Cell therapies in ovarian cancer

Sarivalasis, Apostolos; Morotti, Matteo; Mulvey, Arthur; Imbimbo, Martina; Coukos, George

doi:10.1177/17588359211008399

Cited by 23 publications

(12 citation statements)

References 122 publications

(173 reference statements)

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“…TIL therapy offers an important new therapeutic approach to patients with HGSOC, although, to date, response rates equivalent to those demonstrated in metastatic melanoma using established TIL manufacture techniques have not been achieved in ovarian cancer (Sarivalasis et al, 2021, Pedersen et al, 2018. A contemporary clinical trial of TIL therapy in ovarian cancer has demonstrated limited e cacy compared to metastatic melanoma trials, with all patients achieving a best response of stable disease and a progression free survival between 3-5 months (Pedersen et al, 2018).…”

Section: Discussionmentioning

confidence: 99%

Short term inhibition of immune checkpoint proteins increases ex vivo expansion of tumour infiltrating lymphocytes in high grade serous ovarian cancer

Waddell

Price

Cheadle

et al. 2022

Preprint

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Background: Ovarian cancer remains the most lethal gynaecological malignancy and there is an urgent need for the development of further therapies to improve patient survival. Tumour infiltrating lymphocyte (TIL) therapy has shown clear efficacy in immunogenic cancers, and TIL can be readily expanded ex vivo from samples of high grade serous ovarian cancer (HGSOC). Antibodies against checkpoint proteins are effective in increasing TIL yield and functional response from ovarian cancer TIL cultures, potentially increasing TIL product efficacy. However, it is unknown whether blockade of other key checkpoints, including programmed death ligand-1 (PD-1), T cell immunoglobulin mucin-3 (TIM-3) and lymphocyte activation gene-3 (LAG-3) increase TIL yield in ex vivo cultures from HGSOC samples.Materials and Methods: TIL cultures were generated from fresh tissue samples and were incubated with CD3/CD28 Dynabeads® and IL-2. TIL were grown with or without the addition of 10µg/mL αPD-1, αTIM-3 or αLAG-3 antibodies as either single or repeated applications for 19 days. The phenotype of cultures was analysed by multiparameter flow cytometry. Interferon gamma (IFN-ᵧ) release in response to TIL co-culture with autologous tumour cultures or digests was measured by ELISA. Results: In keeping with previous findings the majority of TIL expressed at least one checkpoint protein. Specifically, TIL expressing PD-1 and TIM-3 retained a functional phenotype with co expression of OX40 and CD28. Expansion of TIL was increased following a single exposure to αPD-1 (1.20 fold) and αLAG-3 (1.31 fold) which was most marked in cultures with otherwise low proliferation. There was no additional increase in proliferation following repeated dosing. In co-culture with autologous tumour, TIL grown in the presence of checkpoint inhibitors showed increased IFN-ᵧ release suggesting increased functional activity in individual cultures. However, this response was not uniform across all cultures. Conclusions: These data suggests that initial blockade of checkpoint proteins is effective in increasing the yield of TIL expanded from HGSOC tumours, suggesting that checkpoint inhibition during TIL manufacture may be a useful method of increasing expansion efficiency.

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Section: Discussionmentioning

confidence: 99%

Short term inhibition of immune checkpoint proteins increases ex vivo expansion of tumour infiltrating lymphocytes in high grade serous ovarian cancer

Waddell

Price

Cheadle

et al. 2022

Preprint

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“…It was found that CDC42EP3 had the most relevance with several TILs, including NK cell, Tcm_CD4 and Tgd. NK-based immunotherapy strategy, especially cytokine-induced killer (CIK) cells, has been extensively studied for decades ( Sarivalasis et al, 2021 ). The clinical efficacy of CIK cells was evaluated in patients with advanced epithelial ovarian cancer in a phase 3 clinical trial.…”

Section: Discussionmentioning

confidence: 99%

Integrative bioinformatics and experimental analysis revealed down-regulated CDC42EP3 as a novel prognostic target for ovarian cancer and its roles in immune infiltration

Yan

Liang

et al. 2021

PeerJ

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Ovarian cancer is a significant clinical challenge as no effective treatments are available to enhance patient survival. Recently, N6-methyladenosine (m6A) RNA modification has been demonstrated to play a pivotal role in tumorigenesis and progression. However, the roles of m6A target genes in ovarian cancer haven’t been clearly illustrated. In this study, we presented a comprehensive bioinformatics and in vitro analysis to evaluate the roles of m6A target genes. Cell division cycle 42 effector protein 3 (CDC42EP3), one probable m6A target gene, was identified to be down-regulated in ovarian cancer tissues and cells. Meanwhile, quantitative PCR (qPCR) and western blot were used to confirm the down-regulated CDC42EP3 in ovarian cancer cells A2780 and TOV112D. The biological function of CDC42EP3 in ovarian cancer was further validated with several algorithms, such as PrognoScan, K-M plotter, LinkedOmics and TISIDB. These findings indicated that lower expression of CDC42EP3 was correlated with poor prognosis in patients with ovarian cancer. In addition, CDC42EP3 expression was significantly associated with a diverse range of tumor-infiltrating immune cells, including natural killer cells (NK), T central memory cells (Tcm), T gamma delta cells (Tgd), etc. Taken together, this study uncovered the potential roles of m6A target gene CDC42EP3 in the regulation of immune microenvironment in the ovarian cancer, and identified CDC42EP3 as a novel prognostic target.

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“…While the therapy was safe and only resulted in grade 1 or 2 toxicities, no reduction in tumor burden was observed in any of the six tested patients [ 25 ]. This and several other clinical trials in OC targeting different antigens have demonstrated the poor success of CAR T-cell therapies in OC, much like in several other solid tumors [ 24 , 26 ]. TCR T-cell therapy in OC on the other hand is still in its early phase with 19 Phase I/II clinical trials registered in (accessed on 15 August 2022).…”

Section: Immunotherapies In Ocmentioning

confidence: 97%

“…On the other hand, CAR T-cell therapy uses antigen-binding regions of antibodies that are fused to intracellular T-cell signaling domains, thereby allowing them to recognize surface antigens independent of HLA presentation. However, while CAR T cells can only elicit an immune response to surface antigens, TCR T cells can recognize antigens from any subcellular compartment [ 24 ]. 32 Phase I/II clinical trials of CAR T-cell therapies have been registered in (accessed on 15 August 2022) directed towards several antigens including B7-H3, TAG72, ALPP, CD133, C-met, FRα, FRβ, HER2, mesothelin, and MUC-1.…”

Section: Immunotherapies In Ocmentioning

confidence: 99%

Dendritic Cell Vaccines: A Promising Approach in the Fight against Ovarian Cancer

Audhut

Deschoemaeker

Allonsius

et al. 2022

Cancers

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Ovarian cancer (OC) is the deadliest gynecological malignancy in developed countries and is the seventh-highest cause of death in women diagnosed with cancer worldwide. Currently, several therapies are in use against OC, including debulking surgery, chemotherapy, as well as targeted therapies. Even though the current standard-of-care therapies improve survival, a vast majority of OC patients relapse. Additionally, immunotherapies have only resulted in meager patient outcomes, potentially owing to the intricate immunosuppressive nexus within the tumor microenvironment. In this scenario, dendritic cell (DC) vaccination could serve as a potential addition to the therapeutic options available against OC. In this review, we provide an overview of current therapies in OC, focusing on immunotherapies. Next, we highlight the potential of using DC vaccines in OC by underscoring the different DC subsets and their functions in OC. Finally, we provide an overview of the advances and pitfalls of current DC vaccine strategies in OC while providing future perspectives that could improve patient outcomes.

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Cell therapies in ovarian cancer

Cited by 23 publications

References 122 publications

Short term inhibition of immune checkpoint proteins increases ex vivo expansion of tumour infiltrating lymphocytes in high grade serous ovarian cancer

Short term inhibition of immune checkpoint proteins increases ex vivo expansion of tumour infiltrating lymphocytes in high grade serous ovarian cancer

Integrative bioinformatics and experimental analysis revealed down-regulated CDC42EP3 as a novel prognostic target for ovarian cancer and its roles in immune infiltration

Dendritic Cell Vaccines: A Promising Approach in the Fight against Ovarian Cancer

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