The PARP1 Inhibitor AZD5305 Impairs Ovarian Adenocarcinoma Progression and Visceral Metastases in Patient-derived Xenografts Alone and in Combination with Carboplatin

Giulia Dellavedova; Alessandra Decio; Laura Formenti; Mark R Albertella; Joanne Wilson; Anna D Staniszewska; Elisabetta Leo; Raffaella Giavazzi; Carmen Ghilardi; Maria Rosa Bani

doi:10.1158/2767-9764.CRC-22-0423

The PARP1 Inhibitor AZD5305 Impairs Ovarian Adenocarcinoma Progression and Visceral Metastases in Patient-derived Xenografts Alone and in Combination with Carboplatin

Cancer Res Commun. 2023 Mar 27;3(3):489-500. doi: 10.1158/2767-9764.CRC-22-0423. eCollection 2023 Mar.

Affiliations

¹ Cancer Metastasis Therapeutics, Oncology Department, Istituto di Ricerche Farmacologiche Mario Negri IRCCS, Milano, Italy.
² Bioscience, Oncology R&D, AstraZeneca, Cambridge, United Kingdom.

^# Contributed equally.

Abstract

PARP inhibitors (PARPi) have changed the management of patients with ovarian cancer and their effectiveness has been demonstrated especially in homologous recombination repair-deficient tumors. These first-generation drugs target PARP1, but also PARP2 and other family members potentially responsible for adverse effects that limit their therapeutic potential and restrict their use in combination with chemotherapeutic agents. We investigated ovarian cancer patient-derived xenografts (OC-PDXs) to assess whether malignant progression could be impaired by a novel inhibitor selective for PARP1 (AZD5305) and to assess the potential of its combination with carboplatin (CPT), the standard-of-care for patients with ovarian cancer. In BRCA-mutated OC-PDXs, AZD5305 achieved greater tumor regressions and longer duration of response as well as a superior impairment of visceral metastasis and improved survival benefit compared with the first-generation dual PARP1/2 inhibitors. The combination of AZD5305 plus CPT was more efficacious than single agents. Subcutaneously growing tumors experienced regression that persisted after therapy stopped. Combination efficacy was greater against tumors that did not respond well to platinum, even at a dose at which AZD5305 monotherapy was ineffective. The combination therapy impaired metastatic dissemination and significantly prolonged the lifespan of mice bearing OC-PDXs in their abdomen. This combination benefit was evident even when CPT was used at suboptimal doses, and was superior to full-dose platinum treatment. These preclinical studies demonstrate that the PARP1-selective inhibitor AZD5305 retains and improves the therapeutic benefit of the first-generation PARPi, providing an opportunity to maximize benefits for this class of anticancer agents.

Significance: Selective PARP1i AZD5305 can exceed the efficacy of first-generation PARPi, which target both PARP1 and PARP2, and potentiates the efficacy of CPT when given in combination. AZD5305 alone or in combination with platinum delayed visceral metastasis, ultimately extending the lifespan of OC-PDX-bearing mice. These preclinical models mimic the progression of the disease occurring in patients after debulking surgery, and are translationally relevant.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenocarcinoma* / drug therapy
Animals
BRCA2 Protein
Carboplatin / therapeutic use
Carcinoma, Ovarian Epithelial / drug therapy
Disease Models, Animal
Female
Heterografts
Humans
Mice
Ovarian Neoplasms* / drug therapy
Platinum / therapeutic use
Poly (ADP-Ribose) Polymerase-1 / therapeutic use
Poly(ADP-ribose) Polymerase Inhibitors / pharmacology

Substances

Poly(ADP-ribose) Polymerase Inhibitors
AZD5305
Carboplatin
Platinum
BRCA2 Protein
PARP1 protein, human
Poly (ADP-Ribose) Polymerase-1