Abstract

Cell membranes in general - the erythrocyte membrane in particular - have the very important properties of being both flexible and durable, enabling large, often complex cell distortion without membrane damage. Indeed, the erythrocyte's ability to rapidly - and repetitively - recover its original shape after squeezing through a small capillary vividly demonstrates the intrinsic elasticity and strength of this cell's membrane. Such properties arise in large part from an organized, deformable network of highly conserved cytoskeletal proteins: alpha- and beta- spectrin form long, seemingly flexible crosslinks between short, stiff actin filaments. A compliant, triangulated latticework results. Additional proteins impart further stability to skeletal interactions while linkage of the network to the overlying plasma membrane involves still more membrane proteins. Defects or deficiencies in these proteins lead to hemolytic anemias, of varying severity, but even for normal red cells major unanswered questions persist as to how the components of the erythrocyte membrane skeleton are organized and how this organization changes during deformation. Because the red cell's protein and lipid constituents are ubiquitous among eukaryotic cells, answers to such questions of organization are also very relevant to a host of other structural molecule diseases. Using fluorescence labeling and microscopy to visualize deformation, we began several years ago to quantitatively elucidate the membrane component reorganization that occurs in cell deformation. Complementary, theoretical studies employing very large scale computer simulation have begun to make detailed molecular connections between a thermodynamic structure and observed mechanics. Pursuing these efforts further, we propose to directly measure red cell membrane network stretching, actin filament orientation before/after deformation, and, via thermal fluctutations, elucidate molecular-scale variations and anisotropies within a network under deformation. The study of selected membrane perturbations and pathologies will help reveal the molecular contributions to the mechanics, and, importantly, the mechanical basis of disease. Theoretical work extending to the molecular scale will guide not only the micromanipulation and cell experiments, but will also motivate direct molecular mechanics experiments by Atomic Force Microscopy on engineered spectrin constructs and its complexes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL062352-03
Application #
6390295
Study Section
Hematology Subcommittee 2 (HEM)
Program Officer
Peterson, Charles M
Project Start
1999-05-10
Project End
2003-04-30
Budget Start
2001-05-01
Budget End
2002-04-30
Support Year
3
Fiscal Year
2001
Total Cost
$233,876
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Engineering (All Types)
Type
Schools of Engineering
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Ivanovska, Irena L; Shin, Jae-Won; Swift, Joe et al. (2015) Stem cell mechanobiology: diverse lessons from bone marrow. Trends Cell Biol 25:523-32
Dasbiswas, K; Majkut, S; Discher, D E et al. (2015) Substrate stiffness-modulated registry phase correlations in cardiomyocytes map structural order to coherent beating. Nat Commun 6:6085
Shin, Jae-Won; Discher, Dennis E (2015) Blood and immune cell engineering: Cytoskeletal contractility and nuclear rheology impact cell lineage and localization: Biophysical regulation of hematopoietic differentiation and trafficking. Bioessays 37:633-42
Spinler, Kyle R; Shin, Jae-Won; Lambert, Michele P et al. (2015) Myosin-II repression favors pre/proplatelets but shear activation generates platelets and fails in macrothrombocytopenia. Blood 125:525-33
Sosale, Nisha G; Rouhiparkouhi, Tahereh; Bradshaw, Andrew M et al. (2015) Cell rigidity and shape override CD47's ""self""-signaling in phagocytosis by hyperactivating myosin-II. Blood 125:542-52
Oltra, NĂºria Sancho; Nair, Praful; Discher, Dennis E (2014) From stealthy polymersomes and filomicelles to ""self"" Peptide-nanoparticles for cancer therapy. Annu Rev Chem Biomol Eng 5:281-99
Dingal, P C Dave P; Discher, Dennis E (2014) Systems mechanobiology: tension-inhibited protein turnover is sufficient to physically control gene circuits. Biophys J 107:2734-43
Majkut, Stephanie; Dingal, P C Dave P; Discher, Dennis E (2014) Stress sensitivity and mechanotransduction during heart development. Curr Biol 24:R495-501
Shin, Jae-Won; Buxboim, Amnon; Spinler, Kyle R et al. (2014) Contractile forces sustain and polarize hematopoiesis from stem and progenitor cells. Cell Stem Cell 14:81-93
Buxboim, Amnon; Swift, Joe; Irianto, Jerome et al. (2014) Matrix elasticity regulates lamin-A,C phosphorylation and turnover with feedback to actomyosin. Curr Biol 24:1909-17

Showing the most recent 10 out of 56 publications