Romina Graziotto scite author profile

Mutations in the CLCN5 gene have been detected in DentÕs disease and its phenotypic variants (X-linked recessive nephrolithiasis, X-linked recessive hypophosphatemic rickets, and idiopathic low-molecular-weight proteinuria of Japanese children). DentÕs disease is a tubular disorder characterized by lowmolecular-weight proteinuria, and nephrolithiasis associated with nephrocalcinosis and hypercalciuria. ClC-5 is the first chloride channel for which a definitive role in the trafficking and acidification-dependent recycling of apical membrane proteins has been established. In the course of CLCN5 SSCP analysis in patients with hypercalciuric nephrolithiasis, we detected a novel mutation at intron 2 of the CLCN5 gene, a T-to-G substitution, located 17 bp upstream of the AG acceptor site. To determine the effect of IVS2-17 T>G mutation on the correct splicing of intron 2, we studied ClC-5 transcripts in a patientÕs peripheral blood leukocytes by means of quantitative comparative RT/PCR, and found a new ClC-5 5Õ UTR isoform characterized by the untranslated exon 1b and by retention of intron 1b. This new isoform-isoform B1-was not correlated with mutation since it was detected also in control leukocytes and in renal tissues of kidney donors, thus confirming its physiological role. By RACE analysis we determined the putative transcriptional start site which is located at intron 1a, 251 nt upstream of the first nucleotide of the untranslated exon 1b. ORF analysis revealed that intron 1b retention in isoform B1 stabilizes the initiation of translation to the AGT at position 297 of the ClC-5 cDNA coding region.

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cDNA Cloning and Characterization of PD1: A Novel Human Testicular Protein with Different Expressions in Various Testiculopathies

Graziotto

Foresta

Scannapieco

et al. 1999

Experimental Cell Research

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Perforin, Granzyme B, and Fas Ligand for Molecular Diagnosis of Acute Renal-Allograft Rejection: Analyses on Serial Biopsies Suggest Methodological Issues

Graziotto

Prete

Rigotti

et al. 2006

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Two lytic pathways are activated in biopsies when AR occurs shortly after Tx, whereas the P/GB mechanism prevails if it occurs later on. Only P and FL in biopsies might be able to predict AR diagnosis, but with a considerable variability in each sample, possibly due to the small portion of tissue core, which may be inadequate for molecular diagnosis. CTL expression in PBL does not correlate with histological AR.

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Early activation of fibrogenesis in transplanted kidneys: A study on serial renal biopsies

Prete

Ceol

Anglani

et al. 2009

Experimental and Molecular Pathology

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