Issue: October 2022
Fact checked byShenaz Bagha

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August 16, 2022
2 min read
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No adverse childhood outcomes through 17 years after prenatal hydroxychloroquine exposure

Issue: October 2022
Fact checked byShenaz Bagha
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Prenatal exposure to hydroxychloroquine in birthing parents with systemic lupus erythematosus results in no significant adverse outcomes in children from breast feeding through 17 years, according to data published in Rheumatology.

The data also revealed that pregnant patients with SLE who received azathioprine had an increase in reports of childhood infection. However, the researchers stated this may be a result of recall bias and requires further study.

Pregnant
Prenatal exposure to hydroxychloroquine in birthing parents with systemic lupus erythematosus results in no significant adverse outcomes in children from breast feeding through 17 years, according to data derived from Reynolds JA, et al. 2022;doi:10.1093/rheumatology/keac372. Source: Adobe Stock

“Both hydroxychloroquine and azathioprine are important drugs in the management of systemic lupus erythematosus (SLE) and are considered to be compatible with pregnancy and breastfeeding,” John A. Reynolds, MRCP, PhD, of the University of Birmingham, in the United Kingdom, told Healio. “There are limited data about longer-term outcomes of children who are exposed to these drugs in utero.”

To examine outcomes among children born to patients with SLE who used hydroxychloroquine or azathioprine during pregnancy and breast-feeding, Reynolds and colleagues conducted a retrospective study of data collected using a questionnaire between 2007 and 2011. Eligible participants were women who met four or more criteria from the updated 1997 American College of Rheumatology classification for SLE prior to pregnancy.

In addition, the researchers assessed participants’ ACR classification criteria, the presence of lupus-related autoantibodies and renal biopsy results for each patient. Additionally, pregnancy data, including drug exposure from conception through breast feeding, and pregnancy outcomes were recorded.

The second portion of the questionnaire was filled out by the participants and included childhood outcomes through the age of 17 years. This survey included information on the presence of neonatal lupus rash, congenital heart block, any congenital malformations and any hospital admissions, as well as the diagnosis for the visit and any evidence demonstrating developmental delays.

In all, the study analyzed 284 live births from 199 patients at 10 sites in the United Kingdom. In all, 150 (60.4%) of the children were exposed to hydroxychloroquine and 87 (31%) were exposed to azathioprine. According to the researchers, there was “no significant difference” in the frequency of malformations or intrauterine growth restrictions between children exposed and those who were not exposed to either drug. However, adjusted models demonstrated that azathioprine exposure was linked to increased reports of childhood infection needing hospital intervention (OR = 2.283; 95% CI, 1.003-5.198).

“This study supports the existing literature that hydroxychloroquine is compatible with pregnancy in patients with SLE,” Reynolds said. “Although pregnant women were more likely to take azathioprine if they had a history of renal disease or hypertension, azathioprine use was not associated with intrauterine growth restriction (IUGR) or low birth weight.

“It is important to recognize that infection was self-reported by the mothers,” he added. “There may be recall bias as mothers taking a drug such as azathioprine might have been more likely to recall episodes of infection.”