Anomalie cardiovascolari in pazienti con malattia renale policistica autosomica dominante

La malattia autosomica dominante policistica renale (ADPKD) è la malattia genetica più comune in nefrologia. Due geni sono stati implicati nello sviluppo della malattia: PKD1 sul cromosoma 16 (85%) e PKD2 sul cromosoma 4 (15%). La ADPKD è clinicamente caratterizzata da coinvolgimento renale ed extrarenale espresso con la comparsa di manifestazioni cistiche e non cistiche. Dal momento che le complicanze cardiovascolari sono la principale causa di morbilità e mortalità, questa revisione si propone di analizzare il coinvolgimento cardiaco e vascolare in ADPKD. L'ipertensione è uno dei sintomi più frequenti e comune e si verifica in circa il 60% dei pazienti prima della comparsa di disfunzione renale. L'effetto dell'ipertensione sulla progressione verso stadi terminali della malattia renale, rende tale fattore di rischio uno dei più importanti e potenzialmente trattabili in ADPKD. L'ipertrofia ventricolare sinistra, spesso rilevata in questi pazienti, rappresenta un altro importante fattore di rischio indipendente per morbilità e mortalità cardiovascolare nella ADPKD. Altre anomalie come la disfunzione diastolica biventricolare, la disfunzione endoteliale e l'aumento dello spessore intima-media carotideo sono presenti anche in giovani pazienti con ADPKD con normale pressione sanguigna e la funzione renale ben conservata. Gli aneurismi intracranici, quelli extracranici e i difetti valvolari cardiaci sono altre manifestazioni cardiovascolari di comune riscontro nei pazienti con ADPKD. Il trattamento precoce dell'ipertensione mediante l'uso di agenti bloccanti del sistema renina-angiotensina-aldosterone potrebbe svolgere un effetto nefroprotettivo e ridurre l'insorgenza di complicanze cardiovascolari nei pazienti con ADPKD

Slowly progressive anti-neutrophil cytoplasmic antibody-associated renal vasculitis: clinico-pathological characterization and outcome.

BACKGROUND: Although rapidly progressive glomerulonephritis is the main renal phenotype of anti-neutrophil cytoplasmic antibody (ANCA)-associated vasculitis (AAV), slow renal disease progression is sometimes observed. These forms have been rarely discussed; we analysed their prevalence, clinico-pathological characteristics and outcome. METHODS: We screened patients with microscopic  polyangiitis (MPA) and granulomatosis with polyangiitis followed at seven referral centres and selected those with estimated glomerular filtration rate (eGFR) reduction 25% as compared with diagnosis, while 4/34 (12%) had started RRT. CONCLUSIONS: AAV may present with slow renal disease progression; this subset is hallmarked by advanced age at diagnosis, positive MPO-ANCA, subclinical interstitial lung lesions and chronic damage at kidney biopsy. Partial renal recovery may occur following immunosuppression

“Renal tubular acidosis: a diagnostic and therapeutic challenge for the Pediatrician

Not availabl

Changing patterns in clinical-histological presentation and renal outcome over the last five decades in a cohort of 499 patients with lupus nephritis

OBJECTIVES: evaluate changes in demographic, clinical and histological presentation, and prognosis of lupus nephritis (LN) over time. PATIENTS AND METHODS: We studied a multicentre cohort of 499 patients diagnosed with LN from 1970 to 2016. The 46-year follow-up was subdivided into three periods (P): P1 1970-1985, P2 1986-2001 and P3 2002-2016, and patients accordingly grouped based on the year of LN diagnosis. Predictors of patient and renal survival were investigated by univariate and multivariate proportional hazards Cox regression analyses. Survival curves were compared using the log-rank test. RESULTS: A progressive increase in patient age at the time of LN diagnosis (p<0.0001) and a longer time between systemic lupus erythematosus onset and LN occurrence (p<0.0001) was observed from 1970 to 2016. During the same period, the frequency of renal insufficiency at the time of LN presentation progressively decreased (p<0.0001) and that of isolated urinary abnormalities increased (p<0.0001). No changes in histological class and activity index were observed, while chronicity index significantly decreased from 1970 to 2016 (p=0.023). Survival without end-stage renal disease (ESRD) was 87% in P1, 94% in P2% and 99% in P3 at 10 years, 80% in P1 and 90% in P2 at 20 years (p=0.0019). At multivariate analysis, male gender, arterial hypertension, absence of maintenance immunosuppressive therapy, increased serum creatinine, and high activity and chronicity index were independent predictors of ESRD. CONCLUSIONS: Clinical presentation of LN has become less severe in the last years, leading to a better long-term renal survival

An atypical Dent\u2019s disease phenotype caused by co-inheritance of mutations at CLCN5 and OCRL genes

Dent's disease is an X-linked renal tubulopathy caused by mutations mainly affecting the CLCN5 gene. Defects in the OCRL gene, which is usually mutated in patients with Lowe syndrome, have been shown to lead to a Dent-like phenotype called Dent disease 2. However, about 20% of patients with Dent's disease carry no CLCN5/OCRL mutations. The disease's genetic heterogeneity is accompanied by interfamilial and intrafamilial phenotypic heterogeneity. We report on a case of Dent's disease with a very unusual phenotype (dysmorphic features, ocular abnormalities, growth delay, rickets, mild mental retardation) in which a digenic inheritance was discovered. Two different, novel disease-causing mutations were detected, both inherited from the patient's healthy mother, that is a truncating mutation in the CLCN5 gene (A249fs*20) and a donor splice-site alteration in the OCRL gene (c.388+3A>G). The mRNA analysis of the patient's leukocytes revealed an aberrantly spliced OCRL mRNA caused by in-frame exon 6 skipping, leading to a shorter protein, but keeping intact the central inositol 5-phosphatase domain and the C-terminal side of the ASH-RhoGAP domain. Only wild-type mRNA was observed in the mother's leukocytes due to a completely skewed X inactivation. Our results are the first to reveal the effect of an epistatic second modifier in Dent's disease too, which can modulate its expressivity. We surmise that the severe Dent disease 2 phenotype of our patient might be due to an addictive interaction of the mutations at two different genes