TY - JOUR
T1 - Membrane-wrapping contributions to malaria parasite invasion of the human erythrocyte
AU - Dasgupta, Sabyasachi
AU - Auth, Thorsten
AU - Gov, Nir S.
AU - Satchwell, Timothy J.
AU - Hanssen, Eric
AU - Zuccala, Elizabeth S.
AU - Riglar, David T.
AU - Toye, Ashley M.
AU - Betz, Timo
AU - Baum, Jake
AU - Gompper, Gerhard
N1 - National Center for Research Resources [5P41RR019664-08]; National Institute of General Medical Sciences from the National Institutes of Health [8 P41 GM103445-08]; NHMRC [APP1047085]; EU [309666]; International Helmholtz Research School of Biophysics and Soft Matter (IHRS BioSoft); Australian Postgraduate Award (APA); Institut Curie; Wellcome Trust [094277, 100993/Z/13/Z]; NHSBT; Wellcome Trust; Agence Nationale de Recherche [JCJC SVSE 5-2011]; Australian Research Council, ARC [FT100100112]X-ray tomography work was supported by grants from the National Center for Research Resources (5P41RR019664-08) and the National Institute of General Medical Sciences (8 P41 GM103445-08) from the National Institutes of Health. Direct funding to support parasitological work was from the NHMRC (Project Grant APP1047085, TB) and, for theoretical work, from the EU FP7 NMP collaborative project PreNanoTox (Project Grant 309666, GG). S.D. acknowledges support by the International Helmholtz Research School of Biophysics and Soft Matter (IHRS BioSoft). E.S.Z. is supported by an Australian Postgraduate Award (APA); N.S.G. thanks the Mayent-Rothschild Visiting Professor Grant at the Institut Curie for funding; T.J.S. is supported by a Wellcome Trust project grant (No. 094277). A.M.T. is supported by an NHSBT R&D grant and the Wellcome Trust; TB. acknowledges support from the Agence Nationale de Recherche (JCJC SVSE 5-2011);J.B. was supported by a Future Fellowship from the Australian Research Council, ARC (FT100100112) and is currently supported by a New Investigator Award from the Wellcome Trust (100993/Z/13/Z). Author contributions: S.D., T.A., N.G., T.J.S., E.H., E.S.Z., D.T.R., A.M.T., T.B., TB., and G.G. worked closely together to design, perform, and interpret experiments; S.D., T.A., N.G., T.B., J.B., and G.G. wrote the paper.
PY - 2014/7/1
Y1 - 2014/7/1
N2 - The blood stage malaria parasite, the merozoite, has a small window of opportunity during which it must successfully target and invade a human erythrocyte. The process of invasion is nonetheless remarkably rapid. To date, mechanistic models of invasion have focused predominantly on the parasite actomyosin motor contribution to the energetics of entry. Here, we have conducted a numerical analysis using dimensions for an archetypal merozoite to predict the respective contributions of the host-parasite interactions to invasion, in particular the role of membrane wrapping. Our theoretical modeling demonstrates that erythrocyte membrane wrapping alone, as a function of merozoite adhesive and shape properties, is sufficient to entirely account for the first key step of the invasion process, that of merozoite reorientation to its apex and tight adhesive linkage between the two cells. Next, parasite-induced reorganization of the erythrocyte cytoskeleton and release of parasite-derived membrane can also account for a considerable energetic portion of actual invasion itself, through membrane wrapping. Thus, contrary to the prevailing dogma, wrapping by the erythrocyte combined with parasite-derived membrane release can markedly reduce the expected contributions of the merozoite actomyosin motor to invasion. We therefore propose that invasion is a balance between parasite and host cell contributions, evolved toward maximal efficient use of biophysical forces between the two cells.
AB - The blood stage malaria parasite, the merozoite, has a small window of opportunity during which it must successfully target and invade a human erythrocyte. The process of invasion is nonetheless remarkably rapid. To date, mechanistic models of invasion have focused predominantly on the parasite actomyosin motor contribution to the energetics of entry. Here, we have conducted a numerical analysis using dimensions for an archetypal merozoite to predict the respective contributions of the host-parasite interactions to invasion, in particular the role of membrane wrapping. Our theoretical modeling demonstrates that erythrocyte membrane wrapping alone, as a function of merozoite adhesive and shape properties, is sufficient to entirely account for the first key step of the invasion process, that of merozoite reorientation to its apex and tight adhesive linkage between the two cells. Next, parasite-induced reorganization of the erythrocyte cytoskeleton and release of parasite-derived membrane can also account for a considerable energetic portion of actual invasion itself, through membrane wrapping. Thus, contrary to the prevailing dogma, wrapping by the erythrocyte combined with parasite-derived membrane release can markedly reduce the expected contributions of the merozoite actomyosin motor to invasion. We therefore propose that invasion is a balance between parasite and host cell contributions, evolved toward maximal efficient use of biophysical forces between the two cells.
UR - http://www.scopus.com/inward/record.url?scp=84904019719&partnerID=8YFLogxK
U2 - 10.1016/j.bpj.2014.05.024
DO - 10.1016/j.bpj.2014.05.024
M3 - مقالة
SN - 0006-3495
VL - 107
SP - 43
EP - 54
JO - Biophysical Journal
JF - Biophysical Journal
IS - 1
ER -