Oops, you're using an old version of your browser so some of the features on this page may not be displaying properly.

MINIMAL Requirements: Google Chrome 24+Mozilla Firefox 20+Internet Explorer 11Opera 15–18Apple Safari 7SeaMonkey 2.15-2.23

Become a member
  1. OncologyPRO
  2. Meeting Resources
  3. ESMO Congress 2024

Poster session 03

1021P - Chemotherapy and hypomethylating agents enhance anti-tumor activity of PRAME ImmTAC

Date

14 Sep 2024

Session

Poster session 03

Topics

Immunotherapy

Tumour Site

Ovarian Cancer;  Non-Small Cell Lung Cancer

Presenters

Adel Benlahrech

Citation

Annals of Oncology (2024) 35 (suppl_2): S674-S711. 10.1016/annonc/annonc1596

Authors

A. Benlahrech, J. Clubley, C. Britton-Rivet, A. Raczka, P.B. Kirk, S. Varadarajan

Author affiliations

  • Translational Medicine, Immunocore Limited, OX14 4RY - Abingdon-on-Thames/GB

Resources

Login to get immediate access to this content.

If you do not have an ESMO account, please create one for free.

Login

Abstract 1021P

Background

Immune-mobilizing monoclonal T cell receptor Against Cancer (ImmTAC) molecules are TCR-CD3 T cell engagers that redirect polyclonal T cells to kill tumors by binding to tumor peptides presented by HLA-A. ImmTAC that targets the cancer testis antigen (CTA) PRAME is in investigational clinical trials as monotherapy and in combination with chemotherapies in advanced solid tumors including melanoma, ovarian, endometrial, and lung (NCT04262466, NCT06112314). This study aims to evaluate whether combining PRAME ImmTAC with chemotherapy or a hypomethylating agent (HMA) enhances tumor cell killing in vitro.

Methods

PRAME ImmTAC-mediated T cell activation and killing of cell lines from lung, ovarian, and endometrial cancers was assessed in vitro with or without decitabine (dec), gemcitabine (gem), doxorubicin (dox), paclitaxel (pac), or carboplatin (carb). PRAME and antigen presentation machinery (APM) genes and proteins (HLA-A, B2M) were quantified by RT-qPCR and flow cytometry.

Results

Dec, an HMA known to increase CTA expression, resulted in up to 4-fold upregulation of PRAME transcripts in lung tumor cell lines. Dec also upregulated APM genes and surface expression in OVCAR3 cells, an ovarian cell line with low HLA-A2 expression. Gem up-regulated HLA-A2 surface expression up to 2-fold in multiple tumor lines. PRAME ImmTAC combination with dec or gem resulted in improved T cell-mediated IFNγ release (up to 3-fold increase in Emax) and tumor killing (up to 2-fold increase), particularly against tumors with low PRAME or APM expression. PRAME ImmTAC combination with either dox, pac, or pac+carb resulted in enhanced tumor cell killing, even at low effector: target (1:1) ratios (up 4-fold increase). The mechanisms by which these chemotherapies enhance PRAME ImmTAC-mediated tumor cell killing is under investigation.

Conclusions

Decitabine increased PRAME and APM, whilst gemcitabine increased APM expression in tumor cells. PRAME ImmTAC-mediated killing of ovarian, endometrial, and lung cell lines was enhanced when combined with dec, gem, dox, pac, pac+carb, with pac exhibiting the highest enhancement. These findings support combining PRAME ImmTAC with HMA or chemotherapy to enhance clinical efficacy.

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

Immunocore Ltd.

Funding

Immunocore Ltd.

Disclosure

A. Benlahrech, J. Clubley, C. Britton-Rivet, A. Raczka, P.B. Kirk, S. Varadarajan: Financial Interests, Personal, Full or part-time Employment: Immunocore Ltd.

Resources from the same session

This site uses cookies. Some of these cookies are essential, while others help us improve your experience by providing insights into how the site is being used.

For more detailed information on the cookies we use, please check our Privacy Policy.

Customise settings

  • Necessary cookies enable core functionality. The website cannot function properly without these cookies, and you can only disable them by changing your browser preferences.