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      Sickle cell dehydration: Pathophysiology and therapeutic applications.

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          Abstract

          Cell dehydration is a distinguishing characteristic of sickle cell disease and an important contributor to disease pathophysiology. Due to the unique dependence of Hb S polymerization on cellular Hb S concentration, cell dehydration promotes polymerization and sickling. In double heterozygosis for Hb S and C (SC disease) dehydration is the determining factor in disease pathophysiology. Three major ion transport pathways are involved in sickle cell dehydration: the K-Cl cotransport (KCC), the Gardos channel (KCNN4) and Psickle, the polymerization induced membrane permeability, most likely mediated by the mechano-sensitive ion channel PIEZO1. Each of these pathways exhibit unique characteristics in regulation by oxygen tension, intracellular and extracellular environment, and functional expression in reticulocytes and mature red cells. The unique dependence of K-Cl cotransport on intracellular Mg and the abnormal reduction of erythrocyte Mg content in SS and SC cells had led to clinical studies assessing the effect of oral Mg supplementation. Inhibition of Gardos channel by clotrimazole and senicapoc has led to Phase 1,2,3 trials in patients with sickle cell disease. While none of these studies has resulted in the approval of a novel therapy for SS disease, they have highlighted the key role played by these pathways in disease pathophysiology.

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          Author and article information

          Journal
          Clin Hemorheol Microcirc
          Clinical hemorheology and microcirculation
          IOS Press
          1875-8622
          1386-0291
          2018
          : 68
          : 2-3
          Affiliations
          [1 ] Department of Laboratory Medicine, Boston Children's Hospital, Harvard Medical School, Boston, MA, USA.
          Article
          CH189007
          10.3233/CH-189007
          29614632
          1baf960f-694a-4931-8145-c0680019beb2
          History

          Gardos channel,K-Cl cotransport,KCC,KCNN4,Membrane transport,Piezo-1,deoxygenation,sickling

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