Clinical Utility of Expanded Carrier Screening: Reproductive Behaviors of At-Risk Couples

Carrier screening identifies couples at increased risk of having a child with a genetic disease and enables them to consider alternative reproductive options. Those who do not make alternative reproductive decisions based on their carrier status may still use this knowledge to prepare for the birth of an affected child and potentially facilitate early intervention (Edwards et al. 2015; Nazareth et al. 2015).

Historically, carrier screening programs targeted a small number of diseases that are highly prevalent in an ethnic-defined population. More recently developed, expanded carrier screening (ECS) assesses risk for dozens or hundreds of diseases across all populations, also known as pan-ethnic, or universal screening (Umbarger et al. 2013). The American College of Obstetricians and Gynecologists (ACOG) recently recognized ECS as an acceptable screening strategy (ACOG Committee Opinion No. 690 2017).

Despite widespread adoption of ECS by many providers, statements from professional organizations suggest additional research is needed (Henneman et al. 2016; Umbarger et al. 2013) in particular, citing the lack of data regarding reproductive outcomes of couples that undergo ECS. Studies of outcomes after population-based carrier screening initiatives for a limited number of disorders have consistently found a reduced incidence of the disease of interest due to the decisions made by the at-risk couples (ARC). Tay-Sachs disease incidence fell by 90% in the Ashkenazi Jewish population due to high screening uptake over the course of multiple decades (Kaback 2000). Screening for thalassemia in Mediterranean and Chinese populations has resulted in similar declines (Cao et al. 2002; Kaback 2000; Liao et al. 2005).

Decision-making among couples at risk for children affected by cystic fibrosis (CF) has been assessed in several studies. Many of the studies only included pregnant couples and often parents who had an affected child. While these studies indicated that the majority of couples would pursue prenatal diagnosis for the condition in question (Ioannou et al. 2015; Sawyer et al. 2006; Scotet et al. 2008), having a previously affected child or relative may influence reproductive decision making. Therefore, while decisions of carrier couples in this context are well-characterized, they do not represent the majority experience of ARC who are unlikely to have personal experience with CF prior to learning their carrier status. (Ioannou et al. 2015).

The available studies that are focused on CF screening in the general population, not based on family history or known carrier status, do demonstrate effectiveness in reducing the incidence of the condition. In the United States, a study in Massachusetts demonstrated a decrease in CF incidence following the screening recommendations by ACOG, American College of Medical Genetics and Genomics (ACMG) and the National Institutes of Health (Hale et al. 2008). Several studies have been conducted outside of the US. Of significance is a five-year study in Edinburgh, UK that showed a drop in CF incidence following the implementation of the screening recommendation (Cunningham and Marshall 1998). A three-year study of a screening program in Australia identified nine ARC, six that were pregnant at the time of screening. All six couples elected prenatal diagnosis, and three preconception couples elected to pursue in vitro fertilization (IVF) with preimplantation genetic diagnosis (PGD) (Massie et al. 2009).

Literature regarding the clinical utility of ECS panels is only beginning to emerge. One recent study by Franasiak et al. (2016) focused on the clinical decision-making of infertile couples found to be carriers through ECS testing as part of their infertility work-up. Eight couples were identified as at-risk carriers and elected to pursue PGD as part of their IVF treatment, indicating that the results of the carrier screening affected clinical decision making in all cases, though the authors noted that not all of the couples completed the planned treatment.

The purpose of this study was to learn about the reproductive decisions of ARC as identified by ECS from a nationwide population. This paper will describe the experience of these ARC after they received their ECS results, characterize their reproductive decisions, and identify factors associated with their decision making.

This was a mixed-methods retrospective study in which participants were invited to self-report their experience and outcomes. The study was approved by the California State University Stanislaus Institutional Review Board, Protocol #1516–007.

Of 207,095 individual patients tested for ECS between April 2014 and August 2015 (either genotyping or sequencing-based, and with a mix of selected diseases), 103,550 notified Counsyl that they were part of a couple and received merged reports. Of these 51,775 couples, our eligibility criteria yielded 537 ARC for possible participation; 465 could be contacted by SMS or email, and the remaining 72 could only be contacted through postal mail (Fig. 1).

The online survey received an 18% (n = 86) total response rate including 16 partial responses in which the respondent either declined consent and was exited from the survey, or provided consent but exited the survey prior to reaching the end. Fifteen percent (n = 70) completed the survey. Of the 72 paper surveys mailed via post, 13% (n = 9) were returned completed. Completion rate was not significantly different between methods (p = 0.72).

Of 79 completed surveys, three were excluded because the respondents did not report the condition for which they were both carriers, instead choosing either “I don’t recall” or “My partner and I were not carriers for the same condition.” An additional 12 that reported a family history of the condition for which they were found to be carriers were excluded from this analysis.

The demographic data of the remaining 64 participants are summarized in Tables 1 and 2. Respondents and their partners were predominantly Caucasian (76% and 70% respectively, selecting this option), educated (89% and 77% respectively, with bachelor’s degree or higher), with annual household incomes exceeding $100,000 (68%). The majority of female partners were 25–34 years of age (81%), had no children at the time of responding to the survey (62%), and had no history of miscarriage (69%). Most ARC had carrier screening as part of a fertility work-up (53%) with other reasons for carrier screening including routine screening (31%), ethnicity-based screening (6.3%), prior miscarriages or stillbirth (4.7%), ultrasound anomalies (3.1%), and consanguinity (1.6%). ARC reported having ECS on the recommendation of a healthcare provider (86%), and almost all pursued genetic counseling after receiving results (95%), the majority through Counsyl’s services (61%).

Sixty participants provided an interpretable answer about their actions or planned actions following results receipt. The remaining four participants either declined to answer the question or did not supply an interpretable response (e.g. selecting “other” without additional explanation when asked about their plans or selecting/indicating contradictory options.) The reproductive decisions reported by ARC were collapsed into two categories: action (36/60) or no action (24/60) based on the ECS results, with the unclear responses (4/64) excluded from the statistical analysis. Actions reported by this group included IVF with PGD (n = 22) and prenatal diagnosis (n = 14).

Potential associations between alternative reproductive options and disease severity, pregnancy status (non-pregnant ARC have more available options), and demographic factors were assessed (Table 3). After Bonferroni correction, the required threshold for significance was .05/10 = α = .005.

Of ARC carrying severe or profound conditions, 76% (32/42) reported alternative reproductive actions, versus 22% (4/18) ARC carrying moderate conditions (Fig. 2), suggesting that disease severity has a significant effect on reproductive actions (p = 0.000145). One severe condition was a clear outlier to this trend: only 29% (2/7) of ARC carrying biotinidase deficiency (BTD) reported a change in their actions, in contrast to the 86% (30/35) of ARC carrying other severe or profound conditions (p = 0.0049). Of ARC carrying profound conditions, 80% (8/10) reported alternative reproductive actions vs. 75% (24/32) of ARC carrying severe conditions (p = 1.00).

Because ECS includes all of the conditions recommended by ACOG and ACMG, the data allow us to compare ARC actions between those diseases with guidelines and those without. For diseases recommended for panethnic screening (CF and spinal muscular atrophy (SMA)), 14 ARC reported taking action on the results while two did not alter their reproductive plans. There was no significant difference (p = 0.270) between rate of action on these recommended conditions as compared to the other severe or profound conditions, with 18 in that group reporting action based on the result and eight reporting no change to reproductive plans (Table 4). If all diseases with guidelines, including ethnicity based screening, are compared, 17 reported taking action based on the result, while three did not. Here again, there was no significant difference (p = 0.284) between ARC carrying diseases with screening recommendations and the ARC carrying non-guideline diseases, with 15 reporting action taken based on their results and seven reporting no change in reproductive plans.

While additional options were available to the non-pregnant couples, pregnancy status was not found to be a significant variable (p = 0.088). Existence of prior children (p = 0.181), occurrence of prior miscarriages (p = 1.00), attainment of graduate education by at least one member of the couple (p = 0.590), and annual income greater than or equal to US$100,000 (p = 0.093) were factors not found to have significant associations.

The data demonstrate that carrier screening results affected clinical decision making for the majority of these ARC. Couples who were carriers of a disease classified as profound or severe were significantly more likely to take action based on the results than those who were carriers of a moderate condition. The qualitative analysis of participants’ open-text responses describing their decision-making rationale corroborated the quantitative analysis: the majority of responses concerned perceived disease severity. Inclusion of a condition in professional society guidelines did not affect the likelihood of changed reproductive decisions.

This study also raises questions about the spectrum of variant-specific effects within recessive diseases and how this may impact reproductive decision making. Only two of nine ARC in our data carrying biotinidase deficiency reported changing their reproductive actions (two others provided unclear responses). The sharp contrast to other severe conditions raised questions as to the source of the discrepancy. While complete BTD is classified as a severe condition, partial deficiency (10–30% enzyme activity) is associated with a mild presentation. One variant, p.Asp444His (D444H, HGVS NC_000003.11:g.15686693G > C) occurs at high frequency (allele frequency of 3.94% = carrier frequency of 7.6% among non-Finnish Europeans in ExAC) (ExAC 2016; Lek et al. 2016). It is a common cause of partial BTD when combined with a classic mutation, and is associated with approximately 50% enzyme activity in homozygotes (Swango et al. 1998), similar to the asymptomatic carrier state. While participants were asked to report the condition they carried, they were not asked to report the specific variants, making it impossible to directly ascertain which ARC carried D444H. However, a review of the records of the original ARC invited to the study (including both respondents and nonrespondents) revealed that in 93% of BTD ARC (53/57), both members of the couple were D444H carriers. Our finding that most (7/9) BTD ARC did not report action taken based on this result is consistent with the hypothesis that all such ARC were D444H double-carriers (p = 0.19). This finding raises the issue of variant-specific effects within genetic conditions that has been well characterized in diseases such as cystic fibrosis. These results suggest a need for additional granularity in disease classification based on known genotype/phenotype correlations within a given condition.

Questions have been raised regarding provider and patient ability to sufficiently understand a wide variety of rare diseases to make informed decisions based on their carrier status (Henneman et al. 2016). One common caution regarding ECS is the overwhelming amount of information needed to counsel on each condition on the panel (Umbarger et al. 2013). Based on the clear differential in reproductive decisions between profound/severe and moderate conditions presented here, it appears that patients understood the relative level of severity and impact of the various diseases identified by ECS. This may also be a result of the high uptake of post-test genetic counseling: 95% of ARC (61/64) pursued genetic counseling after receiving their results.

This study reports the reproductive decisions made by ARC after receiving ECS results to evaluate and demonstrate the clinical utility of ECS. Not only did the majority of ARC identified through ECS alter their reproductive decisions based on these results, but there was no significant difference between the rate of action between severe and profound diseases currently recommended by professional societies and those not yet included in screening guidelines.