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Consideration of Ketogenic Metabolic Therapy as a Complementary or Alternative Approach for Managing Breast Cancer
Seyfried, T.N. ✉
;
Mukherjee, P.
;
Iyikesici, M.S.
;
Slocum, A.
;
Kalamian, M.
;
Spinosa, J.-P.
;
Chinopoulos, C. [Chinopoulos, Christos (Bioenergetika), szerző] Orvosi Biokémiai Intézet (SE / AOK / I)
Angol nyelvű Összefoglaló cikk (Folyóiratcikk) Tudományos
Megjelent:
FRONTIERS IN NUTRITION 2296-861X 2296-861X
7
Paper: 21
, 13 p.
2020
SJR Scopus - Endocrinology, Diabetes and Metabolism: Q1
Azonosítók
MTMT: 31301847
DOI:
10.3389/fnut.2020.00021
WoS:
000525526600001
SE Repozitórium:
8312
Scopus:
85082725502
PubMed:
32219096
Szakterületek:
Biokémia és molekuláris biológia
Breast cancer remains as a significant cause of morbidity and mortality in women. Ultrastructural and biochemical evidence from breast biopsy tissue and cancer cells shows mitochondrial abnormalities that are incompatible with energy production through oxidative phosphorylation (OxPhos). Consequently, breast cancer, like most cancers, will become more reliant on substrate level phosphorylation (fermentation) than on oxidative phosphorylation (OxPhos) for growth consistent with the mitochondrial metabolic theory of cancer. Glucose and glutamine are the prime fermentable fuels that underlie therapy resistance and drive breast cancer growth through substrate level phosphorylation (SLP) in both the cytoplasm (Warburg effect) and the mitochondria (Q-effect), respectively. Emerging evidence indicates that ketogenic metabolic therapy (KMT) can reduce glucose availability to tumor cells while simultaneously elevating ketone bodies, a non-fermentable metabolic fuel. It is suggested that KMT would be most effective when used together with glutamine targeting. Information is reviewed for suggesting how KMT could reduce systemic inflammation and target tumor cells without causing damage to normal cells. Implementation of KMT in the clinic could improve progression free and overall survival for patients with breast cancer. © Copyright © 2020 Seyfried, Mukherjee, Iyikesici, Slocum, Kalamian, Spinosa and Chinopoulos.
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2025-03-30 03:41
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