Discovery and Characterization of an Inhibitor of Glucosylceramide Synthase

Richards, Steven; Larson, Christopher J.; Koltun, Elena S.; Hanel, Art; Chan, Vicky; Nachtigall, Jason; Harrison, Amanda; Aay, Naing; Du, Hongwang; Arcalas, Arlyn; Galan, Adam; Zhang, Jeff; Zhang, Wentao; Won, Kwang‐Ai; Tam, Danny; Qian, Fawn; Wang, Tao; Finn, Patricia D.; Ogilvie, Kathy; Rosen, Jon; Aoyama, Ron; Płonowski, Artur; Cancilla, Belinda; Bentzien, Frauke; Yakes, Michael; Mohan, Raju; Lamb, Peter; Nuss, John M.; Kearney, Patrick C.

doi:10.1021/jm300122u

Cited by 19 publications

(21 citation statements)

References 22 publications

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“…Targeting GCS, due to its central role in the glycosphingolipid synthesis pathway, has emerged as a novel approach for treating metabolic diseases such as Gaucher, Niemann-Pick, and diabetes. In this context, several GCS inhibitors are in clinical use or under development, including miglustat, PDMP, and EXEL-0346 among others (43)(44)(45). Recently, it has been reported that GCS inhibition improved sorafenib effectiveness in vitro and in vivo in experimental hepatocellular carcinoma, recovering drug sensitivity of sorafenib-resistant tumors in mice (46).…”

Section: Discussionmentioning

confidence: 99%

Orthoxenografts of Testicular Germ Cell Tumors Demonstrate Genomic Changes Associated with Cisplatin Resistance and Identify PDMP as a Resensitizing Agent

Piulats

Vidal

García‐Rodríguez

et al. 2018

Clinical Cancer Research

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To investigate the genetic basis of cisplatin resistance as efficacy of cisplatin-based chemotherapy in the treatment of distinct malignancies is often hampered by intrinsic or acquired drug resistance of tumor cells. We produced 14 orthoxenograft transplanting human nonseminomatous testicular germ cell tumors (TGCT) in mice, keeping the primary tumor features in terms of genotype, phenotype, and sensitivity to cisplatin. Chromosomal and genetic alterations were evaluated in matched cisplatin-sensitive and their counterpart orthoxenografts that developed resistance to cisplatin in nude mice. Comparative genomic hybridization analyses of four matched orthoxenografts identified recurrent chromosomal rearrangements across cisplatin-resistant tumors in three of them, showing gains at 9q32-q33.1 region. We found a clinical correlation between the presence of 9q32-q33.1 gains in cisplatin-refractory patients and poorer overall survival (OS) in metastatic germ cell tumors. We studied the expression profile of the 60 genes located at that genomic region. and were the only two genes deregulated in resistant tumors harboring the 9q32-q33.1 gain. Moreover, other four genes ( and ) were deregulated in all five resistant tumors independently of the 9q32-q33.1 amplification. RT-PCRs in tumors and functional analyses in () indicate that the influence of 9q32-q33.1 genes in cisplatin resistance can be driven by either up- or downregulation. We focused on glucosylceramide synthase (GCS) to demonstrate that the GCS inhibitor DL-threo-PDMP resensitizes cisplatin-resistant germline-derived orthoxenografts to cisplatin. Orthoxenografts can be used preclinically not only to test the efficiency of drugs but also to identify prognosis markers and gene alterations acting as drivers of the acquired cisplatin resistance. .

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Section: Discussionmentioning

confidence: 99%

Orthoxenografts of Testicular Germ Cell Tumors Demonstrate Genomic Changes Associated with Cisplatin Resistance and Identify PDMP as a Resensitizing Agent

Piulats

Vidal

García‐Rodríguez

et al. 2018

Clinical Cancer Research

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“…In this molecule, the introduction of at rifluoromethoxy substituent into the p-position of the phenyl group conferred af ivefold reduction in CYP3A4 inhibitory potency relative to that of the Ha nalogue. [26] The synthesis of 22 is shown in Scheme2,w ith the final step relying upon the condensation of AA 28 with amine 29. [26] The synthesis was initiated by reacting 4-(trifluoromethoxy)phenylacetonitrile (23)w ith 1,2-dibromoethane through as equence of intermolecular alkylation and intramolecular cyclization, which was performed in the presence of NaH in THF,t og enerate the cyclopropylr ing.…”

Section: General Aspects Of Asymmetric Synthesis Of Tailor-made Aasmentioning

confidence: 99%

“…[26] The synthesis of 22 is shown in Scheme2,w ith the final step relying upon the condensation of AA 28 with amine 29. [26] The synthesis was initiated by reacting 4-(trifluoromethoxy)phenylacetonitrile (23)w ith 1,2-dibromoethane through as equence of intermolecular alkylation and intramolecular cyclization, which was performed in the presence of NaH in THF,t og enerate the cyclopropylr ing. Hydrolysis of the cyano group with NaOH at 120 8Cf or 48 hr esulted in acid 24.…”

Section: General Aspects Of Asymmetric Synthesis Of Tailor-made Aasmentioning

confidence: 99%

Tailor‐Made Amino Acids and Fluorinated Motifs as Prominent Traits in Modern Pharmaceuticals

Mei

Han

White

et al. 2020

Chemistry A European J

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Structural analysis of modern pharmaceutical practices allows for the identification of two rapidly growing trends: the introduction of tailor‐made amino acids and the exploitation of fluorinated motifs. Curiously, the former represents one of the most ubiquitous classes of naturally occurring compounds, whereas the latter is the most xenobiotic and comprised virtually entirely of man‐made derivatives. Herein, 39 selected compounds, featuring both of these traits in the same molecule, are profiled. The total synthesis, source of the corresponding amino acids and fluorinated residues, and medicinal chemistry aspects and biological properties of the molecules are discussed.

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“…GZ 161, optimized from a large series of carbamates ( 55 ), was shown to reduce brain glucosylceramide levels, improve brain neuropathology, and extend lifespan in the K14 mouse model of Gaucher disease type 2 ( 56 ). A series of lipophilic dipeptides was optimized to yield analogs with low nanomolar inhibition of glucosylceramide synthase and good stability to metabolism by mouse liver microsomes ( 57,58 ). One compound (EXEL-0346) was able to reduce the levels of glucosylceramide, lactosylceramide, and GM3 in the livers of mice after oral dosing.…”

Section: Newer Inhibitorsmentioning

confidence: 99%

The development and use of small molecule inhibitors of glycosphingolipid metabolism for lysosomal storage diseases

Shayman

Larsen

2014

Journal of Lipid Research

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Discovery and Characterization of an Inhibitor of Glucosylceramide Synthase

Cited by 19 publications

References 22 publications

Orthoxenografts of Testicular Germ Cell Tumors Demonstrate Genomic Changes Associated with Cisplatin Resistance and Identify PDMP as a Resensitizing Agent

Orthoxenografts of Testicular Germ Cell Tumors Demonstrate Genomic Changes Associated with Cisplatin Resistance and Identify PDMP as a Resensitizing Agent

Tailor‐Made Amino Acids and Fluorinated Motifs as Prominent Traits in Modern Pharmaceuticals

The development and use of small molecule inhibitors of glycosphingolipid metabolism for lysosomal storage diseases

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