Importantly, the STAT3 complex also induces transcription of the protein SOCS3 that triggers a negative feedback loop of IL-10 regulation
by blocking subsequent phosphorylation of Jak1.11 Several clinical Saracatinib solubility dmso observations regarding pregnancy implicate a role of an anti-inflammatory regulator such as IL-10.13 A significant number of women with rheumatoid arthritis (RA), an inflammation-driven condition, consistently reported diminished symptoms during pregnancy. In contrast, women with systemic lupus erythematosus (SLE), an antibody-driven autoimmune disease, presented with increased symptoms during pregnancy. Taken together, these reports supported the postulate that an anti-inflammatory milieu, perhaps dominated by IL-10,
was amplified during pregnancy most likely as a mechanism of tolerance toward the fetal allograft. Initial studies of the role of IL-10 during pregnancy were carried out in mice. Murine decidual tissues harvested across the spectrum of gestation showed that IL-10 was produced in supernatants and peaked at gestational day (gd)12.14 Administration of recombinant IL-10 in abortion prone CBA×DBA/2 mice significantly abrogated the incidence of spontaneous fetal loss.15 In placental Tanespimycin clinical trial tissue obtained from normal pregnant women, immunohistochemical analysis coupled with ELISA showed MycoClean Mycoplasma Removal Kit that IL-10 was produced in a gestational age–dependent manner. Levels of IL-10 from first and second trimester placental tissues were significantly higher than levels found in third trimester tissues, suggesting that IL-10 is intrinsically downregulated at term to prepare for the onset of labor programmed by production of an inflammatory milieu.16 Further studies elucidated the crucial role
of IL-10 at the maternal–fetal interface as placental and decidual tissue from first trimester missed abortions showed decreased IL-10 production when compared to control tissues obtained from first trimester elective terminations.17 Similarly, a comparison of placental tissue from elective cesarean (pre-labor) and placental tissue obtained post-labor showed higher IL-10 production in pre-labor tissues. Importantly, high IL-10 production in pre-labor tissues correlated to low prostaglandin-2 (PGE-2) levels, whereas the opposite held true for post-labor tissues.18 These data established IL-10 as a key contributor to the balance of pro-inflammatory versus anti-inflammatory signals that orchestrate proper pregnancy outcomes. Figure 1 presents a contemporary view of temporal potential of IL-10 at different stages of pregnancy. Ten years later, the role of IL-10 in pregnancy as an immunosuppressive agent is solidified, and recent studies have focused on its mechanistic properties.