Glucocorticoids Inhibit Basal and Hormone-Induced Serotonin Synthesis in Pancreatic Beta Cells

Ebou, Moina Hasni; Singh-Estivalet, Amrit; Launay, Jean‐Marie; Crinon, Jacques; Tronche, François; Ferré, Pascal; Gautier, Jean‐François; Guillemain, Ghislaine; Bréant, Bernadette; Blondeau, Bertrand; Riveline, Jean‐Pierre

doi:10.1371/journal.pone.0149343

Cited by 8 publications

(1 citation statement)

References 40 publications

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“…Supposedly, this is a consequence of cancer-mediated damage of pancreatic beta cells with elevated susceptibility to heparanase- or oxidant action, which can be seen in cancers and type 1 diabetes (47). These hormonal abnormalities also occur as a consequence of IR and impaired insulin secretion induced excess glucocorticoids (48). This insulin/glucogon imbalance can be restored by a combination of somastatin and insulin that entails a 23-fold increase of the insulin/glucagon ratio without causing any significant host morbidity from hypoglycemia (43).…”

Section: Cancer-induced Distance Alterations In Host Glucose Metabolimentioning

confidence: 99%

Cancer-Induced Reprogramming of Host Glucose Metabolism: “Vicious Cycle” Supporting Cancer Progression

Schwartsburd

2019

Front. Oncol.

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Unrestricted cancer growth requires permanent supply of glucose that can be obtained from cancer-mediated reprogramming of glucose metabolism in the cancer-bearing host. The pathological mechanisms by which cancer cells exert their negative influence on host glucose metabolism are largely unknown. This paper proposes a mechanism of metabolic and hormonal changes that may favor glucose delivery to tumor (not host) cells by creating a cancer-host “vicious cycle” whose prolonged action drives cancer progression and promotes host cachexia. To verify this hypothesis, a feedback model of host-cancer interactions that create the “vicious cycle” via cancer-induced reprogramming of host glucose metabolism is proposed. This model is capable of answering some crucial questions as to how anabolic cancer cells can reprogram the systemic glucose metabolism and why these pathways were not observed in pregnancy. The current paper helps to better understanding a pathogenesis of cancer progression and identify hormonal/metabolic targets for anti-cancer treatment.

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Section: Cancer-induced Distance Alterations In Host Glucose Metabolimentioning

confidence: 99%

Cancer-Induced Reprogramming of Host Glucose Metabolism: “Vicious Cycle” Supporting Cancer Progression

Schwartsburd

2019

Front. Oncol.

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Possible role of arginase 1 positive microglia on depressive/anxiety-like behaviors in atopic dermatitis mouse model

et al. 2022

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β-cell serotonin production is associated with female sex, old age, and diabetes-free condition

Kim

Moon

Kim

et al. 2017

Biochemical and Biophysical Research Communications

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Glucocorticoids Inhibit Basal and Hormone-Induced Serotonin Synthesis in Pancreatic Beta Cells

Cited by 8 publications

References 40 publications

Cancer-Induced Reprogramming of Host Glucose Metabolism: “Vicious Cycle” Supporting Cancer Progression

Cancer-Induced Reprogramming of Host Glucose Metabolism: “Vicious Cycle” Supporting Cancer Progression

Possible role of arginase 1 positive microglia on depressive/anxiety-like behaviors in atopic dermatitis mouse model

β-cell serotonin production is associated with female sex, old age, and diabetes-free condition

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