Simultaneous targeting of mitochondrial metabolism and immune checkpoints as a new strategy for renal cancer therapy

Štemberková-Hubáčková, Soňa; Zobalová, Renata; Dubišová, Mária; Šmigová, J.; Dvořáková, Šárka; Kořínková, Klára; Ezrová, Zuzana; Endaya, Berwini; Blažková, Kristýna; Vlčák, Erik; Brisudová, Petra; Le, Thi Dan Diem; Juhás, Štefan; Rosel, D.; Kelemen, Daniela Cristina; Sovilj, Dana; Vacurová, Eliška; Čajka, Tomáš; Filimonenko, Vlada; Dong, L.; Anděra, Ladislav; Hozák, Pavel; Brabek, J.; Bielcikova, Z.; Štursa, Jan; Werner, Lukáš; Neužil, Jiří

doi:https://dx.doi.org/10.1002/ctm2.645

Počet záznamů: 1

Simultaneous targeting of mitochondrial metabolism and immune checkpoints as a new strategy for renal cancer therapy

1.

SYSNO ASEP	0556526
Druh ASEP	J - Článek v odborném periodiku
Zařazení RIV	J - Článek v odborném periodiku
Poddruh J	Článek ve WOS
Název	Simultaneous targeting of mitochondrial metabolism and immune checkpoints as a new strategy for renal cancer therapy
Tvůrce(i)	Štemberková-Hubáčková, Soňa (BTO-N) Zobalová, Renata (BTO-N)_{RID, ORCID} Dubišová, Mária (BTO-N) Šmigová, J. (CZ) Dvořáková, Šárka (BTO-N)_{ORCID, RID} Kořínková, Klára (BTO-N) Ezrová, Zuzana (BTO-N)_ORCID Endaya, Berwini (BTO-N)_ORCID Blažková, Kristýna (BTO-N) Vlčák, Erik (UMG-J) Brisudová, Petra (BTO-N) Le, Thi Dan Diem (BTO-N) Juhás, Štefan (UZFG-Y)_{RID, ORCID} Rosel, D. (CZ) Kelemen, Daniela Cristina (BTO-N) Sovilj, Dana (BTO-N)_{RID, ORCID} Vacurová, Eliška (BTO-N)_ORCID Čajka, Tomáš (FGU-C)_{RID, ORCID, SAI} Filimonenko, Vlada (UMG-J)_{RID, ORCID} Dong, L. (AU) Anděra, Ladislav (BTO-N)_{ORCID, RID} Hozák, Pavel (UMG-J)_{RID, ORCID} Brabek, J. (CZ) Bielcikova, Z. (CZ) Štursa, Jan (BTO-N) Werner, Lukáš (BTO-N) Neužil, Jiří (BTO-N)_{RID, ORCID}
Celkový počet autorů	27
Číslo článku	e645
Zdroj.dok.	Clinical and Translational Medicine. - : Wiley - ISSN 2001-1326 Roč. 12, č. 3 (2022)
Poč.str.	8 s.
Jazyk dok.	eng - angličtina
Země vyd.	GB - Velká Británie
Klíč. slova	Mitochondrially targeted tamoxifen ; Renal cancer ; Immunotherapy
Vědní obor RIV	FD - Onkologie a hematologie
Obor OECD	Pathology
CEP	GA20-05942S GA ČR - Grantová agentura ČR
	GX21-04607X GA ČR - Grantová agentura ČR
	GA18-02550S GA ČR - Grantová agentura ČR
	GA19-08772S GA ČR - Grantová agentura ČR
	NU21-03-00195 GA MZd - Ministerstvo zdravotnictví
	ED1.1.00/02.0109 GA MŠMT - Ministerstvo školství, mládeže a tělovýchovy
	LTC19048 GA MŠMT - Ministerstvo školství, mládeže a tělovýchovy
	LO1609 GA MŠMT - Ministerstvo školství, mládeže a tělovýchovy
	EF16_013/0001775 GA MŠMT - Ministerstvo školství, mládeže a tělovýchovy
Výzkumná infrastruktura	Czech-BioImaging II - 90129 - Ústav molekulární genetiky AV ČR, v. v. i.
Způsob publikování	Open access
Institucionální podpora	BTO-N - RVO:86652036 ; UMG-J - RVO:68378050 ; UZFG-Y - RVO:67985904 ; FGU-C - RVO:67985823
UT WOS	000774832800001
DOI	https://doi.org/10.1002/ctm2.645
Anotace	Mitochondrially targeted tamoxifen (MitoTam) has recently undergone phase 1/1b clinical trial in patients with various solid tumors. Since patients with clear cell renal carcinoma showed the highest response of the tested diagnoses, we studied the effect of MitoTam on renal cancer in vitro and in vivo to reveal its mechanism of action in more detail and to better understand its benefit for patients. Using primarily the murine RenCa renal cancer cell line and the derived syngeneic mouse tumor model, we studied mechanism of MitoTam toxicity including the mode of death, the role of mitochondria in the effects of the agent, and its efficacy in suppressing syngeneic tumors in mice alone and in combination with the immune checkpoint inhibitors (ICIs), monoclonal antibodies blocking PD-1 and PD-L1. Our findings show a complex effect of MitoTam on mitochondrial function and integrity of renal cancer cells. The agent inhibits complex I-dependent respiration and lowers mitochondrial potential, which results in activation of necroptosis as the major mode of cell death. As a consequence, MitoTam reduces growth of renal tumors as well as metastatic spread of tumor cells via specific targeting of malignant tissue in a mouse model. Moreover, combination of MitoTam with immunotherapy to enhance its anti-cancer efficacy shows significantly increased suppression of tumor growth as well as increased survival of experimental animals compared to single agent treatment. Our data provide a mechanistic rationale for testing of both mono and/or combinatorial therapy with MitoTam plus ICIs in renal carcinomas in Phase 2 trial.
Pracoviště	Biotechnologický ústav
Kontakt	Monika Kopřivová, Monika.Koprivova@ibt.cas.cz, Tel.: 325 873 700
Rok sběru	2023
Elektronická adresa	https://onlinelibrary.wiley.com/doi/10.1002/ctm2.645

Počet záznamů: 1