Psychotropic Drug Use During Breastfeeding: A Review of the Evidence

Filomena Fortinguerra, Antonio Clavenna and Maurizio Bonati

  Pediatrics 2009;124;e547-e556; originally published online Sep 7, 2009;

DOI: 10.1542/peds.2009-0326

  

The online version of this article, along with updated information and services, is

located on the World Wide Web at:

  PEDIATRICS is the official journal of the American Academy of Pediatrics. A monthly

publication, it has been published continuously since 1948. PEDIATRICS is owned, published, and trademarked by the American Academy of Pediatrics, 141 Northwest Point Boulevard, Elk Grove Village, Illinois, 60007. Copyright © 2009 by the American Academy of Pediatrics. All rights reserved. Print ISSN: 0031-4005. Online ISSN: 1098-4275. Psychotropic Drug Use During Breastfeeding: A Review of the Evidence WHAT’S KNOWN ON THIS SUBJECT:

  The evidence on psychotropic medication use during breastfeeding is limited for many drugs, in particular for antipsychotics, hypnotics, and anxiolytics. This lack of data makes it difficult to formulate any generalizations regarding the safety of these medications.

  We systematically collected and evaluated the available information on the safety of psychotropic medication use during breastfeeding to provide physicians with updated and evidence-based information for current problems in daily clinical practice.

  abstract OBJECTIVE:

  The objective of this study was to review the existing liter- ature on the use of various classes of psychotropic medications during breastfeeding to provide information about infant exposure levels and reported adverse events in breastfed infants.

  METHODS:

  A bibliographic search in the Medline (1967 through July 2008), Embase (1975 through July 2008), and PsycINFO (1967 through July 2008) databases was conducted for studies on breastfeeding and psychotropic medications for a total of 96 drugs. References of re- trieved articles, reference books, and dedicated Web sites were also checked. The manufacturers were contacted for drugs without pub- lished information. Original articles and review articles that provide pharmacokinetic data on drug excretion in breast milk and infant safety data were considered, to estimate the “compatibility level” of each drug with breastfeeding.

  RESULTS: A total of 183 original articles were eligible for analysis.

  Documentation was retrieved for 62 (65%) drugs. In all, 19 (31%) psy- chotropic drugs can be used during lactation according to an evidence- based approach. For 28 drugs, the available data do not permit an evaluation of the drug’s safety profile during breastfeeding and, for an additional 15 drugs, the exposure dose or observed adverse effects make their use unsafe. Breastfeeding is essential for the phys- ical and psychological health of both mother and child, and its benefits are well documented.

  

CONCLUSIONS:

  Although most drugs are considered safe during breastfeeding, compatibility with breastfeeding has not been estab- lished for all psychotropic drugs. There is a need for additional re- search and accumulation of experience to guarantee a more rational use of psychotropic drugs during breastfeeding. Pediatrics 2009;124: e547–e556

  AUTHORS: Filomena Fortinguerra, PharmD, Antonio Clavenna, MD, and Maurizio Bonati, MD Laboratory for Mother and Child Health, Public Health Department, Mario Negri Institute for Pharmacological Research, Milan, Italy

KEY WORDS

  breastfeeding, psychotropic drugs, drug therapy, adverse effects, human, systematic review ABBREVIATION SSRI—selective serotonin reuptake inhibitor www.pediatrics.org/cgi/doi/10.1542/peds.2009-0326 doi:10.1542/peds.2009-0326 Accepted for publication Apr 23, 2009 Address correspondence to Filomena Fortinguerra, PharmD, Public Health Department, Laboratory for Mother and Child Health, “Mario Negri” Institute for Pharmacological Research, Via Giuseppe La Masa 19, 20156 Milan, Italy. E-mail: fortinguerra@marionegri.it PEDIATRICS (ISSN Numbers: Print, 0031-4005; Online, 1098-4275).

  Copyright © 2009 by the American Academy of Pediatrics FINANCIAL DISCLOSURE: The authors have indicated they have no financial relationships relevant to this article to disclose.

  ARTICLES

WHAT THIS STUDY ADDS:

  1–6

  and adverse short-term and long-term effects can have a negative impact on the developing infant and child.

  tal disorder in the perinatal period: ⬃10% to 16% of pregnant women ful- fill diagnostic criteria for major or mi- nor depression, but up to 70% report symptoms of depression.

  21 Further-

  more, ⬃7% to 20% of women receive a diagnosis of postpartum depression in the first year after delivery.

  22 Un-

  treated depression and anxiety can have a negative impact on pregnancy,

  23

  24,25

  The World Health Organization recommends exclusive breastfeeding for at least the first 4 to 6 months of life and its continuation for 1 to 2 years thereafter.

  The evidence on psychotropic medica- tion use in breastfeeding mothers is limited: for many drugs only case re- ports or very small studies are avail- able (often only pharmacokinetic data and not with respect to safety), whereas for other drugs on which more information is available, the re- views are not complete and updated. This lack of data makes it difficult to formulate any generalizations regard- ing the safety of these medications

  26–29

  ; therefore, there is a need to collect and evaluate systematically the available information on the risks of psychotropic drugs during breast- feeding. This article reviews the liter- ature to provide more complete and updated information on infant expo- sure levels and reported adverse events in the various psychotropic medication classes.

  METHODS

  Original articles and review articles on breastfeeding and mother and newborn infant exposure to 96 psychotropic drugs were considered. The drugs were classified according to the International Anatomic Therapeutical Classification system in antipsychotics (N05A), anxio- lytics (N05B), hypnotics and sedatives (N05C), antidepressants (N06A), psycho- stimulants (N06B), and antiepileptics (N03; Table 1). Drug combinations and drugs without indications for women of childbearing age were excluded. A bibliographic search in the Medline (1967 through July 2008), Embase (1975 through July 2008), and PsycINFO (1967 through July 2008) databases was performed. The searches per- formed were as follows: [drug name] and [breastfeeding or lactation or breast milk or drug milk level], limiting to [human].

  To make the search more complete, the terms were searched for in the da- tabases’ dictionaries as well as through a free text search of the key words in the articles’ titles and ab- stracts. Manual searches of bibliogra- phies were also conducted to identify additional pertinent studies. All of the references were then analyzed. Moreover, secondary sources, special- ist manuals, reference books, and ded-

  It has been estimated that, each year, more than 500 000 pregnancies in the United States are complicated by psychiatric disorders such as depression, anxiety, and psychosis, which often develop, re- cur, and/or worsen during and after pregnancy. Furthermore, 13% of all psychiatric hospital admissions for women occur during the first postpar- tum year.

  17–19

  orders in the perinatal period, a signif- icant number of women may require pharmacologic treatment.

9 Worldwide, more than half of breast-

  11

  7,8

  In the past few years, several initiatives have been launched to promote breastfeeding, which have led to an increase in this first-choice form of nutrition world- wide. Despite the increased attention toward breastfeeding, however, infor- mation on breast milk drug excretion and knowledge of the adverse effects on the infant are often unavailable or still limited for many drugs that fre- quently are used by women of child- bearing age, and misinformation abounds.

  feeding women take some type of drug,

  10

  and the concern about poten- tial harm to the nursing infant from maternal medications is often cited as a reason to stop lactation,

  even if dis- continuing breastfeeding is often the wrong decision. The Summary of Prod- uct Characteristics should not be con- sidered a reliable source of breast- feeding information; it often indicates that a drug is not recommended dur- ing lactation, suggesting that it be avoided or that breastfeeding be inter- rupted. The warnings are not neces- sarily related to observed or reported adverse effects; they are often used as a defensive measure on the part of the manufacturer when the drug’s safety information is not available. It is important that women be in- formed as to whether they can safely breastfeed while taking their medica- tion.

  16 Given the prevalence of psychiatric dis-

  drugs in lactation therefore seems in- dispensable in efforts to promote breastfeeding.

  13 Concerns that also at-

  tributable to a scarcity of available knowledge about drug safety during lactation are common for all drugs,

  14

  but for a few therapeutic classes such as psychotropic agents, they are relevant.

  15 Psychiatric disorders represent a con-

  siderable public health problem that affects a significant number of preg- nant and lactating women and can have substantial negative physical and psychological sequelae for mother and child. Because of these serious conse- quences, early diagnosis and treat- ment interventions are imperative for the health and well-being of the mother and the child.

20 Depression is the most frequent men-

12 Information on how to deal with

  icated Web sites (eg, LactMed, The MotherRisk Program–Hospital for Sick Children, American Academy of Pediat- rics, Martindale, Meyler’s Side Effects of Drugs) were consulted. Other infor- mation was found in the DRUGDEX da- tabase (Micromedex), a Web site that reports data on drugs from the medi- cal literature, and REPROTOX (Repro- ductive Toxicology Center, Columbia Hospital for Women Medical Center, Washington, DC), a database of refer- ences on reproductive risk that also contains a section with studies related to drug use during breastfeeding. For drugs for which no studies were iden- tified through the procedures de- scribed, the manufacturers were con- tacted directly. The references retrieved were collected and analyzed using the software program Reference Manager 11 (Institute for Scientific Information, Berkeley, CA).

  5. Infant safety data: the incidence of adverse effects reported in breast- fed infants who were exposed to the drug through maternal breast milk, expressed as a ratio of number of breastfed infants, and the type of the observed effects.

  ARTICLES

  The total is ⬎183 because some studies were both pharmacokinetic and adverse effects studies. Numbers in parentheses are drugs with documentation.

  3 2 (1) 1 (1) Antiepileptics 20 47 (14) 43 (12) Overall 96 161 (62) 161 _a

  22 29 (11) 29 (10) Anxiolytics 15 14 (8) 10 (4) Hypnotics and sedatives 13 9 (8) 3 (3) Antidepressants 23 60 (20) 75 (17) Psychostimulants

  Type of Studies ^a Pharmacokinetics Adverse Effects Antipsychotics

  Pharmacotherapeutic Group No. of Drugs

30 When the studies involved sev-

  1. Maternal dosage: the treatment dosage was usually specified in mg/d. When the treatment dose was specified in mg/kg per day, the value was multiplied by 60 kg, the standard weight of an adult wom- an.

  4. incidence and type of adverse ef- fects reported in breastfed infants. Each drug was considered as follows:

  To fit the selection criteria, studies had to provide 2 types of information:

  ●

  pharmacokinetic data on drug ex- cretion in breast milk and

  ●

  adverse effects reported in breast- fed infants who were exposed to the drug through maternal breast milk.

  Data Extraction

  To be used with caution: the avail- able data do not allow an evaluation of the safety profile of the use of the drug during breastfeeding (eg, small number of mother–infant

  ●

  and no relevant adverse effects were reported in breastfed infants.

  30

  Compatible: the drug’s use during breastfeeding is considered safe because the relative infant dosage is ⬍10% of the maternal dosage

  ●

  The “compatibility level” of each drug with breastfeeding was estimated tak- ing into account the following: 1. pharmacokinetic characteristics of the drug; 2. data on drug excretion in breast milk; 3. number of treatment days at sam- pling, according to acute and chronic administration; and

  eral patients who were taking dif- ferent therapeutic dosages, the range between the minimum and the maximum was reported in a table.

  Estimation of the Compatibility Level

  The following data were extracted and tabulated from each study:

  dose (mg/kg) ⫽ %. When possible, the percentage of drug received by the infant relative to the maternal dosage, as an interval between a minimum and maximum of the cal- culated values, was reported. When the study reported the average con- centration of the drug in milk or when a single determination of the drug in milk was conducted, a sin- gle value was indicated. When the study also reported the concentra- tion of the active metabolite(s) in milk, the values for drug and metab- olite(s) were added together in the equation.

  m [mg/mL] ⫻ 900)/maternal daily

  Study Selection

  30

  4. Relative infant dosage (% dose): the daily dosage of drug received by an infant through breast milk, ex- pressed as a percentage of the weight-adjusted maternal daily dosage. It is calculated as follows

  . Table 1 re- ports the range between the mini- mum and maximum M/P. When the studies reported the average con- centration of the drug in plasma and milk only or when a single de- termination of the drug was con- ducted, Table 1 indicates a single value.

  p

  /C

  m

  3. Milk-to-plasma ratio (M/P): the con- centration of the drug in the moth- er’s milk divided by the concentra- tion of the drug in the mother’s plasma measured at the same mo- ment: milk concentration/plasma concentration ⫽ C

  2. Number of mother–infant pairs for which pharmacokinetic data on drug excretion in breast milk were available was also reported.

  : (C pairs, relevant infant adverse ef- fects) or because of the possible ac- cumulation of the drug with pro- longed use (eg, benzodiazepines).

  ●

  Contraindicated: the drug’s use dur- ing breastfeeding is contraindi- cated because the relative infant dosage is ⬎10% of the maternal dosage and relevant adverse effects were reported in breastfed infants.

  RESULTS

  The bibliographic search produced 183 original articles that were eligible for analysis (Table 1). Documentation was available for 62 (65%) of 96 drugs; for the remaining 34 (35%) drugs, even the manufacturer was unable to pro- vide information on use during breast- feeding (Table 2). Twelve drugs re- sulted in exposure levels in breastfed infants that were higher than 10% of the maternal therapeutic dosages, and their use is therefore contraindicated (Table 3). These drugs were antiepilep- tics (7 of 14), anxiolytics (1 of 8), selective serotonin reuptake inhibi- tors (SSRIs; 2 of 6), and antipsychotics (2 of 11). Adverse effects among breastfed infants were reported for 21 (34%) of 62 drugs (Table 4). Thus, for 34 psychotropic drugs, the informa- tion is unavailable, and for an addi- tional 15, their use is unsafe because of exposure dosage or observed ad- verse effects. A total of 19 (31%) psych- otropic drugs can be used during lac- tation according to an evidence-based approach, whereas for 28 drugs, the available data do not allow an evalua- tion of their safety profile during breastfeeding.

  Antidepressants

  Among the drugs with available stud- ies on breastfeeding, antidepressants had a greater number of studies (SSRIs more than tricyclic antidepres- sant). For 20 (87%) of the 23 antide- pressants considered, 60 pharmacoki- netic studies (concerning a total of 342 mother–infant pairs) and 75 articles that reported infant adverse effects (31 reported of 612 monitored) were found. Data on use during breastfeed- ing were unavailable only for ademe- thionine, oxytriptan, and trimipramine. In particular, among the antidepres- sants, sertraline, paroxetine, and flu- voxamine are the first-choice drugs for treatment of depression in breastfeed- ing mothers because they have the lowest degree of excretion into human breast milk. Considering the high rela- tive infant dosage, their long half-life, and the reported adverse effects in in- fants, the use of citalopram, escitalo- pram, and fluoxetine are contraindi- cated during breastfeeding.

  SSRIs were better documented than tricyclic antidepressants, especially regarding their safety profile in breastfed infants; however, the major concern with exposing infants to SSRIs through breast milk is whether long- term exposure to low dosages of these medications may have long-term neu- robehavioral effects. Most of the con- sidered studies were short-term stud- ies; there have been no studies on infants’ long-term exposure to very low dosages of antidepressants. Some studies, however, showed that the platelet serotonin uptake was not de- creased in breastfed infants who were exposed to sertraline or fluoxetine through breast milk. By inference, breastfeeding exposure to these drugs therefore should not affect serotonin metabolism in the infant brain; how- ever, this aspect needs additional in- vestigation.

  31,32

  In any case, if a mother wishes to breastfeed her infant while taking an SSRI, then she should be ad- vised to monitor the infant and to in- form the pediatricians promptly if the infant experiences sedation, nausea, reduced suckling, or other sign of drug toxicity.

  Antipsychotics

  Antipsychotics are the class with the smallest number of studies concern- ing use during breastfeeding. For 11 (50%) of the 22 antipsychotics con- sidered, 29 pharmacokinetic studies (concerning a total of 146 mother– infant pairs) and 29 articles on infant adverse effects (11 reported of 162 monitored) were found.

  Chlorpromazine and olanzapine could be considered the first-choice drugs for treatment of psychotic disorders in

  TABLE 2 Psychotropic Drugs Without Documentation on Their Profile During Breastfeeding

Antipsychotics Anxiolytics Hypnotics/Sedatives Antidepressants Psychostimulants Antiepileptics

Amisulpiride Bromazepam Brotizolam Ademethionine Atomoxetine Buxamin

  Bromperidol Buspirone Estazolam Oxitriptan Modafinil Felbamate

Clotiapine Chlordiazepoxide Flurazepam Trimipramine Magnesium sulfate

Fluphenazine Clotiazepam Nordazepam

  Pregabalin Levomepromazine Hydroxyzine Triazolam Tiagabine Levosulpiride Ketazolam Valpromide Periciazine Meprobamate

  Pimozide Promazine Tiapride Trifluoperazine

  Drug Dosage, mg/d No. of Pairs (Mother–Infant) M/P % Dose Compatibility Level With Breastfeeding

  1 0.9–3.7 0.6–3.0 Caution Trazodone

  7 0.3–1.4 0.1–1.6 Yes Paroxetine 10–50 68 0.1–3.3 0.1–5.5 Yes Sertraline 25–200 43 0.1–5.2 ⬍0.1–3.6

  10 1.7–2.7 2.9–8.3 No Fluoxetine 10–80 83 0.1–6.1 0.8–16.3 No Fluvoxamine 42–200

  0.4 Caution SSRIs Citalopram 18–60 35 0.9–9.4 1.0–10.9 No Escitalopram 5–20

  0.1

  5

  50

  ⬍0.1–1.6 Caution Mianserin 40–60 2 0.8–3.6 0.9–1.4 Caution Nortriptyline 125

  80

  Yes Imipramine 75–200 5 1.2–2.3 0.1–7.5 Yes Maprotiline 100–150 – 0.2–1.5

  2.0 Caution Dosulepin 25–500 32 0.8–4.5 ⬍0.1–5.0

  1.2

  1

  3 0.4–3.0 0.4–4.0 Yes Desipramine 300

  7.5 15 0.3–0.6 0.6–1.4 Yes Tricyclic antidepressants Amitriptyline 75–175 6 0.5–1.7 0.2–1.9 Yes Clomipramine 75–150

  Yes Other antidepressants Duloxetine

  6

  5

  0.5–8.9 Yes Phenobarbital 30–120 34 0.1–0.8 33.6–297.0 No Gabapentin 600–2400

  0.2 Caution References are available upon request to the corresponding author.

  Methylphenidate 15–80 2 1.1–2.7

  3 0.8–1.1 4.0–21.0 No Vigabatrin 200 2 0.1–0.4 0.8–4.0 Caution Zonisamide 300–400 4 0.4–1.0 22.0–32.0 No Psychostimulants

  0.1 Caution Primidone 375–1000 23 0.4–2.3 6.9–37.8 No Topiramate 150–200

  2 0.5–5.0

  8 0.7–1.3 1.3–6.5 Caution Lamotrigine 100–800 42 0.1–1.1 1.8–21.1 No Levetiracetam 1000–3500 33 0.8–3.1 0.5–16.0 No Oxcarbazepine 600–900

  18 0.7–1.0 31.0–99.0 No Phenytoin 100–600 27 ⬍0.1–0.5

  0.3

  33 0.2–2.6 1.1–7.3 Yes Clonazepam 4 2 0.3–0.4 1.3–2.4 Caution Ethosuximide 250–1420

  24 ⬍0.1–0.1 0.1–3.9 Yes Carbamazepine 500–1300

  Valproic acid 500–2400

  1.4–2.5 Caution Venlafaxine 75–450 12 1.6–5.2 3.5–9.2 Yes Antiepileptics

  13 0.7–2.6 0.5–4.4 Yes Reboxetine 4–10 4 ⬍0.1

  0.1 Caution Hypericum 300–900 6 ⱕ0.1 0.1–2.5 Yes Mirtazapine 3–120

  0.1 ⬍0.1 Yes Zopiclone

  20

  Antipsychotics Haloperidol 3–30 11 0.6–8.1 0.2–9.6 Yes Chlorpromazine 40–120

  0.9

  5

  60

  30 3 0.1–0.3 0.4–1.0 Caution Pinazepam 5–10 13 0.1–0.3 0.1–1.2 Caution Prazepam

  7 0.1–0.4 0.3–0.7 Caution Diazepam 1–30 8 0.1–7.7 3.2–12.0 No Lorazepam 3.5–5.0 5 0.1–0.3 0.4–5.3 Caution Oxazepam

  0.5 8 0.2–0.5 ⱕ1.3 Caution Clobazam 30 12 0.1–0.4 7.5–9.9 No Clorazepate dipotassium 20 intramuscularly

  0.8 Caution Anxiolytics Alprazolam

  1

  1.5 Caution Hypnotics and sedatives Flunitrazepam

  15

  Caution Aripiprazole

  65 — 2.3–17.7 No Zuclopenthixol 4–50 7 0.1–0.7 ⬍0.1–0.5

  Yes Perphenazine 16–24 2 0.7–1.1 0.1–0.2 Caution Quetiapine 25–400 8 0.3 0.1–0.5 Caution Risperidone 1.5–4.0 3 0.1–0.5 2.8–4.7 Caution Sulpiride 100

  30 0.2–1.3 3.5–69.0 No Olanzapine 2.5–20.0 14 0.1–0.8 ⬍0.1–4.0

  3 0.4–0.9 0.1–0.2 Yes Clozapine 50–100 2 2.8–4.3 1.0–1.1 No Lithium 600–1500

  0.1

  2

  0.3 Yes Zolpidem

  0.2

  0.5

  5

  10

  1.3 Caution Zaleplon

  3.6 Caution Temazepam 10–20 10 ⬍0.1–0.6

  0.2 Caution Nitrazepam 5 14 0.3–0.5

  2

  5

  15

  0.3 Caution Midazolam

  5 ⬍0.1

  20

  0.2 Caution Lormetazepam

  0.7

  ARTICLES breastfeeding mothers because they have the lowest degree of excretion into human breast milk and scant ad- verse effects in breastfed infants. Con- sidering the high relative infant dos- age and the reported adverse effects in infants, the use of clozapine, lithium, and sulpiride is contraindicated dur- ing breastfeeding. Because psychosis requires long- term treatment and because the data on safety of antipsychotics dur- ing lactation are limited, the benefits of breastfeeding may be weighed against the potential risks of med- ication. All antipsychotic drugs are sedating and have relatively long half-lives, so the infants should be observed for lethargy, sedation, and appropriate development.

  Hypnotics and Anxiolytics

  The available data regarding the use of hypnotic and anxiolytic agents during breastfeeding are scant. For 16 (57%) of the 28 hypnotics and anxiolytics con- sidered, 23 pharmacokinetic studies (concerning a total of 122 mother– infant pairs) and 13 articles on infant adverse effects (6 reported of 57 mon- itored) were retrieved. The available data suggest that the amounts of these medications to which the nursing in- fant is exposed are not very high; how- ever, they must be used with caution by breastfeeding mothers, taking into account that neonates metabolize ben- zodiazepines more slowly than adults and that these drugs are usually used for long-term periods, so they may ac- cumulate in breastfed infants and pro- duce infant sedation, nausea, and poor feeding.

  The use of long-acting benzodiaz- epines, such as diazepam and cloba- zam, is therefore contraindicated in breastfeeding mothers. If a benzodiaz- epine is needed during breastfeeding, then a short-acting one, such as midazolam, oxazepam, pinazepam, or

  Drug Adverse Effects Reported/ Monitored Type ^a Antipsychotic agents

  Haloperidol 3/13 Delayed psychomotor development Chlorpromazine 4/20 (3) Delayed psychomotor development; (1) drowsiness and lethargy. Clozapine 2/4 (2) Sedation and agranulocytosis Lithium 2/32 (1) CNS depression symptoms (hypotonia, lethargy, Olanzapine 0/7 hypothermia, inversion of ECG wave); (1) toxicity in Perphenazine 0/1 concomitance of respiratory infections Quetiapine 0/8 Risperidone 0/4 Sulpiride 0/66 Zuclopenthixol 0/7

  Anxiolytics Alprazolam 3/7 (2) Withdrawal syndrome after cessation of breastfeeding Clorazepate dipotassium 0/7 (irritability, high-pitched crying, agitation, sleep disturbances); (1) sedation Diazepam 2/14 Sedation Lorazepam 0/1

  Hypnotics and sedatives Temazepam 0/10 Zolpidem 1/6 Sedation and poor feeding Zopiclone 0/12

  Tricyclic antidepressants Amitriptyline 0/4 Clomipramine 0/7 Desipramine 0/1 Dosulepin 0/25 Imipramine 0/5 Mianserin 0/2 Nortriptyline 0/21

  SSRIs Citalopram 5/66 (3) Colic, poor suckle, drowsiness and irritability; (1) insomnia; (1) irregular breathing, sleep disturbances, hypotonia and hypertonia

  Escitalopram 1/9 (1) Necrotizing enterocolitis Fluoxetine 15/151 Most frequent: transient irritability, sleep disturbances, and Fluvoxamine 0/12 colic; (6) colic; (1) hypotonia, sedation, poor suckle, and fever; (1) hyperglycemia and glycosuria; (1) peripheral cyanosis and unresponsiveness to stimuli Paroxetine 2/111 Irritability, agitation, feeding problems, nervousness

  Sertraline 2/126 (1) Hypotonia, drowsiness, ear problems, body growth problems; (1) withdrawal syndrome after cessation of breastfeeding (agitation, poor suckle, high-pitched crying, insomnia)

  Other antidepressants Hypericum 6/40 (5) Colic, lethargy, sedation; (1) seizure Mirtazapine 0/13 Reboxetine 0/4 Venlafaxine 0/15 Antiepileptics Valproic acid 1/13 Thrombocytopenic purpura, anemia, and reticulocytosis Carbamazepine 4/39 Most frequent: poor suckle, decreased body weight gain and sedation, spasms after cessation of breastfeeding; (3) transient hepatic dysfunction (2 cases of cholestatic hepatitis, 1 case of hyperbilirubinemia with high levels of ␥ GT); (1) poor suckle; (1) peripheral cyanosis and unresponsiveness to stimuli Clonazepam 0/2

  Ethosuximide 3/6 (2) Hyperexcitability; (1) sedation, decreased body weight gain, poor suckle lormetazepam, should be used. More- over, the minimum dosage required for symptom relief should be used, and the infant should be monitored regu- larly. If an infant experiences sedation, nausea, reduced suckling, or other signs of toxicity, then breastfeeding should be discontinued. Single doses of benzodiazepines do not require any limitation on breastfeeding.

  Antiepileptics

  The antiepileptic therapeutic group is the most investigated during breast- feeding. Data are available for 14 (70%) of the 20 drugs considered: 47 pharmacokinetic studies (concerning a total of 255 mother–infant pairs) and 43 articles on infant adverse effects (26 reported of 220 monitored) were found.

  Valproic acid and carbamazepine are the first-choice drugs for treatment of mothers with epilepsy during breast- feeding because of their low degree of excretion into human breast milk and limited reported adverse effects in in- fants. Considering the high relative in- fant dosage and the reported adverse effects in infants, the use of 6 drugs (ethosuximide, phenobarbital, lam- otrigine, primidone, topiramate, and zonisamide) is contraindicated during breastfeeding.

  Because antiepileptics are used in long-term treatment, the most appro- priate therapy in childbearing women with epilepsy should be evaluated be- fore pregnancy and during the breast- feeding period considering the poten- tial harm of the medication on the fetus and breastfed newborn. If the mother is on therapy with 1 of the con- traindicated drugs (eg, phenobarbi- tal), then the infant should be ob- served for lethargy, sedation, and appropriate development. Although the routine monitoring of infant serum drug levels is not warranted, the infant serum can also be assayed to assess actual neonatal exposure to medica- tion more accurately.

  Psychostimulants

  Studies are available only for methyl- phenidate (2 studies on pharmacoki- netics in 2 pairs and no adverse effects in 1 infant). Methylphenidate shows an M/P that varies from 1.1 to 2.7 and a relative infant dosage that is 0.2% of the maternal dosage; however, the available information is too scant to permit an evaluation of the safety pro- file of the drug.

  DISCUSSION

  No data are available on the use during breastfeeding of one third of psycho- tropic drugs. For the other two thirds, available information varies widely. Al- though many psychotropic drugs are considered safe during breastfeeding because they are excreted to a low ex- tent into breast milk (relative infant dosage ⬍10% of the therapeutic ma- ternal dosage) and no serious adverse events related to exposure to these medications through breast milk have been reported, there are documented differences between drugs within the same class and there is no class action in relation to breastfeeding. Further- more, for each therapeutic category, there are drugs with minimal infant ex- posure via breastfeeding. For these drugs, the dosage to which the infant is exposed is very low and well below what would be expected to have any significant clinical effects. For this rea- son, they are considered first choice for the treatment of breastfeeding mothers (sertraline, chlorpromazine, lormetazepam, and carbamazepine), whereas a few drugs are contraindi- cated (citalopram, clozapine, diaze- pam, and phenobarbital). Although antiepileptics and antide- pressants have been studied exten- sively, to date, less information re- garding the use of antipsychotics, anxiolytics and hypnotics, and psycho- stimulants while breastfeeding is available. The existing literature is of- ten limited to a small number of stud- ies based on a few cases or case re- ports, making it difficult to formulate any generalizations regarding their safety profile in lactation.

  26–29

  These drugs are being used more frequently and need additional investigation. Mothers are increasingly encouraged to nurse, but breastfeeding while tak- ing psychotropic medications is an im- portant issue that has not received the attention that it deserves.

  29 Women Drug Adverse Effects Reported/

  Monitored Type ^a Phenytoin 2/11 Methaemoglobinemia, bleeding, anemia, sedation, poor suckle, and decreased weight gain Phenobarbital 5/50 Most frequent: poor suckle and decreased bodyweight gain,

  Gabapentin 0/6 sedation, methaemoglobinemia, bleeding, anemia, and drowsiness; (4) sedation; (1) withdrawal seizures Lamotrigine 1/46 (1) Motoneuron hyperexcitability, irritability, and poor feeding Levetiracetam 1/19 (1) Hypotonia and poor suckle Oxcarbazepine 0/3 Primidone 9/20 Most frequent: sedation, hypotonia and poor suckle, Topiramate 0/5 decreased body weight gain, and vomiting; (1) spasms after cessation of breastfeeding Psychostimulants

  Methylphenidate 0/1 References are available upon request to the corresponding author. CNS indicates central nervous system; ECG, electrocardiogram. _a The numbers in parentheses indicate the number of infants.

  ARTICLES with postpartum psychiatric disorders are understandably anxious about any uncertainties surrounding the safety of their medications in their infants and often face the dilemma of whether to use psychotropic medication while continuing to breastfeed their infants. Quite often, the first reaction is to stop breastfeeding or to stop any psycho- tropic medications entirely. Moreover, many physicians have been hesitant to prescribe psychotropic medication to women who choose to breastfeed. What is easily forgotten are the risks of untreated psychiatric disorders in the postpartum period.

  33 In such cases, it

  If treatment is deemed appropriate, then the smallest number of medica- tions at the lowest possible dosage consistent with control of the mental illness should be prescribed,

  37 CONCLUSIONS

  this setting, ongoing collaboration with the pediatrician is crucial. If a mother is on therapy with 1 of the contraindicated drugs because she is affected by postpartum affective ill- ness that responds only to a particular drug (this is common for epilepsy), then it is advisable to keep her on that drug rather than to switch. In addition, the woman should be kept on the low- est possible effective dosage of medi- cation, and the infant should be ob- served for possible adverse effects. Although the routine monitoring of in- fant serum drug levels is not war- ranted, if neonatal toxicity related to drug exposure through breast milk is suspected or when the mother is nurs- ing while taking a drug that is contra- indicated during breastfeeding, then infant serum can also be assayed to assess neonatal exposure to medica- tion more accurately.

  20 In

  into breast milk, but concentrations and effects may vary considerably. The amount of medication to which an in- fant is exposed through lactation de- pends on several factors: the maternal dosage, frequency of dosing, rate of absorption into maternal circulation, diffusion from maternal circulation into breast milk, rate of maternal drug metabolism, and absorption of the drug by the infant. Moreover, the fre- quency and timing of the feedings can influence the amount of drug to which the nursing infant is exposed. By re- stricting breastfeeding to times during which breast milk drug concentra- tions would be at their lowest levels or by taking medication immediately af- ter breastfeeding, the infant exposure to the drug may be reduced. As with all drugs taken while breastfeeding, it is prudent to monitor carefully the clini- cal status of infants for signs of drug- related toxicity and adverse effects (generally sedation; irritability; and changes to sleep, feeding, and growth). It is also essential that moth- ers be properly educated about this matter and advised to discontinue a medication if their infant develops signs of toxicity or adverse effects.

  24 All psychotropic drugs are excreted

  and a drug with a proven favorable safety/ efficacy profile should be preferred.

  17

  systematic approach used to collect the available information on psycho- tropic medication use during breast- feeding. The result is a more com- plete, accurate, and updated review of the evidence, and this can repre- sent an important tool for health pro- fessionals for promoting the rational use of psychotropic drugs in breast- feeding mothers. The major objective of this review is to be a reliable source of evidence-based informa- tion for current problems in daily clin- ical practice, especially for psychia- trists, pediatricians, family physicians, and obstetrician-gynecologists, who often play an important role in wom- en’s decision to start or continue breastfeeding while taking psycho- tropic medications.

  is important to safeguard the mental health of the mother while at the same time optimizing the emotional and physical well-being of the infant.

  24 The strength of this review is the

  requires up-to-date knowledge on safety of psychotropic medication use during breastfeeding.

  28 This analysis

  risks (eg, hypersensitivity reactions, adverse central nervous system ef- fects such as lethargy and reduced feeding) and risks of long-term effects on the developing brain.

  35 There are immediate

  general, these medications should not be prescribed without careful consid- eration, but neither should they be au- tomatically avoided. The decision to prescribe psychotropic agents to breastfeeding mothers should depend on an individual risk/ benefit analysis: the known benefits of breastfeeding and medication use for both mother and infant must be weighed against the risk of untreated maternal illness or the risk of infant exposure to medications through breast milk.

  34 In

  The use of psychotropic drugs during lactation will continue to be a contro- versial topic. Given the possible occur- rence of psychiatric illness during the postpartum period, a significant num- ber of women may require pharmaco- logic treatment. The nutritional, immu- nologic, and psychological benefits of breastfeeding have been well docu- mented. Conversely, it is clear from this review that, given the limited data, it is difficult to reach a conclusion on the safety profile of many psychotropic drugs during breastfeeding. There is a need for additional research and re- ported experience. In particular, a long-term monitoring of the neurocog- nitive development of breastfed in- fants is needed; however, certain med- ications can safely be used by mothers who are planning to breastfeed, even if it is also widely known (but parents must to be informed) that no drug is completely free of adverse effects. All psychotropic drugs should be viewed with caution during breastfeeding, tak- ing into account the known benefits of breastfeeding to mothers and infants as well as the possibility that infant ex- posure to clinically significant levels in breast milk may occur.

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Psychotropic Drug Use During Breastfeeding: A Review of the Evidence

Filomena Fortinguerra, Antonio Clavenna and Maurizio Bonati

  Pediatrics 2009;124;e547-e556; originally published online Sep 7, 2009;

DOI: 10.1542/peds.2009-0326