Arijit Kumar Ghosh, Aanchal Verma, Debabrata Majumder, Debasish Maiti, Tathagata Choudhuri, Antara Banerjee, Samiran Saha
{"title":"茶黄素在体内和体外都能诱导艾氏腹水癌细胞自噬","authors":"Arijit Kumar Ghosh, Aanchal Verma, Debabrata Majumder, Debasish Maiti, Tathagata Choudhuri, Antara Banerjee, Samiran Saha","doi":"10.2174/0115734072277726240102062944","DOIUrl":null,"url":null,"abstract":"\n\nTo investigate the efficacy of Theaflavins to induce autophagy and its tumoricidal activity towards Ehrlich’s Ascites Carcinoma cells.\n\n\n\nThe apoptosis-inducing role of Theaflavins against cancer is reported. Autophagy,\na cellular mechanism under stress, occurs either as a survival process or Type-II programmed-cell\ndeath in the presence/absence of apoptosis. The report of Theaflavins inducing autophagy against\ncancer is poor.\n\n\n\nHere, for the first time, the investigation for the anti-tumor efficacy of Theaflavins via\nautophagy in EAC was attempted.\n\n\n\nEAC-bearing mice were treated orally with Theaflavins (10 mg/kg b.w.) every alternate\nday with a total of 27 doses. Body weight, tumor volume and survivability were recorded. Tumoricidal\nand cellular dehydrogenase activity, in vivo and in vitro, were studied using Trypan-blue\nexclusion and MTT assay respectively. Theaflavins-treated EAC cells were subjected to Monodansylcadaverine-\nstaining. LC3II turnover and LC3I conversion were detected by western blotting.\nApoptosis up to 12 h TF-treatment was estimated by AnnexinV binding.\n\n\n\nThis is the first report of Theaflavins inducing autophagy in EAC cells in vivo and in\nvitro. Oral Theaflavins treatment restricted excessive body-weight increase due to tumors, reduced\ntumor volume, and increased survivability of tumor-bearing mice. Theaflavins caused EAC\ncell death (~8% in vitro, ~30% in vivo), significantly reduced metabolic activity, and created conspicuous\nvacuolization in surviving cells. Resultant vacuoles (in vitro, 6 h) were marked as autophagosomes\nby Monodansylcadaverine-staining. Autophagy was confirmed by LC3II augmentation.\nNo significant apoptosis was observed up to 12 h TF-treatment in vitro.\n\n\n\nTheaflavins were efficient inducing autophagy and Type-II PCD in EAC cells. Notably,\nTheaflavins induced autophagy prior to apoptosis in vitro.\n","PeriodicalId":10772,"journal":{"name":"Current Bioactive Compounds","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2024-01-17","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Theaflavins Induce Autophagy in Ehrlich’s Ascites Carcinoma Cells both\\nIn vivo and In vitro\",\"authors\":\"Arijit Kumar Ghosh, Aanchal Verma, Debabrata Majumder, Debasish Maiti, Tathagata Choudhuri, Antara Banerjee, Samiran Saha\",\"doi\":\"10.2174/0115734072277726240102062944\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"\\n\\nTo investigate the efficacy of Theaflavins to induce autophagy and its tumoricidal activity towards Ehrlich’s Ascites Carcinoma cells.\\n\\n\\n\\nThe apoptosis-inducing role of Theaflavins against cancer is reported. Autophagy,\\na cellular mechanism under stress, occurs either as a survival process or Type-II programmed-cell\\ndeath in the presence/absence of apoptosis. The report of Theaflavins inducing autophagy against\\ncancer is poor.\\n\\n\\n\\nHere, for the first time, the investigation for the anti-tumor efficacy of Theaflavins via\\nautophagy in EAC was attempted.\\n\\n\\n\\nEAC-bearing mice were treated orally with Theaflavins (10 mg/kg b.w.) every alternate\\nday with a total of 27 doses. Body weight, tumor volume and survivability were recorded. Tumoricidal\\nand cellular dehydrogenase activity, in vivo and in vitro, were studied using Trypan-blue\\nexclusion and MTT assay respectively. Theaflavins-treated EAC cells were subjected to Monodansylcadaverine-\\nstaining. LC3II turnover and LC3I conversion were detected by western blotting.\\nApoptosis up to 12 h TF-treatment was estimated by AnnexinV binding.\\n\\n\\n\\nThis is the first report of Theaflavins inducing autophagy in EAC cells in vivo and in\\nvitro. Oral Theaflavins treatment restricted excessive body-weight increase due to tumors, reduced\\ntumor volume, and increased survivability of tumor-bearing mice. Theaflavins caused EAC\\ncell death (~8% in vitro, ~30% in vivo), significantly reduced metabolic activity, and created conspicuous\\nvacuolization in surviving cells. Resultant vacuoles (in vitro, 6 h) were marked as autophagosomes\\nby Monodansylcadaverine-staining. Autophagy was confirmed by LC3II augmentation.\\nNo significant apoptosis was observed up to 12 h TF-treatment in vitro.\\n\\n\\n\\nTheaflavins were efficient inducing autophagy and Type-II PCD in EAC cells. 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Theaflavins Induce Autophagy in Ehrlich’s Ascites Carcinoma Cells both
In vivo and In vitro
To investigate the efficacy of Theaflavins to induce autophagy and its tumoricidal activity towards Ehrlich’s Ascites Carcinoma cells.
The apoptosis-inducing role of Theaflavins against cancer is reported. Autophagy,
a cellular mechanism under stress, occurs either as a survival process or Type-II programmed-cell
death in the presence/absence of apoptosis. The report of Theaflavins inducing autophagy against
cancer is poor.
Here, for the first time, the investigation for the anti-tumor efficacy of Theaflavins via
autophagy in EAC was attempted.
EAC-bearing mice were treated orally with Theaflavins (10 mg/kg b.w.) every alternate
day with a total of 27 doses. Body weight, tumor volume and survivability were recorded. Tumoricidal
and cellular dehydrogenase activity, in vivo and in vitro, were studied using Trypan-blue
exclusion and MTT assay respectively. Theaflavins-treated EAC cells were subjected to Monodansylcadaverine-
staining. LC3II turnover and LC3I conversion were detected by western blotting.
Apoptosis up to 12 h TF-treatment was estimated by AnnexinV binding.
This is the first report of Theaflavins inducing autophagy in EAC cells in vivo and in
vitro. Oral Theaflavins treatment restricted excessive body-weight increase due to tumors, reduced
tumor volume, and increased survivability of tumor-bearing mice. Theaflavins caused EAC
cell death (~8% in vitro, ~30% in vivo), significantly reduced metabolic activity, and created conspicuous
vacuolization in surviving cells. Resultant vacuoles (in vitro, 6 h) were marked as autophagosomes
by Monodansylcadaverine-staining. Autophagy was confirmed by LC3II augmentation.
No significant apoptosis was observed up to 12 h TF-treatment in vitro.
Theaflavins were efficient inducing autophagy and Type-II PCD in EAC cells. Notably,
Theaflavins induced autophagy prior to apoptosis in vitro.
Current Bioactive CompoundsPharmacology, Toxicology and Pharmaceutics-Pharmacology, Toxicology and Pharmaceutics (all)
CiteScore
1.90
自引率
0.00%
发文量
112
期刊介绍:
The journal aims to provide comprehensive review articles on new bioactive compounds with proven activities in various biological screenings and pharmacological models with a special emphasis on stereoeselective synthesis. The aim is to provide a valuable information source of bioactive compounds synthesized or isolated, which can be used for further development of pharmaceuticals by industry and academia. The journal should prove to be essential reading for pharmacologists, natural product chemists and medicinal chemists who wish to be kept informed and up-to-date with the most important developments on new bioactive compounds of natural or synthetic origin, including their stereoeselective synthesis.