Respiratory complex I regulates dendritic cell maturation in explant model of human tumor immune microenvironment

Author:

Turpin Rita,Liu Ruixian,Munne Pauliina M,Peura Aino,Rannikko Jenna H,Philips Gino,Boeckx Bram,Salmelin Natasha,Hurskainen Elina,Suleymanova Ilida,Aung July,Vuorinen Elisa M,Lehtinen Laura,Mutka Minna,Kovanen Panu E,Niinikoski Laura,Meretoja Tuomo J,Mattson Johanna,Mustjoki SatuORCID,Saavalainen Päivi,Goga Andrei,Lambrechts Diether,Pouwels Jeroen,Hollmén Maija,Klefström JuhaORCID

Abstract

BackgroundCombining cytotoxic chemotherapy or novel anticancer drugs with T-cell modulators holds great promise in treating advanced cancers. However, the response varies depending on the tumor immune microenvironment (TIME). Therefore, there is a clear need for pharmacologically tractable models of the TIME to dissect its influence on mono- and combination treatment response at the individual level.MethodsHere we establish a patient-derived explant culture (PDEC) model of breast cancer, which retains the immune contexture of the primary tumor, recapitulating cytokine profiles and CD8+T cell cytotoxic activity.ResultsWe explored the immunomodulatory action of a synthetic lethal BCL2 inhibitor venetoclax+metformin drug combination ex vivo, discovering metformin cannot overcome the lymphocyte-depleting action of venetoclax. Instead, metformin promotes dendritic cell maturation through inhibition of mitochondrial complex I, increasing their capacity to co-stimulate CD4+T cells and thus facilitating antitumor immunity.ConclusionsOur results establish PDECs as a feasible model to identify immunomodulatory functions of anticancer drugs in the context of patient-specific TIME.

Funder

Business Finland

Finnish Cancer Institute

Horizon 2020 Framework Programme

iCAN digital precision cancer medicine flagship

Ida Montinin Säätiö

Jane ja Aatos Erkon Säätiö

Research Council of Finland

Sigrid Juséliuksen Säätiö

Sihtasutus Archimedes

Syöpäjärjestöt

The Finnish Cancer Organizations

U.S. Department of Defense

Publisher

BMJ

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