Anti‐TNF treatment during pregnancy and birth outcomes: A population‐based study from Denmark, Finland, and Sweden

Bröms, Gabriella; Kieler, Helle; Ekbom, Anders; Gissler, Mika; Hellgren, Karin; Lahesmaa-Korpinen, Anna-Maria; Pedersen, Lars; Schmitt‐Egenolf, Marcus; Sørensen, Henrik Toft; Granath, Fredrik

doi:10.1002/pds.4930

Cited by 50 publications

(62 citation statements)

References 47 publications

(86 reference statements)

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“…The current data show that pregnancies exposed to anti-TNFα are not associated with an increased risk of fetal malformations, preterm delivery or pregnancy loss [ 128 , 129 , 130 ]. One of the main concerns, when the fetus is exposed in utero to biological therapy, is the risk of neonatal infections, particularly in the first year of life [ 131 ].…”

Section: Pathological Transfer Of Igg—biological Therapy In Pregnamentioning

confidence: 99%

Benefits and Risks of IgG Transplacental Transfer

et al. 2020

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Maternal passage of immunoglobulin G (IgG) is an important passive mechanism for protecting the infant while the neonatal immune system is still immature and ineffective. IgG is the only antibody class capable of crossing the histological layers of the placenta by attaching to the neonatal Fc receptor expressed at the level of syncytiotrophoblasts, and it offers protection against neonatal infectious pathogens. In pregnant women with autoimmune or alloimmune disorders, or in those requiring certain types of biological therapy, transplacental passage of abnormal antibodies may cause fetal or neonatal harm. In this review, we will discuss the physiological mechanisms and benefits of transplacental transfer of maternal antibodies as well as pathological maternal situations where this system is hijacked, potentially leading to adverse neonatal outcomes.

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Section: Pathological Transfer Of Igg—biological Therapy In Pregnamentioning

confidence: 99%

Benefits and Risks of IgG Transplacental Transfer

et al. 2020

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“…As a result, IFX concentrations in infants, whose mothers have been exposed to IFX during pregnancy, are often supramaternal and IFX can be detected for up to 1 year postpartum 6,7 . IFX exposure of the fetus and newborn have not been associated with severe adverse outcomes for the child, and reported associations with lower birth weight, shorter gestational term, and increased risk of delivery by cesarean section may have been attributable to confounding by disease activity 8–12 . However, pharmacological use during pregnancy is often done carefully and with extra safety precautions.…”

Section: Introductionmentioning

confidence: 99%

“…6,7 IFX exposure of the fetus and newborn have not been associated with severe adverse outcomes for the child, and reported associations with lower birth weight, shorter gestational term, and increased risk of delivery by cesarean section may have been attributable to confounding by disease activity. [8][9][10][11][12] However, pharmacological use during pregnancy is often done carefully and with extra safety precautions. Current European guidelines advocate pausing IFX in the third trimester whereas North American guidelines recommend pausing in the last 6-10 weeks prior to delivery.…”

Section: Introductionmentioning

confidence: 99%

Infliximab clearance decreases in the second and third trimesters of pregnancy in inflammatory bowel disease

et al. 2021

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Background Infliximab therapy during pregnancy in inflammatory bowel disease is challenged by a dilemma between maintaining adequate maternal disease control while minimizing fetal infliximab exposure. We investigated the effects of pregnancy on infliximab pharmacokinetics. Methods The study population comprised 23 retrospectively identified pregnancies. Patients with inflammatory bowel disease were generally in clinical remission at pregnancy conception (74%) and received steady infliximab maintenance therapy (5 mg/kg q8w n = 17; q6w n = 4; q10w n = 1; 10 mg/kg q8w n = 1). Trough blood samples had been obtained in the same patients prior to pregnancy ( n = 119), the first trimester ( n = 16), second trimester ( n = 18), third trimester ( n = 7), and post-pregnancy ( n = 12). Data were analyzed using nonlinear mixed-effects population pharmacokinetic modelling. Results Dose-normalized infliximab concentrations were significantly higher during the second trimester (median 15 µg/mL/kg, interquartile range 10–21) compared to pre-pregnancy (7, 2–12; p = 0.003), the first trimester (9, 1–12; p = 0.04), or post-pregnancy (6, interquartile range 3–11; p > 0.05) in patients with inflammatory bowel disease. Similar trends were observed in the third trimester (13, 7–36; p > 0.05). A one-compartment model with linear elimination described the pharmacokinetics of infliximab (volume of distribution = 18.2 L; clearance 0.61 L/day). Maternal infliximab exposure was influenced by the second and third trimester of pregnancy and anti-infliximab antibodies, and not by pregnancy-imposed physiological changes in, for example, body weight or albumin. Infliximab clearance decreased significantly during the second and third trimesters by up to 15% as compared to pre- and post-pregnancy and the first trimester. The increased maternal infliximab exposure was weakly associated with lowered clinical disease activity. Pharmacokinetic model simulations of virtual patients indicated the increased maternal infliximab trough concentrations imposed by pregnancy will not completely counteract the decrease in infliximab concentration if therapy is paused in the third trimester. Conclusion Infliximab clearance decreases significantly in the second and third trimesters, leading to increasing maternal infliximab concentrations in any given regimen. Maternal infliximab levels may thus be maintained as constant in a de-intensified regimen by therapeutic drug monitoring guidance in inflammatory bowel disease.

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“…Potential effects of TNFi on pregnancy outcomes should be considered. Increased risks associated with TNFi of preterm birth, caesarean section and small for gestational age children have been previously reported (Bröms et al, 2020). However, given the study design and the fact that high disease activity is known to negatively influence pregnancy outcomes (Smeele and Dolhain, 2019), these effects might not be drug-derived, but due to confounding by indication.…”

Section: Discussionmentioning

confidence: 94%

IL-6 but Not TNFα Levels Are Associated With Time to Pregnancy in Female Rheumatoid Arthritis Patients With a Wish to Conceive

et al. 2020

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Fertility issues are common amongst women with rheumatoid arthritis (RA). Interleukin 6 (IL-6) and tumor necrosis factor alpha (TNFα), known key players in RA pathogenesis, have been associated with reproductive disorders. This study investigates the role of these cytokines in decreased fertility in women with active RA. Preconception cytokine measurements of 61 patients from the PARA-cohort, a prospective study on RA and pregnancy, were studied in relation to time to pregnancy as a measure for fertility. IL-6 levels were higher in patients with a time to pregnancy longer than 1 year (p = 0.016). Survival analysis of patients stratified by high or low serum IL-6 levels, shows a prolonged time to pregnancy in the high IL-6 group (p = 0.045). Univariate cox regression analysis of IL-6 in relation to time to pregnancy as well as multivariate cox regression analysis correcting for age, disease activity, nulliparity, NSAID use and prednisone use were performed, with hazards ratios for log transformed IL-6 of 0.68 (95% CI: 0.51–0.93, p = 0.015) and 0.66 (95% CI: 0.43–0.99, p = 0.044), respectively. For TNFα, no association with time to pregnancy was found. This study shows that high IL-6, but not TNFα, is associated with decreased fertility in women with RA. This finding provides a rationale to therapeutically target the IL-6 pathway in the time period before pregnancy. More research in the form of large cohort studies on drug safety and the effect of bDMARDS on fertility is needed for implementation of treatment strategies directed at fertility issues in women with RA.

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Anti‐TNF treatment during pregnancy and birth outcomes: A population‐based study from Denmark, Finland, and Sweden

Cited by 50 publications

References 47 publications

Benefits and Risks of IgG Transplacental Transfer

Benefits and Risks of IgG Transplacental Transfer

Infliximab clearance decreases in the second and third trimesters of pregnancy in inflammatory bowel disease

IL-6 but Not TNFα Levels Are Associated With Time to Pregnancy in Female Rheumatoid Arthritis Patients With a Wish to Conceive

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