GJC2 Missense Mutations Cause Human Lymphedema

Overview

Journal Am J Hum Genet

Publisher Cell Press

Specialty Genetics

Date 2010 Jun 12

PMID 20537300

Citations 72

Authors

Robert E Ferrell

Catherine J Baty

Mark A Kimak

Jenny M Karlsson

Elizabeth C Lawrence

Marlise Franke-Snyder

Stephen D Meriney

Eleanor Feingold

David N Finegold

Affiliations

Soon will be listed here.

Abstract

Lymphedema is the clinical manifestation of defects in lymphatic structure or function. Mutations identified in genes regulating lymphatic development result in inherited lymphedema. No mutations have yet been identified in genes mediating lymphatic function that result in inherited lymphedema. Survey microarray studies comparing lymphatic and blood endothelial cells identified expression of several connexins in lymphatic endothelial cells. Additionally, gap junctions are implicated in maintaining lymphatic flow. By sequencing GJA1, GJA4, and GJC2 in a group of families with dominantly inherited lymphedema, we identified six probands with unique missense mutations in GJC2 (encoding connexin [Cx] 47). Two larger families cosegregate lymphedema and GJC2 mutation (LOD score = 6.5). We hypothesize that missense mutations in GJC2 alter gap junction function and disrupt lymphatic flow. Until now, GJC2 mutations were only thought to cause dysmyelination, with primary expression of Cx47 limited to the central nervous system. The identification of GJC2 mutations as a cause of primary lymphedema raises the possibility of novel gap-junction-modifying agents as potential therapy for some forms of lymphedema.

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