Interleukin-33-induced expression of PIBF1 by decidual B cells protects against preterm labor

B Huang, AN Faucette, MD Pawlitz, B Pei, JW Goyert… - Nature medicine, 2017 - nature.com
B Huang, AN Faucette, MD Pawlitz, B Pei, JW Goyert, JZ Zhou, NG El-Hage, J Deng, J Lin…
Nature medicine, 2017nature.com
Preterm birth (PTB) is a leading cause of neonatal death worldwide. Intrauterine and
systemic infection and inflammation cause 30–40% of spontaneous preterm labor (PTL),
which precedes PTB. Although antibody production is a major immune defense mechanism
against infection, and B cell dysfunction has been implicated in pregnancy complications
associated with PTL,, the functions of B cells in pregnancy are not well known,,,. We found
that choriodecidua of women undergoing spontaneous PTL harbored functionally altered B …
Abstract
Preterm birth (PTB) is a leading cause of neonatal death worldwide. Intrauterine and systemic infection and inflammation cause 30–40% of spontaneous preterm labor (PTL), which precedes PTB. Although antibody production is a major immune defense mechanism against infection, and B cell dysfunction has been implicated in pregnancy complications associated with PTL,, the functions of B cells in pregnancy are not well known,,,. We found that choriodecidua of women undergoing spontaneous PTL harbored functionally altered B cell populations. B cell–deficient mice were markedly more susceptible than wild-type (WT) mice to PTL after inflammation, but B cells conferred interleukin (IL)-10-independent protection against PTL. B cell deficiency in mice resulted in a lower uterine level of active progesterone-induced blocking factor 1 (PIBF1), and therapeutic administration of PIBF1 mitigated PTL and uterine inflammation in B cell–deficient mice. B cells are a significant producer of PIBF1 in human choriodecidua and mouse uterus in late gestation. PIBF1 expression by B cells is induced by the mucosal alarmin IL-33 (ref. ). Human PTL was associated with diminished expression of the α-chain of IL-33 receptor on choriodecidual B cells and a lower level of active PIBF1 in late gestation choriodecidua. These results define a vital regulatory cascade involving IL-33, decidual B cells and PIBF1 in safeguarding term pregnancy and suggest new therapeutic approaches based on IL-33 and PIBF1 to prevent human PTL.
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