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Gomez‐Lopez, Nardhy; Romero, Roberto; Tarca, Adi L.; Miller, Derek; Panaitescu, Bogdan; Schwenkel, George; Gudicha, Dereje W.; Hassan, Sonia S.; Pacora, Percy; Jung, Eunjung; Hsu, Chaur‐Dong
American journal of reproductive immunology, December 2019, Letnik: 82, Številka: 6Journal Article
Problem Pyroptosis, inflammatory programmed cell death, is initiated through the inflammasome and relies on the pore‐forming actions of the effector molecule gasdermin D. Herein, we investigated whether gasdermin D is detectable in women with spontaneous preterm labor and sterile intra‐amniotic inflammation or intra‐amniotic infection. Method of study Amniotic fluid samples (n = 124) from women with spontaneous preterm labor were subdivided into the following groups: (a) those who delivered at term (n = 32); and those who delivered preterm (b) without intra‐amniotic inflammation (n = 41), (c) with sterile intra‐amniotic inflammation (n = 32), or (d) with intra‐amniotic infection (n = 19), based on amniotic fluid IL‐6 concentrations and the microbiological status of amniotic fluid (culture and PCR/ESI‐MS). Gasdermin D concentrations were measured using an ELISA kit. Multiplex immunofluorescence staining was also performed to determine the expression of gasdermin D, caspase‐1, and interleukin‐1β in the chorioamniotic membranes. Flow cytometry was used to detect pyroptosis (active caspase‐1) in decidual cells from women with preterm labor and birth. Results (a) Gasdermin D was detected in the amniotic fluid and chorioamniotic membranes from women who underwent spontaneous preterm labor/birth with either sterile intra‐amniotic inflammation or intra‐amniotic infection, but was rarely detected in those without intra‐amniotic inflammation. (b) Amniotic fluid concentrations of gasdermin D were higher in women with intra‐amniotic infection than in those with sterile intra‐amniotic inflammation, and its expression in the chorioamniotic membranes was associated with caspase‐1 and IL‐1β (inflammasome mediators). (c) Decidual stromal cells and leukocytes isolated from women with preterm labor and birth are capable of undergoing pyroptosis given their expression of active caspase‐1. Conclusion Pyroptosis can occur in the context of sterile intra‐amniotic inflammation and intra‐amniotic infection in patients with spontaneous preterm labor and birth
