, Wasser, Walter G., Shemer, Revital, Hawkins, Gregory A., Divers, Jasmin, Parekh, Rulan S., Man Li, Sampson, Matthew G., Kretzler, Matthias, Pollak, Martin R., Shah, Shrijal, Blackler, Daniel, Nichols, Brendan, Wilmot, Michael, Alper, Seth L., and Freedman, Barry I.

Subjects

*CHRONIC kidney failure, *APOLIPOPROTEINS, *GENOTYPES, *ALLELES, *DISEASES in African Americans, *GENETICS

Abstract

Background. Inheritance of apolipoprotein L1 gene (APOL1) renal-risk variants in a recessive pattern strongly associates with non-diabetic end-stage kidney disease (ESKD). Further evidence supports risk modifiers in APOL1-associated nephropathy; some studies demonstrate that heterozygotes possess excess risk for ESKD or show earlier age at ESKD, relative to those with zero risk alleles. Nearby loci are also associated with ESKD in non- African Americans. Methods. We assessed the role of the APOL3 null allele rs11089781 on risk of non-diabetic ESKD. Four cohorts containing 2781 ESKD cases and 2474 controls were analyzed. Results. Stratifying by APOL1 risk genotype (recessive) and adjusting for African ancestry identified a significant additive association between rs11089781 and ESKD in each stratum and in a meta-analysis [meta-analysis P = 0.0070; odds ratio (OR) = 1.29]; ORs were consistent across APOL1 risk strata. The biological significance of this association is supported by the finding that the APOL3 gene is co-regulated with APOL1, and that APOL3 protein was able to bind to APOL1 protein. Conclusions. Taken together, the genetic and biological data support the concept that other APOL proteins besides APOL1 may also influence the risk of non-diabetic ESKD. [ABSTRACT FROM AUTHOR]

Published

2018

17. Molecular Dynamic Simulation Reveals Structure Differences in APOL1 Variants and Implication in Pathogenesis of Chronic Kidney Disease

Author

Richard Mayanja, Christopher Kintu, Oudou Diabate, Opeyemi Soremekun, Olugbenga Oluseun Oluwagbemi, Mamadou Wele, Robert Kalyesubula, Daudi Jjingo, Tinashe Chikowore, and Segun Fatumo

Subjects

Genetics, molecular dynamic simulation, molecular docking, chronic kidney disease, APOL1, mutation, Genetics (clinical)

Abstract

Background: According to observational studies, two polymorphisms in the apolipoprotein L1 (APOL1) gene have been linked to an increased risk of chronic kidney disease (CKD) in Africans. One polymorphism involves the substitution of two amino-acid residues (S342G and I384M; known as G1), while the other involves the deletion of two amino-acid residues in a row (N388 and Y389; termed G2). Despite the strong link between APOL1 polymorphisms and kidney disease, the molecular mechanisms via which these APOL1 mutations influence the onset and progression of CKD remain unknown. Methods: To predict the active site and allosteric site on the APOL1 protein, we used the Computed Atlas of Surface Topography of Proteins (CASTp) and the Protein Allosteric Sites Server (PASSer). Using an extended molecular dynamics simulation, we investigated the characteristic structural perturbations in the 3D structures of APOL1 variants. Results: According to CASTp’s active site characterization, the topmost predicted site had a surface area of 964.892 Å2 and a pocket volume of 900.792 Å3. For the top three allosteric pockets, the allostery probability was 52.44%, 46.30%, and 38.50%, respectively. The systems reached equilibrium in about 125 ns. From 0–100 ns, there was also significant structural instability. When compared to G1 and G2, the wildtype protein (G0) had overall high stability throughout the simulation. The root-mean-square fluctuation (RMSF) of wildtype and variant protein backbone Cα fluctuations revealed that the Cα of the variants had a large structural fluctuation when compared to the wildtype. Conclusion: Using a combination of different computational techniques, we identified binding sites within the APOL1 protein that could be an attractive site for potential inhibitors of APOL1. Furthermore, the G1 and G2 mutations reduced the structural stability of APOL1.

Published

2022

18. Association Between APOL1 Genotype and Kidney Diseases and Annual Kidney Function Change: A Systematic Review and Meta-Analysis of the Prospective Studies

Author

Rachel E. Patzer, Kenneth A. Newell, Julien Hogan, Stephen O. Pastan, Allyson Hart, Ram Jagannathan, and Kanya Rajagopalan

Subjects

medicine.medical_specialty, end-stage renal diseases, 030232 urology & nephrology, Renal function, Review, Disease, 030204 cardiovascular system & hematology, urologic and male genital diseases, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Genotype, medicine, APOL1, Prospective cohort study, disparities, African Americans, business.industry, Incidence (epidemiology), Absolute risk reduction, female genital diseases and pregnancy complications, Nephrology, Meta-analysis, Relative risk, business, chronic kidney disease

Abstract

Background Two coding risk variants in the Apo L1 gene (APOL1) underlie most of the excess risk for kidney diseases in recent African ancestry patients. Strength and consistency of the relationship between APOL1 high-risk genotypes and the risk of chronic kidney diseases (CKD) and end-stage renal disease (ESRD) are not uniform. Objective To conduct a systematic review and meta-analysis of prospective studies assessing the association of APOL1 genotypes and the risk of developing CKD, ESRD, and CKD to ESRD in adults. Methods Systematic search of MEDLINE, EMBASE, and Google Scholar was performed for prospective studies assessing the associations between APOL1 genotypes and CKD, ESRD, and progression from CKD to ESRD. Secondary analyses were to evaluate the annual kidney function change by APOL1 gene status. Random effects models were used to estimate pooled risk ratios (RRs) and weighted mean differences for outcomes of interest. Results The search yield 10 prospective during a follow-up period ranging from 4.4 to 25 years. The high-risk APOL1 genotype was associated with the incidence of CKD (RR:1.41[95% CI: 1.14-1.75]), the progression from CKD to ESRD (RR: 1.70[95% CI:1.44; 2.01]) compared with the low-risk APOL1 genotype. There was no appreciable association between high-risk APOL1 genotype with the incidence of ESRD. Furthermore, high-risk APOL1 genotype was associated with a marginal decrement in the annual eGFR decline (-0.55[95% CI: -0.94 to -0.16]) mL/min/1.73m2 compared with low-risk APOL1 genotype status. Conclusion In summary, African Americans carrying APOL1 high-risk genotypes are at increased risk of developing CKD and ESRD. Given that the APOL1 risk alleles are common among individuals with African ancestry, with ~18% of African Americans carrying high-risk alleles, these findings highlight the potential identification of subgroups of patients who may benefit from APOL1 screening and developing culturally-appropriate interventions.

Published

2021

19. The Expanding Role of APOL1 Risk in Chronic Kidney Disease and Cardiovascular Disease.

Author

Estrella, Michelle M. and Parekh, Rulan S.

Abstract

Variants of the APOL1 gene, found primarily in individuals of African descent, are associated with various forms of kidney disease and kidney disease progression. Recent studies evaluating the association of APOL1 with cardiovascular disease have yielded conflicting results, and the potential role in cardiovascular disease remains unclear. In this review, we summarize the observational studies linking the APOL1 risk variants with chronic kidney and cardiovascular disease among persons of African descent. [ABSTRACT FROM AUTHOR]

Published

2017

20. Apolipoprotein L1 Gene Effects on Kidney Transplantation.

Author

Freedman, Barry I., Locke, Jayme E., Reeves-Daniel, Amber M., and Julian, Bruce A.

Abstract

The pathogenesis of many common etiologies of nephropathy has been informed by recent molecular genetic breakthroughs. It now is apparent that the ethnic disparity in the risk for nondiabetic chronic kidney disease between African Americans and European Americans is explained largely by variation in the apolipoprotein L1 gene (APOL1). The presence of two APOL1 renal risk variants markedly increases an individual's risk for kidney disease. In transplantation, kidneys from deceased African Americans with two APOL1 renal risk variants have shorter survival intervals after engraftment, regardless of the ethnicity of the recipient. Precision medicine will transform the clinical practice of nephrology and kidney transplantation, and play an important role in the allocation of kidneys from deceased and living kidney donors with recent African ancestry. This article reviews existing data on APOL1 in deceased-donor and living-donor kidney transplantation. It considers the impact of including APOL1 genotyping in decisions on the allocation and discard of deceased-donor kidneys, as well as the selection of living donors. [ABSTRACT FROM AUTHOR]

Published

2017

21. APOL1 renal risk variants exacerbate podocyte injury by increasing inflammatory stress

Author

Hidefumi Wakashin, Myung K. Shin, Jurgen Heymann, Hila Roshanravan, Avi Z. Rosenberg, Jeffrey B. Kopp, Parnaz Daneshpajouhnejad, and Maarten Hoek

Subjects

Protein isoform, Nephrology, Gene isoform, Genetically modified mouse, medicine.medical_specialty, Apolipoprotein L1, Interleukin-1beta, Kidney Glomerulus, 030232 urology & nephrology, Mice, Transgenic, In Vitro Techniques, 030204 cardiovascular system & hematology, Kidney, lcsh:RC870-923, Nephrectomy, Podocyte, Mice, 03 medical and health sciences, 0302 clinical medicine, Stress, Physiological, Chronic kidney disease, Internal medicine, medicine, Animals, Humans, Protein Isoforms, RNA, Messenger, APOL1, Inflammation, NLRP12, Messenger RNA, biology, business.industry, Podocytes, Intracellular Signaling Peptides and Proteins, lcsh:Diseases of the genitourinary system. Urology, Cell biology, medicine.anatomical_structure, biology.protein, Inflammatory stress, business, Interleukin-1 beta, Research Article

Abstract

Background Apolipoprotein L1, APOL1, is a trypanosome lytic factor present in human and certain other primates. APOL1 gene variants, present in individuals of recent sub-Saharan African descent, increase risk for glomerular disease and associate with the disease progression, but the molecular mechanisms have not been defined. Objectives We focus on the mechanism how APOL1 variant proteins enhance podocyte injury in the stressed kidney. Methods First, we investigated the expression of APOL1 protein isoform and the localization of APOL1 protein in the kidney. Next, we examined the role of APOL1 in the podocyte stress and the inflammatory signaling in the kidney after hemi-nephrectomy. Results We identified a novel RNA variant that lacks a secretory pathway signal sequence and we found that the predicted APOL1-B3 protein isoform was expressed in human podocytes in vivo and by BAC-APOL1 transgenic mice. APOL1-B3-G2 transgenic mice, carrying a renal risk variant, manifested podocyte injury and increased pro-IL-1β mRNA in isolated glomeruli and increased IL-1β production in the remnant kidney after uninephrectomy. APOL1-B3 interacted with NLRP12, a key regulator of Toll-like receptor signaling. Conclusions These results suggest a possible mechanism for podocyte injury by which one of the APOL1 protein isoforms, APOL1-B3 and its renal risk variants, enhances inflammatory signaling.

Published

2020

22. Assessment of Barriers to Donation for Potential Black Kidney Donors

Author

Rob Elias, Priscilla Smith, Kate Bramham, and J. Kearney

Subjects

Transplantation, Kidney, medicine.medical_specialty, Genotype, business.industry, lcsh:Diseases of the genitourinary system. Urology, lcsh:RC870-923, medicine.anatomical_structure, Nephrology, Family medicine, Donation, Chronic Kidney Disease, Hypertension, Research Letter, Ethnicity, medicine, APOL1, business

Published

2021

23. THE APOLIPOPROTEIN L1 GENE AND CARDIOVASCULAR DISEASE.

Author

Robinson, Todd W. and Freedman, Barry I.

Subjects

*APOLIPOPROTEINS, *CARDIOVASCULAR diseases, *KIDNEY diseases, *ATHEROSCLEROSIS, *LIPOPROTEINS

Abstract

Relative to those with European ancestry, African Americans have an excess incidence of nondiabetic chronic kidney disease predominantly due to two coding renal-risk variants in the apolipoprotein L1 gene (APOL1). This APOL1-kidney disease association is independent of systemic hypertension or blood pressure. Recent reports describe extra-renal effects of the APOL1 G1 and G2 renal-risk variants on cardiovascular disease (CVD), subclinical atherosclerosis, lipoprotein particle concentrations, and survival. However, results have been less consistent than those seen in kidney disease, and the observed APOL1 associations with CVD vary from risk to protective. This manuscript reviews the relationships between APOL1 renal-risk variants and CVD, with an emphasis on study-specific factors that may have contributed to disparate observations. It is possible that APOL1 renal- risk variants impact the systemic vasculature, not only the kidneys. As novel therapies for APOL1-associated nephropathy are developed, APOL1 variant protein effects on large blood vessels and risk of CVD will need to be considered. [ABSTRACT FROM AUTHOR]

Published

2016

24. APOL1 Renal Risk Variants Are Associated With Chronic Kidney Disease in Children and Youth With Perinatal HIV Infection.

Author

Purswani, Murli U., Patel, Kunjal, Winkler, Cheryl A., Spector, Stephen A., Hazra, Rohan, Seage III, George R., Mofenson, Lynne, Karalius, Brad, Scott, Gwendolyn B., Van Dyke, Russell B., and Kopp, Jeffrey B.

Abstract

APOL1 renal risk alleles are associated with chronic kidney disease (CKD) in adults, with the strongest effect being for HIVassociated nephropathy. Their role in youth with perinatal HIV-1 infection (PHIV) has not been studied. In a nested case-control study of 451 PHIV participants in the Pediatric HIV/AIDS Cohort Study, we found a 3.5-fold increased odds of CKD in those carrying high-risk APOL1 genotypes using a recessive model [95% confidence interval (CI): 1.2 to 10.0]. We report an unadjusted incidence of 1.2 CKD cases/ 100 person-years (95% CI: 0.5 to 2.5) in PHIV youth carrying APOL1 high-risk genotypes, with important implications for sub-Saharan Africa. [ABSTRACT FROM AUTHOR]

Published

2016

25. APOL1 nephropathy risk variants are associated with altered high-density lipoprotein profiles in African Americans.

Author

Gutiérrez, Orlando M., Judd, Suzanne E., Irvin, Marguerite R., Degui Zhi, Limdi, Nita, Palmer, Nicholette D., Rich, Stephen S., Sale, Michèle M., and Freedman, Barry I.

Subjects

*KIDNEY diseases, *KIDNEY disease treatments, *DISEASES in African Americans, *GENE expression, *APOLIPOPROTEINS, *PATIENTS

Abstract

Background. Two independent coding variants in the apolipoprotein L1 gene (APOL1), G1 and G2, strongly associate with nephropathy in African Americans; associations with cardiovascular disease are more controversial. Although APOL1 binds plasma high-density lipoproteins (HDLs), data on APOL1 risk variant associations with HDL subfractions are sparse. Methods. Two APOL1 G1 single nucleotide polymorphisms and the G2 insertion/deletion polymorphism were genotyped in 2010 Reasons for Geographic and Racial Differences in Stroke (REGARDS) Study participants with nuclear magnetic resonance spectroscopy-based lipoprotein subfraction measurements. Linear regression was used to model associations between numbers of APOL1 G1/G2 risk variants and HDL subfractions, adjusting for demographic, clinical and ancestral covariates. Results. Female sex and higher percentage of African ancestry were positively associated with the number of APOL1 G1/G2 risk alleles. In the unadjusted analysis, mean (standard error) small HDL concentrations (μmol/L) for participants with zero, one and two G1/G2 risk alleles were 19.0 (0.2), 19.7 (0.2) and 19.9 (0.4), respectively (P = 0.02). Adjustment for age, sex, diabetes and African ancestry did not change the results but strengthened the statistical significance (P = 0.004). No significant differences in large or medium HDL, very lowdensity lipoprotein or low-density lipoprotein particle concentrations were observed by APOL1 genotype. Conclusions. Greater numbers of APOL1 G1/G2 risk alleles were associated with higher small HDL particle concentrations in African Americans. These results may suggest novel areas of investigation to uncover reasons for the association between APOL1 risk variants with adverse outcomes in African Americans. [ABSTRACT FROM AUTHOR]

Published

2016

26. APOL1 Long-term Kidney Transplantation Outcomes Network (APOLLO): Design and Rationale

Author

Jonathan S. Bromberg, Darshana Dadhania, Donald W. Bowden, Laurie P Russell, Emilio D. Poggio, Barry I. Freedman, Timothy E. Craven, Madhav C. Menon, Krista L. Lentine, Bruce A. Julian, Jasmin Divers, Roslyn B. Mannon, Sylvia E. Rosas, Afshin Parsa, Nishadi Rajapakse, Nichole Jefferson, Amber Reeves-Daniel, Alessia Fornoni, Ana S. Iltis, Giselle Guerra, Elling Eidbo, Robert J. Stratta, Chi-yuan Hsu, Lijun Ma, Mitzie Spainhour, Michael D. Gautreaux, Daniel C. Brennan, Paul L. Kimmel, Nicholette D. Palmer, Mariella Ortigosa-Goggins, Matthew R. Weir, J. Brian Moore, Sumit Mohan, Carl D. Langefeld, Meyeon Park, Stephen O. Pastan, Patrick O. Gee, Amir A. Alexander, Mona D. Doshi, David K. Klassen, S. Carrie Smith, Deirdre Sawinski, Marva Moxey-Mims, David M. Reboussin, Kelly A. Birdwell, Rasheed Gbadegesin, Brad C. Astor, Kenneth A. Newell, Patrick P. Koty, Gordon Bowen, Jonah Odim, and Barbara Murphy

Subjects

United Network for Organ Sharing, medicine.medical_specialty, graft failure, 030232 urology & nephrology, kidney transplantation, 030204 cardiovascular system & hematology, lcsh:RC870-923, outcomes, 03 medical and health sciences, 0302 clinical medicine, Clinical Research, medicine, Family history, APOL1, Kidney transplantation, African Americans, urogenital system, business.industry, lcsh:Diseases of the genitourinary system. Urology, medicine.disease, Institutional review board, 3. Good health, Histocompatibility, Transplantation, Nephrology, Family medicine, Donation, business, chronic kidney disease, Kidney disease

Abstract

Introduction Much of the higher risk for end-stage kidney disease (ESKD) in African American individuals relates to ancestry-specific variation in the apolipoprotein L1 gene (APOL1). Relative to kidneys from European American deceased-donors, kidneys from African American deceased-donors have shorter allograft survival and African American living-kidney donors more often develop ESKD. The National Institutes of Health (NIH)–sponsored APOL1 Long-term Kidney Transplantation Outcomes Network (APOLLO) is prospectively assessing kidney allograft survival from donors with recent African ancestry based on donor and recipient APOL1 genotypes. Methods APOLLO will evaluate outcomes from 2614 deceased kidney donor-recipient pairs, as well as additional living-kidney donor-recipient pairs and unpaired deceased-donor kidneys. Results The United Network for Organ Sharing (UNOS), Association of Organ Procurement Organizations, American Society of Transplantation, American Society for Histocompatibility and Immunogenetics, and nearly all U.S. kidney transplant programs, organ procurement organizations (OPOs), and histocompatibility laboratories are participating in this observational study. APOLLO employs a central institutional review board (cIRB) and maintains voluntary partnerships with OPOs and histocompatibility laboratories. A Community Advisory Council composed of African American individuals with a personal or family history of kidney disease has advised the NIH Project Office and Steering Committee since inception. UNOS is providing data for outcome analyses. Conclusion This article describes unique aspects of the protocol, design, and performance of APOLLO. Results will guide use of APOL1 genotypic data to improve the assessment of quality in deceased-donor kidneys and could increase numbers of transplanted kidneys, reduce rates of discard, and improve the safety of living-kidney donation., Graphical abstract

Published

2019

27. APOL1, Acid Load, and CKD Progression

Author

Loren Lipworth, Thomas G. Stewart, Mindy Pike, Adriana M. Hung, Cassianne Robinson-Cohen, Jennifer Morse, Khaled Abdel-Kader, Patrick Ormsby, Edward D. Siew, and T. Alp Ikizler

Subjects

medicine.medical_specialty, Population, 030232 urology & nephrology, Renal function, 030204 cardiovascular system & hematology, lcsh:RC870-923, Gastroenterology, End stage renal disease, 03 medical and health sciences, 0302 clinical medicine, Clinical Research, dietary acid load, Internal medicine, medicine, APOL1, education, Acidosis, 2. Zero hunger, education.field_of_study, end-stage renal disease, business.industry, Hazard ratio, Metabolic acidosis, lcsh:Diseases of the genitourinary system. Urology, medicine.disease, 3. Good health, Nephrology, Cohort, acidosis, medicine.symptom, business, chronic kidney disease, Kidney disease

Abstract

Introduction High dietary acid load and metabolic acidosis are associated with an accelerated decline in kidney function and may contribute to the observed heterogeneity in end-stage renal disease (ESRD) risk according to APOL1 genotype. Our objective was to examine the associations of metabolic acidosis and dietary acid load with kidney disease progression, according to APOL1 genotype, among individuals with chronic kidney disease (CKD). Methods We studied 1048 African American participants in the Chronic Renal Insufficiency Cohort. Metabolic acidosis was defined as blood levels of serum bicarbonate less than 22 mEq/L, and dietary acid load was quantified by potential renal acid load (PRAL) using data from the Diet Health Questionnaire. APOL1 status was defined as having 2 risk variants, consisting of either possible combination of the G1 and G2 risk alleles. We tested associations of APOL1 and dietary and metabolic acidosis with CKD progression, defined as time to ESRD or 50% decline in eGFR. Results During a median follow-up period of 7 years, 379 participants had an incident CKD progression event (6.4 events per 100 person-years). After full adjustment, among participants with 2 APOL1 variants, the analysis failed to detect an association between metabolic acidosis or dietary acid load and CKD progression (hazard ratio [HR], 1.03; 95% confidence interval [CI], 0.96–1.11 per 1 mEq/L higher serum bicarbonate and an HR, 1.03; 95% CI, 0.92–1.15 per 10 mEq/L higher PRAL). Similar associations were noted among participants without the APOL1 high-risk genotype. Conclusion In a population at high risk of developing ESRD, metabolic acidosis and dietary acid load were not associated with CKD progression., Graphical abstract

Published

2019

28. COVID-19 Pandemic: Is Africa Different?

Author

Shoyab Wadee, Oluwasegun Afolaranmi, Jesutofunmi A. Omiye, Anthony J.O. Were, Elliot Koranteng Tannor, Ebun L. Bamgboye, Mogamat Razeen Davids, Abdou Niang, and Saraladevi Naicker

Subjects

Male, Coronavirus disease 2019 (COVID-19), Population, Pneumonia, Viral, SARS-COV-2 virus, World health, 03 medical and health sciences, 0302 clinical medicine, COVID-19 Testing, Chronic kidney disease, Surveys and Questionnaires, Health care, Case fatality rate, Pandemic, Severity of illness, Opinion Paper, Humans, 030212 general & internal medicine, APOL1, education, Pandemics, Demography, Quality of Health Care, education.field_of_study, Travel, 030505 public health, Cultural Characteristics, business.industry, SARS-CoV-2, Mortality rate, COVID-19, General Medicine, Acute Kidney Injury, COVAN, Geography, Africa, Communicable Disease Control, Female, 0305 other medical science, business

Abstract

COVID-19 has now spread to all the continents of the world with the possible exception of Antarctica. However, Africa appears different when compared with all the other continents. The absence of exponential growth and the low mortality rates contrary to that experienced in other continents, and contrary to the projections for Africa by various agencies, including the World Health Organization (WHO) has been a puzzle to many. Although Africa is the second most populous continent with an estimated 17.2% of the world's population, the continent accounts for only 5% of the total cases and 3% of the mortality. Mortality for the whole of Africa remains at a reported 19,726 as at August 01, 2020. The onset of the pandemic was later, the rate of rise has been slower and the severity of illness and case fatality rates have been lower in comparison to other continents. In addition, contrary to what had been documented in other continents, the occurrence of the renal complications in these patients also appeared to be much lower. This report documents the striking differences between the continents and within the continent of Africa itself and then attempts to explain the reasons for these differences. It is hoped that information presented in this review will help policymakers in the fight to contain the pandemic, particularly within Africa with its resource-constrained health care systems.

Published

2021

29. APOL1 renal risk variants exacerbate podocyte injury by increasing inflammatory stress

Author

Wakashin, Hidefumi, Heymann, Jurgen, Roshanravan, Hila, Daneshpajouhnejad, Parnaz, Rosenberg, Avi, Shin, Myung Kyun, Hoek, Maarten, and Kopp, Jeffrey B.

Published

2020

30. APOL1 Kidney Disease Risk Variants: An Evolving Landscape.

Author

Dummer, Patrick D., Limou, Sophie, Rosenberg, Avi Z., Heymann, Jurgen, Nelson, George, Winkler, Cheryl A., and Kopp, Jeffrey B.

Abstract

Summary Apolipoprotein L1 ( APOL1 ) genetic variants account for much of the excess risk of chronic and end-stage kidney disease, which results in a significant global health disparity for persons of African ancestry. We estimate the lifetime risk of kidney disease in APOL1 dual-risk allele individuals to be at least 15%. Experimental evidence suggests a direct role of APOL1 in pore formation, cellular injury, and programmed cell death in renal injury. The APOL1 BH3 motif, often associated with cell death, is unlikely to play a role in APOL1-induced cytotoxicity because it is not conserved within the APOL family and is dispensable for cell death in vitro. We discuss two models for APOL1 trypanolytic activity: one involving lysosome permeabilization and another involving colloid-osmotic swelling of the cell body, as well as their relevance to human pathophysiology. Experimental evidence from human cell culture models suggests that both mechanisms may be operative. A systems biology approach whereby APOL1-associated perturbations in gene and protein expression in affected individuals are correlated with molecular pathways may be productive to elucidate APOL1 function in vivo. [ABSTRACT FROM AUTHOR]

Published

2015

31. Apolipoprotein L1, income and early kidney damage.

Author

Tamrat, Ruth, Peralta, Carmen A., Tajuddin, Salman M., Evans, Michele K., Zonderman, Alan B., and Crews, Deidra C.

Subjects

APOLIPOPROTEINS, KIDNEY diseases, SOCIOECONOMICS, HEALTH of African Americans, ALBUMINURIA

Abstract

Background: The degree to which genetic or environmental factors are associated with early kidney damage among African Americans (AAs) is unknown. Methods: Among 462 AAs in the Healthy Aging in Neighborhoods of Diversity across the Life Span (HANDLS) study, we examined the cross-sectional association between apolipoprotein L1 (APOL1) risk variants and income with: 1) mildly reduced eGFR (<75 mL/min/1.73 m², creatinine-cystatin C equation) and 2) elevated urine albumin-to-creatinine ratio (ACR) (≥17 in men and ≥25 mg/g in women). High risk APOL1 status was defined by 2 copies of high-risk variants; low risk if 0 or 1 copy. Income groups were dichotomized as < $14,000/year (lowest income group) or = $14,000/year. Logistic regression models were adjusted for age, sex, and % European ancestry. Results: Overall, participants' mean age was 47 years and 16% (n = 73) had high risk APOL1 status. Mean eGFR was 99 mL/min/1.73 m². Mildly reduced eGFR was prevalent among 11% (n = 51). The lowest income group had higher adjusted odds (aOR) of mildly reduced eGFR than the higher income group (aOR 1.8, 95% CI 1.2-2.7). High-risk APOL1 was not significantly associated with reduced eGFR (aOR 1.5, 95% CI 0.9-2.5). Among 301 participants with ACR data, 7% (n = 21) had elevated ACR. Compared to low-risk, persons with high-risk APOL1 had higher odds of elevated ACR (aOR 3.8, 95% CI 2.0-7.3). Income was not significantly associated with elevated ACR (aOR 1.8, 95% CI 0.7-4.5). There were no significant interactions between APOL1 and income. Conclusions: Both genetic and socioeconomic factors may be important determinants of early kidney damage among AAs. [ABSTRACT FROM AUTHOR]

Published

2015

32. A focus on the association of Apol1 with kidney disease in children

Author

Agathe B Nkoy, François B. Lepira, Michel Ntetani Aloni, Elena Levtchenko, René M. Ngiyulu, Orly K Kazadi, Lamberthus P Van den Heuvel, Jean-Lambert E Gini, Fanny Oliveira Arcolino, Pepe M. Ekulu, and Oyindamola C Adebayo

Subjects

Nephrology, medicine.medical_specialty, 030232 urology & nephrology, Renal function, Disease, 030204 cardiovascular system & hematology, Kidney, urologic and male genital diseases, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Chronic kidney disease, Epidemiology, medicine, Genetics, Albuminuria, Humans, Genetic Predisposition to Disease, Renal Insufficiency, Chronic, APOL1, Child, Children, business.industry, Sickle cell disease, Apolipoprotein L1, medicine.disease, female genital diseases and pregnancy complications, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], Increased risk, HIV-associated nephropathy, Pediatrics, Perinatology and Child Health, medicine.symptom, business, Kidney disease

Abstract

Contains fulltext : 231532.pdf (Publisher’s version ) (Closed access) Individuals of African origin have an increased risk of developing various progressive chronic kidney diseases (CKD). This risk has been attributed to genetic variants (G1, G2) in apolipoprotein-L1 (APOL1) gene. In the pediatric population, especially in children affected by sickle cell disease (SCD), by human immunodeficiency virus (HIV), or with various glomerular diseases, APOL1 risk variants have been associated with the development of hypertension, albuminuria, and more rapid decline of kidney function. The present review focuses on existing APOL1-related epidemiological data in children with CKD. It also includes data from studies addressing racial disparities in CKD, the APOL1-related innate immunity, and the relationship between APOL1 and CKD and pathogenic pathways mediating APOL1-related kidney injury.

Published

2021

33. The biology of APOL1 with insights into the association between APOL1 variants and chronic kidney disease.

Author

Madhavan, Sethu and O'Toole, John

Subjects

*KIDNEY diseases, *APOLIPOPROTEIN genetics, *HUMAN genetic variation, *BLOOD proteins, *AFRICANS, *GENEALOGY, *DISEASES

Abstract

Recent studies have identified genetic variants in APOL1 that may contribute to the increased incidence of kidney disease in populations with African ancestry. Here, we review the biology of APOL1 present in the circulation and localized to the kidney as it may contribute to the pathogenesis of APOL1-associated kidney disease. [ABSTRACT FROM AUTHOR]

Published

2014

34. APOL1 Kidney-Risk Variants Induce Mitochondrial Fission

Author

Ann L. Craddock, Lance D. Miller, Lijun Ma, Jasmin Divers, Gregory A. Hawkins, Young A Choi, James A. Snipes, Ashok K. Hemal, Barry I. Freedman, Manish S. Bharadwaj, Mariana Murea, Snezana Petrovic, Pamela J. Hicks, Hannah C. Ainsworth, Carl D. Langefeld, John S. Parks, Moin A. Saleem, Anthony J.A. Molina, Dongmei Cheng, and Jeff W. Chou

Subjects

Kidney Disease, Cell, 030232 urology & nephrology, Renal and urogenital, 030204 cardiovascular system & hematology, Mitochondrion, 03 medical and health sciences, 0302 clinical medicine, Translational Research, Gene expression, medicine, Genetics, 2.1 Biological and endogenous factors, Aetiology, APOL1, Gene knockout, African Americans, business.industry, Prevention, HEK 293 cells, Cell biology, mitochondria, FSGS, medicine.anatomical_structure, mitochondrial fusion, Nephrology, Cell culture, Mitochondrial fission, business, chronic kidney disease, Biotechnology

Abstract

Introduction APOL1 G1 and G2 nephropathy-risk variants cause mitochondrial dysfunction and contribute to kidney disease. Analyses were performed to determine the genetic regulation of APOL1 and elucidate potential mechanisms in APOL1-nephropathy. Methods A global gene expression analysis was performed in human primary renal tubule cell lines derived from 50 African American individuals. Follow-up gene knock out, cell-based rescue, and microscopy experiments were performed. Results APOL1 genotypes did not alter APOL1 expression levels in the global gene expression analysis. Expression quantitative trait locus (eQTL) analysis in polyinosinic-polycytidylic acid (poly IC)–stimulated renal tubule cells revealed that single nucleotide polymorphism (SNP) rs513349 adjacent to BAK1 was a trans eQTL for APOL1 and a cis eQTL for BAK1; APOL1 and BAK1 were co-expressed in cells. BAK1 knockout in a human podocyte cell line resulted in diminished APOL1 protein, supporting a pivotal effect for BAK1 on APOL1 expression. Because BAK1 is involved in mitochondrial dynamics, mitochondrial morphology was examined in primary renal tubule cells and HEK293 Tet-on cells of various APOL1 genotypes. Mitochondria in APOL1 wild-type (G0G0) tubule cells maintained elongated morphology when stimulated by low-dose poly IC, whereas those with G1G1, G2G2, and G1G2 genotypes appeared to fragment. HEK293 Tet-on cells overexpressing APOL1 G0, G1, and G2 were created; G0 cells appeared to promote mitochondrial fusion, whereas G1 and G2 induced mitochondrial fission. The mitochondrial dynamic regulator Mdivi-1 significantly preserved cell viability and mitochondrial cristae structure and reversed mitochondrial fission induced by overexpression of G1 and G2. Conclusion Results suggest the mitochondrial fusion/fission pathway may be a therapeutic target in APOL1-nephropathy., Graphical abstract

Published

2020

35. Kidney disease and electrolytes in COVID-19: more than meets the eye

Author

Sol Carriazo, Alberto Ortiz, and Mehmet Kanbay

Subjects

medicine.medical_specialty, Thrombotic microangiopathy, medicine.medical_treatment, 030232 urology & nephrology, Cardiorenal syndrome, 030204 cardiovascular system & hematology, Peritoneal dialysis, 03 medical and health sciences, 0302 clinical medicine, medicine, APOL1, Intensive care medicine, Editorial Comments, cardiorenal, Kidney, Transplantation, business.industry, Acute kidney injury, SIADH, COVID-19, Eculizumab, medicine.disease, haemodialysis, medicine.anatomical_structure, acute kidney injury, peritoneal dialysis, Nephrology, Syndrome of inappropriate antidiuretic hormone secretion, Fanconi, business, chronic kidney disease, medicine.drug, Kidney disease

Abstract

COVID-19 is a global pandemic fuelled in some countries by government actions. The current issue of Clinical Kidney Journal presents 15 articles on COVID-19 and kidney disease from three continents, providing a global perspective of the impact of severe acute respiratory syndrome coronavirus 2 on electrolytes and different kidney compartments (glomeruli, tubules and vascular compartments) and presenting clinically as a syndrome of inappropriate antidiuretic hormone secretion, acute kidney injury, acute kidney disease, collapsing glomerulopathy and thrombotic microangiopathy, among others, in the context of a brand-new cardiorenal syndrome. Kidney injury may need acute dialysis that may overwhelm haemodialysis (HD) and haemofiltration capabilities. In this regard, acute peritoneal dialysis (PD) may be lifesaving. Additionally, pre-existent chronic kidney disease increases the risk of more severe COVID-19 complications. The impact of COVID-19 on PD and HD patients is also discussed, with emphasis on preventive measures. Finally, current therapeutic approaches and potential future therapeutic approaches undergoing clinical trials, such as complement targeting by eculizumab, are also presented.

Published

2020

36. COVID-19 and the Kidney: Recent Advances and Controversies.

Author

Menez, Steven and Parikh, Chirag R.

Subjects

SARS-CoV-2, KIDNEY diseases, COVID-19

Abstract

Kidney involvement is common in coronavirus disease-2019 (COVID-19), and our understanding of the effects of COVID-19 on short- and long-term kidney outcomes has evolved over the course of the pandemic. Initial key questions centered on the spectrum and degree of acute kidney injury (AKI) in patients hospitalized with severe COVID-19. Investigators worldwide have explored the association between COVID-19-associated AKI and short-term outcomes, including inpatient mortality and disease severity. Even as treatments evolved, vaccinations were developed, and newer viral variants arose, subsets of patients were identified as at continued high risk for major adverse kidney outcomes. In this review, we explore key topics of continued relevance including the following: (1) a comparison of COVID-19-associated AKI with AKI developing in other clinical settings; (2) the ongoing controversy over kidney tropism in the setting of COVID-19 and the potential for competitive binding of the severe acute respiratory syndrome coronavirus 2 virus with angiotensin converting enzyme-2 to prevent viral cell entry; and (3) the identification of high-risk patients for adverse outcomes to inform long-term outpatient management. Patients at particularly high risk for adverse kidney outcomes include those with APOL1 high-risk genotype status. Biomarkers of injury, inflammation, tubular health, and repair measured in both the blood and urine may hold prognostic significance. [ABSTRACT FROM AUTHOR]

Published

2022

37. Genetic variation in APOL1 and MYH9 genes is associated with chronic kidney disease among Nigerians.

Author

Tayo, Bamidele, Kramer, Holly, Salako, Babatunde, Gottesman, Omri, McKenzie, Colin, Ogunniyi, Adesola, Bottinger, Erwin, and Cooper, Richard

Abstract

Purpose: A region of chromosome 22 which includes APOL1 and MYH9 genes was recently identified as a risk locus for non-diabetic forms of kidney disease, including idiopathic and HIV-associated focal segmental glomerular sclerosis and kidney disease clinically attributed to hypertension among African Americans. The purposes of the current study were, therefore, to examine the frequency of these variants and to determine whether they are associated with chronic kidney disease (CKD) among native Africans. Methods: To investigate the possible evidence of association between variants in these genes and non-diabetic CKD among West Africans, we performed a case/control analysis in a sample of 166 Nigerians without history of European admixture. Our study included a total of 9 variants on APOL1 ( n = 4) and MYH9 ( n = 5) genes. Results: We observed significantly strong associations with previously reported APOL1 variants rs73885319 and rs60910145, and their two-allele 'G1' haplotype ( P < 0.005). We did not observe significant evidence of association between non-diabetic CKD and any of the MYH9 variants or haplotypes after accounting for multiple testing in our sample. Conclusions: In conclusion, APOL1 risk variants are associated with non-diabetic forms of CKD among Nigerians of Yoruba ethnicity. Further information on APOL1/MYH9 variants may lead to screening programs, which could lead to earlier detection and interventions for non-diabetic kidney disease. [ABSTRACT FROM AUTHOR]

Published

2013

38. Target Organ Damage in African American Hypertension: Role of APOL1.

Author

Freedman, Barry and Murea, Mariana

Abstract

Apolipoprotein L1 ( APOL1) gene association studies and results of the African American Study of Kidney Disease and Hypertension are disproving the longstanding concept that mild to moderate essential hypertension contributes substantially to end-stage renal disease susceptibility in African Americans. APOL1 coding variants underlie a spectrum of kidney diseases, including that attributed to hypertension (labeled arteriolar or hypertensive nephrosclerosis), focal segmental glomerulosclerosis, and HIV-associated nephropathy. APOL1 nephropathy risk variants persist because of protection afforded from the parasite that causes African sleeping sickness. This breakthrough will lead to novel treatments for hypertensive African Americans with low-level proteinuria, for whom effective therapies are lacking. Furthermore, APOL1 nephropathy risk variants contribute to racially variable allograft survival rates after kidney transplantation and assist in detecting nondiabetic forms of nephropathy in African Americans with diabetes. Discovery of APOL1-associated nephropathy was a major success of the genetics revolution, demonstrating that secondary hypertension is typically present in nondiabetic African Americans with nephropathy. [ABSTRACT FROM AUTHOR]

Published

2012

39. APOL1 Renal-Risk Variants Do Not Associate With Incident Cardiovascular Disease or Mortality in the Systolic Blood Pressure Intervention Trial

Author

Vasilios Papademetriou, Paul L. Kimmel, Jeffrey T. Bates, Barry M. Wall, James P. Lash, Karen Servilla, Amret T. Hawfield, Barry I. Freedman, Nicholas M. Pajewski, John R. Sedor, Michael V. Rocco, and Michel Chonchol

Subjects

Acute coronary syndrome, medicine.medical_specialty, Acute decompensated heart failure, 030232 urology & nephrology, Renal function, 030204 cardiovascular system & hematology, lcsh:RC870-923, albuminuria, 03 medical and health sciences, 0302 clinical medicine, Clinical Research, cardiovascular disease, Internal medicine, Genetic model, Medicine, Myocardial infarction, APOL1, African Americans, business.industry, SPRINT, Hazard ratio, lcsh:Diseases of the genitourinary system. Urology, medicine.disease, 3. Good health, Blood pressure, Nephrology, Albuminuria, Cardiology, medicine.symptom, business, chronic kidney disease

Abstract

Introduction Relationships between apolipoprotein L1 gene (APOL1) renal-risk variants (RRVs) and cardiovascular disease (CVD) remain controversial. To clarify associations between APOL1 and CVD, a total of 2568 African American Systolic Blood Pressure Intervention Trial (SPRINT) participants were assessed for the incidence of CVD events (primary composite including nonfatal myocardial infarction, acute coronary syndrome not resulting in myocardial infarction, nonfatal stroke, nonfatal acute decompensated heart failure, and CVD death), renal outcomes, and all-cause mortality. Methods Cox proportional hazards regression models were used, adjusting for age, sex, African ancestry proportion, and treatment group (systolic blood pressure target of

Published

2017

40. Frequency of ClinVar Pathogenic Variants in Chronic Kidney Disease Patients Surveyed for Return of Research Results at a Cleveland Public Hospital

Author

Dana C, Crawford, John, Lin, Jessica N, Cooke Bailey, Tyler, Kinzy, John R, Sedor, John F, O'Toole, and William S, Bush

Subjects

Adult, Male, African Americans, Genotype, Population Health, Hospitals, Public, Computational Biology, Genetic Variation, ClinVar, Apolipoprotein L1, Polymorphism, Single Nucleotide, Article, Pharmacogenomic Testing, return of results, Black or African American, electronic health records, Gene Frequency, Humans, Female, Genetic Predisposition to Disease, Renal Insufficiency, Chronic, APOL1, Alleles, chronic kidney disease

Abstract

Return of results is not common in research settings as standards are not yet in place for what to return, how to return, and to whom. As a pioneer of large-scale of return of research results, the Precision Medicine Initiative Cohort now known of All of Us plans to return pharmacogenomic results and variants of clinical significance to its participants starting late 2019. To better understand the local landscape of possibilities regarding return of research results, we assessed the frequency of pathogenic variants and APOL1 renal risk variants in a small diverse cohort of chronic kidney disease patients (CKD) ascertained from a public hospital in Cleveland, Ohio genotyped on the Illumina Infinium MegaEX. Of the 23,720 ClinVar-designated variants directly assayed by the MegaEX, 8,355 (35%) had at least one alternate allele in the 130 participants genotyped. Of these, 18 ClinVar variants deemed pathogenic by multiple submitters with no conflicts in interpretation were distributed across 27 participants. The majority of these pathogenic ClinVar variants (14/18) were associated with autosomal recessive disorders. Of note were four African American carriers of TTR rs76992529 associated with amyloidogenic transthyretin amyloidosis, otherwise known as familial transthyretin amyloidosis (FTA). FTA, an autosomal dominant disorder with variable penetrance, is more common among African-descent populations compared with European-descent populations. Also common in this CKD population were APOL1 renal risk alleles G1 (rs73885319) and G2 (rs71785313) with 60% of the study population carrying at least one renal risk allele. Both pathogenic ClinVar variants and APOL1 renal risk alleles were distributed among participants who wanted actionable genetic results returned, wanted genetic results returned regardless of actionability, and wanted no results returned. Results from this local genetic study highlight challenges in which variants to report, how to interpret them, and the participant’s potential for follow-up, only some of the challenges in return of research results likely facing larger studies such as All of Us.

Published

2019

41. Sequencing rare and common APOL1 coding variants to determine kidney disease risk

Author

Ping An, Colm O'hUigin, Jeffrey B. Kopp, Laurence Lecordier, Taras K. Oleksyk, George W. Nelson, Victor A. David, Cheryl A. Winkler, Elizabeth A. Binns-Roemer, Sophie Limou, Wilfried Guiblet, and Etienne Pays

Subjects

Male, Trypanosoma brucei rhodesiense, Apolipoprotein L1, Biopsy, Trypanosoma brucei gambiense, Bioinformatics, urologic and male genital diseases, Focal segmental glomerulosclerosis, Gene Frequency, Risk Factors, APOL1, Genetics, education.field_of_study, biology, Glomerulosclerosis, Focal Segmental, personalized medicine, Exons, Phenotype, Nephrology, Female, Lipoproteins, HDL, Population, selection, trypanolysis, Polymorphism, Single Nucleotide, Risk Assessment, Article, White People, Nephropathy, Host-Parasite Interactions, medicine, Humans, Genetic Predisposition to Disease, AIDS-Associated Nephropathy, education, Allele frequency, Genotyping, Genetic Association Studies, Haplotype, association, population genetics, Sequence Analysis, DNA, medicine.disease, United States, Black or African American, FSGS, Apolipoproteins, Haplotypes, Case-Control Studies, biology.protein, HIVAN, chronic kidney disease, Kidney disease

Abstract

A third of African Americans with sporadic focal segmental glomerulosclerosis (FSGS) or HIV-associated nephropathy (HIVAN) do not carry APOL1 renal risk genotypes. This raises the possibility that other APOL1 variants may contribute to kidney disease. To address this question, we sequenced all APOL1 exons in 1, 437 Americans of African and European decent, including 464 patients with biopsy-proven FSGS/HIVAN. Testing for association with 33 common and rare variants with FSGS/HIVAN revealed no association independent of strong recessive G1 and G2 effects. Seeking additional variants that might have been under selection by pathogens and could represent candidates for kidney disease risk, we also sequenced an additional 1, 112 individuals representing 53 global populations. Except for G1 and G2, none of the 7 common codon-altering variants showed evidence of selection or could restore lysis against trypanosomes causing human African trypanosomiasis. Thus, only APOL1 G1 and G2 confer renal risk and other common and rare APOL1 missense variants, including the archaic G3 haplotype, do not contribute to sporadic FSGS and HIVAN in the United States population. Hence, in most potential clinical or screening applications, our study suggests that sequencing APOL1 exons is unlikely to bring additional information compared to genotyping only APOL1 G1 and G2 risk alleles.

Published

2015

42. Apolipoprotein L1 gene variants associate with prevalent kidney but not prevalent cardiovascular disease in the Systolic Blood Pressure Intervention Trial

Author

Jasmin Divers, George A. Kaysen, Jackson T. Wright, Nicholas M. Pajewski, Carl D. Langefeld, Barry I. Freedman, Amret T. Hawfield, David M. Reboussin, Michael V. Rocco, Ana C. Ricardo, Dominic S. Raj, Diane E. Bild, John R. Sedor, and Paul L. Kimmel

Subjects

medicine.medical_specialty, Mean arterial pressure, Apolipoprotein L1, Renal function, Article, albuminuria, chemistry.chemical_compound, cardiovascular disease, Internal medicine, medicine, APOL1, African Americans, Creatinine, biology, SPRINT, business.industry, Odds ratio, medicine.disease, Endocrinology, Blood pressure, chemistry, Nephrology, Albuminuria, Cardiology, biology.protein, medicine.symptom, business, chronic kidney disease, Kidney disease

Abstract

Apolipoprotein L1 gene (APOL1) G1 and G2 coding variants are strongly associated with chronic kidney disease (CKD) in African Americans. Here APOL1 association was tested with baseline estimated glomerular filtration rate (eGFR), urine albumin:creatinine ratio (UACR), and prevalent cardiovascular disease (CVD) in 2,571 African Americans from the Systolic Blood Pressure Intervention Trial (SPRINT), a trial assessing effects of systolic blood pressure reduction on renal and CVD outcomes. Logistic regression models that adjusted for potentially important confounders tested for association between APOL1 risk variants and baseline clinical CVD (myocardial infarction, coronary or carotid artery revascularization) and CKD (eGFR under 60 ml/min/1.73m2 and/or UACR over 30 mg/g). African American SPRINT participants were 45.3% female with mean (median) age of 64.3 (63) years, mean arterial pressure 100.7 (100) mmHg, eGFR 76.3 (77.1) ml/min/1.73m2, UACR 49.9 (9.2) mg/g, and 8.2% had clinical CVD. APOL1 (recessive inheritance) was positively associated with CKD (odds ratio 1.37, 95% confidence interval 1.08–1.73) and log UACR estimated slope [β] 0.33) and negatively associated with eGFR (β −3.58), all significant. APOL1 risk variants were not significantly associated with prevalent CVD (1.02, 0.82–1.27). Thus, SPRINT data show that APOL1 risk variants are associated with mild CKD but not prevalent CVD in African American with a UACR under 1000 mg/g.

Published

2015

43. The biology of APOL1 with insights into the association between APOL1 variants and chronic kidney disease

Author

M. Madhavan, Sethu and O’Toole, John F.

Published

2014

44. Apolipoprotein L1 gene variants associate with hypertension-attributed nephropathy and the rate of kidney function decline in African Americans

Author

George W. Nelson, Weijia Zhang, Richard G. Freedman, Paul E. Klotman, Michael S. Lipkowitz, Rulan S. Parekh, Donald W. Bowden, Michael J. Choi, Barry I. Freedman, Mary E. Comeau, Carl D. Langefeld, Brad C. Astor, W. H. Linda Kao, Jeffrey B. Kopp, Cheryl A. Winkler, Sudha K. Iyengar, and Erwin P. Bottinger

Subjects

Male, Time Factors, Hypertension, Renal, Apolipoprotein L1, 030232 urology & nephrology, Blood Pressure, 030204 cardiovascular system & hematology, Kidney, chemistry.chemical_compound, 0302 clinical medicine, Gene Frequency, Risk Factors, APOL1, Nephritis, biology, Molecular Motor Proteins, Middle Aged, 3. Good health, Treatment Outcome, medicine.anatomical_structure, Nephrology, Creatinine, Female, Lipoproteins, HDL, Glomerular Filtration Rate, Adult, medicine.medical_specialty, hypertension, Renal function, human genetics, AASK (African American Study of Kidney Disease and Hypertension), Article, Nephropathy, 03 medical and health sciences, Internal medicine, medicine, Humans, Antihypertensive Agents, Aged, Myosin Heavy Chains, business.industry, Case-control study, Genetic Variation, Odds ratio, medicine.disease, Black or African American, Endocrinology, Apolipoproteins, chemistry, Case-Control Studies, biology.protein, business, chronic kidney disease, Kidney disease

Abstract

Despite intensive antihypertensive therapy there was a high incidence of renal end points in participants of the African American Study of Kidney Disease and Hypertension (AASK) cohort. To better understand this, coding variants in the apolipoprotein L1 ( APOL1 ) and the nonmuscle myosin heavy chain 9 ( MYH9 ) genes were evaluated for an association with hypertension-attributed nephropathy and clinical outcomes in a case–control study. Clinical data and DNA were available for 675 AASK participant cases and 618 African American non-nephropathy control individuals. APOL1 G1 and G2, and MYH9 E1 variants along with 44 ancestry informative markers, were genotyped with allele frequency differences between cases and controls analyzed by logistic regression multivariable models adjusting for ancestry, age, and gender. In recessive models, APOL1 risk variants were significantly associated with kidney disease in all cases compared to controls with an odds ratio of 2.57. In AASK cases with more advanced disease, such as a baseline urine protein to creatinine ratio over 0.6g/g or a serum creatinine over 3mg/dl during follow-up, the association was strengthened with odds ratios of 6.29 and 4.61, respectively. APOL1 risk variants were consistently associated with renal disease progression across medication classes and blood pressure targets. Thus, kidney disease in AASK participants was strongly associated with APOL1 renal risk variants.

Published

2012

45. Genetic variation in APOL1 and MYH9 genes is associated with chronic kidney disease among Nigerians

Author

Omri Gottesman, Colin A. McKenzie, Richard S. Cooper, Babatunde L. Salako, Holly Kramer, Erwin P. Bottinger, Adesola Ogunniyi, and Bamidele O. Tayo

Subjects

Adult, Male, Nephrology, medicine.medical_specialty, Pathology, Apolipoprotein L1, Urology, Black People, Nigeria, Locus (genetics), MYH9, Chronic kidney disease, Internal medicine, Genetic variation, Nephrology - Original Paper, Humans, Medicine, APOL1, Renal Insufficiency, Chronic, Myosin Heavy Chains, biology, business.industry, Molecular Motor Proteins, Nigerians, Haplotype, Genetic Variation, Genetic renal disease, medicine.disease, Apolipoproteins, biology.protein, Female, Lipoproteins, HDL, business, Chromosome 22, Kidney disease

Abstract

Purpose A region of chromosome 22 which includes APOL1 and MYH9 genes was recently identified as a risk locus for non-diabetic forms of kidney disease, including idiopathic and HIV-associated focal segmental glomerular sclerosis and kidney disease clinically attributed to hypertension among African Americans. The purposes of the current study were, therefore, to examine the frequency of these variants and to determine whether they are associated with chronic kidney disease (CKD) among native Africans. Methods To investigate the possible evidence of association between variants in these genes and non-diabetic CKD among West Africans, we performed a case/control analysis in a sample of 166 Nigerians without history of European admixture. Our study included a total of 9 variants on APOL1 (n = 4) and MYH9 (n = 5) genes. Results We observed significantly strong associations with previously reported APOL1 variants rs73885319 and rs60910145, and their two-allele “G1” haplotype (P