Abstract

Erythrocyte spectrin-actin junctions play a critical role in the maintenance of cell shape andmembrane properties. Their organization and membrane linkage is therefore of fundamentalimportance to erythrocyte physiology. Our recent evidence indicates that dematin performs apivotal function by linking these junctions to the membrane. Here, we propose that dematinperforms its biological function by linking the spectrin-actin junctions to the membrane viaglucose transporter-1 (GLUT1) in human erythrocytes. We will test this hypothesis under thefollowing three aims: A1: GLUT1 interaction with the spectrin-actin junctions in humanerythrocytes. We have identified GLUT1 as the primary membrane receptor for dematin andadducin in human erythrocytes. We propose to identify the interacting domains of GLUT1,dematin, and adducin, and disrupt the GLUT1-cytoskeletal bridge by biochemical means, thusassessing its impact on the membrane stability and shape of human erythrocytes. A2. Dematinand adducin binding receptor(s) in mouse erythrocytes and adipocytes. We propose thatdematin and adducin bind to a novel membrane receptor(s) in mouse erythrocytes. We willidentify this receptor using immunoprecipitation, mass spectrometry, and chemical crosslinkingassays. We will test the binding of dematin and adducin with several potential membraneproteins identified in our proteomics screen of mouse erythrocyte membrane vesicles. We willalso investigate the binding of dematin and adducin with GLUT4, and investigate their functionaleffects on GLUT4 recycling and glucose uptake in adipocytes. These experiments will clarify therole of alternate receptors that link the spectrin-actin junctions in mouse erythrocytes andadipocytes. A3. Physiological implications of complete dematin deficiency. Recently, weobserved an obesity phenotype in the dematin headpiece domain null mice. To elucidate thespecific role of the headpiece domain of dematin, we propose to generate a new mouse modelwith complete dematin deficiency using the conventional gene targeting techniques. We willcompare the anemia and obesity phenotypes in the headpiece and dematin null mice focusingparticularly on the impaired GLUT4 trafficking and diabetes. Together, these studies are likely tounveil a novel function of dematin, adducin, and glucose transporters in the regulation of anemiaand metabolic disorders with broader implications for other headpiece domain-containingproteins.

Public Health Relevance

Erythrocyte membrane has served as a paradigm for discovering the function of its proteins in many non-erythroid cells. This project will investigate the role of dematin, adducin, and glucose transporters in the formation of a novel membrane-cytoskeletal bridge with functional implications in hemolytic anemia, diabetes, and obesity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
7R01HL095050-03
Application #
8183080
Study Section
Erythrocyte and Leukocyte Biology Study Section (ELB)
Program Officer
Qasba, Pankaj
Project Start
2009-08-05
Project End
2013-04-30
Budget Start
2010-12-15
Budget End
2011-04-30
Support Year
3
Fiscal Year
2010
Total Cost
$409,224
Indirect Cost

  Institution

Name
Tufts University
Department
Physiology
Type
Schools of Medicine
DUNS #
039318308
City
Boston
State
MA
Country
United States
Zip Code
02111

  Publications

Nwankwo, Jennifer O; Gremmel, Thomas; Gerrits, Anja J et al. (2017) Calpain-1 regulates platelet function in a humanized mouse model of sickle cell disease. Thromb Res 160:58-65
Lu, Yunzhe; Hanada, Toshihiko; Fujiwara, Yuko et al. (2016) Gene disruption of dematin causes precipitous loss of erythrocyte membrane stability and severe hemolytic anemia. Blood 128:93-103
Nwankwo, Jennifer O; Lei, Jianxun; Xu, Jian et al. (2016) Genetic inactivation of calpain-1 attenuates pain sensitivity in a humanized mouse model of sickle cell disease. Haematologica 101:e397-e400
Baldwin, Michael R; Li, Xuerong; Hanada, Toshihiko et al. (2015) Merozoite surface protein 1 recognition of host glycophorin A mediates malaria parasite invasion of red blood cells. Blood 125:2704-11
Baldwin, Michael; Russo, Crystal; Li, Xuerong et al. (2014) Plasmodium falciparum signal peptide peptidase cleaves malaria heat shock protein 101 (HSP101). Implications for gametocytogenesis. Biochem Biophys Res Commun 450:1427-32
Baldwin, Michael; Yamodo, Innocent; Ranjan, Ravi et al. (2014) Human erythrocyte band 3 functions as a receptor for the sialic acid-independent invasion of Plasmodium falciparum. Role of the RhopH3-MSP1 complex. Biochim Biophys Acta 1843:2855-70
De Franceschi, Lucia; Franco, Robert S; Bertoldi, Mariarita et al. (2013) Pharmacological inhibition of calpain-1 prevents red cell dehydration and reduces Gardos channel activity in a mouse model of sickle cell disease. FASEB J 27:750-9
Kemp, C M; Oliver, W T; Wheeler, T L et al. (2013) The effects of Capn1 gene inactivation on skeletal muscle growth, development, and atrophy, and the compensatory role of other proteolytic systems. J Anim Sci 91:3155-67
Kuchay, S M; Wieschhaus, A J; Marinkovic, M et al. (2012) Targeted gene inactivation reveals a functional role of calpain-1 in platelet spreading. J Thromb Haemost 10:1120-32
Yamada, Kaori H; Kozlowski, Dorothy A; Seidl, Stacey E et al. (2012) Targeted gene inactivation of calpain-1 suppresses cortical degeneration due to traumatic brain injury and neuronal apoptosis induced by oxidative stress. J Biol Chem 287:13182-93

Showing the most recent 10 out of 14 publications