abstract

• Endometrial cancer is the fourth most frequent neoplasia for women worldwide, and over the past two decades it incidence has increased. The most common histological type of endometrial cancer is endometrioid adenocarcinoma, also known as type 1 endometrial cancer. Endometrioid endometrial cancer is associated with diverse epidemiological risk factors including estrogen use, obesity, diabetes, cigarette smoking, null parity, early menarche, and late menopause. Clinical effectiveness of chemotherapy is variable, indicating that novel molecular therapies against specific cellular processes associated to cell survival and resistance to therapy, such as autophagy, urged to ameliorate the rates of success in endometrial cancer treatment. Autophagy (also known as macroautophagy) is a specialized mechanism that maintains cell homeostasis which is activated in response to cellular stressors including nutrients deprivation, amino acids starvation, hypoxia, and metabolic stress to prolong cell survival via lysosomal degradation of cytoplasmic macromolecules and organelles. However, in human cancer cells, autophagy has a controversial function due to its dual role as self-protective or apoptotic. Conventional antitumor therapies including hormones, chemotherapy and ionizing radiation, may activate autophagy as a pro-survival tumor response contributing to treatment resistance. Intriguingly, if autophagy continues above reversibility of cell viability, autophagy can result in apoptosis of tumor cells. Here, we have reviewed the mechanisms of autophagy described in endometrial cancers, including the role of PI3K/AKT/mTOR, AMPK-mTOR, and p53 signaling pathways that trigger or inhibit the process and thus representing potential molecular targets in therapeutic clinical approaches. In addition, we discussed the recent findings indicating that autophagy can be modulated using repurposing drugs which may leads to faster experimentation and validation, as well as more easy access of the medications to patients. Finally, the promising role of dietary compounds and microRNAs in autophagy modulation is also discussed. In conclusion, although the research about autophagy is scarce but ongoing in endometrial cancer, the actual findings highlight the promising usefulness of novel molecules for directing targeted therapies. © Copyright © 2019 Nuñez-Olvera, Gallardo-Rincón, Puente-Rivera, Salinas-Vera, Marchat, Morales-Villegas and López-Camarillo.

authors

• Gallardo-Rincón D.
• López-Camarillo C.
• Marchat L.A.
• Morales Villegas Raúl
• Núñez-Olvera S.I.
• Puente-Rivera J.
• Salinas-Vera Y.M.

publication date

• 2019-01-01

funding provided via

• Universidad Autónoma de la Ciudad de México, UACM  Grant

published in

• Frontiers in Oncology  Journal

keywords

• AKT/mTOR pathway; autophagy; endometrial cancer; microRNAs; therapy 2 hydroxylinoleic acid; agaricus blazi murill extract; antineoplastic agent; bortezomib; chloroquine; cisplatin; Cordyceps sinensis extract; DNA mismatch repair protein MSH2; echinocystic acid; Eclipta prostrata extract; everolimus; fluorouracil; Ganoderma lucidum extract; gestagen; isoliquiritigenin; itraconazole; liraglutide; metformin; methylnitrosourea; mhy 2256; nifedipine; paclitaxel; platinum; protopanaxadiol; rapamycin; resveratrol; sorafenib; temozolomide; unclassified drug; unindexed drug; vorinostat; AMPK signaling; apoptosis; autophagy; cell cycle arrest; cell growth; clinical effectiveness; depolymerization; downstream processing; endometrium cancer; endoplasmic reticulum stress; enzyme activity; gene knockdown; gene mutation; gene silencing; histology; human; immunofluorescence test; leukemia; lung metastasis; mismatch repair; natural killer cell; obesity; Pi3K/Akt signaling; protein expression; receptor down regulation; Review; risk factor; therapy effect; transmission electron microscopy; tumor growth; tumor suppressor gene

Digital Object Identifier (DOI)

• 10.3389/fonc.2019.01326

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volume

• 9