Mechanism of the Tissue-Specific Action of the Selective Androgen Receptor Modulator S-101479

Furuya, Kazuyuki; Yamamoto, Norio; Ohyabu, Yuki; Morikyu, Teruyuki; Ishige, Hirohide; Albers, M.; Endo, Yasuhisa

doi:10.1248/bpb.b12-00885

Cited by 34 publications

(22 citation statements)

References 56 publications

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“…15 • SARMs with tetrahydroquinolinone core structure, such as S-40503, 15 S-101479, 21 and S-49288. 22 • SARMs with indole core structure, such as RAD35010 15 and Ly2452473. 21 • SARMs with steroidal core structure, such as MK-0773, 15,23 Cl-4-AS-1, TMF-4AS-1, YK-11, and S-42.…”

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confidence: 99%

Human in vivo metabolism study of LGD‐4033

Fragkaki

Sakellariou

Kiousi

et al. 2018

Drug Testing and Analysis

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Selective androgen receptor modulators (SARMs) are an emerging class of therapeutics targeted to cachexia, sarcopenia, and hypogonadism treatment. LGD-4033 is a SARM which has been included on the Prohibited List annually released by the World Anti-Doping Agency (WADA). The aim of the present work was the investigation of the metabolism of LGD-4033 in a human excretion study after administration of an LGD-4033 supplement, the determination of the metabolites' excretion profiles with special interest in the determination of its long-term metabolites, and the comparison of the excretion time of the phase I and phase II metabolites. The results were also compared to those derived from previous LGD-4033 studies concerning both in vitro and in vivo experiments. Supplement containing LGD-4033 was administered to one human male volunteer and urine samples were collected up to almost 21 days. Analysis of the hydrolyzed (with β-glucuronidase) as well as of the non-hydrolyzed samples was performed using liquid chromatography-high resolution mass spectrometry (LC-HRMS) in negative ionization mode and revealed that, in both cases, the two isomers of the dihydroxylated metabolite (M5) were preferred target metabolites. The glucoconjugated parent LGD-4033 and its gluco-conjugated metabolites M1 and M2 can be also considered as useful target analytes in non-hydrolyzed samples. The study also presents two trihydroxylated metabolites (M6) identified for the first time in human urine; one of them was recently reported in an LGD-4033 metabolism study in horse urine and plasma. KEYWORDS human doping, LGD-4033, liquid chromatography-mass spectrometry, SARM, selective androgen receptor modulator

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confidence: 99%

Human in vivo metabolism study of LGD‐4033

Fragkaki

Sakellariou

Kiousi

et al. 2018

Drug Testing and Analysis

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“…7,14,32,35,37 SERMs and SARMS have convincingly demonstrated that small molecules can elicit tissue-or gene-selective effects, and recently, several groups have developed inhibitors that disrupt interactions between NRs and coactivator proteins. 7,14,31,32,35,37,38 For example, the bone-specific actions of the SARM S-101479 are the result of its failure to recruit TIF2, SRC-1, and NCoA3. 38 We have previously described an AR-TIF2 PPI biosensor (PPIB) HCS assay that can be used to screen for compounds that can induce, inhibit the formation of, or disrupt preexisting PPIs between AR and TIF2.…”

Section: Introductionmentioning

confidence: 99%

“…7,14,31,32,35,37,38 For example, the bone-specific actions of the SARM S-101479 are the result of its failure to recruit TIF2, SRC-1, and NCoA3. 38 We have previously described an AR-TIF2 PPI biosensor (PPIB) HCS assay that can be used to screen for compounds that can induce, inhibit the formation of, or disrupt preexisting PPIs between AR and TIF2. 20 However, the previous AR-TIF2 PPIB studies were conducted in the U-2 OS osteosarcoma cell line, and we wanted to determine whether the assay might perform differently when performed in a CaP cell background and whether AR-TIF2 PPI inhibitor or disruptor hits would behave differently.…”

Section: Introductionmentioning

confidence: 99%

Reconfiguring the AR-TIF2 Protein–Protein Interaction HCS Assay in Prostate Cancer Cells and Characterizing the Hits from a LOPAC Screen

Fancher

Hua

Camarco

et al. 2016

ASSAY and Drug Development Technologies

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The continued activation of androgen receptor (AR) transcription and elevated expression of AR and transcriptional intermediary factor 2 (TIF2) coactivator observed in prostate cancer (CaP) recurrence and the development of castration-resistant CaP (CRPC) support a screening strategy for small-molecule inhibitors of AR-TIF2 protein-protein interactions (PPIs) to find new drug candidates. Small molecules can elicit tissue selective effects, because the cells of distinct tissues express different levels and cohorts of coregulatory proteins. We reconfigured the AR-TIF2 PPI biosensor (PPIB) assay in the PC-3 CaP cell line to determine whether AR modulators and hits from an AR-TIF2 PPIB screen conducted in U-2 OS cells would behave differently in the CaP cell background. Although we did not observe any significant differences in the compound responses between the assay performed in osteosarcoma and CaP cells, the U-2 OS AR-TIF2 PPIB assay would be more amenable to screening, because both the virus and cell culture demands are lower. We implemented a testing paradigm of counter-screens and secondary hit characterization assays that allowed us to identify and deprioritize hits that inhibited/disrupted AR-TIF2 PPIs and AR transcriptional activation (AR-TA) through antagonism of AR ligand binding or by non-specifically blocking nuclear receptor trafficking. Since AR-TIF2 PPI inhibitor/disruptor molecules act distally to AR ligand binding, they have the potential to modulate AR-TA in a cell-specific manner that is distinct from existing anti-androgen drugs, and to overcome the development of resistance to AR antagonism. We anticipate that the application of this testing paradigm to characterize the hits from an AR-TIF2 PPI high-content screening campaign will enable us to prioritize the AR-TIF2 PPI inhibitor/disruptor leads that have potential to be developed into novel therapeutics for CaP and CRPC.

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“…A recent report has demonstrated that the SARM, S-101479, which shows low N/C interaction, induced recruitment of fewer cofactors than DHT. 34) This observation suggests that the difference in Fst mRNA regulation between YK11 and DHT stems from cofactor recruitment differences.…”

Section: Discussionmentioning

confidence: 98%

Selective Androgen Receptor Modulator, YK11, Regulates Myogenic Differentiation of C2C12 Myoblasts by Follistatin Expression

Kanno

Ota

Someya

et al. 2013

Biological & Pharmaceutical Bulletin

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The myogenic differentiation of C2C12 myoblast cells is induced by the novel androgen receptor (AR) partial agonist, (17α,20E)-17,20-[(1-methoxyethylidene)bis-(oxy)]-3-oxo-19-norpregna-4,20-diene-21-carboxylic acid methyl ester (YK11), as well as by dihydrotestosterone (DHT). YK11 is a selective androgen receptor modulator (SARM), which activates AR without the N/C interaction. In this study, we further investigated the mechanism by which YK11 induces myogenic differentiation of C2C12 cells. The induction of key myogenic regulatory factors (MRFs), such as myogenic differentiation factor (MyoD), myogenic factor 5 (Myf5) and myogenin, was more significant in the presence of YK11 than in the presence of DHT. YK11 treatment of C2C12 cells, but not DHT, induced the expression of follistatin (Fst), and the YK11-mediated myogenic differentiation was reversed by anti-Fst antibody. These results suggest that the induction of Fst is important for the anabolic effect of YK11.

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Mechanism of the Tissue-Specific Action of the Selective Androgen Receptor Modulator S-101479

Cited by 34 publications

References 56 publications

Human in vivo metabolism study of LGD‐4033

Human in vivo metabolism study of LGD‐4033

Reconfiguring the AR-TIF2 Protein–Protein Interaction HCS Assay in Prostate Cancer Cells and Characterizing the Hits from a LOPAC Screen

Selective Androgen Receptor Modulator, YK11, Regulates Myogenic Differentiation of C2C12 Myoblasts by Follistatin Expression

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