Chaperoning steroidal physiology: Lessons from mouse genetic models of Hsp90 and its cochaperones

Sánchez, Edwin R.

doi:10.1016/j.bbamcr.2011.11.006

Cited by 86 publications

(106 citation statements)

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“…Our data indicate that under basal conditions, increased expression of Fkbp5 mRNA is associated with increased weight gain and increased total caloric intake. This agrees with the 51KO mouse model, which is leaner compared with WT littermates , Sanchez 2012). When we compared the correlation coefficients between basal and stressed conditions, there was in fact no difference for Fkbp5 and caloric intake between conditions.…”

Section: Discussionsupporting

confidence: 76%

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Interplay between diet-induced obesity and chronic stress in mice: potential role of FKBP51

Balsevich

Uribe

Wagner

et al. 2014

Journal of Endocrinology

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While it is known that stress promotes obesity, the effects of stress within an obesogenic context are not so clear and molecular targets at the interface remain elusive. The FK506-binding protein 51 (FKBP51, gene: Fkbp5) has been identified as a target gene implicated in the development of stress-related psychiatric disorders and is a possible candidate for involvement in stress and metabolic regulation. The aims of the current study are to investigate the interaction between chronic stress and an obesogenic context and to additionally examine whether FKBP51 is involved in this interaction. For this purpose, male C57BL/6 mice were exposed to a high-fat diet for 8 weeks before being challenged with chronic social defeat stress. Herein, we demonstrate that chronic stress induces hypophagia and weight loss, ultimately improving features arising from an obesogenic context, including glucose tolerance and levels of insulin and leptin. We show that Fkbp5 expression is responsive to diet and stress in the hypothalamus and hippocampus respectively. Furthermore, under basal conditions, higher levels of hypothalamic Fkbp5 expression were related to increased body weight gain. Our data indicate that Fkbp5 may represent a novel target in metabolic regulation.

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Section: Discussionsupporting

confidence: 76%

“…Interestingly, mice deficient in FKBP51 display a moderately lean phenotype under basal conditions , Sanchez 2012. In this regard, Fkbp5 is an interesting candidate gene to study in the context of stress and metabolic regulation.…”

Section: Introductionmentioning

confidence: 99%

Interplay between diet-induced obesity and chronic stress in mice: potential role of FKBP51

Balsevich

Uribe

Wagner

et al. 2014

Journal of Endocrinology

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“…3D), as seen in vitro. These mutations also impair PP5's ability to dephosphorylate phospho-GR-Ser211, another known target of PP5 discussed in detail later (2). These data are in agreement with our previous work, in which overexpression of PP5 in HCT116 colon cancer cells enhanced Cdc37 dephosphorylation (8).…”

Section: -23)supporting

confidence: 83%

“…Having established that particular residues in the catalytic cleft are necessary for Cdc37 recognition, the question arises whether these residues are able to confer specificity of phosphatase activity (i.e., does their mutation have differential effects on different substrates?). PP5 also dephosphorylates GR, another Hsp90 client, at Ser203, Ser211, and Ser226 and subsequently, controls its activity and nucleocytoplasmic translocation (2). To examine specificity, we, therefore, investigated the consequences of mutations in the PP5 catalytic cleft on its ability to dephosphorylate GR-Ser211.…”

Section: Hyper-or Hypoactivity Of Pp5 Mutants Enhances Hsp90 Binding Tomentioning

confidence: 99%

“…Hsp90 | PP5 | Cdc37 | chaperone | phosphatase P rotein phosphatase 5 (PP5) has pleiotropic roles in cellular signaling, including DNA damage repair, proliferation of breast cancer cells, circadian cycling, response to cytotoxic stresses, Rac-dependent potassium ion channel activity, and activation of steroid hormone receptors [e.g., glucocorticoid receptor (GR) and estrogen receptor] (1,2). It is a member of the phosphoprotein phosphatase (PPP) family of serine/threonine phosphatases, which has members that share a highly conserved catalytic core and catalytic mechanism dependent on two metal ions, commonly Mn 2+ .…”

mentioning

confidence: 99%

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Structural and functional basis of protein phosphatase 5 substrate specificity

Oberoi

Dunn

Woodford

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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The serine/threonine phosphatase protein phosphatase 5 (PP5) regulates hormone-and stress-induced cellular signaling by association with the molecular chaperone heat shock protein 90 (Hsp90). PP5-mediated dephosphorylation of the cochaperone Cdc37 is essential for activation of Hsp90-dependent kinases. However, the details of this mechanism remain unknown. We determined the crystal structure of a Cdc37 phosphomimetic peptide bound to the catalytic domain of PP5. The structure reveals PP5 utilization of conserved elements of phosphoprotein phosphatase (PPP) structure to bind substrate and provides a template for many PPP-substrate interactions. Our data show that, despite a highly conserved structure, elements of substrate specificity are determined within the phosphatase catalytic domain itself. Structure-based mutations in vivo reveal that PP5-mediated dephosphorylation is required for kinase and steroid hormone receptor release from the chaperone complex. Finally, our data show that hyper-or hypoactivity of PP5 mutants increases Hsp90 binding to its inhibitor, suggesting a mechanism to enhance the efficacy of Hsp90 inhibitors by regulation of PP5 activity in tumors.Hsp90 | PP5 | Cdc37 | chaperone | phosphatase P rotein phosphatase 5 (PP5) has pleiotropic roles in cellular signaling, including DNA damage repair, proliferation of breast cancer cells, circadian cycling, response to cytotoxic stresses, Rac-dependent potassium ion channel activity, and activation of steroid hormone receptors [e.g., glucocorticoid receptor (GR) and estrogen receptor] (1, 2). It is a member of the phosphoprotein phosphatase (PPP) family of serine/threonine phosphatases, which has members that share a highly conserved catalytic core and catalytic mechanism dependent on two metal ions, commonly Mn 2+ . Most PPP family members exhibit high, nonspecific phosphatase activity. Specificity is provided by a large cohort of regulatory and other interacting proteins that function to inhibit basal activity and recruit substrates, thereby finely tuning the enzymes (3). This combinatorial approach enables a small number of catalytic subunits to have the breadth of specificity equivalent to that seen in kinases, which are greater in number by an order of magnitude. Structures of complexes between regulatory and catalytic domains have illuminated the importance of regulatory subunits in facilitating substrate recruitment (3). However, to date, there is no structural information describing how a substrate binds at the active site of a PPP; therefore, a central question remains of how local interactions between the substrate and the catalytic domain contribute to the molecular basis of dephosphorylation.PP5 is unique among the PPP family because it has a low basal activity caused by an autoinhibitory N-terminal tetratricopeptide (TPR) domain (4). Its activity is promoted by a number of cellular factors, including fatty acids and the molecular chaperone heat shock protein 90 (Hsp90) (5), both of which release autoinhibition by interacting with the TPR...

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In silico identification and biochemical characterization of the human dicarboxylate clamp TPR protein interaction network

et al. 2018

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Dicarboxylate clamp tetratricopeptide repeat (dc TPR ) motif‐containing proteins are well‐known partners of the heat shock protein (Hsp) 70 and Hsp90 molecular chaperones. Together, they facilitate a variety of intracellular processes, including protein folding and maturation, protein targeting, and protein degradation. An extreme C‐terminal sequence, the EEVD motif, is identical in Hsp70 and Hsp90, and is indispensable for their interaction with dc TPR proteins. However, almost no information is available on the existence of other potential dc TPR ‐interacting proteins. We searched the human protein database for proteins with C‐terminal sequences similar to that of Hsp70/Hsp90 to identify potential partners of dc TPR proteins. The search identified 112 proteins containing a Hsp70/Hsp90‐like signature at their C termini. Gene Ontology enrichment analysis of identified proteins revealed enrichment of distinct protein classes, such as molecular chaperones and proteins of the ubiquitin–proteasome system, highlighting the possibility of functional specialization of proteins containing a Hsp70/Hsp90‐like signature. We confirmed interactions of selected proteins containing Hsp70/Hsp90‐like C termini with dc TPR proteins both in vitro and in situ . Analysis of interactions of 10‐amino‐acid peptides corresponding to the C termini of identified proteins with dc TPR proteins revealed significant differences in binding strength between various peptides. We propose a hierarchical mode of interaction within the dc TPR protein network. These findings describe a novel dc TPR protein interaction networks and provide a rationale for selective regulation of protein–protein interactions within this network.

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Chaperoning steroidal physiology: Lessons from mouse genetic models of Hsp90 and its cochaperones

Cited by 86 publications

References 100 publications

Interplay between diet-induced obesity and chronic stress in mice: potential role of FKBP51

Interplay between diet-induced obesity and chronic stress in mice: potential role of FKBP51

Structural and functional basis of protein phosphatase 5 substrate specificity

In silico identification and biochemical characterization of the human dicarboxylate clamp TPR protein interaction network

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