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Actin assembly-inducing protein

April 14, 2024

The Actin assembly-inducing protein (ActA) is a protein encoded and used by Listeria monocytogenes to propel itself through a mammalian host cell. ActA is a bacterial surface protein comprising a membrane-spanning region.[1] In a mammalian cell the bacterial ActA interacts with the Arp2/3 complex and actin monomers to induce actin polymerization on the bacterial surface generating an actin comet tail. The gene encoding ActA is named actA or prtB.[2]

Actin assembly-inducing protein
EVH1 domain-ActA peptide complex
Identifiers
SymbolActA
NCBI gene2798121
UniProtP33379
Search for
StructuresSwiss-model
DomainsInterPro

Introduction edit

As soon as L. monocytogenes bacteria are ingested by humans, they get internalized into intestinal epithelium cells and rapidly try to escape their internalization vacuole.[3][4] In the cytosol they start to polymerize actin on their surface by the help of the ActA protein. It has been shown that ActA is not only necessary but also sufficient to induce motility of bacteria in the absence of other bacterial factors.[5]

Discovery edit

ActA was discovered by analysing lecithinase-negative Tn917-lac Listeria mutants because of the phenotype that they were unable to spread from cell to cell. These mutant bacteria still escaped from the phagosomes as efficiently as wild-type bacteria and multiplied within the infected cells but they were not surrounded by actin like wild-type bacteria. Further analysis showed, that Tn917-lac had inserted into actA, the second gene of an operon. The third gene of this operon, plcB, encodes the L. monocytogenes lecithinase. To determine whether actA itself, plcB or other co-transcribed downstream regions are involved in actin assembly, mutations in the appropriate genes were generated. All mutants except the actA mutants were similar to wild-type concerning association with F-actin and cell-cell spreading. Complementation with actA restored wild-type phenotype in the actA mutants.[1]

Function edit

 
Fig. 1 Actin assembly induced by bacterial protein ActA (shown in green). Mammalian proteins involved in this process are: Profilin (P), Vasodilator-stimulated phosphoprotein (VASP) and actin-related-protein 2 and 3 complex (Arp2/3 complex) as well as actin.

ActA is a protein which acts as a mimic of Wiskott-Aldrich syndrome protein (WASP), a nucleation promoting factor (NPF) present in host cells. NPFs in the mammalian cell recruit and bind to the already existing actin-related-protein 2 and 3 complex (Arp2/3 complex) and induce an activating conformational change of the Arp2/3 complex.[6] Due to this conformational change, NPFs initiate polymerization of a new actin filament at a 70° angle, which leads to the characteristic Y-branched actin structures in the leading edge of motile cells. ActA localizes to the old pole of the bacterium and spans both the bacterial cell membrane and the cell wall, lateral diffusion is inhibited; thus ActA localizes in a polarized and anchored manner on the bacterial surface. Consequently, actin polymerization only starts in this region on the surface of the bacterium.[7] Expression of ActA is induced only after entering a mammalian host cell.[8]

Actin filament assembly generates the force that pushes the bacterium in the mammalian host cytoplasm forward. Continuous actin polymerization is sufficient for motility in the cytoplasm and even for infection of adjacent cells.[9]

Research edit

New data indicates that ActA plays a role also in vacuolar disruption. A deletion mutant of ActA was defective in permeabilizing the vacuole. An 11 amino acid stretch of the N-terminus of the acidic region (32-42) was shown to be important for disruption of the phagosome.[10]

Structure edit

The primary proteinous product of the actA gene consists of 639 amino acids and includes the signal peptide (first N-terminal 29 amino acids) and the ActA chain (C-terminal 610 amino acids). Therefore, the sequence of the mature ActA protein consist of 610 amino acids. ActA has a molecular weight of 70,349 Da and is a surface protein.[1][2]

ActA is a natively unfolded protein which can be divided into three functional domains (Fig. 2):[1][11][12]

  • N-terminal domain that is highly charged: amino acid residues 1-234
  • central domain with proline-rich repeats: amino acid residues 235-394
  • C-terminal domain with a transmembrane domain: amino acid residues 395-610

N-terminal domain edit

 
Fig. 2 The ActA protein and its functional domains

The first 156 amino acids of the N-terminal domain consist of three regions[10][13] (Fig. 2):

  • A-region with a stretch of acidic residues: 32-45
  • AB-region, an actin monomer-binding region: 59-102
  • C-region, a cofilin homology sequence: 145-156

The N-terminal portion of ActA plays an important role in actin polymerization.[14] The domain displays consensus elements present in eukaryotic WASP family NPFs which include an actin monomer-binding region as well as an Arp2/3 binding C (central or cofilin homology) and A (acidic) region.[7] The actin monomer-binding region of ActA has functional properties like the WASP-Homology-2 (WH2) or V domain, but differs in the sequence.[15] Thus in WASP-family NPFs the order of the domains is WH2 followed by C, and then by A, which is not the case in ActA.

Central domain edit

The central proline-rich region of ActA is crucial for ensuring efficient bacterial motility. There are four proline-rich repeats containing either FPPPP or FPPIP motifs. These regions mimic those of the host cell cytoskeletal protein zyxin, vinculin and palladin, known to associate with focal adhesions or stress fibers.[16] The vasodilator-stimulated phosphoprotein (VASP) can bind through its Ena/VASP homology 1 domain (EVH1 domain) to the central proline-rich region and recruits profilin, an actin monomer binding protein, which itself promotes polymerization at barbed ends of actin filaments. Furthermore, VASP seems to interact with F-actin through its carboxy-terminal EVH2 domain, which provides a linkage of the bacterium to the tail.[17] This statement is supported by the fact that ActA can bind multiple Ena/VASP proteins simultaneously and has a high affinity between ActA and Ena/VASP. VASP has been shown to reduce the frequency actin-Y-branches in vitro and thus increases the proportion of filaments which are organized in a parallel alignment in comet tails.[18][19]

C-terminal domain edit

The C-terminal domain of ActA has a hydrophobic region which anchors the protein in the bacterial membrane.[20][21][22]

In summary, besides

  • the absence of sequence homology in the actin-binding-region and
  • an alteration in the sequence of ARP2/3 activating domains typical for WASP-family NPFs (V(WH2)-C-A),
  • a major difference between ActA and host NPFs is that ActA does not have elements that bind to regulatory proteins such as Rho family GTPases. This structural difference between ActA and host NPFs can be advantageous for L. monocytogenes and its pathogenesis because the actin nucleation activity of L. monocytogenes is independent of host regulation.[7]

Analogues edit

WASP/N-WASP, which is functionally mimicked by ActA, is highly conserved in eukaryotes. It is an important actin-cytoskeleton organizer and is critical for processes such as endocytosis and cell motility. Activated by Cdc42, a Rho-family small GTPase, WASP/N-WASP activates the Arp2/3 complex, which leads to rapid actin polymerization.[23]

Actin-based motility of other pathogens edit

In Shigella the protein IcsA activates N-WASP, which in non-infected mammalian cells is activated by the GTPase Cdc42. Active N-WASP/WASP leads to actin polymerization by activating the Arp2/3 complex. In contrast, the Listeria ActA protein interacts with and activates directly the Arp2/3 complex.[7]

The Rickettsia RickA protein is also able to activate the Arp2/3 complex in a WASP-like manner. In contrast to Listeria, the actin filaments are organized in long, unbranched parallel bundles. The Arp2/3 complex is only localized near the bacterial surface and thus it is assumed that a more frequent Arp2/3 complex-independent elongation occurs.[16]

In Burkholderia pseudomallei BimA initiates actin polymerization in vitro. It is assumed that intracellular migration of this bacterium functions independently of the Arp2/3 complex.[16]

See also edit

References edit

  1. ^ a b c d Kocks C, Gouin E, Tabouret M, Berche P, Ohayon H, Cossart P (February 1992). "L. monocytogenes-induced actin assembly requires the actA gene product, a surface protein". Cell. 68 (3): 521–31. doi:10.1016/0092-8674(92)90188-I. PMID 1739966. S2CID 27231730.
  2. ^ a b Uniprot P33379
  3. ^ Cossart P, Sansonetti PJ (April 2004). "Bacterial invasion: the paradigms of enteroinvasive pathogens". Science. 304 (5668): 242–8. Bibcode:2004Sci...304..242C. doi:10.1126/science.1090124. PMID 15073367. S2CID 34536253.
  4. ^ Cossart P, Pizarro-Cerdá J, Lecuit M (January 2003). "Invasion of mammalian cells by Listeria monocytogenes: functional mimicry to subvert cellular functions". Trends in Cell Biology. 13 (1): 23–31. doi:10.1016/S0962-8924(02)00006-5. PMID 12480337.
  5. ^ Zigmond SH (February 2004). "Formin-induced nucleation of actin filaments". Current Opinion in Cell Biology. 16 (1): 99–105. doi:10.1016/j.ceb.2003.10.019. PMID 15037312.
  6. ^ Goley ED, Rodenbusch SE, Martin AC, Welch MD (October 2004). "Critical conformational changes in the Arp2/3 complex are induced by nucleotide and nucleation promoting factor". Molecular Cell. 16 (2): 269–79. doi:10.1016/j.molcel.2004.09.018. PMID 15494313.
  7. ^ a b c d Gouin E, Welch MD, Cossart P (February 2005). "Actin-based motility of intracellular pathogens". Current Opinion in Microbiology. 8 (1): 35–45. doi:10.1016/j.mib.2004.12.013. PMID 15694855.
  8. ^ Rafelski SM, Theriot JA (February 2006). "Mechanism of polarization of Listeria monocytogenes surface protein ActA". Molecular Microbiology. 59 (4): 1262–79. doi:10.1111/j.1365-2958.2006.05025.x. PMC 1413586. PMID 16430699.
  9. ^ Goldberg MB (December 2001). "Actin-Based Motility of Intracellular Microbial Pathogens". Microbiology and Molecular Biology Reviews. 65 (4): 595–626. doi:10.1128/MMBR.65.4.595-626.2001. PMC 99042. PMID 11729265.
  10. ^ a b Poussin MA, Goldfine H (January 2010). "Evidence for involvement of ActA in maturation of the Listeria monocytogenes phagosome". Cell Research. 20 (1): 109–12. doi:10.1038/cr.2009.142. PMC 2802179. PMID 20029388.
  11. ^ Ireton K, Cossart P (1997). "Host-pathogen interactions during entry and actin-based movement of Listeria monocytogenes". Annual Review of Genetics. 31: 113–38. doi:10.1146/annurev.genet.31.1.113. PMID 9442892.
  12. ^ Footer MJ, Lyo JK, Theriot JA (2008-08-29). "Close packing of Listeria monocytogenes ActA, a natively unfolded protein, enhances F-actin assembly without dimerization". The Journal of Biological Chemistry. 283 (35): 23852–23862. doi:10.1074/jbc.M803448200. ISSN 0021-9258. PMC 2527104. PMID 18577520.
  13. ^ Welch MD (2007). "Actin-Based Motility and Cell-to-Cell Spread of Listeria monocytogenes". In Goldfine H, Shen H (eds.). Listeria monocytogenes: Pathogenesis and Host Response. New York: Springer. pp. 197–223. doi:10.1007/978-0-387-49376-3_10. ISBN 978-0-387-49373-2.
  14. ^ Welch MD, Rosenblatt J, Skoble J, Portnoy DA, Mitchison TJ (July 1998). "Interaction of human Arp2/3 complex and the Listeria monocytogenes ActA protein in actin filament nucleation". Science. 281 (5373): 105–8. Bibcode:1998Sci...281..105W. doi:10.1126/science.281.5373.105. PMID 9651243.
  15. ^ Zalevsky J, Grigorova I, Mullins RD (February 2001). "Activation of the Arp2/3 complex by the Listeria acta protein. Acta binds two actin monomers and three subunits of the Arp2/3 complex". The Journal of Biological Chemistry. 276 (5): 3468–75. doi:10.1074/jbc.M006407200. PMID 11029465.
  16. ^ a b c Lambrechts A, Gevaert K, Cossart P, Vandekerckhove J, Van Troys M (May 2008). "Listeria comet tails: the actin-based motility machinery at work". Trends in Cell Biology. 18 (5): 220–7. doi:10.1016/j.tcb.2008.03.001. PMID 18396046.
  17. ^ Laurent V, Loisel TP, Harbeck B, et al. (March 1999). "Role of Proteins of the Ena/VASP Family in Actin-based Motility of Listeria monocytogenes". The Journal of Cell Biology. 144 (6): 1245–58. doi:10.1083/jcb.144.6.1245. PMC 2150578. PMID 10087267.
  18. ^ Skoble J, Auerbuch V, Goley ED, Welch MD, Portnoy DA (October 2001). "Pivotal role of VASP in Arp2/3 complex–mediated actin nucleation, actin branch-formation, and Listeria monocytogenes motility". The Journal of Cell Biology. 155 (1): 89–100. doi:10.1083/jcb.200106061. PMC 2150787. PMID 11581288.
  19. ^ Bear J.E., Svitkina T.M., Krause M., et al. (May 2002). "Antagonism between Ena/VASP proteins and actin filament capping regulates fibroblast motility". Cell. 109 (4): 509–21. doi:10.1016/S0092-8674(02)00731-6. hdl:1721.1/83477. PMID 12086607. S2CID 2848293.
  20. ^ Vazquez-Boland JA, Kocks C, Dramsi S, et al. (January 1992). "Nucleotide sequence of the lecithinase operon of Listeria monocytogenes and possible role of lecithinase in cell-to-cell spread". Infection and Immunity. 60 (1): 219–30. doi:10.1128/iai.60.1.219-230.1992. PMC 257526. PMID 1309513.
  21. ^ Domann E, Wehland J, Rohde M, et al. (May 1992). "A novel bacterial virulence gene in Listeria monocytogenes required for host cell microfilament interaction with homology to the proline-rich region of vinculin". The EMBO Journal. 11 (5): 1981–90. doi:10.1002/j.1460-2075.1992.tb05252.x. PMC 556658. PMID 1582425.
  22. ^ Kocks C, Hellio R, Gounon P, Ohayon H, Cossart P (July 1993). "Polarized distribution of Listeria monocytogenes surface protein ActA at the site of directional actin assembly". Journal of Cell Science. 105 (3): 699–710. doi:10.1242/jcs.105.3.699. PMID 8408297.
  23. ^ Kurisu S, Takenawa T (2009). "The WASP and WAVE family proteins". Genome Biology. 10 (6): 226. doi:10.1186/gb-2009-10-6-226. PMC 2718491. PMID 19589182.

External links edit

  • YouTube video from Nature, Listeria monocytogenes [2:00–4:12]

April 14, 2024
actin, assembly, inducing, protein, acta, protein, encoded, used, listeria, monocytogenes, propel, itself, through, mammalian, host, cell, acta, bacterial, surface, protein, comprising, membrane, spanning, region, mammalian, cell, bacterial, acta, interacts, w. The Actin assembly inducing protein ActA is a protein encoded and used by Listeria monocytogenes to propel itself through a mammalian host cell ActA is a bacterial surface protein comprising a membrane spanning region 1 In a mammalian cell the bacterial ActA interacts with the Arp2 3 complex and actin monomers to induce actin polymerization on the bacterial surface generating an actin comet tail The gene encoding ActA is named actA or prtB 2 Actin assembly inducing proteinEVH1 domain ActA peptide complexIdentifiersSymbolActANCBI gene2798121UniProtP33379Search forStructuresSwiss modelDomainsInterPro Contents 1 Introduction 1 1 Discovery 2 Function 2 1 Research 3 Structure 3 1 N terminal domain 3 2 Central domain 3 3 C terminal domain 4 Analogues 4 1 Actin based motility of other pathogens 5 See also 6 References 7 External linksIntroduction editAs soon as L monocytogenes bacteria are ingested by humans they get internalized into intestinal epithelium cells and rapidly try to escape their internalization vacuole 3 4 In the cytosol they start to polymerize actin on their surface by the help of the ActA protein It has been shown that ActA is not only necessary but also sufficient to induce motility of bacteria in the absence of other bacterial factors 5 Discovery edit ActA was discovered by analysing lecithinase negative Tn917 lac Listeria mutants because of the phenotype that they were unable to spread from cell to cell These mutant bacteria still escaped from the phagosomes as efficiently as wild type bacteria and multiplied within the infected cells but they were not surrounded by actin like wild type bacteria Further analysis showed that Tn917 lac had inserted into actA the second gene of an operon The third gene of this operon plcB encodes the L monocytogenes lecithinase To determine whether actA itself plcB or other co transcribed downstream regions are involved in actin assembly mutations in the appropriate genes were generated All mutants except the actA mutants were similar to wild type concerning association with F actin and cell cell spreading Complementation with actA restored wild type phenotype in the actA mutants 1 Function edit nbsp Fig 1 Actin assembly induced by bacterial protein ActA shown in green Mammalian proteins involved in this process are Profilin P Vasodilator stimulated phosphoprotein VASP and actin related protein 2 and 3 complex Arp2 3 complex as well as actin ActA is a protein which acts as a mimic of Wiskott Aldrich syndrome protein WASP a nucleation promoting factor NPF present in host cells NPFs in the mammalian cell recruit and bind to the already existing actin related protein 2 and 3 complex Arp2 3 complex and induce an activating conformational change of the Arp2 3 complex 6 Due to this conformational change NPFs initiate polymerization of a new actin filament at a 70 angle which leads to the characteristic Y branched actin structures in the leading edge of motile cells ActA localizes to the old pole of the bacterium and spans both the bacterial cell membrane and the cell wall lateral diffusion is inhibited thus ActA localizes in a polarized and anchored manner on the bacterial surface Consequently actin polymerization only starts in this region on the surface of the bacterium 7 Expression of ActA is induced only after entering a mammalian host cell 8 Actin filament assembly generates the force that pushes the bacterium in the mammalian host cytoplasm forward Continuous actin polymerization is sufficient for motility in the cytoplasm and even for infection of adjacent cells 9 Research edit New data indicates that ActA plays a role also in vacuolar disruption A deletion mutant of ActA was defective in permeabilizing the vacuole An 11 amino acid stretch of the N terminus of the acidic region 32 42 was shown to be important for disruption of the phagosome 10 Structure editThe primary proteinous product of the actA gene consists of 639 amino acids and includes the signal peptide first N terminal 29 amino acids and the ActA chain C terminal 610 amino acids Therefore the sequence of the mature ActA protein consist of 610 amino acids ActA has a molecular weight of 70 349 Da and is a surface protein 1 2 ActA is a natively unfolded protein which can be divided into three functional domains Fig 2 1 11 12 N terminal domain that is highly charged amino acid residues 1 234 central domain with proline rich repeats amino acid residues 235 394 C terminal domain with a transmembrane domain amino acid residues 395 610N terminal domain edit nbsp Fig 2 The ActA protein and its functional domainsThe first 156 amino acids of the N terminal domain consist of three regions 10 13 Fig 2 A region with a stretch of acidic residues 32 45 AB region an actin monomer binding region 59 102 C region a cofilin homology sequence 145 156The N terminal portion of ActA plays an important role in actin polymerization 14 The domain displays consensus elements present in eukaryotic WASP family NPFs which include an actin monomer binding region as well as an Arp2 3 binding C central or cofilin homology and A acidic region 7 The actin monomer binding region of ActA has functional properties like the WASP Homology 2 WH2 or V domain but differs in the sequence 15 Thus in WASP family NPFs the order of the domains is WH2 followed by C and then by A which is not the case in ActA Central domain edit The central proline rich region of ActA is crucial for ensuring efficient bacterial motility There are four proline rich repeats containing either FPPPP or FPPIP motifs These regions mimic those of the host cell cytoskeletal protein zyxin vinculin and palladin known to associate with focal adhesions or stress fibers 16 The vasodilator stimulated phosphoprotein VASP can bind through its Ena VASP homology 1 domain EVH1 domain to the central proline rich region and recruits profilin an actin monomer binding protein which itself promotes polymerization at barbed ends of actin filaments Furthermore VASP seems to interact with F actin through its carboxy terminal EVH2 domain which provides a linkage of the bacterium to the tail 17 This statement is supported by the fact that ActA can bind multiple Ena VASP proteins simultaneously and has a high affinity between ActA and Ena VASP VASP has been shown to reduce the frequency actin Y branches in vitro and thus increases the proportion of filaments which are organized in a parallel alignment in comet tails 18 19 C terminal domain edit The C terminal domain of ActA has a hydrophobic region which anchors the protein in the bacterial membrane 20 21 22 In summary besides the absence of sequence homology in the actin binding region and an alteration in the sequence of ARP2 3 activating domains typical for WASP family NPFs V WH2 C A a major difference between ActA and host NPFs is that ActA does not have elements that bind to regulatory proteins such as Rho family GTPases This structural difference between ActA and host NPFs can be advantageous for L monocytogenes and its pathogenesis because the actin nucleation activity of L monocytogenes is independent of host regulation 7 Analogues editWASP N WASP which is functionally mimicked by ActA is highly conserved in eukaryotes It is an important actin cytoskeleton organizer and is critical for processes such as endocytosis and cell motility Activated by Cdc42 a Rho family small GTPase WASP N WASP activates the Arp2 3 complex which leads to rapid actin polymerization 23 Actin based motility of other pathogens edit In Shigella the protein IcsA activates N WASP which in non infected mammalian cells is activated by the GTPase Cdc42 Active N WASP WASP leads to actin polymerization by activating the Arp2 3 complex In contrast the Listeria ActA protein interacts with and activates directly the Arp2 3 complex 7 The Rickettsia RickA protein is also able to activate the Arp2 3 complex in a WASP like manner In contrast to Listeria the actin filaments are organized in long unbranched parallel bundles The Arp2 3 complex is only localized near the bacterial surface and thus it is assumed that a more frequent Arp2 3 complex independent elongation occurs 16 In Burkholderia pseudomallei BimA initiates actin polymerization in vitro It is assumed that intracellular migration of this bacterium functions independently of the Arp2 3 complex 16 See also editListeria monocytogenesReferences edit a b c d Kocks C Gouin E Tabouret M Berche P Ohayon H Cossart P February 1992 L monocytogenes induced actin assembly requires the actA gene product a surface protein Cell 68 3 521 31 doi 10 1016 0092 8674 92 90188 I PMID 1739966 S2CID 27231730 a b Uniprot P33379 Cossart P Sansonetti PJ April 2004 Bacterial invasion the paradigms of enteroinvasive pathogens Science 304 5668 242 8 Bibcode 2004Sci 304 242C doi 10 1126 science 1090124 PMID 15073367 S2CID 34536253 Cossart P Pizarro Cerda J Lecuit M January 2003 Invasion of mammalian cells by Listeria monocytogenes functional mimicry to subvert cellular functions Trends in Cell Biology 13 1 23 31 doi 10 1016 S0962 8924 02 00006 5 PMID 12480337 Zigmond SH February 2004 Formin induced nucleation of actin filaments Current Opinion in Cell Biology 16 1 99 105 doi 10 1016 j ceb 2003 10 019 PMID 15037312 Goley ED Rodenbusch SE Martin AC Welch MD October 2004 Critical conformational changes in the Arp2 3 complex are induced by nucleotide and nucleation promoting factor Molecular Cell 16 2 269 79 doi 10 1016 j molcel 2004 09 018 PMID 15494313 a b c d Gouin E Welch MD Cossart P February 2005 Actin based motility of intracellular pathogens Current Opinion in Microbiology 8 1 35 45 doi 10 1016 j mib 2004 12 013 PMID 15694855 Rafelski SM Theriot JA February 2006 Mechanism of polarization of Listeria monocytogenes surface protein ActA Molecular Microbiology 59 4 1262 79 doi 10 1111 j 1365 2958 2006 05025 x PMC 1413586 PMID 16430699 Goldberg MB December 2001 Actin Based Motility of Intracellular Microbial Pathogens Microbiology and Molecular Biology Reviews 65 4 595 626 doi 10 1128 MMBR 65 4 595 626 2001 PMC 99042 PMID 11729265 a b Poussin MA Goldfine H January 2010 Evidence for involvement of ActA in maturation of the Listeria monocytogenes phagosome Cell Research 20 1 109 12 doi 10 1038 cr 2009 142 PMC 2802179 PMID 20029388 Ireton K Cossart P 1997 Host pathogen interactions during entry and actin based movement of Listeria monocytogenes Annual Review of Genetics 31 113 38 doi 10 1146 annurev genet 31 1 113 PMID 9442892 Footer MJ Lyo JK Theriot JA 2008 08 29 Close packing of Listeria monocytogenes ActA a natively unfolded protein enhances F actin assembly without dimerization The Journal of Biological Chemistry 283 35 23852 23862 doi 10 1074 jbc M803448200 ISSN 0021 9258 PMC 2527104 PMID 18577520 Welch MD 2007 Actin Based Motility and Cell to Cell Spread of Listeria monocytogenes In Goldfine H Shen H eds Listeria monocytogenes Pathogenesis and Host Response New York Springer pp 197 223 doi 10 1007 978 0 387 49376 3 10 ISBN 978 0 387 49373 2 Welch MD Rosenblatt J Skoble J Portnoy DA Mitchison TJ July 1998 Interaction of human Arp2 3 complex and the Listeria monocytogenes ActA protein in actin filament nucleation Science 281 5373 105 8 Bibcode 1998Sci 281 105W doi 10 1126 science 281 5373 105 PMID 9651243 Zalevsky J Grigorova I Mullins RD February 2001 Activation of the Arp2 3 complex by the Listeria acta protein Acta binds two actin monomers and three subunits of the Arp2 3 complex The Journal of Biological Chemistry 276 5 3468 75 doi 10 1074 jbc M006407200 PMID 11029465 a b c Lambrechts A Gevaert K Cossart P Vandekerckhove J Van Troys M May 2008 Listeria comet tails the actin based motility machinery at work Trends in Cell Biology 18 5 220 7 doi 10 1016 j tcb 2008 03 001 PMID 18396046 Laurent V Loisel TP Harbeck B et al March 1999 Role of Proteins of the Ena VASP Family in Actin based Motility of Listeria monocytogenes The Journal of Cell Biology 144 6 1245 58 doi 10 1083 jcb 144 6 1245 PMC 2150578 PMID 10087267 Skoble J Auerbuch V Goley ED Welch MD Portnoy DA October 2001 Pivotal role of VASP in Arp2 3 complex mediated actin nucleation actin branch formation and Listeria monocytogenes motility The Journal of Cell Biology 155 1 89 100 doi 10 1083 jcb 200106061 PMC 2150787 PMID 11581288 Bear J E Svitkina T M Krause M et al May 2002 Antagonism between Ena VASP proteins and actin filament capping regulates fibroblast motility Cell 109 4 509 21 doi 10 1016 S0092 8674 02 00731 6 hdl 1721 1 83477 PMID 12086607 S2CID 2848293 Vazquez Boland JA Kocks C Dramsi S et al January 1992 Nucleotide sequence of the lecithinase operon of Listeria monocytogenes and possible role of lecithinase in cell to cell spread Infection and Immunity 60 1 219 30 doi 10 1128 iai 60 1 219 230 1992 PMC 257526 PMID 1309513 Domann E Wehland J Rohde M et al May 1992 A novel bacterial virulence gene in Listeria monocytogenes required for host cell microfilament interaction with homology to the proline rich region of vinculin The EMBO Journal 11 5 1981 90 doi 10 1002 j 1460 2075 1992 tb05252 x PMC 556658 PMID 1582425 Kocks C Hellio R Gounon P Ohayon H Cossart P July 1993 Polarized distribution of Listeria monocytogenes surface protein ActA at the site of directional actin assembly Journal of Cell Science 105 3 699 710 doi 10 1242 jcs 105 3 699 PMID 8408297 Kurisu S Takenawa T 2009 The WASP and WAVE family proteins Genome Biology 10 6 226 doi 10 1186 gb 2009 10 6 226 PMC 2718491 PMID 19589182 External links editYouTube video from Nature Listeria monocytogenes 2 00 4 12 Retrieved from https en wikipedia org w index php title Actin assembly inducing protein amp oldid 1199195720, wikipedia, wiki, book, books, library,

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