[PDF] Estrogen Receptor Antagonists Are Anti-Cryptococcal Agents That Directly Bind EF Hand Proteins and Synergize with Fluconazole In Vivo. by Butts, Arielle; Koselny, Kristy; Chabrier-Rosello, Yeissa; Semighini, Camile P.; Brown, Jessica C. S.; Wang, Xuying; Annadurai, Sivakumar; DiDone, Louis; Tabroff, Julie; Childers, Wayne E.; Abou-Gharbia, Magid; Wellington, Melanie; Cardenas, Maria E.; Madhani, Hiten D.; Heitman, Joseph; Krysan, Damian J. - eBookmela

Estrogen Receptor Antagonists Are Anti-Cryptococcal Agents That Directly Bind EF Hand Proteins and Synergize with Fluconazole In Vivo. by Butts, Arielle; Koselny, Kristy; Chabrier-Rosello, Yeissa; Semighini, Camile P.; Brown, Jessica C. S.; Wang, Xuying; Annadurai, Sivakumar; DiDone, Louis; Tabroff, Julie; Childers, Wayne E.; Abou-Gharbia, Magid; Wellington, Melanie; Cardenas, Maria E.; Madhani, Hiten D.; Heitman, Joseph; Krysan, Damian J.

Estrogen Receptor Antagonists Are Anti-Cryptococcal Agents That Directly Bind EF Hand Proteins and Synergize with Fluconazole In Vivo.                                  by    Butts, Arielle; Koselny, Kristy; Chabrier-Rosello, Yeissa; Semighini, Camile P.; Brown, Jessica C. S.; Wang, Xuying; Annadurai, Sivakumar; DiDone, Louis; Tabroff, Julie; Childers, Wayne E.; Abou-Gharbia, Magid; Wellington, Melanie; Cardenas, Maria E.; Madhani, Hiten D.; Heitman, Joseph; Krysan, Damian J.
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Author: Butts, Arielle, Koselny, Kristy, Chabrier-Rosello, Yeissa, Semighini, Camile P., Brown, Jessica C. S., Wang, Xuying, Annadurai, Sivakumar, DiDone, Louis, Tabroff, Julie, Childers, Wayne E., Abou-Gharbia, Magid, Wellington, Melanie, Cardenas, Maria E., Madhani, Hiten D., Heitman, Joseph, Krysan, Damian J.

Added by: jake

Added Date: 2014-10-24

Language: eng

Collections: pubmed, journals

ISSN Number: 2150-7511 (Electronic)

Pages Count: 300

PPI Count: 300

PDF Count: 1

Total Size: 12.44 MB

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Volume: 5

Contributor: American Society for Microbiology (ASM)

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Estrogen Receptor Antagonists Are Anti-Cryptococcal Agents That Directly Bind EF Hand Proteins and Synergize with Fluconazole In Vivo.                                  by    Butts, Arielle; Koselny, Kristy; Chabrier-Rosello, Yeissa; Semighini, Camile P.; Brown, Jessica C. S.; Wang, Xuying; Annadurai, Sivakumar; DiDone, Louis; Tabroff, Julie; Childers, Wayne E.; Abou-Gharbia, Magid; Wellington, Melanie; Cardenas, Maria E.; Madhani, Hiten D.; Heitman, Joseph; Krysan, Damian J.

July 10, 2020

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Estrogen Receptor Antagonists Are Anti-Cryptococcal Agents That Directly Bind EF Hand Proteins and Synergize with Fluconazole In Vivo.                                  by    Butts, Arielle; Koselny, Kristy; Chabrier-Rosello, Yeissa; Semighini, Camile P.; Brown, Jessica C. S.; Wang, Xuying; Annadurai, Sivakumar; DiDone, Louis; Tabroff, Julie; Childers, Wayne E.; Abou-Gharbia, Magid; Wellington, Melanie; Cardenas, Maria E.; Madhani, Hiten D.; Heitman, Joseph; Krysan, Damian J.

July 10, 2020

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This article is from mBio, volume 5.

Abstract

Cryptococcosis is an infectious disease of global significance for which new therapies are needed. Repurposing previously developed drugs for new indications can expedite the translation of new therapies from bench to beside. Here, we characterized the anti-cryptococcal activity and antifungal mechanism of estrogen receptor antagonists related to the breast cancer drugs tamoxifen and toremifene. Tamoxifen and toremifene are fungicidal and synergize with fluconazole and amphotericin B in vitro. In a mouse model of disseminated cryptococcosis, tamoxifen at concentrations achievable in humans combines with fluconazole to decrease brain burden by ~1 log10. In addition, these drugs inhibit the growth of Cryptococcus neoformans within macrophages, a niche not accessible by current antifungal drugs. Toremifene and tamoxifen directly bind to the essential EF hand protein calmodulin, as determined by thermal shift assays with purified C. neoformans calmodulin (Cam1), prevent Cam1 from binding to its well-characterized substrate calcineurin (Cna1), and block Cna1 activation. In whole cells, toremifene and tamoxifen block the calcineurin-dependent nuclear localization of the transcription factor Crz1. A large-scale chemical genetic screen with a library of C. neoformans deletion mutants identified a second EF hand-containing protein, which we have named calmodulin-like protein 1 (CNAG_05655), as a potential target, and further analysis showed that toremifene directly binds Cml1 and modulates its ability to bind and activate Cna1. Importantly, tamoxifen analogs (idoxifene and methylene-idoxifene) with increased calmodulin antagonism display improved anti-cryptococcal activity, indicating that calmodulin inhibition can be used to guide a systematic optimization of the anti-cryptococcal activity of the triphenylethylene scaffold.

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