A phase I study of the HDM2 antagonist SAR405838 combined with the MEK inhibitor pimasertib in patients with advanced solid tumours

Weger, Vincent A. de; Jonge, Maja de; Langenberg, Marlies H.G.; Schellens, Jan H.M.; Lolkema, Martijn P.; Varga, Andréa; Demers, Brigitte; Thomas, Koruth; Hsu, Karl; Tuffal, Gilles; Goodstal, Samantha; Macé, Sandrine; Deutsch, Éric

doi:10.1038/s41416-018-0355-8

Cited by 45 publications

(32 citation statements)

References 19 publications

(22 reference statements)

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“…The most frequently occurring adverse events observed were diarrhoea (81%), blood creatine phosphokinase (77%), nausea (62%) and vomiting (62%). This study indicated that the safety profile of SAR405838 combined with pimasertib was consistent with the safety profiles of both the drugs (de Weger et al, 2019).…”

Section: Sar405838supporting

confidence: 73%

Targeting Mouse Double Minute 2: Current Concepts in DNA Damage Repair and Therapeutic Approaches in Cancer

Peng

Lang

et al. 2020

Front. Pharmacol.

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Defects in DNA damage repair may cause genome instability and cancer development. The tumor suppressor gene p53 regulates cell cycle arrest to allow time for DNA repair. The oncoprotein mouse double minute 2 (MDM2) promotes cell survival, proliferation, invasion, and therapeutic resistance in many types of cancer. The major role of MDM2 is to inhibit p53 activity and promote its degradation. In this review, we describe the influence of MDM2 on genomic instability, the role of MDM2 on releasing p53 and binding DNA repair proteins to inhibit repair, and the regulation network of MDM2 including its transcriptional modifications, protein stability, and localization following DNA damage in genome integrity maintenance and in MDM2-p53 axis control. We also discuss p53-dependent and p53 independent oncogenic function of MDM2 and the outcomes of clinical trials that have been used with clinical inhibitors targeting p53-MDM2 to treat certain cancers.

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Section: Sar405838supporting

confidence: 73%

Targeting Mouse Double Minute 2: Current Concepts in DNA Damage Repair and Therapeutic Approaches in Cancer

Peng

Lang

et al. 2020

Front. Pharmacol.

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“…The components of this pathway play a very important role in the genesis of cancer, which has been reported many times before [183,184,185]. p53 and the MAPK components are the most frequently mutated tumor suppressor and oncogene pathways in human cancers [81]. For this reason, there is a great potential in simultaneous targeting of these two pathways to provide useful therapeutic approaches.…”

Section: Drug Combinations For the Supporting Of Anti-cancer Activmentioning

confidence: 99%

Helping the Released Guardian: Drug Combinations for Supporting the Anticancer Activity of HDM2 (MDM2) Antagonists

Kocik

Machula

Wiśniewska

et al. 2019

Cancers

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The protein p53, known as the “Guardian of the Genome”, plays an important role in maintaining DNA integrity, providing protection against cancer-promoting mutations. Dysfunction of p53 is observed in almost every cancer, with 50% of cases bearing loss-of-function mutations/deletions in the TP53 gene. In the remaining 50% of cases the overexpression of HDM2 (mouse double minute 2, human homolog) protein, which is a natural inhibitor of p53, is the most common way of keeping p53 inactive. Disruption of HDM2-p53 interaction with the use of HDM2 antagonists leads to the release of p53 and expression of its target genes, engaged in the induction of cell cycle arrest, DNA repair, senescence, and apoptosis. The induction of apoptosis, however, is restricted to only a handful of p53wt cells, and, generally, cancer cells treated with HDM2 antagonists are not efficiently eliminated. For this reason, HDM2 antagonists were tested in combinations with multiple other therapeutics in a search for synergy that would enhance the cancer eradication. This manuscript aims at reviewing the recent progress in developing strategies of combined cancer treatment with the use of HDM2 antagonists.

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“…Development of small molecules disrupting the MDM2–P53 interactions has been highly pursued from academia to industry in recent years 5 , 9 , 10 , 11 , 12 , 13 , 14 . Some of these inhibitors including DS-3032 (also known as Milademetan, DS-3032b) 15 , 16 , NVP-CGM097 17 , 18 , 19 , SAR405838 20 , 21 , 22 , RG7112 23 , 24 , MK-8242 25 , 26 , RG7388 27 and AMG 232 28 , 29 , 30 ( Fig. 2 ) are under clinical evaluation for anticancer treatment.…”

Section: Introductionmentioning

confidence: 99%

Small-molecule MDM2/X inhibitors and PROTAC degraders for cancer therapy: advances and perspectives

Fang

Liao

2020

Acta Pharmaceutica Sinica B

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Blocking the MDM2/X–P53 protein–protein interaction has been widely recognized as an attractive therapeutic strategy for the treatment of cancers. Numerous small-molecule MDM2 inhibitors have been reported since the release of the structure of the MDM2–P53 interaction in 1996, SAR405838, NVP-CGM097, MK-8242, RG7112, RG7388, DS-3032b, and AMG232 currently undergo clinical evaluation for cancer therapy. This review is intended to provide a comprehensive and updated overview of MDM2 inhibitors and proteolysis targeting chimera (PROTAC) degraders with a particular focus on how these inhibitors or degraders are identified from starting points, strategies employed, structure–activity relationship (SAR) studies, binding modes or co-crystal structures, biochemical data, mechanistic studies, and preclinical/clinical studies. Moreover, we briefly discuss the challenges of designing MDM2/X inhibitors for cancer therapy such as dual MDM2/X inhibition, acquired resistance and toxicity of P53 activation as well as future directions.

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A phase I study of the HDM2 antagonist SAR405838 combined with the MEK inhibitor pimasertib in patients with advanced solid tumours

Cited by 45 publications

References 19 publications

Targeting Mouse Double Minute 2: Current Concepts in DNA Damage Repair and Therapeutic Approaches in Cancer

Targeting Mouse Double Minute 2: Current Concepts in DNA Damage Repair and Therapeutic Approaches in Cancer

Helping the Released Guardian: Drug Combinations for Supporting the Anticancer Activity of HDM2 (MDM2) Antagonists

Small-molecule MDM2/X inhibitors and PROTAC degraders for cancer therapy: advances and perspectives

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