Women

Fear of infertility is common among patients with IBD and may adversely impact family planning decisions. In reality, women with quiescent IBD and no prior pelvic surgery have similar infertility rates (5%–14%) as the general population. Active disease does impair fertility, likely via multifactorial mechanisms, such as pelvic inflammation, poor nutrition, decreased libido, dyspareunia, and depression. A small study demonstrated decreased ovarian reserve in women with Crohn disease, especially those with active disease. Pelvic surgery significantly increases female infertility due to scarring and adhesions. A meta-analysis of ileal pouch anal anastomosis (IPAA) surgery in ulcerative colitis found a 48% postoperative infertility rate, threefold higher than the 15% rate in medically treated patients. Laparoscopic total proctocolectomy with IPAA may preserve fertility compared with open surgery. Abdominal surgeries that spare the pelvis, such as colectomy with ileorectal anastomosis, may also preserve female fertility. Women of childbearing potential should be counseled before surgery about the infertility risk of IPAA, and less invasive procedures may be considered. However, given the retrospective nature of the studies and older techniques, true rates of infertility following IPAA are not known. IPAA does not appear to impact success rates of in vitro fertilization.

Women who experience difficulty conceiving or spontaneous abortion should be assessed for occult disease activity, hypovitaminosis D, and celiac disease, all of which are associated with infertility. If women remain unable to conceive after 6 months of calculated attempts, reproductive endocrinology referral is warranted.

Men

Less is known about male fertility in IBD. Zinc deficiency in Crohn disease may impair sperm function. Certain medications have been shown to affect sperm quantity and quality. Sulfasalazine causes reversible infertility due to dose-dependent oligospermia, reduced sperm motility, and altered sperm morphology. Methotrexate may reduce sperm quality, although any such effects are reversible when the drug is discontinued. Some experts recommend that men stop methotrexate at least 3 months before attempting conception. Antitumor necrosis factor α (anti-TNF) medications may accelerate germ cell apoptosis in the seminiferous tubules, which might theoretically decrease sperm count. However, a small study of 10 men did not find a decrement in sperm concentration following infliximab infusion. It remains unknown whether medication-induced changes in sperm quality have any effect on fertility, and additional research is needed.

Inflammatory Bowel Disease Detrimentally Impacts Pregnancy

Women with IBD, including those in remission, experience a higher rate of adverse pregnancy outcomes than the general population. A recent meta-analysis including 15,007 women with IBD found increased odds of preterm birth (odds ratio [OR] 1.85, 95% confidence interval [CI] 1.67–2.05), small for gestational age infants (OR 1.36, 95% CI 1.16–1.60), and still birth (OR 1.57, 95% CI 1.03–2.38). The risk of congenital anomalies was also increased (OR 1.29, 95% CI 1.05–1.58), although there was evidence of publication bias. Multiple recent population-based studies failed to detect an increased risk of congenital anomalies in IBD pregnancies. IBD is associated with higher rates of pregnancy complications, such as preeclampsia, preterm premature rupture of membranes, and venous thromboembolism. Inadequate maternal weight gain has been identified as a predictor of adverse outcomes. Additional hypothesized mediators of increased risk include inflammation, anemia, hypoalbuminemia, poor nutrition, and medication exposures. Based on these findings, all IBD pregnancies should be monitored by a maternal-fetal medicine specialist. Serial ultrasonography should be considered in the third trimester to assess fetal growth.

Pregnancy May Impact Inflammatory Bowel Disease

It remains uncertain whether pregnancy itself adversely affects the course of IBD. Among women in remission at conception, the risk of subsequent disease exacerbation during pregnancy is 20% in Crohn disease and 33% in ulcerative colitis. The ongoing prospective, multicenter Pregnancy in Inflammatory Bowel Disease and Neonatal Outcomes (PIANO) registry of more than 1475 pregnant women with IBD also found a higher rate of ulcerative colitis activity relative to Crohn activity. Overlapping immune pathways, such as placental production of proinflammatory cytokines, have been hypothesized as a potential explanation for this finding. Alternatively, this may reflect less aggressive ulcerative colitis treatment, as most of these patients were on mesalamine monotherapy. A meta-analysis of 1720 patients with IBD found that disease activity during pregnancy strongly correlates with disease activity at the time of conception. Active disease affected 46% to 55% of pregnancies commenced during active disease, compared with 23% to 29% of pregnancies conceived during remission. Overall, IBD relapse rates during pregnancy are similar to rates for nonpregnant women.

Disease behavior during pregnancy and the postpartum period is likely confounded by the frequent and inappropriate discontinuation of maintenance medications, which increases the risk of flare. Providers must educate patients about the risk of disease to the pregnancy and the importance of medication adherence to optimize preconception disease control and maintain remission throughout pregnancy.

Medications

With the exception of methotrexate and thalidomide, most medications used to treat IBD are considered low risk and may be continued during pregnancy and breastfeeding ( Table 1 ). Of note, the US Food and Drug Administration recently implemented a revised medication labeling rule that removes the previously used pregnancy categories (A, B, C, D, X). We will not reference the pregnancy categories in the following discussion.

Biologics

Anti–tumor necrosis factor agents

Of the 4 anti-TNF medications approved for IBD, infliximab and adalimumab provide most pregnancy safety information. Although mainly limited to case series, available data on the anti-TNF class suggest low risk for use during pregnancy. However, the long-term implications of intrauterine exposure remain unknown, especially with respect to immune system development and function.

Series with more than 100 IBD pregnancies each exposed to infliximab, adalimumab, and certolizumab pegol found no adverse effect on pregnancy outcomes. Golimumab is predicted to have a similar safety profile. More than 500 women in the PIANO registry have been exposed to anti-TNF medications during pregnancy: more than 260 infliximab, more than 150 adalimumab, more than 65 certolizumab pegol, and 29 multiple agents. There is no increased risk of congenital anomalies compared with the unexposed IBD cohort. A systematic review including more than 1500 anti-TNF exposed pregnancies found no pattern of adverse pregnancy outcomes or congenital anomalies. A recent meta-analysis showed a similar rate of unfavorable pregnancy outcomes between women taking anti-TNF therapy and unexposed controls (OR 1.00; 95% CI 0.72–1.41), including preterm delivery (OR 1.00; 95% CI 0.62–1.62), low birth weight (OR 1.05; 95% CI 0.62–1.78), and congenital anomalies (OR 1.10; 95% CI 0.58–2.09).

Combination therapy with an anti-TNF and thiopurine may be associated with a higher risk of preterm birth (OR 2.4; 95% CI 1.3–4.3) and any pregnancy complication (OR 1.7; 95% CI 1.0–2.2), in addition to the risk of delayed infant infections described previously.

There is clinically insignificant anti-TNF excretion into breast milk, with milk concentrations less than 1% of maternal plasma concentrations. Furthermore, antibodies ingested orally are unlikely to be bioavailable. In the PIANO registry, breastfed infants exposed to anti-TNF monoclonal antibodies have similar rates of growth and milestone achievement compared with unexposed breastfed infants, with no increased risk of infection.

Transplacental drug transfer

Monoclonal immunoglobulin G1 (IgG1) medications (infliximab, adalimumab, golimumab) are actively transported across the placenta along with other maternal antibodies, beginning in the second trimester. Fetal IgG1 concentrations increase logarithmically, with 80% of transfer occurring in the third trimester. Cord blood infliximab and adalimumab concentrations at birth exceed maternal levels by up to fourfold, and these agents remain detectable in infants for up to 12 months. This raises concern about potential adverse effects on neonatal immune system development. In the PIANO registry, third trimester anti-TNF exposure did not detrimentally affect infant growth rate, immune development, number of infections, or achievement of developmental milestones. A small study of 25 anti-TNF exposed children reported appropriate serologic response to vaccination and normal cellular immunity.

Until the implications of intrauterine anti-TNF exposure are better understood, it is reasonable for women in sustained remission to consider third trimester dosing adjustments to reduce neonatal exposure ( Table 2 ). Therapeutic drug monitoring with trough serum concentrations in the late second or early third trimester may also help guide dosing before delivery. However, any decision to alter medication dosing schedule should be individualized and balanced against the risks, which include triggering active disease or maternal immunization with diminished future drug effectiveness.

Table 2

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