Article ID Journal Published Year Pages File Type
3964266 Journal of Reproductive Immunology 2014 9 Pages PDF
Abstract

•Maternofetal tolerance is not tolerance but the regulation of inflammation.•The purpose of decidual NK cells is to protect against infection.•IFN-γ altering decidual arteries and VEGF ↑fetal trophoblast growth are inessential.•Complement-triggered inflammation destroys angiogenesis: sFlt1 does not.•RCTs/systematic reviews can give flawed RIF and RM treatment evaluations.

According to Mark Twain, “It ain’t what you don’t know that gets you into trouble. It's what you know for sure that just ain’t so.” Four items believed by reproductive immunologists are analyzed. (1) In a semiallogeneic (outbred) mating, maternofetal tolerance is required to prevent immune rejection manifesting as infertility, recurrent pregnancy loss, preeclampsia and fetal growth restriction. (2) Regulation of natural killer (NK) cells at the fetomaternal interface by interaction with fetal trophoblast paternal class I MHC is obligatory for pregnancy success. (3) Failure of angiogenesis triggered by complement activation is a key mechanism in pregnancy pathology. (4) Randomized controlled (double-blind) clinical trials and systematic reviews exemplified by the Cochrane database provide reliable evidence on which to base treatment and promulgate guidelines. Those who heed not the lessons of history are doomed to repeat the same mistakes in the future. History shows that we do this and expect a different outcome.

Related Topics
Life Sciences Immunology and Microbiology Immunology
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