Management of dermatological conditions in pregnancy

20.1 Introduction

Every system in the body undergoes drastic changes during pregnancy, including the integumentary system. These dermatological changes are a result of varying factors, such as alterations in collagen formation, increase in sebaceous and eccrine gland secretion, shifts in hormone production, and increased circulatory blood volume [ ]. This can lead to the development of new or worsening of current dermatological conditions during pregnancy. While these conditions are oftentimes minor and resolve after pregnancy, some can be of significant concern for the woman during the antepartum period [ ]. This may prompt the pregnant woman to seek treatment from the health care provider, who will need to utilize sound clinical judgment on how to safely manage dermatological conditions during pregnancy and the postpartum period. Overall, management can be addressed with one of four approaches: (1) delay treatment until after pregnancy; (2) consider nonpharmacologic alternatives; (3) judiciously prescribe medications; or (4) discontinue breastfeeding during the postpartum period and prescribe accordingly.

Even when considering one of the before mentioned approaches, the clinical decision regarding medication use during pregnancy is hazed by the paucity of randomized clinical trials that include pregnant women. Furthermore, the new Federal Drug Administration (FDA) Pregnancy Category that replaced the previous A, B, C, D, and X system in 2015 has been faced with criticism for being confusing when it comes to interpreting medication safety and fetal risk assessment [ ]. This is especially alarming since findings from a large, prospective cohort study of nulliparous women suggested that more than 90% of the study participants took at least one medication while pregnant [ ]. Therefore, it is imperative that guidance be provided to health care providers with regards to the practice of prescribing medications to patients who are pregnant or breastfeeding. The choice to take medications should be a joint decision between the patient and health care provider [ ].

The purpose of this chapter is to provide direction for health care providers who are faced with the dilemma of prescribing medications for managing dermatological conditions for patients during the antepartum and postpartum periods. Although a plethora of conditions impacting the integumentary system during pregnancy exists, this chapter will focus on managing the most common alterations. These include acne, psoriasis, dermatoses, bacterial infections, viral infections, fungal infections, and parasitic infections. When describing medication safety risk for the pregnant patient, the FDA categorical method will be utilized.

20.2 Acne

Acne is a common dermatological condition that can vary from mild comedones to severe inflammation and scarring [ ]. The pregnancy state can exacerbate clinical manifestations of acne. The basis for deciding to treat acne during pregnancy and the postpartum period is based on the severity of the condition. However, prescribing medications for acne can be perplexing since there are a limited number of safe pharmacologic choices available for patients who are pregnant or breastfeeding [ ].

20.2.1 Topical agents

Because of their low systemic absorption, topical medications should be the initial line of treatment when managing mild to moderate acne during pregnancy and lactation. Meredith and Ormerod [ ] described several considerations that should be taken into account with the use of topical agents, such as the “amount of agent applied; surface area of application; length of application time; frequency of application; application to broken skin/erosions; choice of vehicle used; and thickness of stratum corneum” (p. 353).

Although antibacterial agents, such as erythromycin (category B) 1%–3% in petroleum jelly once daily, clindamycin (B) 1% once daily, and metronidazole (category B) 0.75%, may be prescribed, monotherapy with topical antibacterial medications is of concern due to the problem of antibiotic resistance [ ]. Another concern exists regarding the use of topical metronidazole among pregnant women since animal studies have suggested a link between oral metronidazole and carcinogenicity with no adequate studies of pregnant women to support its use [ ]. Therefore, topical metronidazole should be regarded as an alternative to topical erythromycin and clindamycin when treating acne in pregnancy. Topical metronidazole should be avoided altogether for lactating women due to its secretion in breast milk, having comparable concentration levels to plasma levels with oral use [ ]. Limited data exist regarding the use of topical dapsone (category C) and nadifloxacin (category N) by pregnant and lactating women.

Comedolytics, such as azelaic acid (category B) and benzoyl peroxide 2.5% (category C), are considered safe in pregnancy and lactation due to their low systemic absorption. In fact, findings from a study estimated that the systemic absorption of topical benzoyl peroxide is approximately 5% [ ]. Topical benzoyl peroxide is also a popular pharmacologic agent in managing acne because it possesses some antiinflammatory properties.

Another class of medications used to treat comedones of mild to moderate acne is topical retinoids, such as tretinoin (category C), isotretinoin (category C), tazarotene (category X), and adapalene (category C). Tazarotene has been assigned an FDA category X; thereby, it is contraindicated in pregnancy. Conflicting reports exist regarding the safe use of topical retinoids among pregnant women. Several reports have suggested a correlation between topical tretinoin and congenital birth defects, such as cardiac anomalies, diaphragmatic hernia, and ear and limb malformations, in the neonates of women who used these agents during early pregnancy [ ]. On the contrary, findings from a case control study did not suggest an increased risk for birth defects among infants exposed to topical tretinoin from maternal use [ ]. Furthermore, findings from a prospective observational study comparing women who were exposed to topical retinoid in the first trimester of pregnancy to a control group of pregnant women indicated no statistically significant difference in neonatal birth defects among these two groups [ ]. On the other hand, when assessing the safety of adapalene use in pregnancy, an association between this medication and anophthalmia has been suggested [ ]. Even the manufacturers of topical retinoids caution their use in pregnancy.

Since data regarding the excretion levels of tazarotene into breast milk are unknown, it is not recommended for use by lactating women. Tretinoin and adapalene have low levels of systemic absorption. Therefore, they are regarded as being safe for use in women who are breastfeeding.

20.2.2 Oral agents

For women who have acne unresponsive to topical agents, oral medications may be considered. One category of medications used for systemic treatment is antibiotics. However, caution regarding antibiotic resistance holds true for oral antibiotics, as with topical antibiotic agents. With the exception of early pregnancy, erythromycin (category B) 400 mg every 8 h before meals is the oral antibiotic of choice in helping to manage acne. When prescribing erythromycin for this indication, it recommended that it be combined with a topical agent, if possible, to address concerns regarding antibiotic resistance [ ]. Another concern pertains to the use of erythromycin estolate, which should not be used in pregnancy due to risks of maternal hepatotoxicity [ ]. Azithromycin (category B) with varying dosing regimens may be another option, but there are less data supporting its safe use in pregnancy when compared to erythromycin [ ]. Another choice may be amoxicillin (category B) 250–500 mg twice daily alone or in combination with another agent, although data support that its use in early pregnancy may increase the risk for oral clefts [ ].

Trimethoprim (category C) use in early pregnancy has been associated with spontaneous abortions [ ], fetal cardiovascular defects, oral clefts, and urinary tract anomalies in women who did not take a folic acid supplement [ ]. Therefore, trimethoprim/sulfamethoxazole 160/800 mg twice a day should only be prescribed if other options are lacking and the benefits outweigh the risks. Moreover, sulfonamides can remain in the neonatal circulation in the first few days following birth if maternal ingestion of the drug takes place near term [ ]. This can lead to the development of jaundice, hemolytic anemia, hyperbilirubinemia, and theoretically, kernicterus in the newborn. As a result, this drug should not be administered to pregnant women near the end of their pregnancies.

Tetracycline (category D) should be avoided altogether in pregnancy due to embryo and fetal toxicity, including staining of deciduous teeth and impaired skeletal development [ ]. If fetal exposure to this medication takes place after the 20th week of pregnancy, the deciduous teeth become yellow and progressively darken because tetracycline binds to calcium orthophosphate, subsequently becoming actively deposited in teeth and bones [ ]. The effects on the fetal skeletal bone are considered reversible, but it can retard growth of the fibula in premature infants [ ]. Studies have also suggested its use in pregnancy can cause acute fatty metamorphosis of the liver in the pregnant woman [ ].

Oral retinoids are a popular choice for managing acne in the nonpregnant patient. Due to its severe teratogenic effects, isotretinoin (category X) is contraindicated for use in pregnancy. Isotretinoin has been linked to fetal craniofacial, cardiac, central nervous system, and thymus and parathyroid gland malformations [ ]. Manufacturers of the drug advise women to avoid pregnancy 1 month before, during, and 1 month after taking isotretinoin and that women must use two different forms of contraception during this time [ ]. Prescribers of isotretinoin in the United States are required to participate in the iPledge [ ] program, a computer-based risk management system designed to prevent use by pregnant women. Oral retinoids are not recommended for use during the lactating period.

20.3 Psoriasis

Psoriasis is an autoimmune disease characterized by thick, pruritic, scaly plaques on the skin. The increased estrogen levels that occur during pregnancy are thought to lead to an immune tolerant state, resulting in an improvement of these symptoms for many pregnant women [ ]. Results of a study examining pregnant women with psoriasis found 55% demonstrated improvement, 21% had no change, and 23% experienced worsening of symptoms during pregnancy [ ]. For pregnant women who do require treatment, pharmacologic management can be challenging for the prescriber.

20.3.1 Topical agents

In general, topical agents, such as moisturizers, calcipotriene (category C), and low-to-moderate-potency corticosteroids (category C), are the first line of treatment to manage localized psoriasis for pregnant and breastfeeding women [ ]. A study assessing the outcomes of pregnant women exposed to topical corticosteroids found no increased risk of low birth weight infants, fetal anomalies, or preterm birth [ ]. However, more potent topical corticosteroids applied to a large body surface area have similar effects as systemic oral preparations and should be used with caution by pregnant women [ ]. Calcipotriene (category C), a synthetic derivative of vitamin D3, is considered a safe topical agent for use by pregnant women [ , ]. Another option is topical tacrolimus (category C), a calcineurin inhibitor that is primarily effective as a local agent in treating psoriasis in the facial or intertriginous areas [ ]. Results of animal studies have indicated no reports of teratogenicity associated with topical tacrolimus [ ]. Other topical agents, such as crude coal tar (category C) and tazarotene (category X), should not be used during pregnancy since teratogenic risks are seemingly unknown [ ].

The second-line treatment option for managing psoriasis in pregnancy is both narrow and broadband ultraviolet B phototherapy, which can be used alone or in combination with topical agents [ ]. Since penetration of the ultraviolet light is limited to the maternal skin, this is considered safe for the fetus and breastfeeding newborn [ ]. However, decreased maternal folic acid levels have been associated with repeated exposure to broadband ultraviolet B with recommendations for folic acid monitoring by the prescriber [ ]. Psoralen and ultraviolet A light should not be used in pregnancy due to associated mutagenic properties [ ].

20.4 Oral agents

If psoriasis is persistent or worsens during pregnancy, systemic treatment may be warranted. Cyclosporine (category C) 2.5–5 mg/kg/day is considered the initial oral agent of choice [ ]. The drug passively crosses the placental blood barrier resulting in 10%–50% of the maternal plasma concentration and lacks mutagenic or teratogenic properties [ ]. Contrary to its acceptable use in pregnancy, oral cyclosporine should be avoided in lactating women since it possesses immunosuppressive characteristics, potentially impacting the breastfed newborn [ ].

Oral corticosteroids, such as prednisone (category D), prednisolone (category D), or methylprednisolone (category C), are not used in the treatment of common psoriasis in pregnancy due to reports indicating an association with their use and gastroesophageal reflux, low birth weight, intrauterine growth restriction, and oral clefts among neonates exposed in utero [ ]. Although a metaanalysis failed to find an increased risk for serious fetal anomalies, the authors raised concern with using oral corticosteroids during the first trimester of pregnancy [ ]. These medications may be used by lactating women with a recommended 3–4 h interval from ingestion to a breastfeeding episode [ ].

Mycophenolate mofetil (category D) has been associated with congenital anomalies and first trimester spontaneous abortion; thereby, should not be used by pregnant women or those attempting to conceive [ ]. Similarly, methotrexate (category X) and acitretin (category X) should be avoided by pregnant and lactating women. Methotrexate is an abortifacient with mutagenic and teratogenic properties, such as anencephaly, cleft palate, and ear and skeletal malformations, and should not be used by women or men for 3 months prior to conception [ ]. Due to storage in adipose tissue, stricter guidelines are used for acitretin by which pregnancy should be avoided up to 3 years after discontinuing treatment due to risks for severe fetal anomalies, such as craniofacial, ear, thymus, central nervous system, and cardiovascular system malformations [ ].

Biologic agents, such as etanercept (category B), infliximab (category B), and adalimumab (category B), are becoming an increasingly popular choice in treating psoriasis. However, severely limited data on their use in pregnancy make prescribing to the pregnant and lactation populations somewhat perplexing. The majority of studies examining the administration of these medications to pregnant women are from their use in managing irritable bowel syndrome and rheumatoid arthritis [ ]. One report indicated that newborns exposed to infliximab and adalimumab in utero had significantly higher concentrations of these drugs when compared to their mothers, with levels still detectable during the first 2–7 months of life [ ]. While the placental transfer of etanercept to the fetus is much lower [ ], there has been a case report of a neonate who developed VACTERL syndrome while exposed to etanercept in utero [ ]. This condition, which causes vertebral anomalies, anal atresia, cardiac anomalies, tracheoesophageal fistula, esophageal atresia, renal anomalies, and limb anomalies, was also observed in animal studies involving etanercept [ ]. Moreover, a study involving 41 women who took etanercept or infliximab while pregnant found 59% of their newborns displayed at least one clinical manifestation of VACTERL syndrome [ ]. A case of partial VACTERL association was also reported in an infant whose mother took adalimumab while pregnant [ , ]. It is noteworthy that there have been no other reported anomalies in newborns exposed to etanercept in utero [ , ]. A comparison of women who took infliximab while pregnant also noted no increased risk of fetal or neonatal anomalies [ ]. The potential for immunosuppression in the newborn exposed to biologic agents is also of concern, especially after an infant who was exposed to infliximab in utero died from disseminated bacillus Calmette-Guerin infection after being vaccinated [ ].

Due to the low levels of etanercept and infliximab in breast milk, evidence supports their safe use by breastfeeding women [ ]. Although evidence seemingly supports the use of these biologic agents in pregnant and nursing women, due to the lack of long-term and rigorous studies, it makes arriving at a definitive conclusion regarding their safe use difficult to determine. Further lacking are empirical data on the use of newer biologic agents, such as ustekinumab, secukinumab, and ixekizumab, with pregnant and lactating women [ ].

20.5 Dermatoses

Dermatologic conditions that only occur in pregnancy and the immediate postpartum period are referred to as dermatoses of pregnancy. In 2006, these conditions were reclassified by Ambros-Rudolph, Mullegger, Vaughan-Jones, Kerl, and Black to include four conditions: (1) pemphigoid gestationis (PG); (2) polymorphic eruption of pregnancy (PEP); (3) intrahepatic cholestasis of pregnancy (ICP); and (4) atopic eruption of pregnancy (AEP) [ ]. While there are vast differences among these conditions, the underlying commonality is the intense pruritus associated with these dermatoses. Therefore, the hallmark treatment includes the use of antihistamines since they are considered the first line of treatment in managing pruritus associated with dermatological conditions during pregnancy [ ].

Systemic antihistamines are classified as first generation and second generation, with the primary difference being that first-generation antihistamines, such as chlorpheniramine (category B), diphenhydramine (category B), dexchlorpheniramine (category B), and hydroxyzine (category C), have sedating effects, while second-generation antihistamines, such as loratadine (category B), cetirizine (category B), fexofenadine (category C), and azelastine (category C), do not [ ]. This impact on the central nervous system should be taken into consideration by prescribers since it may pose a safety risk and interfere with the patient's quality of life by producing long-lasting sedative effects associated with first-generation oral antihistamines [ ]. Even so, when prescribing a first-generation oral antihistamine, the prescriber should educate the patient to take this medication prior to sleeping.

However, more empirical data exist assessing the use of first-generation antihistamines, likely because they have been used longer when compared to newer, second-generation antihistamines. A metaanalysis of 24 studies with more than 200,000 pregnant women who took an oral first-generation antihistamine during the first trimester of their pregnancies discovered no increased fetal or maternal risk [ ]. Moreover, this result was corroborated by the findings of several studies [ ]. Nonetheless, because oral diphenhydramine has been associated with retinopathy of prematurity, formerly known as retrolental fibroplasia, it should be avoided during the last 2 weeks of pregnancy [ ]. It should also not be used during this time frame because it may cause withdrawal symptoms, such as irritability and difficulty feeding, in newborns exposed to this medication in utero [ ]. Additionally, high doses of diphenhydramine can cause uterine contractions, resulting in premature births [ ]. Another first-generation antihistamine, hydroxyzine, should not be taken in the first trimester of pregnancy due to its association with fetal anomalies [ ].

First-generation systemic antihistamines are not recommended for use by lactating women primarily due to the lack of supporting evidence [ ]. It is recognized that these drugs may lead to drowsiness and lethargy in the breast-fed newborn [ ]. It has also been proposed that first-generation oral antihistamines may cause decreased maternal milk production due to their impact on dopamine secretion [ ].

With regards to second-generation antihistamines, systemic loratadine and cetirizine are considered safe during the second and third trimesters of pregnancy and lactation [ ]. Initial concerns regarding the risk of hypospadias in newborns exposed to maternal oral use of loratadine in utero were refuted by the Centers for Disease Control and Prevention after assessing data from the National Birth Defects Prevention Study [ ]. As with first-generation antihistamines, these second-generation medications should not be taken in large doses near the time of delivery [ ].

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