Functional and biophysical analyses of the class XIV Toxoplasma gondii Myosin D

Angelika Herm-Götz; Frêdêric Delbac; Stefan Weiss; Miklos Nyitrai; Rolf Stratmann; Stanislas Tomavo; L. David Sibley; Michael A. Geeves; Dominique Soldati

doi:10.1007/s10974-005-9046-1

Functional and biophysical analyses of the class XIV Toxoplasma gondii Myosin D

Angelika Herm-Götz, Frêdêric Delbac, Stefan Weiss, Miklos Nyitrai, Rolf Stratmann, Stanislas Tomavo, L. David Sibley, Michael A. Geeves, Dominique Soldati

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Abstract

The obligate intracellular parasite Toxoplasma gondii uses gliding motility to migrate across the biological barriers of the host and to invade cells. This unique form of locomotion requires an intact actin cytoskeleton and involves at least one motor protein (TgMyoA) that belongs to the class XIV of the myosin superfamily. TgMyoA is anchored in the inner membrane complex and is essential for the gliding motion, host cell invasion and egress of T. gondii tachyzoites. TgMyoD is the smallest T. gondii myosin and is structurally very closely related to TgMyoA. We show here that TgMyoD exhibits similar transient kinetic properties as the fast single-headed TgMyoA. To determine if TgMyoD also contributes to parasite gliding motility, the TgMyoD gene was disrupted by double homologous recombination. In contrast to TgMyoA, TgMyoD gene is dispensable for tachyzoite propagation and motility. Parasites lacking TgMyoD glide normally and their virulence is not compromised in mice. The fact that TgMyoD is predominantly expressed in bradyzoites explains the absence of a phenotype observed with myodko in tachyzoites and does not exclude a role of this motor in gliding that would be restricted to the cyst forming but nevertheless motile stage of the parasite.

Original language	English
Pages (from-to)	139-151
Number of pages	13
Journal	Journal of Muscle Research and Cell Motility
Volume	27
Issue number	2
DOIs	https://doi.org/10.1007/s10974-005-9046-1
State	Published - Feb 2006

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@article{1363e4c359454d4bac520669af43d88c,

title = "Functional and biophysical analyses of the class XIV Toxoplasma gondii Myosin D",

abstract = "The obligate intracellular parasite Toxoplasma gondii uses gliding motility to migrate across the biological barriers of the host and to invade cells. This unique form of locomotion requires an intact actin cytoskeleton and involves at least one motor protein (TgMyoA) that belongs to the class XIV of the myosin superfamily. TgMyoA is anchored in the inner membrane complex and is essential for the gliding motion, host cell invasion and egress of T. gondii tachyzoites. TgMyoD is the smallest T. gondii myosin and is structurally very closely related to TgMyoA. We show here that TgMyoD exhibits similar transient kinetic properties as the fast single-headed TgMyoA. To determine if TgMyoD also contributes to parasite gliding motility, the TgMyoD gene was disrupted by double homologous recombination. In contrast to TgMyoA, TgMyoD gene is dispensable for tachyzoite propagation and motility. Parasites lacking TgMyoD glide normally and their virulence is not compromised in mice. The fact that TgMyoD is predominantly expressed in bradyzoites explains the absence of a phenotype observed with myodko in tachyzoites and does not exclude a role of this motor in gliding that would be restricted to the cyst forming but nevertheless motile stage of the parasite.",

author = "Angelika Herm-G{\"o}tz and Fr{\^e}d{\^e}ric Delbac and Stefan Weiss and Miklos Nyitrai and Rolf Stratmann and Stanislas Tomavo and Sibley, {L. David} and Geeves, {Michael A.} and Dominique Soldati",

note = "Funding Information: The sequence data (EtMyoD) were produced by BBSRC funded collaboration between the Pathogen Sequencing Unit at the Wellcome Trust Sanger Institute and the Institute for Animal Health and can be obtained from http://www.genedb.org/genedb/ete-nella/. This work was mainly funded by the Deutsche Forschungsgemeinschaft. (DFG grant number SO 366/ 1–1, SO366/1–2) and the Wellcome Trust and Swiss National Fund to DS. AHG is currently supported by BioFuture (BMBF). Dr. F. Delbac was supported by a grant of the von Humboldt fundation. We thank Dr. Meissner for his cooperation.",

year = "2006",

month = feb,

doi = "10.1007/s10974-005-9046-1",

language = "English",

volume = "27",

pages = "139--151",

journal = "Journal of Muscle Research and Cell Motility",

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number = "2",

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T1 - Functional and biophysical analyses of the class XIV Toxoplasma gondii Myosin D

AU - Herm-Götz, Angelika

AU - Delbac, Frêdêric

AU - Weiss, Stefan

AU - Nyitrai, Miklos

AU - Stratmann, Rolf

AU - Tomavo, Stanislas

AU - Sibley, L. David

AU - Geeves, Michael A.

AU - Soldati, Dominique

N1 - Funding Information: The sequence data (EtMyoD) were produced by BBSRC funded collaboration between the Pathogen Sequencing Unit at the Wellcome Trust Sanger Institute and the Institute for Animal Health and can be obtained from http://www.genedb.org/genedb/ete-nella/. This work was mainly funded by the Deutsche Forschungsgemeinschaft. (DFG grant number SO 366/ 1–1, SO366/1–2) and the Wellcome Trust and Swiss National Fund to DS. AHG is currently supported by BioFuture (BMBF). Dr. F. Delbac was supported by a grant of the von Humboldt fundation. We thank Dr. Meissner for his cooperation.

PY - 2006/2

Y1 - 2006/2

N2 - The obligate intracellular parasite Toxoplasma gondii uses gliding motility to migrate across the biological barriers of the host and to invade cells. This unique form of locomotion requires an intact actin cytoskeleton and involves at least one motor protein (TgMyoA) that belongs to the class XIV of the myosin superfamily. TgMyoA is anchored in the inner membrane complex and is essential for the gliding motion, host cell invasion and egress of T. gondii tachyzoites. TgMyoD is the smallest T. gondii myosin and is structurally very closely related to TgMyoA. We show here that TgMyoD exhibits similar transient kinetic properties as the fast single-headed TgMyoA. To determine if TgMyoD also contributes to parasite gliding motility, the TgMyoD gene was disrupted by double homologous recombination. In contrast to TgMyoA, TgMyoD gene is dispensable for tachyzoite propagation and motility. Parasites lacking TgMyoD glide normally and their virulence is not compromised in mice. The fact that TgMyoD is predominantly expressed in bradyzoites explains the absence of a phenotype observed with myodko in tachyzoites and does not exclude a role of this motor in gliding that would be restricted to the cyst forming but nevertheless motile stage of the parasite.

AB - The obligate intracellular parasite Toxoplasma gondii uses gliding motility to migrate across the biological barriers of the host and to invade cells. This unique form of locomotion requires an intact actin cytoskeleton and involves at least one motor protein (TgMyoA) that belongs to the class XIV of the myosin superfamily. TgMyoA is anchored in the inner membrane complex and is essential for the gliding motion, host cell invasion and egress of T. gondii tachyzoites. TgMyoD is the smallest T. gondii myosin and is structurally very closely related to TgMyoA. We show here that TgMyoD exhibits similar transient kinetic properties as the fast single-headed TgMyoA. To determine if TgMyoD also contributes to parasite gliding motility, the TgMyoD gene was disrupted by double homologous recombination. In contrast to TgMyoA, TgMyoD gene is dispensable for tachyzoite propagation and motility. Parasites lacking TgMyoD glide normally and their virulence is not compromised in mice. The fact that TgMyoD is predominantly expressed in bradyzoites explains the absence of a phenotype observed with myodko in tachyzoites and does not exclude a role of this motor in gliding that would be restricted to the cyst forming but nevertheless motile stage of the parasite.

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U2 - 10.1007/s10974-005-9046-1

DO - 10.1007/s10974-005-9046-1

M3 - Article

C2 - 16470333

AN - SCOPUS:33746101814

SN - 0142-4319

VL - 27

SP - 139

EP - 151

JO - Journal of Muscle Research and Cell Motility

JF - Journal of Muscle Research and Cell Motility

IS - 2

ER -

Functional and biophysical analyses of the class XIV Toxoplasma gondii Myosin D

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