Cla4p, a <i>Saccharomyces cerevisiae</i> Cdc42p-Activated Kinase Involved in Cytokinesis, Is Activated at Mitosis†

Benton, Benjamin K.; Tinkelenberg, Arthur H.; Gonzalez, Isabel; Cross, Frederick R.

doi:10.1128/mcb.17.9.5067

Cited by 111 publications

(108 citation statements)

References 71 publications

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“…6A), as reported previously (46). These loss of function phenotypes were not due to complete loss of Cla4 kinase activity, because the PH⌬ mutant has been shown previously to have detectable (albeit reduced) kinase activity, whereas the PBD⌬ mutant has elevated kinase activity relative to wild type Cla4 (46).…”

Section: Resultssupporting

confidence: 63%

“…In contrast, expression of mutant Cla4-GFP in which the PH domain or PBD was deleted failed to rescue the elongated bud phenotype (only 40% of cells had normal buds, similar to empty vector controls; Fig. 6A), as reported previously (46). These loss of function phenotypes were not due to complete loss of Cla4 kinase activity, because the PH⌬ mutant has been shown previously to have detectable (albeit reduced) kinase activity, whereas the PBD⌬ mutant has elevated kinase activity relative to wild type Cla4 (46).…”

Section: Resultsmentioning

confidence: 63%

“…The rationale for doing so was severalfold. In contrast to other proteins such as Boi1 that bind Cdc42 by poorly understood mechanisms, Cla4 uses its conserved PBD to bind Cdc42 (46). Furthermore, Cla4 probably binds Cdc42 by a mechanism highly similar to that used by mammalian PAK1 because the residues in PAK1 that bind Cdc42 are conserved in Cla4 (Fig.…”

Section: Resultsmentioning

confidence: 99%

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The p21-activated Protein Kinase-related Kinase Cla4 Is a Coincidence Detector of Signaling by Cdc42 and Phosphatidylinositol 4-Phosphate

Wild

Lemmon

et al. 2004

Journal of Biological Chemistry

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Signal transduction pathways that co-regulate a given biological process often are organized into networks by molecules that act as coincidence detectors. Phosphoinositides and the Rho-type GTPase Cdc42 regulate overlapping processes in all eukaryotic cells. However, the coincidence detectors that link these pathways into networks remain unknown. Here we show that the p21-activated protein kinase-related kinase Cla4 of yeast integrates signaling by Cdc42 and phosphatidylinositol 4-phosphate (PI4P). We found that the Cla4 pleckstrin homology (PH) domain binds in vitro to several phosphoinositide species. To determine which phosphoinositides regulate Cla4 in vivo, we analyzed phosphatidylinositol kinase mutants (stt4, mss4, and pik1). This indicated that the plasma membrane pool of PI4P, but not phosphatidylinositol 4,5-bisphosphate or the Golgi pool of PI4P, is required for localization of Cla4 to sites of polarized growth. A combination of the Cdc42-binding and PH domains of Cla4 was necessary and sufficient for localization to sites of polarized growth. Point mutations affecting either domain impaired the ability of Cla4 to regulate cell morphogenesis and the mitotic exit network (localization of Lte1). Therefore, Cla4 must retain the ability to bind both Cdc42 and phosphoinositides, the hallmark of a coincidence detector. PI4P may recruit Cla4 to the plasma membrane where Cdc42 activates its kinase activity and refines its localization to cortical sites of polarized growth. In mammalian cells, the myotonic dystrophy-related Cdc42-binding kinase possesses p21-binding and PH domains, suggesting that this kinase may be a coincidence detector of signaling by Cdc42 and phosphoinositides.

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Section: Resultssupporting

confidence: 63%

Section: Resultsmentioning

confidence: 63%

Section: Resultsmentioning

confidence: 99%

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The p21-activated Protein Kinase-related Kinase Cla4 Is a Coincidence Detector of Signaling by Cdc42 and Phosphatidylinositol 4-Phosphate

Wild

Lemmon

et al. 2004

Journal of Biological Chemistry

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“…In S. cerevisiae, there are five Cdc42 effectors with recognizable CRIB domains ( Figure 7A). Interestingly, Cla4 and Skm1 have PH domains at a position similar to that of the Ste20 BR domain, and the PH domain of Cla4 is essential for its function (Benton et al, 1997;Wild et al, 2004). Therefore, we wondered if the other two Cdc42 targets, Gic1 and Gic2, might also contain membrane-binding domains in an analogous position.…”

Section: Br Domains In the Yeast Cdc42 Effectors Gic1 And Gic2mentioning

confidence: 99%

Identification of Novel Membrane-binding Domains in Multiple Yeast Cdc42 Effectors

Takahashi

Pryciak

2007

MBoC

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The Rho-type GTPase Cdc42 is a central regulator of eukaryotic cell polarity and signal transduction. In budding yeast, Cdc42 regulates polarity and mitogen-activated protein (MAP) kinase signaling in part through the PAK-family kinase Ste20. Activation of Ste20 requires a Cdc42/Rac interactive binding (CRIB) domain, which mediates its recruitment to membrane-associated Cdc42. Here, we identify a separate domain in Ste20 that interacts directly with membrane phospholipids and is critical for its function. This short region, termed the basic-rich (BR) domain, can target green fluorescent protein to the plasma membrane in vivo and binds PIP 2 -containing liposomes in vitro. Mutation of basic or hydrophobic residues in the BR domain abolishes polarized localization of Ste20 and its function in both MAP kinase-dependent and independent pathways. Thus, Cdc42 binding is required but is insufficient; instead, direct membrane binding by Ste20 is also required. Nevertheless, phospholipid specificity is not essential in vivo, because the BR domain can be replaced with several heterologous lipid-binding domains of varying lipid preferences. We also identify functionally important BR domains in two other yeast Cdc42 effectors, Gic1 and Gic2, suggesting that cooperation between protein-protein and protein-membrane interactions is a prevalent mechanism during Cdc42-regulated signaling and perhaps for other dynamic localization events at the cell cortex.

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“…A PAK homolog Cla4 (Benton et al, 1997) directly phosphorylates and regulates Swe1 stability . In addition, Clb-Cdc28 complexes associate with and phosphorylate Swe1 (Sia et al, 1998;McMillan et al, 2002), suggesting the existence of a positive feedback mechanism.…”

Section: G2/m Transitionmentioning

confidence: 99%

Yeast polo-like kinases: functionally conserved multitask mitotic regulators

et al. 2005

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The polo-like kinases (Plks) are a conserved subfamily of Ser/Thr protein kinases that play pivotal roles in regulating various cellular and biochemical events at multiple stages of M phase. Genetic and biochemical data revealed that both the budding yeast and the fission yeast polo kinase homologs (Cdc5 and Plo1, respectively) bear remarkable functional similarities with those in metazoan organisms, suggesting that the role of Plks is largely conserved throughout evolution. Thus, studies on Plks in genetically amenable lower eucaryotic organisms may yield valuable insights into the function of Plks in higher eucaryotic organisms. In this review, common properties and distinct functions of Cdc5 and Plo1 will be discussed and compared to properties and functions of Plks in higher eucaryotic organisms.

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Cla4p, a Saccharomyces cerevisiae Cdc42p-Activated Kinase Involved in Cytokinesis, Is Activated at Mitosis†

Cited by 111 publications

References 71 publications

The p21-activated Protein Kinase-related Kinase Cla4 Is a Coincidence Detector of Signaling by Cdc42 and Phosphatidylinositol 4-Phosphate

The p21-activated Protein Kinase-related Kinase Cla4 Is a Coincidence Detector of Signaling by Cdc42 and Phosphatidylinositol 4-Phosphate

Identification of Novel Membrane-binding Domains in Multiple Yeast Cdc42 Effectors

Yeast polo-like kinases: functionally conserved multitask mitotic regulators

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