# Strategic selection of MDM2 inhibitors enhances the efficacy of FAK inhibition in mesothelioma based on TP53 genotype

**Authors:** Xuerao Ning, Thảo Thi Thanh Nguyễn, Takao Morinaga, Yuji Tada, Hideaki Shimada, Kenzo Hiroshima, Naoto Yamaguchi, Masatoshi Tagawa, Zu Ye, Zu Ye, Zu Ye, Zu Ye

PMC · DOI: 10.1371/journal.pone.0343551 · PLOS One · 2026-02-23

## TL;DR

This study shows that combining FAK and MDM2 inhibitors can effectively treat mesothelioma, but the choice of MDM2 inhibitor depends on the TP53 genotype of the tumor.

## Contribution

The study demonstrates that the efficacy of FAK and MDM2 inhibitor combinations in mesothelioma depends on TP53 genotype and MDM2 inhibitor type.

## Key findings

- Defactinib inhibits cell growth and induces FAK dephosphorylation regardless of TP53 genotype.
- Nutlin-3a synergizes with defactinib in wild-type TP53 cells but antagonizes in mutated TP53 cells.
- RITA retains synergistic activity with defactinib in mutated TP53 cells.

## Abstract

Mesothelioma has characteristic genetic changes including inactivation of neurofibromatosis type 2 (NF2) and deletion of the INK4A/ARF region. Cells deficient of NF2 protein (MERLIN) depend on focal adhesion kinase (FAK) for cell adhesion and FAK inhibitors suppress the cell growth. The INK4A/ARF deletion activates MDM2 functions which ubiquitinate and degrade p53, and consequently the cellular p53 levels decrease. The deletion therefore induces loss of p53 functions although a majority of mesothelioma has wild-type TP53 genotype. An MDM2 inhibitor which blocked the ubiquitination increased p53 levels, restored p53 functions and facilitated cell growth arrest. Moreover, FAK and p53 expressions were reciprocally regulated. We examined growth suppressive effects of a FAK inhibitor, defactinib, and MDM2 inhibitors, nutlin-3a and reactivation of p53 and induction of tumor cell apoptosis (RITA), with representative wild-type and mutated TP53 mesothelioma and investigated molecular changes induced by the agents. We analyzed possible combinatory effects of the inhibitors and molecular changes caused by the combination. Our study showed that defactinib inhibited cell growth and induced FAK dephosphorylation irrespective of the TP53 genotype, and that the inhibited FAK phosphorylation was not associated with MERLIN levels or with p53 up-regulation, but linked with AKT dephosphorylation. Nutlin-3a preferentially suppressed growth of wild-type TP53 cells and augment p53 expression without DNA damage, whereas RITA-mediated p53 up-regulation was linked with the damage. A combination of defactinib and the MDM2 inhibitors showed that nutlin-3a showed synergistic/additive effects in wild-type and antagonistic effects in mutated TP53 cells, whereas RITA retained synergistic activity in mutated TP53 cells. These results suggest that the therapeutic success of combined FAK and MDM2 inhibition in mesothelioma depends on the precise matching of MDM2 inhibitors with the TP53 genotypes, and highlight the need for genotype-based selection of MDM2 inhibitors.

## Linked entities

- **Genes:** NF2 (NF2, moesin-ezrin-radixin like (MERLIN) tumor suppressor) [NCBI Gene 4771], Cdkn2a (cyclin dependent kinase inhibitor 2A) [NCBI Gene 12578], MDM2 (MDM2 proto-oncogene) [NCBI Gene 4193], TP53 (tumor protein p53) [NCBI Gene 7157], TP53 (tumor protein p53) [NCBI Gene 7157], PTK2 (protein tyrosine kinase 2) [NCBI Gene 5747], AKT1 (AKT serine/threonine kinase 1) [NCBI Gene 207]
- **Proteins:** Nf2 (neurofibromin 2), PTK2 (protein tyrosine kinase 2), TP53 (tumor protein p53), MDM2 (MDM2 proto-oncogene), AKT1 (AKT serine/threonine kinase 1)
- **Chemicals:** defactinib (PubChem CID 25117126), nutlin-3a (PubChem CID 11433190)
- **Diseases:** mesothelioma (MONDO:0005065)

## Full-text entities

- **Genes:** RITA1 (RBPJ interacting and tubulin associated 1) [NCBI Gene 84934] {aka C12orf52, RITA}, p53-ps (Wistar clone pR53P1 p53 pseudogene) [NCBI Gene 301300], MDM2 (MDM2 proto-oncogene) [NCBI Gene 4193] {aka ACTFS, HDMX, LSKB, hdm2}, Casp9 (caspase 9) [NCBI Gene 12371] {aka APAF-3, CASP-9, Caspase-9, ICE-LAP6, Mch6}, Parp1 (poly (ADP-ribose) polymerase family, member 1) [NCBI Gene 11545] {aka 5830444G22Rik, ARTD1, Adprp, Adprt1, PARP, PPOL}, Mdm2 (MDM2 proto-oncogene) [NCBI Gene 17246] {aka 1700007J15Rik, Mdm-2}, MSLN (mesothelin) [NCBI Gene 10232] {aka MPF, SMRP}, PARP1 (poly(ADP-ribose) polymerase 1) [NCBI Gene 142] {aka ADPRT, ADPRT 1, ADPRT1, ARTD1, PARP, PARP-1}, ATM (ATM serine/threonine kinase) [NCBI Gene 472] {aka AT1, ATA, ATC, ATD, ATDC, ATE}, AKT1 (AKT serine/threonine kinase 1) [NCBI Gene 207] {aka AKT, PKB, PKB-ALPHA, PRKBA, RAC, RAC-ALPHA}, ZNF331 (zinc finger protein 331) [NCBI Gene 55422] {aka RITA, ZNF361, ZNF463}, VEGFA (vascular endothelial growth factor A) [NCBI Gene 7422] {aka L-VEGF, MVCD1, VEGF, VPF}, Trp53-ps (transformation related protein 53, pseudogene) [NCBI Gene 22060], CHEK2 (checkpoint kinase 2) [NCBI Gene 11200] {aka CDS1, CHK2, HuCds1, LFS2, PP1425, RAD53}, TP53 (tumor protein p53) [NCBI Gene 7157] {aka BCC7, BMFS5, LFS1, P53, TRP53}, CDKN2A (cyclin dependent kinase inhibitor 2A) [NCBI Gene 1029] {aka ARF, CAI2, CDK4I, CDKN2, CMM2, INK4}, Ptk2 (PTK2 protein tyrosine kinase 2) [NCBI Gene 14083] {aka FADK 1, FAK, FRNK, Fadk, p125FAK}, SLURP1 (secreted LY6/PLAUR domain containing 1) [NCBI Gene 57152] {aka ANUP, ARS, ArsB, LY6-MT, LY6LS, MDM}, CASP9 (caspase 9) [NCBI Gene 842] {aka APAF-3, APAF3, ICE-LAP6, MCH6, PPP1R56}, H2AX (H2A.X variant histone) [NCBI Gene 3014] {aka H2A.X, H2A/X, H2AFX}, NF2 (NF2, moesin-ezrin-radixin like (MERLIN) tumor suppressor) [NCBI Gene 4771] {aka ACN, BANF, SCH, SWNV, merlin-1}, TFRC (transferrin receptor) [NCBI Gene 7037] {aka CD71, IMD46, T9, TFR, TFR1, TR}, PTK2 (protein tyrosine kinase 2) [NCBI Gene 5747] {aka FADK, FADK 1, FAK, FAK1, FRNK, PPP1R71}, H3P16 (H3 histone pseudogene 16) [NCBI Gene 644914] {aka H3.6, H3F3AP6, p21}, CDH1 (cadherin 1) [NCBI Gene 999] {aka Arc-1, BCDS1, CD324, CDHE, ECAD, LCAM}, PTK2B (protein tyrosine kinase 2 beta) [NCBI Gene 2185] {aka CADTK, CAKB, FADK2, FAK2, PKB, PTK}, H2ax (H2A.X variant histone) [NCBI Gene 15270] {aka H2A.X, H2afx, Hist5-2ax, gammaH2ax}, Nf2 (neurofibromin 2) [NCBI Gene 18016] {aka merlin}, SQSTM1 (sequestosome 1) [NCBI Gene 8878] {aka A170, DMRV, EBIAP, FTDALS3, NADGP, OSIL}, CD274 (CD274 molecule) [NCBI Gene 29126] {aka ADMIO5, B7-H, B7H1, PD-L1, PDCD1L1, PDCD1LG1}, Akt1 (Akt serine/threonine kinase 1) [NCBI Gene 11651] {aka Akt, LTR-akt, PKB, PKB/Akt, PKBalpha, Rac}
- **Diseases:** lung cancer (MESH:D008175), Cancer (MESH:D009369), growth retardation (MESH:D006130), non-small cell lung cancer (MESH:D002289), lung squamous cell carcinoma (MESH:D002294), Malignant mesothelioma (MESH:D000086002), Epithelioid (MESH:D012509), pleural effusion (MESH:D010996), cytotoxic (MESH:D064420), sarcomatoid (MESH:D002292), Mesothelioma (MESH:D008654)
- **Chemicals:** NSC 652287 (MESH:C118989), Defactinib (MESH:C584510), platinum (MESH:D010984), trypan blue (MESH:D014343), idasanutlin (MESH:C586849), sodium dodecyl sulfate (MESH:D012967), pemetrexed (MESH:D000068437), MSTO-211H (-), VS-4718 (MESH:C559284), Nutlin-3a (MESH:C482205)
- **Species:** Mycoplasma (genus) [taxon 2093], Homo sapiens (human, species) [taxon 9606]
- **Mutations:** R273S, G245S
- **Cell lines:** JMN-1B — Homo sapiens (Human), Pleural biphasic mesothelioma, Cancer cell line (CVCL_M006), NCI-H2052 — Homo sapiens (Human), Pleural sarcomatoid mesothelioma, Cancer cell line (CVCL_1518), MSTO-211H — Homo sapiens (Human), Pleural biphasic mesothelioma, Cancer cell line (CVCL_1430), EHMES-10 — Homo sapiens (Human), Pleural malignant mesothelioma, Cancer cell line (CVCL_M208), EHMES-1 — Homo sapiens (Human), Pleural malignant mesothelioma, Cancer cell line (CVCL_M207), NCI-226 — Homo sapiens (Human), Pleural epithelioid mesothelioma, Cancer cell line (CVCL_1544), Met-5A — Homo sapiens (Human), Transformed cell line (CVCL_3749), H2452 — Homo sapiens (Human), Pleural biphasic mesothelioma, Cancer cell line (CVCL_1553), H28 — Homo sapiens (Human), Pleural malignant mesothelioma, Cancer cell line (CVCL_1555)

## Full text

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## Figures

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## References

40 references — full list in the complete paper: https://tomesphere.com/paper/PMC12928570/full.md

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Source: https://tomesphere.com/paper/PMC12928570