Effect of a Single Apolipoprotein L1 Gene Nephropathy Variant on the Risk of Advanced Lupus Nephritis in Brazilians

Vajgel, Gisele; Lima, Salvador Vilar Correia; Santana, Diego Jeronimo S.; Oliveira, Camila Barbosa Lyra de; Costa, Denise Maria Nascimento; Hicks, Pamela J.; Cavalcante, Maria Alina Gomes de Mattos; Langefeld, Carl D.; Valente, Lucila Maria; Crovella, Sérgio; Kirsztajn, Gianna Mastroianni; Freedman, Barry I.; Sandrin-Garcia, Paula

doi:10.3899/jrheum.190684

Cited by 19 publications

(14 citation statements)

References 41 publications

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“…(38) Consistently, progressive nephritis was worsened with every copy of risk allele in Brazilian AA/H lupus patients. (39) In this context, our data implicating a role for APOL1 within T cells involved in adaptive immune responses against a donor organ, demonstrate that previous data regarding R-nAPOL1 and allograft outcomes need to be reinterpreted, and its role in infiltrating inflammatory mononuclear cells in native kidney glomerulonephritis investigated.…”

Section: Discussionmentioning

confidence: 66%

Recipient APOL1 risk alleles associate with death-censored renal allograft survival and rejection episodes

Zhang¹,

Sun²,

Fu³

et al. 2021

Journal of Clinical Investigation

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Apolipoprotein L1 (APOL1) risk-alleles in donor kidneys associate with graft loss but whether recipient risk-allele expression impacts transplant outcomes is unclear. To test whether recipient APOL1 risk-alleles independently correlate with transplant outcomes, we analyzed genome-wide SNP genotyping data of donors and recipients from two kidney transplant cohorts, Genomics of Chronic Allograft Rejection (GOCAR) and Clinical Trials in Organ Transplantation (CTOT1/17). We estimated genetic ancestry (quantified as proportion of African ancestry or pAFR) by ADMIXTURE and correlated APOL1 genotypes and pAFR with outcomes. In the GOCAR discovery set, we observed that the number of recipient APOL1 G1/G2 alleles (R-nAPOL1) associated with increased risk of death-censored allograft loss (DCAL), independent of ancestry (HR = 2.14; P = 0.006), and within the subgroup of African American and Hispanic (AA/H) recipients (HR = 2.36; P = 0.003). R-nAPOL1 also associated with increased risk of any T cell-mediated rejection (TCMR) event. These associations were validated in CTOT1/17. Ex vivo studies of peripheral blood mononuclear cells revealed unanticipated high APOL1 expression in activated CD4 + /CD8 + T cells and natural killer cells. We detected enriched immune response gene pathways in risk-allele carriers vs. noncarriers on the kidney transplant waitlist and among healthy controls. Our findings demonstrate an immunomodulatory role for recipient APOL1 risk-alleles associating with TCMR and DCAL. This finding has broader implications for immune mediated injury to native kidneys.

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Section: Discussionmentioning

confidence: 66%

Recipient APOL1 risk alleles associate with death-censored renal allograft survival and rejection episodes

Zhang¹,

Sun²,

Fu³

et al. 2021

Journal of Clinical Investigation

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“…Similarly, our observation that moderate expression of G0G1 or G0G2 caused cytotoxicity could help explain the elevated risk of APOL1 nephropathy in some carriers of one RRVs relative to carriers of G0G0. 13,14,26 Our results also raise new questions. We observed that tet induced a lower level of G0 protein relative to G2 protein in G0G2-containing HEK293 cells.…”

Section: Disclosuresmentioning

confidence: 75%

Kidney Disease-Associated APOL1 Variants Have Dose-Dependent, Dominant Toxic Gain-of-Function

Datta

Kataria

Zhang

et al. 2020

JASN

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BackgroundTwo coding renal risk variants (RRVs) of the APOL1 gene (G1 and G2) are associated with large increases in CKD rates among populations of recent African descent, but the underlying molecular mechanisms are unknown. Mammalian cell culture models are widely used to study cytotoxicity of RRVs, but results have been contradictory. It remains unclear whether cytotoxicity is RRV-dependent or driven solely by variant-independent overexpression. It is also unknown whether expression of the reference APOL1 allele, the wild-type G0, could prevent cytotoxicity of RRVs.MethodsWe generated tetracycline-inducible APOL1 expression in human embryonic kidney HEK293 cells and examined the effects of increased expression of APOL1 (G0, G1, G2, G0G0, G0G1, or G0G2) on known cytotoxicity phenotypes, including reduced viability, increased swelling, potassium loss, aberrant protein phosphorylation, and dysregulated energy metabolism. Furthermore, whole-genome transcriptome analysis examined deregulated canonical pathways.ResultsAt moderate expression, RRVs but not G0 caused cytotoxicity in a dose-dependent manner that coexpression of G0 did not reduce. RRVs also have dominant effects on canonical pathways relevant for the cellular stress response.ConclusionsIn HEK293 cells, RRVs exhibit a dominant toxic gain-of-function phenotype that worsens with increasing expression. These observations suggest that high steady-state levels of RRVs may underlie cellular injury in APOL1 nephropathy, and that interventions that reduce RRV expression in kidney compartments may mitigate APOL1 nephropathy.

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“…While single polymorphisms may not be sufficient to cause autoimmunity alone, accumulating numbers of risk variants may cause the immune system to become overwhelmed, leading to immune dysregulation [ 24 , 75 ]. Furthermore, interferon signaling upregulation inpatients with LN may trigger nephropathy associated with apolipoprotein L1 ( APOL1 ) risk-alleles (which are prevalent in individuals with Sub-Saharan African ancestry) by upregulating APOL1 mRNA expression and increasing genotype-associated disease severity [ 76 ]. Risk-associated variants in interferon-related genes have also been identified for other autoimmune diseases, including SSc, for which family history remains the strongest known risk factor [ 32 ].…”

Section: The Interferon Pathway and Its Role In Autoimmunity: Systemic Lupus Erythematosus And Beyondmentioning

confidence: 99%

The Pathogenesis, Molecular Mechanisms, and Therapeutic Potential of the Interferon Pathway in Systemic Lupus Erythematosus and Other Autoimmune Diseases

Ramaswamy

Tummala

Streicher

et al. 2021

IJMS

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Therapeutic success in treating patients with systemic lupus erythematosus (SLE) is limited by the multivariate disease etiology, multi-organ presentation, systemic involvement, and complex immunopathogenesis. Agents targeting B-cell differentiation and survival are not efficacious for all patients, indicating a need to target other inflammatory mediators. One such target is the type I interferon pathway. Type I interferons upregulate interferon gene signatures and mediate critical antiviral responses. Dysregulated type I interferon signaling is detectable in many patients with SLE and other autoimmune diseases, and the extent of this dysregulation is associated with disease severity, making type I interferons therapeutically tangible targets. The recent approval of the type I interferon-blocking antibody, anifrolumab, by the US Food and Drug Administration for the treatment of patients with SLE demonstrates the value of targeting this pathway. Nevertheless, the interferon pathway has pleiotropic biology, with multiple cellular targets and signaling components that are incompletely understood. Deconvoluting the complexity of the type I interferon pathway and its intersection with lupus disease pathology will be valuable for further development of targeted SLE therapeutics. This review summarizes the immune mediators of the interferon pathway, its association with disease pathogenesis, and therapeutic modalities targeting the dysregulated interferon pathway.

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Effect of a Single Apolipoprotein L1 Gene Nephropathy Variant on the Risk of Advanced Lupus Nephritis in Brazilians

Cited by 19 publications

References 41 publications

Recipient APOL1 risk alleles associate with death-censored renal allograft survival and rejection episodes

Recipient APOL1 risk alleles associate with death-censored renal allograft survival and rejection episodes

Kidney Disease-Associated APOL1 Variants Have Dose-Dependent, Dominant Toxic Gain-of-Function

The Pathogenesis, Molecular Mechanisms, and Therapeutic Potential of the Interferon Pathway in Systemic Lupus Erythematosus and Other Autoimmune Diseases

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