a mir-1207-5p binding site polymorphism abolishes regulation of hbegf and is associated with disease severity in cfhr5 nephropathymir - 1207 - 5 - p结合位点多态性破坏hbegf监管和cfhr5肾病与疾病严重程度相关.pdfVIP
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a mir-1207-5p binding site polymorphism abolishes regulation of hbegf and is associated with disease severity in cfhr5 nephropathymir - 1207 - 5 - p结合位点多态性破坏hbegf监管和cfhr5肾病与疾病严重程度相关
A miR-1207-5p Binding Site Polymorphism Abolishes
Regulation of HBEGF and Is Associated with Disease
Severity in CFHR5 Nephropathy
1 1 2 1
Gregory Papagregoriou , Kamil Erguler , Harsh Dweep , Konstantinos Voskarides , Panayiota
1 3 4 2 5 .
Koupepidou , Yiannis Athanasiou , Alkis Pierides , Norbert Gretz , Kyriacos N. Felekkis * ,
1 .
Constantinos Deltas *
1 Molecular Medicine Research Center and Laboratory of Molecular and Medical Genetics, Department of Biological Sciences, University of Cyprus, Nicosia, Cyprus,
2 Medical Research Center, University of Heidelberg, Mannheim, Germany, 3 Department of Nephrology, Nicosia General Hospital, Nicosia, Cyprus, 4 Department of
Nephrology, Hippocrateon Hospital, Nicosia, Cyprus, 5 Department of Life and Health Sciences, University of Nicosia, Nicosia, Cyprus
Abstract
Heparin binding epidermal growth factor (HBEGF) is expressed in podocytes and was shown to play a role in glomerular
physiology. MicroRNA binding sites on the 39UTR of HBEGF were predicted using miRWalk algorithm and followed by
DNA sequencing in 103 patients diagnosed with mild or severe glomerulopathy. A single nucleotide polymorphism,
miRSNP C1936T (rs13385), was identified at the 39UTR of HBEGF that corresponds to the second base of the hsa-miR-
1207-5p seed region. When AB8/13 undifferentiated podocytes were transfected with miRNA mimics of hsa-miR-1207-5p,
the HBEGF protein levels were reduced by about 50%. A DNA fragment containing the miRSNP allele-1936C was cloned
into the pMIR-Report
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