Patient-derived tumor organoids with p53 mutations, and not wild-type p53, are sensitive to synergistic combination PARP inhibitor treatment

Author:

Rowdo Florencia P. MadorskyORCID,Xiao GuORCID,Khramtsova Galina FORCID,Nguyen JohnORCID,Olopade Olufunmilayo IORCID,Martini RachelORCID,Stonaker BrianORCID,Boateng RichardORCID,Oppong Joseph K.ORCID,Adjei Ernest K.ORCID,Awuah BaffourORCID,Kyei IshmaelORCID,Aitpillah Frances S.ORCID,Adinku Michael O.ORCID,Ankomah KwasiORCID,Osei-Bonsu Ernest B.ORCID,Gyan Kofi K.ORCID,Altorki Nasser K.ORCID,Cheng EstherORCID,Ginter Paula S.ORCID,Hoda SyedORCID,Newman LisaORCID,Elemento OlivierORCID,Davis Melissa B.ORCID,Martin M. LauraORCID,Bargonetti JillORCID

Abstract

AbstractPoly (ADP-ribose) polymerase inhibitors (PARPi) are used for patients withBRCA1/2mutations, but patients with other mutations may benefit from PARPi treatment. Another mutation that is present in more cancers thanBRCA1/2is mutation to theTP53gene. In 2D breast cancer cell lines, mutant p53 (mtp53) proteins tightly associate with replicating DNA and Poly (ADP-ribose) polymerase (PARP) protein. Combination drug treatment with the alkylating agent temozolomide and the PARPi talazoparib kills mtp53 expressing 2D grown breast cancer cell lines. We evaluated the sensitivity to the combination of temozolomide plus PARPi talazoparib treatment to breast and lung cancer patient-derived tumor organoids (PDTOs). The combination of the two drugs was synergistic for a cytotoxic response in PDTOs with mtp53 but not for PDTOs with wtp53. The combination of talazoparib and temozolomide induced more DNA double-strand breaks in mtp53 expressing organoids than in wild-type p53 expressing organoids as shown by increased ψ-H2AX protein expression. Moreover, breast cancer tissue microarrays (TMAs) showed a positive correlation between stable p53 and high PARP1 expression in sub-groups of breast cancers, which may indicate sub-classes of breast cancers sensitive to PARPi therapy. These results suggest that mtp53 could be a biomarker to predict response to the combination of PARPi talazoparib-temozolomide treatment.

Publisher

Cold Spring Harbor Laboratory

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