Areca nut (AN) is an addictive carcinogen used by about 200-600 million people worldwide. Some AN components are shown to induce apoptosis; however, we previously demonstrated that AN extract (ANE) and the 30-100kDa fraction of ANE (ANE 30-100K) induced autophagy-like responses, such as swollen cell morphology, empty cytoplasm, acidic vesicles, and LC3-II accumulation, in an oral cancer cell line, OECM-1. To further assess the responses of other cell types to ANE 30-100K, we used both normal and malignant cells as the targets of ANE 30-100K and found that normal oral fibroblasts (CMT415), peripheral blood lymphocytes (PBLs), Jurkat leukemia T cells, and esophageal carcinoma cells (CE81T/VGH) exhibited similar responses after ANE 30-100K challenge. ANE 30-100K drastically increased acidic vesicle-containing PBLs isolated from two independent donors (from 0.1% to 92.1% and 2.9% to 64.2%). Furthermore, both ANE- and ANE 30-100K-induced LC3-II accumulation in CMT415 and CE81T/VGH was further increased in the presence of the lysosomal protease inhibitors (pepstatin A, E64d, and leupeptin). On the other hand, ANE 30-100K also increased the level of intracellular reactive oxygen species (ROS), and the ROS scavengers, N-acetylcysteine (NAC) and Tiron, inhibited ANE 30-100K-induced cell death and LC3-II accumulation. Collectively, these results suggest the existence of an autophagy-inducing AN ingredient (AIAI) in ANE 30-100K, which renders ANE as an autophagic flux inducer through ROS in both normal and malignant cells.
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Mechanistic and compositional studies of the autophagy-inducing areca nut ingredient.
J Dent Sci
December 2020
Department of Biotechnology, Chia Nan University of Pharmacy, Tainan, Taiwan, Republic of China.
Background/purpose: We previously found that the partially purified 30-100 kDa fraction of areca-nut-extract (ANE 30-100K) induces autophagy in different types of cells including oral carcinoma OECM-1 cells. This study was to analyze the composition and possible mechanisms of ANE 30-100K-induced autophagy (AIA).
Materials And Methods: Phenol-sulfuric acid method and high performance anion exchange chromatography were utilized to analyze the composition of ANE 30-100K.
Chronic Stimulation of the Autophagy-inducing Ingredient of Areca Nut Promotes Tumor Growth Through Up-regulation of Tumoral Autophagy.
Anticancer Res
January 2020
Department of Biotechnology, Chia Nan University of Pharmacy, Tainan, Taiwan, R.O.C.
Article Synopsis
- Autophagy can play conflicting roles in tumors, either promoting or suppressing their growth; the study investigates how areca-nut-extract (ANE 30-100K) induces autophagy and its impact on tumor cell resistance in stressed conditions.
- In experiments with esophageal CE81T/VGH cells and nude mice, researchers found that CAS-treated tumor cells showed increased autophagy markers and resilience against harsh environments, which could be reversed by using autophagy inhibitors.
- Ultimately, the study highlights that CAS treatment may enhance tumor growth and suggests that inhibiting autophagy, especially when combined with other cancer drugs like cisplatin, could provide effective therapeutic strategies against these tumors.
Clathrin-mediated endocytosis is required for ANE 30-100K-induced autophagy.
J Oral Pathol Med
January 2018
Department of Dentistry, Taipei Medical University, Taipei, Taiwan.
Background: We identified an autophagy-inducing areca nut (AN) ingredient (AIAI) in the 30-100 kDa fraction of AN extract (ANE 30-100K). This study was to analyze the role of endocytosis in ANE 30-100K-induced autophagy.
Methods: We used benzyl alcohol, dynasore, and shRNA of clathrin and dynamin to assess whether ANE 30-100K-induced cytotoxicity and accumulation of microtubule-associated protein 1 light chain 3 (LC3)-II were affected in oral (OECM-1) and esophageal (CE81T/VGH) carcinoma cells.
Impacts of autophagy-inducing ingredient of areca nut on tumor cells.
PLoS One
April 2016
Department of Medical Research, Chi Mei Medical Center, Tainan, Taiwan; Division of Natural Science, College of Liberal Education, Shu-Te University, Kaohsiung, Taiwan.
Areca nut (AN) is a popular carcinogen used by about 0.6-1.2 billion people worldwide.
View Article and Find Full Text PDFAutophagy induction by the 30-100kDa fraction of areca nut in both normal and malignant cells through reactive oxygen species.
Oral Oncol
November 2010
Department of Biotechnology, Chia Nan University of Pharmacy, Tainan, Taiwan, ROC.
Areca nut (AN) is an addictive carcinogen used by about 200-600 million people worldwide. Some AN components are shown to induce apoptosis; however, we previously demonstrated that AN extract (ANE) and the 30-100kDa fraction of ANE (ANE 30-100K) induced autophagy-like responses, such as swollen cell morphology, empty cytoplasm, acidic vesicles, and LC3-II accumulation, in an oral cancer cell line, OECM-1. To further assess the responses of other cell types to ANE 30-100K, we used both normal and malignant cells as the targets of ANE 30-100K and found that normal oral fibroblasts (CMT415), peripheral blood lymphocytes (PBLs), Jurkat leukemia T cells, and esophageal carcinoma cells (CE81T/VGH) exhibited similar responses after ANE 30-100K challenge.
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