Обстеження батьків на носійство перед зачаттям або перед пологами

ЗаJeffrey S. Dungan, MD, Northwestern University, Feinberg School of Medicine
Переглянуто/перевірено січ. 2024

Carrier testing is part of routine prenatal care and is ideally done before conception. The extent of carrier testing is related to how the woman and her partner weigh factors such as

  • The probability of a fetal abnormality based on risk factors and the results of any previous testing

  • The probability of a complication from invasive fetal testing

  • The importance of knowing the results (eg, would the pregnancy be terminated if an abnormality was diagnosed, would not knowing the results cause anxiety)

For these reasons, the decision is individual, and recommendations often cannot be generalized to all women, even those with similar risk.

A screening history is part of the evaluation. The history is summarized as a pedigree (see figure Symbols for constructing a family pedigree). Information should include the health status and presence of genetic disorders or carrier status of both parents, of first-degree relatives (parents, siblings, offspring), and of second-degree relatives (aunts, uncles, grandparents), as well as ethnic and racial background and consanguineous matings. Outcomes of previous pregnancies are noted. If genetic disorders are suspected, relevant medical records must be reviewed.

Testing potential parents for a genetic carrier state that may result in affected offspring is best done before conception; however, many people wait until after conception to have carrier screening. Traditionally, screening tests are offered to parents at risk of being asymptomatic carriers for certain common mendelian disorders (see table Preconception or Prenatal Genetic Screening of Potential Parents). Because parent ethnicity is often complex and not well-defined and because prenatal genetic testing is becoming much less expensive and quicker, some clinicians are starting to screen all potential (and expectant) parents, regardless of ethnicity (called universal carrier screening). Therefore, current approaches to carrier screening include offering all patients the same larger list of conditions to be evaluated. Often, dozens of genes and disorders (some with more severe phenotypic consequences than others) are included (1). Increasing the amount of testing and evaluation is expected to increase the complexity of pre-test counseling. The American College of Medical Genetics and Genomics recommends a tiered carrier screening system based on carrier frequency and has provided tables listing disorders to be included in carrier screening panels (2).

(See also Prenatal Genetic Counseling.)

Довідкові матеріали загального характеру

  1. 1. American College of Obstetricians and Gynecologists/Committee on Genetics: Committee opinion no. 690: Carrier Screening in the age of genomic medicine. Obstet Gynecol 129 (3):e35–e40, 2017. doi: 10.1097/AOG.0000000000001951

  2. 2. Gregg AR, Aarabi M, Klugman S, et al: Screening for autosomal recessive and X-linked conditions during pregnancy and preconception: A practice resource of the American College of Medical Genetics and Genomics (ACMG). [published correction appears in Genet Med 2021 Aug 27]. Genet Med 23(10):1793-1806, 2021. doi:10.1038/s41436-021-01203-z

Обстеження перед пологами для виявлення генетичних аномалій в плода

After conception, pregnant women should be offered noninvasive screening tests for fetal chromosomal disorders using one of several methods (eg, ell-free DNA serum tests, analyte screening) (1). If such a screening test is positive, it may be followed up with fetal diagnostic genetic testing, which are invasive tests using a sample of fetal cells (see table Indications for Fetal Genetic Diagnostic Tests). These diagnostic tests provide a definitive diagnosis of genetic abnormalities. Additionally, if screening of either parent (done before or after conception) detects a genetic abnormality, pregnant patients may choose to do fetal genetic diagnostic tests (eg, chorionic villous sampling or amniocentesis) without first doing a noninvasive fetal screening test (eg, cfDNA or serum screening).

Screening tests for fetal chromosomal disorders include screening for fetal Down syndrome, trisomy 18, and trisomy 13 with analysis of cell-free DNA (cfDNA) in maternal plasma, which can be done as early as 10 weeks gestation. Another screening method, called analyte screening, uses multiple maternal serum markers (alpha-fetoprotein, beta-human chorionic gonadotropin [beta-hCG], estriol, inhibin A) to detect neural tube defects, Down syndrome (and other chromosomal abnormalities), and some other birth defects. Analyte screening is done at 15 to 20 weeks gestation.

Fetal genetic diagnostic tests are usually recommended if risk of a fetal chromosomal abnormality is increased (see table Indications for Fetal Genetic Diagnostic Tests). Fetal genetic diagnostic tests, unlike screening tests, are usually invasive and involve fetal risk. Thus, in the past, these tests were not routinely recommended for women without risk factors or a known genetic abnormality in one of the parents. However, because fetal genetic diagnostic tests are now more widely available and safety has improved, it is recommended to offer fetal genetic testing to all pregnant patients, regardless of risk.

Fetal genetic diagnostic tests include chorionic villus sampling, amniocentesis, or, rarely, percutaneous umbilical blood sampling. In addition, for pregnancies conceived through assisted reproductive technologies (eg, in vitro fertilization), preimplantation genetic diagnosis is an option.

Fetal genetic diagnostic tests can detect all trisomies, many other chromosomal abnormalities, and several hundred mendelian abnormalities. Submicroscopic chromosomal abnormalities are missed by traditional karyotype testing and can be identified only by microarray technologies, such as array comparative genomic hybridization and single nucleotide polymorphism (SNP)-based arrays. Array comparative genomic hybridization in prenatal testing is most frequently used to evaluate fetuses with structural abnormalities. Arrays detect numeric chromosome abnormalities (eg, trisomies) as well as unbalanced structural chromosome disorders, such as microdeletions. Studies have reported about 6% incidence of array abnormalities that would have been missed with traditional karyotyping in structurally abnormal fetuses.

Preimplantation genetic diagnosis may be available for partners who are using in vitro fertilization.

Таблиця
Таблиця
Таблиця
Таблиця

Довідкові матеріали щодо аналізів

  1. 1. American College of Obstetricians and Gynecologists’ Committee on Practice Bulletins—Obstetrics; Committee on Genetics; Society for Maternal-Fetal Medicine: Screening for fetal chromosomal abnormalities: ACOG Practice Bulletin, Number 226. Obstet Gynecol. 2020;136(4):e48-e69. doi:10.1097/AOG.0000000000004084