Open AccessFamilial C3 Glomerulopathy Associated with CFHR5 Mutations
Author(s) -
Yiannis Athanasiou,
Konstantinos Voskarides,
Daniel P. Gale,
Loukas Damianou,
Charalambos Patsias,
Michalis Zavros,
Patrick H. Maxwell,
H. Terence Cook,
Panayiota Demosthenous,
Andreas Hadjisavvas,
Kyriacos Kyriacou,
Ioanna Zouvani,
Alkis Pierides,
Constantinos Deltas
Publication year - 2011
Publication title -
clinical journal of the american society of nephrology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.755
H-Index - 151
eISSN - 1555-905X
pISSN - 1555-9041
DOI - 10.2215/cjn.09541010
Subject(s) - medicine , glomerulopathy , proteinuria , nephropathy , renal function , gastroenterology , dialysis , immunology , kidney , endocrinology , diabetes mellitus
Complement factor H and related proteins (CFHR) are key regulators of the alternative complement pathway, where loss of function mutations lead to a glomerulopathy with isolated mesangial C3 deposits without immunoglobulins. Gale et al. (12) reported on 26 patients with the first familial, hematuric glomerulopathy caused by a founder mutation in the CFHR5 gene in patients of Cypriot descent living in the United Kingdom. CFHR5 nephropathy is clinically characterized by continuous microscopic hematuria whereas some patients present with additional episodes of synpharyngitic macrohematuria, associated with infection and pyrexia. A subgroup of patients, particularly men, develop additional proteinuria, hypertension, and chronic renal disease or ESRD.
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