| Literature DB >> 26450986 |
Fiona C Brown1, Ashlee J Conway1, Loretta Cerruti1, Janelle E Collinge2, Catriona McLean3, James S Wiley4, Ben T Kile2, Stephen M Jane5, David J Curtis6.
Abstract
We used an N-ethyl-N-nitrosurea-based forward genetic screen in mice to identify new genes and alleles that regulate erythropoiesis. Here, we describe a mouse line expressing an activated form of the K-Cl cotransporter Slc12a4 (Kcc1), which results in a semi-dominant microcytosis of red cells. A missense mutation from methionine to lysine in the cytoplasmic tail of Kcc1 impairs phosphorylation of adjacent threonines required for inhibiting cotransporter activity. We bred Kcc1(M935K) mutant mice with a humanized mouse model of sickle cell disease to directly explore the relevance of the reported increase in KCC activity in disease pathogenesis. We show that a single mutant allele of Kcc1 induces widespread sickling and tissue damage, leading to premature death. This mouse model reveals important new insights into the regulation of K-Cl cotransporters and provides in vivo evidence that increased KCC activity worsened end-organ damage and diminished survival in sickle cell disease.Entities:
Mesh:
Substances:
Year: 2015 PMID: 26450986 DOI: 10.1182/blood-2014-10-609362
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113