Protocols for High-Risk Pregnancies. Группа авторов

Protocols for High-Risk Pregnancies

Protocols for High-Risk Pregnancies - Группа авторов

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an MDE: depressed mood, diminished interest, significant weight change, insomnia or hypersomnia, psychomotor retardation or agitation, fatigue, feelings of guilt or worthlessness, decreased concentration, and recurrent thoughts of death or suicide. An affected woman should have at least five of these symptoms, including either depressed mood and/or diminished interest, most of the time for two weeks. If a woman has a history of manic/hypomanic episodes as well as MDEs, she suffers from bipolar disorder but is presenting in the depressed phase. Mania is characterized by elevated/expansive/irritable mood, increased energy, grandiosity, decreased need for sleep, pressured speech, and increased participation in goal‐related or risky activities. If she has never had manic or hypomanic episodes, and she meets the above criteria, then her diagnosis is unipolar major depressive disorder.

      Women with MDE who suffer from bipolar disorder will require treatment with a mood stabilizer and an antidepressant. Valproate and carbamazepine are effective mood stabilizers but also established teratogens and should not be used early in pregnancy. Lamotrigine is FDA approved for treatment of individuals with bipolar disorder and may be useful although it must be titrated up slowly and it is specifically useful for bipolar depression and not bipolar mania. Lithium is the gold standard treatment for bipolar disorder but has been associated with fetal cardiac defects. It may be best to avoid this agent early in pregnancy, although the absolute risk of lithium is now considered to be lower than it was after publication of results from the lithium registry. The risk of a major malformation, including a major heart anomaly, is about 70% higher than in those who are not exposed to lithium although some investigations find no increased risk for malformations. Moreover, many of the malformations are very rare so increased risk is difficult to establish, even in large cohorts. First‐ and second‐generation antipsychotics (e.g., olanzapine, risperidone) have good mood‐stabilizing properties and appear to have lower teratogenic risk than anticonvulsants. If mood improves, there is no need to add an antidepressant.

      Women with unipolar MDE who are not sufficiently treated with psychotherapy or women with bipolar disorder who did not respond to a mood stabilizer alone will need treatment with an antidepressant. The reproductive safety profile of the older tricyclic antidepressants is no better than for the newer, serotonin or serotonin‐norepinephrine reuptake inhibitors. However, older agents have more side effects. It is reasonable to start with either a selective serotonin reuptake inhibitor or bupropion. If a woman is struggling to avoid nicotine cigarettes, use of bupropion may help treat her nicotine addiction and her depression. Given data associating paroxetine use in pregnancy with malformations of the heart, many experts recommend that this agent not be prescribed to pregnant women in the first trimester. However, if a woman presents well into her first trimester of pregnancy on a particular agent, there may be little benefit to switching to a different agent since in utero exposure has already occurred. In any case, women should be counseled to minimize use of other harmful licit and illicit substances such as cigarettes, alcohol or recreational drugs. Use of such substances is more common in women with depression and patients may not realize that cigarettes, alcohol or other drugs are as harmful, if not more problematic, than antidepressant agents.

      It is ideal to see a woman a week after initiation of pharmacotherapy for MDE to determine the presence and magnitude of side effects to the medication and assess further deterioration in psychiatric status. Subsequently, she can be seen again after two weeks and then monthly. Some degree of mood improvement may be noticeable within a few weeks. However, it may take 6–8 weeks to see full response to treatment. The patient should be assessed for suicidal thoughts at each visit. While some clinicians have concerns that asking about suicidal thoughts will “suggest” this action to patients, this is not the case. Appropriate emergency medical care can be arranged if the patient endorses suicidal thoughts. If the obstetrician is unable to provide follow‐up care at these intervals, the patient may be referred to a psychiatrist who can communicate with the obstetrician regarding the patient’s progress. Once response has been obtained, the patient’s mood can be reevaluated at routine obstetrics visits.

      The risk period for an episode of MDE coincides with the period of women’s fertility. While some women benefit from psychotherapy and can avoid pharmacotherapy in pregnancy, this is not always the case. Women who have underlying bipolar disorder and those with severe recurrent major depressive disorder will likely require medication management. Antipsychotic agents have a lower risk profile than anticonvulsant mood stabilizers, which should be avoided early in pregnancy. Antidepressants are not major teratogens but clinicians need to apprise patients of potential risks and benefits of treatment, including perinatal complications such as preterm birth or transient neonatal distress.

      1  American Psychiatric Association. Diagnostic and Statistical Manual of Mental Disorders, 5th edn. Washington, DC: American Psychiatric Association, 2013.

      2 Chambers C, Hernandez‐Diaz H, Marter LV, et al. Selective serotonin‐reuptake inhibitors and risk of persisitent pulmonary hypertension of the newborn. N Engl J Med 2006; 354:579–87.

      3 Hermann A, Gorun A, Benudis A. Lithium use and non‐use for pregnant and postpartum women with bipolar disorder. Curr Psychiatry Rep 2019; 21(11):114.

      4 Kallen B, Reis M. Neonatal complications after maternal concomitant use of SSRI and other central nervous system active drugs during the second or third trimester of pregnancy. J Clin Psychopharmacol 2012; 32(5):608–14.

      5  McKenna K, Koren G, Tetelbaum M, et al. Pregnancy outcome of women using atypical antipsychotic drugs: a prospective comparative study. J Clin Psychiatry 2005; 66(4):444–9; quiz 546.

      6 Ross LE, Grigoriadis S, Mamisashvili L, et al. Selected pregnancy and delivery outcomes after exposure to antidepressant medication: a systematic review and meta‐analysis. JAMA Psychiatry 2013; 70(4):436–43.

      7 Yonkers K, Blackwell K, Glover J, Forray A. Antidepressant use in pregnant and postpartum women. Annu Rev Clin Psychol 2014; 10:369–92.

      8 Yonkers KA, Norwitz ER, Smith MV, et al. Depression and serotonin reuptake inhibitor treatment as risk factors for preterm birth. Epidemiology 2012; 23(5):677–85.
PART 2 Antenatal Testing

       Mary E. Norton

      Department of Obstetrics, Gynecology, and Reproductive Sciences, University of California, San Francisco, CA, USA

      Aneuploidy refers to an abnormal number of chromosomes, e.g., the presence of more or fewer than the usual diploid complement of 46. Presence of a single additional chromosome is known as trisomy and is an important cause of congenital malformations. The most common autosomal trisomies are Down syndrome (trisomy 21), Edward syndrome (trisomy 18), and Patau syndrome (trisomy 13). Sex chromosomal aneuploidies such as 47,XXY (Klinefelter syndrome) and 45,X (Turner syndrome) as well as an entire extra set of chromosomes (triploidy) can also be seen. In addition, deletions and duplications of portions

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