Direct Effects of Mifepristone on Mice Embryogenesis: An In Vitro Evaluation by Single-Embryo RNA Sequencing Analysis

Su, Yu-Ting; Chen, Jia-Shing; Lan, Kuo‐Chung; Lee, Yung-Kuo; Chu, Tian‐Huei; Ho, Yu-Cheng; Wu, Cheng-Chun; Huang, Fay

doi:10.3390/biomedicines11030907

Cited by 1 publication

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References 66 publications

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“…Mifepristone may directly interfere with embryogenesis in addition to endometrial receptivity and embryonic implantation. 145 Mifepristone regulates macrophagemediated NK cell function in the decidua. The NK cells' cytotoxicity and migration ability significantly increased by macrophages pre-treated with mifepristone in a dose-dependent manner.…”

Section: Oral Porcine Afp-toxin Complexesmentioning

confidence: 99%

Alpha-Fetoprotein: A Revolutionary Anti-Cancer Drug

Pak¹

2023

MRAJ

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Alpha-fetoprotein is an oncofetal protein the embryo produces during fetal development. The protein serves two critical functions simultaneously: it delivers nutrients to growing embryo cells and immature myeloid-derived suppressor cells, so the mother’s immune system doesn’t attack the embryo. The protein is present in minuscule amounts in adults and elevated alpha-fetoprotein levels serve as pregnancy or tumor markers. Exogenous alpha-fetoprotein has a new application as an immunotherapy drug. It can deliver drugs in a natural shuttle manner to myeloid-derived suppressor cells and stimulate them to calm the hyperactive immune response during many physiological and pathological conditions. On the other hand, alpha-fetoprotein loaded with toxins kills myeloid-derived suppressor cells and unleashes natural killer cells and cytotoxic lymphocytes to erase cancer. Most cancers have cells that specifically bind alpha-fetoprotein, and this protein targets chemotherapy to them also. So, alpha-fetoprotein with toxins combines both potent cancer immunotherapy and targeted chemotherapy activities. Alpha-fetoprotein can be chemically conjugated with or bind toxins non-covalently. Both preparations have demonstrated superior efficacy and safety compared to chemotherapy alone. Alpha-fetoprotein-toxin immuno/chemotherapy is not personalized. There is no need to preselect patients for cancer treatments as they have elevated myeloid-derived suppressor cell levels. The anti-cancer efficacy of porcine alpha-fetoprotein non-covalent complexes with selected toxins administered orally is a remarkable discovery that needs research. Cancer treatment and prevention are different issues, and they could need different approaches. Alpha-fetoprotein administration with drugs or toxins could be as effective in early cancer and metastasis prevention as mifepristone pills in pregnancy prevention.

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Section: Oral Porcine Afp-toxin Complexesmentioning

confidence: 99%

Alpha-Fetoprotein: A Revolutionary Anti-Cancer Drug

Pak¹

2023

MRAJ

View full text Add to dashboard Cite

show abstract

Direct Effects of Mifepristone on Mice Embryogenesis: An In Vitro Evaluation by Single-Embryo RNA Sequencing Analysis

Cited by 1 publication

References 66 publications

Alpha-Fetoprotein: A Revolutionary Anti-Cancer Drug

Alpha-Fetoprotein: A Revolutionary Anti-Cancer Drug

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