Membranous nephropathy and lupus-like syndrome after hematopoietic cell transplantation: a case report

<p>Abstract</p> <p>Introduction</p> <p>The kidney is increasingly recognised as a target organ of chronic graft-versus-host disease after hematopoietic cell transplantation in the context of the development of the nephrotic syndrome. Chronic graft-versus-host disease is associated with autoimmune phenomena similar, but not identical, to those observed in various rheumatologic disorders, implicating autoimmunity as an important component of the disease.</p> <p>Case presentation</p> <p>We report the case of a 57-year-old Caucasian man who developed the nephrotic syndrome due to membranous nephropathy in association with recurrent chronic graft-versus-host disease, along with a lupus-like syndrome manifested with pancytopenia, hair loss, positive anti-DNA antibodies and sub-epithelial and mesangial immune deposits. To the best of our knowledge, this is the first case reported in the literature. The nephrotic syndrome subsided soon after he was treated with a short course of cyclosporin with steroids. Unfortunately he died seven months later due to a relapse of leukemia.</p> <p>Conclusions</p> <p>Our case report confirms the notion that chronic graft-versus-host disease is characterized by the appearance of autoimmune phenomena similar, but not identical, to those seen in autoimmune diseases. The decision for more immunosuppression has to be weighed against the need for preservation of the graft versus leukemia phenomenon.</p

A functional variant in NEPH3 gene confers high risk of renal failure in primary hematuric glomerulopathies. Evidence for predisposition to microalbuminuria in the general population.

BACKGROUND: Recent data emphasize that thin basement membrane nephropathy (TBMN) should not be viewed as a form of benign familial hematuria since chronic renal failure (CRF) and even end-stage renal disease (ESRD), is a possible development for a subset of patients on long-term follow-up, through the onset of focal and segmental glomerulosclerosis (FSGS). We hypothesize that genetic modifiers may explain this variability of symptoms. METHODS: We looked in silico for potentially deleterious functional SNPs, using very strict criteria, in all the genes significantly expressed in the slit diaphragm (SD). Two variants were genotyped in a cohort of well-studied adult TBMN patients from 19 Greek-Cypriot families, with a homogeneous genetic background. Patients were categorized as "Severe" or "Mild", based on the presence or not of proteinuria, CRF and ESRD. A larger pooled cohort (HEMATURIA) of 524 patients, including IgA nephropathy patients, was used for verification. Additionally, three large general population cohorts [Framingham Heart Study (FHS), KORAF4 and SAPHIR] were used to investigate if the NEPH3-V353M variant has any renal effect in the general population. RESULTS AND CONCLUSIONS: Genotyping for two high-scored variants in 103 TBMN adult patients with founder mutations who were classified as mildly or severely affected, pointed to an association with variant NEPH3-V353M (filtrin). This promising result prompted testing in the larger pooled cohort (HEMATURIA), indicating an association of the 353M variant with disease severity under the dominant model (p = 3.0x10-3, OR = 6.64 adjusting for gender/age; allelic association: p = 4.2x10-3 adjusting for patients' kinships). Subsequently, genotyping 6,531 subjects of the Framingham Heart Study (FHS) revealed an association of the homozygous 353M/M genotype with microalbuminuria (p = 1.0x10-3). Two further general population cohorts, KORAF4 and SAPHIR confirmed the association, and a meta-analysis of all three cohorts (11,258 individuals) was highly significant (p = 1.3x10-5, OR = 7.46). Functional studies showed that Neph3 homodimerization and Neph3-Nephrin heterodimerization are disturbed by variant 353M. Additionally, 353M was associated with differential activation of the unfolded protein response pathway, when overexpressed in stressed cultured undifferentiated podocyte cells, thus attesting to its functional significance. Genetics and functional studies support a "rare variant-strong effect" role for NEPH3-V353M, by exerting a negative modifier effect on primary glomerular hematuria. Additionally, genetics studies provide evidence for a role in predisposing homozygous subjects of the general population to micro-albuminuria

<i>MYH9</i> rs11089788 statistical analysis for a replicate cohort (D) and for the sum of cohorts B and D, that gave statistical significance.

<p>Patients in cohort D belong to families that segregate microscopic hematuria but no known mutation has been found in any of the genes <i>COL4A3</i>, <i>COL4A4</i>, or <i>CFHR5</i>, so far.</p

Description of cohorts and patients under study.

<p>Please note that cohort B1 is the male only patients with CFHR5 nephropathy.</p><p>MH: Microscopic Hematuria, ESKD: End Stage Kidney Disease, XLAS: X-linked Alport syndrome.</p>1<p>“Mild” patients born before 01/1963. Gender difference (Mild vs Severe) is not significant (p = 0.141).</p>2<p>“Mild” patients born before 01/1975. Gender difference (Mild vs Severe) is significant (p = 0.001).</p>3<p>“Severe” patients: ESKD≤40 yo.</p>4<p>“Mild” patients born before 01/1979. Gender difference (Mild vs Severe) is significant (p = 0.001).</p

Genotype distribution of the studied <i>MYH9</i> variants, by cohort and by severity.

<p>Genotype distribution of the studied <i>MYH9</i> variants, by cohort and by severity.</p

Genotype associations for the three <i>MYH9</i> variants genotyped in this study.

<p>P-values were calculated by Pearson Chi-Square test. The whole CFHR5 cohort (B) was genotyped only for <i>MYH9</i> rs11089788, the only SNP that gave p-value close to 0.1 for the male CFHR5 patients (B1).</p>*<p>P-values calculated by Fisher's Exact Test (2-sided) due to existence of genotypes values less than 10.</p>**<p>Odds ratio (OR) cannot be estimated due to zero genotypic values in the “Severe” category.</p

Validation of the International IgA Nephropathy Prediction Tool in the Greek Registry of IgA Nephropathy

Background: Immunoglobulin A nephropathy (IgAN) is among the commonest glomerulonephritides in Greece and an important cause of end-stage kidney disease (ESKD) with an insidious chronic course. Thus, the recently published International IgAN prediction tool could potentially provide valuable risk stratification and guide the appropriate treatment module. This study aimed to externally validate this prediction tool using a patient cohort from the IgAN registry of the Greek Society of Nephrology.&amp; nbsp;Methods: We validated the predictive performance of the two full models (with or without race) derived from the International IgAN Prediction Tool study in the Greek Society of Nephrology registry of patients with IgAN using external validation of survival prediction models (Royston and Altman). The discrimination and calibration of the models were tested using the C-statistics and stratified analysis, coefficient of determination (RD2) for model fit, and the regression coefficient of the linear predictor (beta(PI)), respectively.&amp; nbsp;Results: The study included 264 patients with a median age of 39 (30-51) years where 65.2% are men. All patients were of Caucasian origin. The 5-year risk of the primary outcome (50% reduction in estimated glomerular filtration rate or ESKD) was 8%. The RD2 for the full models with and without race when applied to our cohort was 39 and 35%, respectively, and both were higher than the reported RD2 for the models applied to the original validation cohorts (26.3, 25.3, and 35.3%, respectively). Harrel’s C statistic for the full model with race was 0.71, and for the model without race was 0.70. Renal survival curves in the subgroups (&lt; 16th, similar to 16 to &lt; 50th, similar to 50 to &lt; 84th, and &gt; 84th percentiles of linear predictor) showed adequate separation. However, the calibration proved not to be acceptable for both the models, and the risk probability was overestimated by the model.&amp; nbsp;Conclusions: The two full models with or without race were shown to accurately distinguish the highest and higher risk patients from patients with low and intermediate risk for disease progression in the Greek registry of IgAN

Flowchart of the genotyping strategy followed to investigate the significance of the two SNPs in four genes that emerged to have functional significance based on the <i>in silico</i> assay (see material and methods).

<p>Black arrow symbolizes the <i>NEPH3</i>-V353M variant which initially derived indicative significant association and was investigated further (black not filled arrows symbolize the meta-analysis). Light grey arrows symbolize the three SNPs found not to be significantly associated in sub-cohort A and not tested further. Dot-lined arrows symbolize the two SNPs that were found to be non-polymorphic in this cohort and not tested further.</p

Co-immunoprecipitation experiments, testing for the binding effectiveness of Neph3 protein with methionine (M) at the 353 position.

<p><b>(A)</b> Left panel: FLAG-Neph3[353<b>V</b>] and FLAG-Neph3[353<b>M</b>] were immuno-precipitated with anti-FLAG antibody and then they were analyzed by western blot using an anti-HA antibody (for HA-Neph3[353<b>V</b>] and HA-Neph3[353<b>M</b>]) in order to check all possible hetero- and homo-dimer interactions. Neph3[353<b>M</b>]-Neph3[353<b>M</b>] homodimers are strongly increased compared with the Neph3[353<b>V</b>]-Neph3[353<b>M</b>] and the Neph3[353<b>V</b>]-Neph3[353<b>V</b>] ones. Right panel: FLAG-Neph3[353<b>V</b>] and FLAG-Neph3[353<b>M</b>] were immuno-precipitated with anti-FLAG antibody and then they were analyzed by western blot using an anti-V5 antibody (for sV5-Nephrin]. Nephrin-Neph3[353<b>M</b>] heterodimers are slightly increased compared with the Nephrin -Neph3[353<b>V</b>] ones. Anti-V5 and anti-FLAG western blots from lysates (input) were used for loading normalization. V5-NPHP1 (nephrocystin) served as an experiment control. <b>(B)</b> Statistics of densitometry of the blots in Fig 3A, n = 3. Intensity (±SEM) is given as a percentage of wild-type intensity, which is set by definition at 1.0 (100%). There is statistical significance (unpaired t-test) for the homodimerization and heterodimerization comparisons described in Fig 3A. For more details see text.</p