BACKGROUND: Focal segmental glomerulosclerosis (FSGS) is a leading cause of steroid-resistant nephrotic syndrome. Hereditary FSGS is frequently caused by mutations in important structural podocyte proteins, including the slit diaphragm-associated transient receptor potential channel C6 (TRPC6). METHODS: In five patients with biopsy-proven autosomal-dominant FSGS from five different Dutch families, all 13 exons of TRPC6 were sequenced. Upon identification of a novel TRPC6 sequence variant, the resultant amino acid change was introduced in the wild-type TRPC6 protein and functionally tested using patch-clamp analyses and cell-surface biotinylation experiments. RESULTS: None of the previously described TRPC6 mutations were found in our cohort. In one family, we identified a novel c.524G>A sequence variant resulting in a p.Arg175Gln (R175Q) substitution in the TRPC6 protein. This sequence variant was absent in 449 control subjects and from public SNP databases. The mutation was located in the third ankyrin repeat domain (ANK3) in the cytoplasmic N-tail of TRPC6, important for protein-protein interaction and regulation of ion channel activity. Patch-clamp analyses of the mutant channel indeed showed an increased TRPC6 channel-mediated current. However, cell-surface expression of the mutant channel was not increased. CONCLUSIONS: We identified a novel TRPC6 p.Arg175Gln gain-of-function mutation that shows increased TRPC6-mediated current, which is not due to altered cell-surface expression. This is the first mutation identified in ANK3 of the TRPC6 N-tail and is most likely responsible for the late-onset autosomal dominant FSGS in this family.
BACKGROUND:Focal segmental glomerulosclerosis (FSGS) is a leading cause of steroid-resistant nephrotic syndrome. Hereditary FSGS is frequently caused by mutations in important structural podocyte proteins, including the slit diaphragm-associated transient receptor potential channel C6 (TRPC6). METHODS: In five patients with biopsy-proven autosomal-dominant FSGS from five different Dutch families, all 13 exons of TRPC6 were sequenced. Upon identification of a novel TRPC6 sequence variant, the resultant amino acid change was introduced in the wild-type TRPC6 protein and functionally tested using patch-clamp analyses and cell-surface biotinylation experiments. RESULTS: None of the previously described TRPC6 mutations were found in our cohort. In one family, we identified a novel c.524G>A sequence variant resulting in a p.Arg175Gln (R175Q) substitution in the TRPC6 protein. This sequence variant was absent in 449 control subjects and from public SNP databases. The mutation was located in the third ankyrin repeat domain (ANK3) in the cytoplasmic N-tail of TRPC6, important for protein-protein interaction and regulation of ion channel activity. Patch-clamp analyses of the mutant channel indeed showed an increased TRPC6 channel-mediated current. However, cell-surface expression of the mutant channel was not increased. CONCLUSIONS: We identified a novel TRPC6p.Arg175Gln gain-of-function mutation that shows increased TRPC6-mediated current, which is not due to altered cell-surface expression. This is the first mutation identified in ANK3 of the TRPC6 N-tail and is most likely responsible for the late-onset autosomal dominant FSGS in this family.
Authors: Brian Leei Lin; Damian Matera; Julia F Doerner; Nan Zheng; Donato Del Camino; Sumita Mishra; Hong Bian; Svetlana Zeveleva; Xiaoguang Zhen; Nathaniel T Blair; Jayhong A Chong; David P Hessler; Djahida Bedja; Guangshuo Zhu; Grace K Muller; Mark J Ranek; Lynn Pantages; Mary McFarland; Matthew R Netherton; Angela Berry; Diane Wong; Georg Rast; Hu Sheng Qian; Steven M Weldon; Jay J Kuo; Achim Sauer; Chris Sarko; Magdalene M Moran; David A Kass; Steven S Pullen Journal: Proc Natl Acad Sci U S A Date: 2019-04-26 Impact factor: 11.205
Authors: Marc Riehle; Anja K Büscher; Björn-Oliver Gohlke; Mario Kaßmann; Maria Kolatsi-Joannou; Jan H Bräsen; Mato Nagel; Jan U Becker; Paul Winyard; Peter F Hoyer; Robert Preissner; Dietmar Krautwurst; Maik Gollasch; Stefanie Weber; Christian Harteneck Journal: J Am Soc Nephrol Date: 2016-02-18 Impact factor: 10.121
Authors: Brianna E Talbot; David H Vandorpe; Brian R Stotter; Seth L Alper; Johannes S Schlondorff Journal: J Biol Chem Date: 2019-07-02 Impact factor: 5.157
Authors: Kasi C McPherson; Corbin A Shields; Bibek Poudel; Ashley C Johnson; Lateia Taylor; Cassandra Stubbs; Alyssa Nichols; Denise C Cornelius; Michael R Garrett; Jan M Williams Journal: Am J Physiol Renal Physiol Date: 2020-02-18
Authors: Cesar P Canales; Paola Krall; Pamela Kairath; Irene C Perez; Miryam A Fragoso; Paulina Carmona-Mora; Phillip Ruiz; Jochen Reiser; Juan I Young; Katherina Walz Journal: Br J Med Med Res Date: 2014-10-30