Mutations in fetal genes involved in innate immunity and host defense against microbes increase risk of preterm premature rupture of membranes ( PPROM )

Background Twin studies have revealed a significant contribution of the fetal genome to risk of preterm birth. Preterm premature rupture of membranes ( PPROM ) is the leading identifiable cause of preterm delivery. Infection and inflammation of the fetal membranes is commonly found associated with PPROM . Methods We carried out whole exome sequencing ( WES ) of genomic DNA from neonates born of African‐American mothers whose pregnancies were complicated by PPROM (76) or were normal term pregnancies ( N  = 43) to identify mutations in 35 candidate genes involved in innate immunity and host defenses against microbes. Targeted genotyping of mutations in the candidates discovered by WES was conducted on an additional 188 PPROM cases and 175 controls. Results We identified rare heterozygous nonsense and frameshift mutations in several of the candidate genes, including CARD 6, CARD 8, DEFB 1, FUT 2, MBL 2, NLP 10, NLRP 12, and NOD 2 . We discovered that some mutations ( CARD 6, DEFB 1, FUT 2, MBL 2, NLRP 10, NOD 2 ) were present only in PPROM cases. Conclusions We conclude that rare damaging mutations in innate immunity and host defense genes, the majority being heterozygous, are more frequent in neonates born of pregnancies complicated by PPROM . These findings suggest that the risk of preterm birth in African‐Americans may be conferred by mutations in multiple genes encoding proteins involved in dampening the innate immune response or protecting the host against microbial infection and microbial products.