Maternal sepsis incidence, aetiology and outcome for mother and fetus: a prospective study

Knowles, S; O’Sullivan, Niamh; Meenan, AM; Hanniffy, Rosena; Robson, Michael

doi:10.1111/1471-0528.12892

Cited by 155 publications

(181 citation statements)

References 24 publications

(97 reference statements)

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“…All experiments in pregnant animals were conducted on day 16 of pregnancy (E16). This period was chosen as most cases of severe sepsis occur during the third trimester of human pregnancy [25].…”

Section: Time Matingmentioning

confidence: 99%

“…Time to labor and pup survival were assessed in a vehicle (PBS) group and demonstrated no difference to untreated control data in our group (mean time to delivery in PBS-treated group 57.2 ± 6.6 compared with untreated group 55.6 ± 0.8). LPS administration demonstrated a dose-dependent reduction in time to delivery (Supplementary Table S3), but at high doses of 20 μg and above LPS caused maternal deaths (20,25,50, or 100 μg LPS; at least one maternal death per group, numbers shown in Supplementary Table S3). The dose of 10 μg caused no maternal deaths, was most reproducible preterm delivery, and had least variation in labor time, pup survival, and caused no maternal mortality (mean time to delivery 23 ± 2.07, Supplementary Table S3).…”

Section: Maternal Intraperitoneal Lipopolysaccharide Administrationmentioning

confidence: 99%

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The response of the innate immune and cardiovascular systems to LPS in pregnant and nonpregnant mice†

Zöllner

Howe

Edey

et al. 2017

Biology of Reproduction

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Sepsis is the leading cause of direct maternal mortality, but there are no data directly comparing the response to sepsis in pregnant and nonpregnant (NP) individuals. This study uses a mouse model of sepsis to test the hypothesis that the cardiovascular response to sepsis is more marked during pregnancy. Female CD1 mice had radiotelemetry probes implanted and were time mated. NP and day 16 pregnant CD-1 mice received intraperitoneal lipopolysaccharide (LPS; 10 μg, serotype 0111: B4). In a separate study, tissue and serum (for RNA, protein and flow cytometry studies), aorta and uterine vessels (for wire myography) were collected after LPS or vehicle control administration. Administration of LPS resulted in a greater fall in blood pressure in pregnant mice compared to NP mice. This occurred with similar changes in the circulating levels of cytokines, vasoactive factors, and circulating leukocytes, but with a greater monocyte and lesser neutrophil margination in the lungs of pregnant mice. Baseline markers of cardiac dysfunction and apoptosis as well as cytokine expression were higher in pregnant mice, but the response to LPS was similar in both groups as was the ex vivo assessment of vascular function. In pregnant mice, nonfatal sepsis is associated with a more marked hypotensive response but not a greater immune response. We conclude that endotoxemia induces a more marked hypotensive response in pregnant compared to NP mice. These changes were not associated with a more marked systemic inflammatory response in pregnant mice, although monocyte lung margination was greater. The more marked hypotensive response to LPS may explain the greater vulnerability to some infections exhibited by pregnant women. Pregnancy enhances LPS-induced hypotension, 2017, Vol. 97, No. 2 Summary SentenceIn pregnant mice, nonfatal sepsis is associated with a more marked hypotensive response but not a greater immune response.

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Section: Time Matingmentioning

confidence: 99%

Section: Maternal Intraperitoneal Lipopolysaccharide Administrationmentioning

confidence: 99%

The response of the innate immune and cardiovascular systems to LPS in pregnant and nonpregnant mice†

Zöllner

Howe

Edey

et al. 2017

Biology of Reproduction

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“…and Candida spp., 14,15 UTI associated with institutional vaginal delivery, 16 and puerperal sepsis mostly associated with vaginal infections. 17 In conditions of poverty where access to health care is limited, coinfection is likely common. Yet research on coinfections during pregnancy and lactation has primarily focused on the associations of HIV and malaria with other pathogens including intestinal nematodes [18][19][20] or associations with other infections of the intestine 21 or the reproductive tract.…”

Section: Introductionmentioning

confidence: 99%

Interactions Among Urogenital, Intestinal, Skin, and Oral Infections in Pregnant and Lactating Panamanian Ngäbe Women: A Neglected Public Health Challenge

Gonzalez‐Fernandez¹,

Koski²,

Sinisterra³

et al. 2015

The American Society of Tropical Medicine and Hygiene

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Abstract. Interrelationships among bacteria, protozoa, helminths, and ectoparasites were explored in a cross-sectional survey of 213 pregnant and 99 lactating indigenous women. Prevalences in pregnancy and lactation, respectively, were: vaginitis (89.2%; 46.8%), vaginal trichomoniasis (75.3%; 91.1%), bacterial vaginosis (BV; 60.6%; 63.3%), hookworm (56.6%; 47.8%), asymptomatic bacteriuria/urinary tract infection (AB/UTI; 56.2%; 36.2%), cervicitis (33.3%; 6.3%), vaginal yeast (24.9%; 11.4%), Ascaris (32.5%; 17.4%), vaginal diplococci (20.4%; 31.6%), caries (19.7%; 18.2%), scabies (17.4%; 8.1%), and Trichuris (12.5%; 8.7%). Multiple regressions revealed positive associations during pregnancy (trichomoniasis and AB/UTI; diplococci and Ascaris) and lactation (yeast and scabies). Negative associations were detected in pregnancy (BV and trichomoniasis; hookworm and diplococci) and lactation (BV and yeast). Vaginal Lactobacillus reduced odds of diplococci in pregnancy and lactation, but increased Ascaris eggs per gram (epg) and odds of trichomoniasis in pregnancy and yeast in lactation. These associations raised a concern that treatment of one condition may increase the risk of another.

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“…In a recently reported study 17% of sepsis were diagnosed antepartum, 36% intrapartum and 47% were diagnosed in the postpartum period . The source of infection was most often the genital tract (61%), followed by the urinary tract in 25% of cases . Maternal sepsis was also a risk for the fetus, as it was associated with an increased risk of preterm delivery (OR 2.8), and a high perinatal mortality rate (OR 5.8) .…”

mentioning

confidence: 95%

Procalcitonin; a feasible biomarker for severe bacterial infections in Obstetrics and Gynecology?

Tujula

Kokki

Räsänen

et al. 2018

Acta Obstet Gynecol Scand

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Maternal sepsis incidence, aetiology and outcome for mother and fetus: a prospective study

Cited by 155 publications

References 24 publications

The response of the innate immune and cardiovascular systems to LPS in pregnant and nonpregnant mice†

The response of the innate immune and cardiovascular systems to LPS in pregnant and nonpregnant mice†

Interactions Among Urogenital, Intestinal, Skin, and Oral Infections in Pregnant and Lactating Panamanian Ngäbe Women: A Neglected Public Health Challenge

Procalcitonin; a feasible biomarker for severe bacterial infections in Obstetrics and Gynecology?

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