The hsp90-FKBP52 Complex Links the Mineralocorticoid Receptor to Motor Proteins and Persists Bound to the Receptor in Early Nuclear Events

Galigniana, Mario D.; Erlejman, Alejandra G.; Monte, Martín; Gómez-Sánchez, Celso E.; Piwien-Pilipuk, Graciela

doi:10.1128/mcb.01190-09

Cited by 136 publications

(150 citation statements)

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“…after the overexpression of the p50/dynactin-2 subunit of dynactin [36]. In all these cases, the nuclear localization of the receptor was not fully inhibited, but it was only impaired (Figure 2-B).…”

Section: The Hsp90•fkbp52•dynein/dynactin Molecular Machinery Of Tranmentioning

confidence: 85%

“…This suggests the existence of two mechanisms of transport, a rapid Hsp90•FKBP52•dynein complex-dependent mechanism ( Figure 2-B, blue continuous line) and an alternative, slower and heterocomplexindependent mechanism ( Figure 2B, red dotted line), perhaps due to simple diffusion. Importantly, when the nuclear translocation rate of these receptors is impaired, they are highly sensitive to proteasomal degradation [20,36]. The same Hsp90•FKBP52•dynein complex constitutes the molecular machinery responsible for the retrotransport of the proapoptotic factor p53 [65], suggesting that it may play a general role in the retrotransport mechanism of a number of Hsp90-associated factors.…”

Section: The Hsp90•fkbp52•dynein/dynactin Molecular Machinery Of Tranmentioning

confidence: 99%

“…Even though the biological function of these IMMs remains poorly understood, it is accepted that they are not related to immunosuppression, a property that concerns to the smallest members of the family, CyPA and FKBP12 (see [48] for a recent update). Importantly, it was demonstrated that the intermediate chain of the motor protein dynein coimmunoprecipitates with the Hsp90•FKBP52 complex bound to the GR [21,61,63] and MR [36] suggesting that the motor protein powers the retrograde movement of the receptor. Actually, the use of inhibitors of the ATPase activity of dynein and/or the disruption of the complex impairs the retrotransport of the receptor [36,64].…”

Section: The Hsp90•fkbp52•dynein/dynactin Molecular Machinery Of Tranmentioning

confidence: 99%

“…Importantly, it was demonstrated that the intermediate chain of the motor protein dynein coimmunoprecipitates with the Hsp90•FKBP52 complex bound to the GR [21,61,63] and MR [36] suggesting that the motor protein powers the retrograde movement of the receptor. Actually, the use of inhibitors of the ATPase activity of dynein and/or the disruption of the complex impairs the retrotransport of the receptor [36,64]. and Hsp70 (and their associated cochaperone Hsp40) are assembled thanks to the presence of Hop/p60 (heat-shock organizing protein, formerly called p60).…”

Section: The Hsp90•fkbp52•dynein/dynactin Molecular Machinery Of Tranmentioning

confidence: 99%

“…Regardless of their primary localization, however, these receptors (and other nuclear factors) undergo a permanent and dynamic nucleocytoplasmic shuttling. Clearly, such diversity is most likely related to a dissimilar import/export balance, which could be due to the expression balance of TPR-domain immunophilins [36,37], as we will discuss later in this article. The biological relevance of the nucleocytoplasmic shuttling is implied by the fact that the intersection of the predicted interactome for the Hsp90/Hsp70 chaperone machinery and the interactome of steroid receptors represents˜20% of genes whose products are related to intracellular transport and/or nucleocytoplasmic shuttling [38].…”

Section: Introductionmentioning

confidence: 99%

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The Emerging Role of TPR-Domain Immunophilins in the Mechanism of Action of Steroid Receptors

Mazaira

Lagadari

Erlejman

et al. 2014

Nuclear Receptor Research

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Abstract. In the absence of ligand, some members of nuclear receptor family such as corticosteroid receptors are primarily located in the cytoplasm, and they rapidly accumulate in the nucleus upon ligand-binding. Other members of the family such as the estrogen receptor are mostly nuclear. Regardless of their primary location, these oligomeric proteins undergo a dynamic nuclearcytoplasmic shuttling, and their transport through the cytoplasmic compartment has always been assumed to occur in a stochastic manner by simple diffusion. Although heuristic, this oversimplified model has never been demonstrated. Moreover, it has always been assumed that the first step related to receptor activation is the dissociation of the Hsp90-based heterocomplex, a process referred to as 'transformation.' Nonetheless, recent experimental evidence indicates that the chaperone machinery is required for the retrotransport of the receptor throughout the cytoplasm and facilitates its active passage through the nuclear pore. Therefore, transformation is actually a nuclear event. A group of Hsp90-binding cochaperones belonging to the immunophilin family plays a cardinal role not only in the mechanism for receptor movement, but also in nuclear events leading to interactions with nuclear sites of action and the regulation of transcriptional activity. In this article we analyze the importance of molecular chaperones and TPR-domain immunophilins in the molecular mechanism of action of steroid receptors.

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Section: The Hsp90•fkbp52•dynein/dynactin Molecular Machinery Of Tranmentioning

confidence: 85%

Section: The Hsp90•fkbp52•dynein/dynactin Molecular Machinery Of Tranmentioning

confidence: 99%

Section: The Hsp90•fkbp52•dynein/dynactin Molecular Machinery Of Tranmentioning

confidence: 99%

Section: The Hsp90•fkbp52•dynein/dynactin Molecular Machinery Of Tranmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

The Emerging Role of TPR-Domain Immunophilins in the Mechanism of Action of Steroid Receptors

Mazaira

Lagadari

Erlejman

et al. 2014

Nuclear Receptor Research

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The Prospect of FKBP51 as a Drug Target

et al. 2012

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The FK506 binding protein 51 (FKBP51) is best known as an Hsp90-associated co-chaperone that regulates the responsiveness of steroid hormone receptors. In human genetic association studies, FKBP51 has repeatedly been associated with emotion processing and numerous stress-related affective disorders. It has also been implicated in contributing to the glucocorticoid hyposensitivity observed in New World primates. More recently, several research groups have consistently shown a protective effect of FKBP51 knockout or knockdown on stress endocrinology and stress-coping behavior in animal models of depression and anxiety. The principal druggability of FKBP51 is exemplified by the prototypic FKBP ligands FK506 and rapamycin. Moreover, FKBP51 is highly suited for X-ray co-crystallography, which should facilitate the rational drug design of improved FKBP51 ligands. In summary, FKBP51 has emerged as a promising new drug target for stress-related disorders that should be amenable to drug discovery.

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The Multifaceted Mineralocorticoid Receptor

Gómez-Sánchez

2014

Comprehensive Physiology

247

220

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The primary adrenal cortical steroid hormones, aldosterone, and the glucocorticoids cortisol and corticosterone, act through the structurally similar mineralocorticoid (MR) and glucocorticoid receptors (GRs). Aldosterone is crucial for fluid, electrolyte, and hemodynamic homeostasis and tissue repair; the significantly more abundant glucocorticoids are indispensable for energy homeostasis, appropriate responses to stress, and limiting inflammation. Steroid receptors initiate gene transcription for proteins that effect their actions as well as rapid non-genomic effects through classical cell signaling pathways. GR and MR are expressed in many tissues types, often in the same cells, where they interact at molecular and functional levels, at times in synergy, others in opposition. Thus the appropriate balance of MR and GR activation is crucial for homeostasis. MR has the same binding affinity for aldosterone, cortisol, and corticosterone. Glucocorticoids activate MR in most tissues at basal levels and GR at stress levels. Inactivation of cortisol and corticosterone by 11β-HSD2 allows aldosterone to activate MR within aldosterone target cells and limits activation of the GR. Under most conditions, 11β-HSD1 acts as a reductase and activates cortisol/corticosterone, amplifying circulating levels. 11β-HSD1 and MR antagonists mitigate inappropriate activation of MR under conditions of oxidative stress that contributes to the pathophysiology of the cardiometabolic syndrome; however, MR antagonists decrease normal MR/GR functional interactions, a particular concern for neurons mediating cognition, memory, and affect.

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The hsp90-FKBP52 Complex Links the Mineralocorticoid Receptor to Motor Proteins and Persists Bound to the Receptor in Early Nuclear Events

Cited by 136 publications

References 69 publications

The Emerging Role of TPR-Domain Immunophilins in the Mechanism of Action of Steroid Receptors

The Emerging Role of TPR-Domain Immunophilins in the Mechanism of Action of Steroid Receptors

The Prospect of FKBP51 as a Drug Target

The Multifaceted Mineralocorticoid Receptor

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