A conserved motif promotes HpaB‐regulated export of type III effectors from <i>Xanthomonas</i>

Prochaska, Heike; Thieme, Sabine; Daum, Sebastian; Grau, Jan; Schmidtke, Cornelius; Hallensleben, Magnus; John, Peter; Bacia, Kirsten; Bonas, Ulla

doi:10.1111/mpp.12725

Cited by 7 publications

(18 citation statements)

References 68 publications

(103 reference statements)

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“…Interestingly, a recent study has shown that many recently discovered T3Es target to bacterial membrane where chaperone HpaB promotes recognition of T3Es by T3SS [ 23 ]. The free HpaB targets to the cytoplasmic and/or inner components of T3SS, which presumably is used to regulate secretion and/or translocation of T3SS substrates [ 11 , 12 , 14 , 22 , 48 , 49 ].…”

Section: Resultsmentioning

confidence: 99%

“…Interestingly, a recent study has shown that many recently discovered T3Es target to bacterial membrane where chaperone HpaB promotes recognition of T3Es by T3SS [23]. The free HpaB…”

Section: The C-terminal Domain Of Hpab Is Dispensable For Interaction With T3ss Components In Xccmentioning

confidence: 99%

“…Recent work has shown that T3Es of X. campestris pv. vesicatoria (Xcv), prior to interaction with HpaB, locate to the bacterial cytoplasmic membrane by specifically binding to cardiolipin [23]. Several studies in animal pathogenic bacteria have shown that the T3E wraps around the chaperone dimer in an extended conformation before targeting to the secretion platform, leading to the proposal that there is a three-dimensional signal for T3SS recognition [1,15,[24][25][26].…”

Section: Introductionmentioning

confidence: 99%

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The C-terminal domain of the type III secretion chaperone HpaB contributes to dissociation of chaperone-effector complex in Xanthomonas campestris pv. campestris

et al. 2021

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Many animal and plant pathogenic bacteria employ a type three secretion system (T3SS) to deliver type three effector proteins (T3Es) into host cells. Efficient secretion of many T3Es in the plant pathogen Xanthomonas campestris pv. campestris (Xcc) relies on the global chaperone HpaB. However, how the domain of HpaB itself affects effector translocation/secretion is poorly understood. Here, we used genetic and biochemical approaches to identify a novel domain at the C-terminal end of HpaB (amino acid residues 137–160) that contributes to virulence and hypersensitive response (HR). Both in vitro secretion assay and in planta translocation assay showed that the secretion and translocation of T3E proteins depend on the C-terminal region of HpaB. Deletion of the C-terminal region of HpaB did not affect binding to T3Es, self-association or interaction with T3SS components. However, the deletion of C-terminal region sharply reduced the mounts of free T3Es liberated from the complex of HpaB with the T3Es, a reaction catalyzed in an ATP-dependent manner by the T3SS-associated ATPase HrcN. Our findings demonstrate the C-terminal domain of HpaB contributes to disassembly of chaperone-effector complex and reveal a potential molecular mechanism underpinning the involvement of HpaB in secretion of T3Es in Xcc.

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Section: Resultsmentioning

confidence: 99%

“…Interestingly, a recent study has shown that many recently discovered T3Es target to bacterial membrane where chaperone HpaB promotes recognition of T3Es by T3SS [23]. The free HpaB…”

Section: The C-terminal Domain Of Hpab Is Dispensable For Interaction With T3ss Components In Xccmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The C-terminal domain of the type III secretion chaperone HpaB contributes to dissociation of chaperone-effector complex in Xanthomonas campestris pv. campestris

et al. 2021

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“…Notably, an interaction with T3S chaperones was also described for FliJ, Spa13, and InvI, suggesting that HrpO/FliJ/YscO family members are involved in a network of interactions with T3SS components and chaperones (Evans et al, ; Evans & Hughes, ). In Xcv , the T3S chaperone HpaB is essential for the efficient secretion and translocation of multiple effector proteins and was previously identified as interaction partner of T3SS components including the ATPase, the C ring, and the cytoplasmic domains of components of the export apparatus (Büttner et al, ; Büttner et al, ; Hartmann & Büttner, ; Lonjon et al, ; Lorenz & Büttner, ; Lorenz et al, ; Prochaska et al, ). The presence of multiple binding sites for HpaB in the T3SS suggests that HrpB7 does not play an exclusive role in the recruitment of chaperone complexes but might rather be of general importance for T3S.…”

Section: Discussionmentioning

confidence: 99%

“…Hrc and Hrp proteins are essential for T3S as structural components, whereas the accessory Hpa (Hrp associated) proteins are often involved in the control of T3S. One example is the T3S chaperone HpaB, which binds to type III effectors and presumably targets them to the T3S ATPase (Büttner et al, 2004;Büttner et al, 2006;Lonjon et al, 2017;Lorenz & Büttner, 2009;Prochaska et al, 2018;Scheibner et al, 2018). HpaB contributes to the translocation of most effector proteins and is, therefore, essential for pathogenicity.…”

Section: Introductionmentioning

confidence: 99%

HrpB7 from Xanthomonas campestris pv. vesicatoria is an essential component of the type III secretion system and shares features of HrpO/FliJ/YscO family members

Drehkopf

Otten

Hausner

et al. 2020

Cellular Microbiology

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The Gram‐negative bacterium Xanthomonas campestris pv. vesicatoria translocates effector proteins via a type III secretion system (T3SS) into eukaryotic cells. The T3SS spans both bacterial membranes and consists of more than 20 proteins, 9 of which are conserved in plant and animal pathogens and constitute the core subunits of the secretion apparatus. T3S in X. campestris pv. vesicatoria also depends on nonconserved proteins with yet unknown function including HrpB7, which contains predicted N‐ and C‐terminal coiled‐coil regions. In the present study, we provide experimental evidence that HrpB7 forms stable oligomeric complexes. Interaction and localisation studies suggest that HrpB7 interacts with inner membrane and predicted cytoplasmic (C) ring components of the T3SS but is dispensable for the assembly of the C ring. Additional interaction partners of HrpB7 include the cytoplasmic adenosinetriphosphatase HrcN and the T3S chaperone HpaB. The interaction of HrpB7 with T3SS components as well as complex formation by HrpB7 depends on the presence of leucine heptad motifs, which are part of the predicted N‐ and C‐terminal coiled‐coil structures. Our data suggest that HrpB7 forms multimeric complexes that associate with the T3SS and might serve as a docking site for the general T3S chaperone HpaB.

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A packaging signal-binding protein regulates the assembly checkpoint of integrative filamentous phages

Yeh,

Feehley,

Feehley

et al. 2024

Preprint

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Many integrative filamentous phages not only lack Ff coliphage homologues essential for assembly but also have distinct packaging signals (PS). Their encapsidation remains completely uncharacterized to date. Here we report the first evidence of a PS-dependent checkpoint for integrative filamentous phage assembly. Suppressor screening of PS-deficient phages identified an unknown protein, PSB15 (PS-binding15kDa), crucial for encapsidation. The WAGFXF motif of the PSB15 N-terminus directly binds to PS DNA with conformational change, while suppressor mutations relieve DNA binding specificity constraints to rescue assembly arrest. PSB15 interacts with phospholipid cardiolipin via its basic helix and C-terminus, and recruits PS DNA to the inner membrane (IM). The PSB15-PS complex is released from the IM by interaction between its hydrophobic linker and thioredoxin (Trx), a host protein that is required for Ff assembly but whose mechanisms are still unclear. Live cell imaging shows that thioredoxin and DNA binding regulate the dwelling time of PSB15 at cell poles, suggesting that they both facilitate the dissociation of PSB15 from the IM. Loss of PSB15 or its PS-binding and IM-targeting/dissociation activity compromised virus egress, indicating that the PS/PSB15/Trx complex establishes a regulatory phage assembly checkpoint critical for integrative phage infection and life cycles.

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A conserved motif promotes HpaB‐regulated export of type III effectors from Xanthomonas

Cited by 7 publications

References 68 publications

The C-terminal domain of the type III secretion chaperone HpaB contributes to dissociation of chaperone-effector complex in Xanthomonas campestris pv. campestris

The C-terminal domain of the type III secretion chaperone HpaB contributes to dissociation of chaperone-effector complex in Xanthomonas campestris pv. campestris

HrpB7 from Xanthomonas campestris pv. vesicatoria is an essential component of the type III secretion system and shares features of HrpO/FliJ/YscO family members

A packaging signal-binding protein regulates the assembly checkpoint of integrative filamentous phages

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