Teri Puhalsky, BSN, RN, CRNI

The autoimmune diseases we treat every day have implications across the patient’s lifespan. Women in their childbearing years are faced with a problem that doesn’t have an easy solution. Do they risk adverse pregnancy outcomes and their own health to have a baby, knowing they have a complex and sometimes difficult-to-treat disease? Many providers discourage women from becoming pregnant, but they lack the data to support their position. Studies like this one are essential so that the real risks and potential outcomes to the baby and the mother can be discussed.

In my practice, when the patient begins discussing the desire to become pregnant, we immediately send her to a high-risk pregnancy provider so that all the expectations can be discussed up front and she can get the needed support.

Pre-pregnancy counseling, referrals to high-risk pregnancy providers, multidisciplinary management of her disease and medications, and close monitoring especially during the first trimester are critical pieces of the care plan.

Ellen M. Field, MD

Although there are a multitude of studies regarding pregnancy outcomes in patients with anti-phospholipid syndrome and systemic lupus erythematosus, little data are available for pregnancy outcomes in systemic sclerosis. Studies to date have had conflicting data and the more recent studies, including prospective data from two published studies, concluded successful outcomes similar to the general population, with no increase in maternal mortality. Older studies, mainly observational case studies, showed poor outcomes, both maternal and fetal, with increased infertility, miscarriage and maternal complications.

This study was designed to retrospectively compare pregnancy and disease outcomes of women with SSc with those of patients with APS and SLE, including a healthy control group, all followed prospectively through their pregnancies.

Prior data showed discordant risk for preterm birth, intrauterine growth restriction (IUGR), small for gestational age (SGA) newborns and preeclampsia. Some data suggest higher risk for progression in women with early onset — less than 4 years — diffuse cutaneous scleroderma and positive anti-topoisomerase antibodies.

In general, APS and SLE are frequently associated with poor outcomes including recurring fetal loss, preeclampsia, placental insufficiency and IUGR.

Demographics included 21 pregnant women with SSc, 26 pregnant women with SLE, 31 pregnant women with APS and 40 healthy controls who were all age matched.

Results included 21 patients with SSc, with a total of 33 pregnancies, four of which were conceived through assisted reproductive technology. A total of 121 control pregnancies included 40 pregnancies from 26 patients with SLE, 41 pregnancies from 31 patients with APS, and 40 healthy controls. Mean disease duration at conception in SSc was 6 years, 9.4 years for SLE and 2.5 years for APS.

Results showed an increased risk overall for adverse pregnancy outcomes for SSc including miscarriage, SGA newborns, preeclampsia and premature deliveries.

I would agree with the authors that the main strength of the study was that patients were followed prospectively with real-time assessments as compared to prior studies where data were collected through questionnaires or database information. The limitations include small study size and the retrospective analysis.

There is a significant need for larger cohort population studies in patients with SSc, who represent an increasing population of pregnancies in autoimmune disease. Additionally, there is a need for pre-pregnancy counseling and management by high-risk maternal fetal medicine clinicians.