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Twins as Participants in Randomized Controlled Trials: A Review of Published Literature

Published online by Cambridge University Press:  28 December 2017

Athula Sumathipala*
Affiliation:
Research Institute for Primary Care & Health Sciences, Keele University, Staffordshire, UK South Staffordshire and Shropshire NHS Foundation Trust, Stafford, UK Institute for Research and Development, Colombo, Sri Lanka
Lisa Yelland
Affiliation:
South Australian Health and Medical Research Institute, Adelaide, South Australia, Australia School of Public Health, The University of Adelaide, Adelaide, South Australia, Australia
Debra Green
Affiliation:
South Staffordshire and Shropshire NHS Foundation Trust, Stafford, UK
Tom Shepherd
Affiliation:
Research Institute for Primary Care & Health Sciences, Keele University, Staffordshire, UK
Kaushalya Jayaweera
Affiliation:
Institute for Research and Development, Colombo, Sri Lanka
Paulo Ferreira
Affiliation:
Faculty of Health Sciences, Musculoskeletal Health Research Group, University of Sydney, Sydney, New South Wales, Australia
Jeffrey M. Craig
Affiliation:
Murdoch Children's Research Institute and Department of Paediatrics, University of Melbourne, Royal Children's Hospital, Melbourne, Victoria, Australia
*
address for correspondence: Professor Athula Sumathipala, Research Institute for Primary Care & Health Sciences Faculty of Medicine & Health Sciences, Keele University, Staffordshire, ST5 5BG, UK. E-mail: [email protected]

Abstract

Monozygotic (MZ) and dizygotic (DZ) twins participate in research that partitions variance in health, disease, and behavior into genetic and environmental components. However, there are other innovative roles for twins in medical research. One such way is involving MZ and/or DZ twins in co-twin control-designed randomized controlled trials (RCTs). To our knowledge, no reviews have been conducted that summarizes the involvement of twins in RCTs. Therefore, we conducted a systematic literature search using the U.S. Clinical Trials Database, NHS electronic databases, MEDLINE, EMBASE, and PsychINFO for RCTs on publications involving MZ and/or DZ twins as RCT participants. Out of the 186,027 clinical trials registered in the U.S. clinical trial register ClinicaTrails.gov, only six RCTs used twins as participants. From 1,598 articles identified in our search, 50 peer-reviewed English language publications met our pre-defined inclusion criteria. Sample sizes for RCTs have ranged from a total number of participants from 2 to 1,162; however, 32 (64%) studies had a sample size of 100 or less, and of those, 12 (24%) had fewer than 10. Both MZ and DZ twins have been recruited to the RCTs. In most instances (33/50) each twin from a pair were assigned to different study arms. Most of those studies included MZ twins only. Despite the methodological advantages, the use of MZ and DZ twins as participants in interventional RCTs appeared limited. The continuous development of innovative twin designs, especially RCTs, indicates that twin research can extend beyond the more widely recognized heritability estimates.

Type
Articles
Copyright
Copyright © The Author(s) 2017 

Twins studies are best known for using the classical twin design, based on comparisons between the similarity of monozygotic (MZ) and dizygotic (DZ) twins to partition the variance in health, disease, and behavior into genetic and environmental components, predominantly using observational study designs (Boomsma et al., Reference Boomsma, Busjahn and Peltonen2002; van Dongen et al., Reference van Dongen, Slagboom, Draisma, Martin and Boomsma2012)

Studies involving twins have become increasingly relevant due to the continuous work of twin registries and studies that have, collectively, amassed data and biological material on hundreds of thousands of twins, and have provided a valuable resource for studying complex genetic phenotypes and their underlying biology (Hur & Craig, Reference Hur and Craig2013). The availability of longitudinal data through the International Society of Twin Studies and International Network of Twin Registries (INTR) is also proving to be a valuable resource, not only for new studies but also for global collaborations (Buchwald et al., Reference Buchwald, Kaprio, Hopper, Sung, Goldberg, Fortier and Harris2014). Data derived from a collaboration of 54 international twin cohort databases participating in the CODATwins Project is a prime example (Jelenkovic et al., 2015, Reference Jelenkovic, Hur, Sund, Yokoyama, Siribaddana, Hotopf and Silventoinen2016; Silventoinen et al., Reference Silventoinen, Jelenkovic, Sund, Honda, Aaltonen, Yokoyama and Kaprio2015, Reference Silventoinen, Jelenkovic, Sund, Hur, Yokoyama, Honda and Kaprio2016; Yokoyama et al., Reference Yokoyama, Jelenkovic, Sund, Sung, Hopper, Ooki and Silventoinen2016).

Within-pair comparisons of phenotypically discordant MZ and DZ twin pairs through an observational co-twin controlled design can illuminate the non-shared environmental differences influencing human traits. However, such comparisons are arguably more efficient in intervention co-twin control studies using phenotypically concordant pairs, where one twin is randomly assigned to receive the intervention and the other twin acts as their control. A comparison between the co-twin control design in intervention and non-intervention studies, along with other novel utilities of this design, have been discussed in detail previously (Plomin & Haworth, Reference Plomin and Haworth2010).

The term ‘intervention’ refers broadly to any clinical maneuver offered to study participants that may have an effect on their health status (Jadad, Reference Jadad1998). Randomized controlled trials (RCTs) are considered the gold standard for testing interventions and ‘the most rigorous way of determining whether a cause–effect relationship exists between treatment and outcome and for assessing the cost effectiveness of a treatment’ (Sibbald & Roland, Reference Sibbald and Roland1998, p. 201). Random allocation provides participants the same chance of being assigned to each of the treatment groups (Altman, Reference Altman1991). The purpose of random allocation is to ensure that the characteristics of participants are as similar as possible across treatment groups prior to the initiation of an intervention (baseline). If randomization is done properly, it reduces the risk of a serious imbalance in known and unknown factors that could influence the clinical course of the participants. Therefore, any significant differences between treatment groups in the outcome of interest can be attributed to the intervention and not to any unidentified factor(s).

However, involving MZ twins in a co-twin control-designed RCT has advantages over the traditional RCT involving unrelated individuals. The co-twin control design can increase statistical power and provide perfect control for many of the potential confounding factors that could be imbalanced between treatment groups by chance, especially genetic makeup and age. The latter is particularly relevant to RCTs in children, where age matching is often a challenge. However, recruiting children in RCTs has ethical implications and needs especially strict ethical oversight.

DZ twins may also allow for matching due to shared environment as well as some genetic component and age, which can potentially justify the choice for recruiting DZ twins rather than siblings for a study. However, challenges such as teasing out individual factors in the context of complex interacting contributors may arise when using DZ twins in RCTs. It is also believed that the co-twin control RCT approach will have the additional advantage of requiring a relatively smaller sample size without reducing the statistical power (Plomin & Haworth, Reference Plomin and Haworth2010). However, if twins from the same pair are randomly assigned to the same treatment group or independently of each other, rather than to different treatment groups as in the co-twin control design, the benefits in sample size for an RCT involving twins may be lost (Yelland et al., Reference Yelland, Sullivan, Price and Lee2017). Intervention studies involving twins do exist in the literature. One such trial testing the effect of Vitamin C intake on common cold symptoms found that the relative power of this design compared to an unpaired design could be 2–14 times stronger, which means an unpaired study design would require much larger sample sizes to detect the same effect (Carr et al., Reference Carr, Martin and Whitfield1981; Martin et al., Reference Martin, Carr, Oakeshott and Clark1982).

However, in our opinion the full advantages and the rationale for involving twins in RCTs have not been adequately discussed or explored. Therefore, we carried out this review as the first step to identify studies using twins as participants for RCTs. In-depth analyses of the quality of individual studies and methodological issues of these studies or meta-analysis was not an aim of this review. In addition, a meta-analysis is not possible due to the heterogeneity of such studies and the varying interventions tested, resulting in no single treatment effect to be estimated. Instead, we aimed to identify all published material including RCTs involving only twins as participants up until 2015, using the selection criteria described below, and to summarize basic trial characteristics including sample size, inclusion criteria, whether trials include only MZ, DZ or both, and randomization method (i.e., whether same-pair twins were randomly assigned to the same treatment group independent of each other, or to different treatment groups in a co-twin control design).

Materials and Methods

A comprehensive search was carried out using the following databases: USA clinical trial (https://clinicaltrials.gov/), MEDLINE (1946–2015), EMBASE (1974–2015), and PsychINFO (1806–2015). We also performed an extensive search using PubMed (all publications until March 2015). Searches were confined to articles in English.

In the NHS library electronic database searches (MEDLINE, EMBASE, and PsychINFO), the search terms ‘twins’, ‘randomi*’, ‘control*’, and ‘trial*’ with Boolean operator AND was used in ‘title and abstract’. Each database was searched individually using the search terms. This allowed for all alternative spelling (randomised and randomized), variations of control (control, controls, and controlled) and singular or plural trial (trial and trials) to be searched simultaneously. The search terms used for the PubMed search also took all of these variations into account (as per the NHS library search).

Data Extraction

Data were extracted by one reviewer (DG), and then checked independently by a second reviewer (AS). All publications identified in the searches were searched for duplicates. Eligibility for inclusion in the review was decided by DG and AS. Full versions of publications selected were obtained and reviewed independently by three authors (AS, DG, and TS). Any discrepancy in judgments was resolved through consensus. Abstracts eligible for inclusion were confined to those reporting on a RCT that had used only twins as study participants but not mothers pregnant with twins. Information was extracted from each of the studies relating to authors, study location, database, twin registry (if any), condition, primary outcome, sample size, eligible age, eligible sex, zygosity, twin assignment (same treatment groups, different treatment groups, or independent allocation), masking, and control arm.

Results

U.S. Clinical Trial Database

The initial search using the U.S. clinical trial database (186,027 clinical trials registered) resulted in a total of 90 clinical trials. Of these, 50 studies were registered with twins as study participants, and 40 studies were registered with mothers who were pregnant with twins as study participants. Of the 90 twin studies, there were 29 RCTs. Of these, 23 had used mothers pregnant with twins as the study participants and only six studies had recruited twins as the study participants (Figure 1).

FIGURE 1 PRISMA diagram to illustrate the literature search process and the resulting number of reviewed articles from USA Clinical Trial database.

Extended Search Using Other Databases

After taking into account all duplicates and discounting papers including mothers pregnant with twins, the NHS library searches gave a total of 51 papers on RCTs using twins as study participants; 47 from MEDLINE, and a further 4 papers not found in MEDLINE were found in EMBASE. No additional papers were found in PsychINFO.

PubMed searches gave an additional eight papers using twins as study participants that were not found in either the MEDLINE or EMBASE search. The search term ‘Twins and Randomized Control Trial’ found two papers; the term ‘Twins and Randomised Controlled Trial’ found five; and the term ‘Twins and Randomised Control Trials’ found one. The search terms ‘Twins and Randomised Controlled Trial’ and ‘Twins and Randomised controlled trials’ gave the exact same result when substituting the ‘s’ for a ‘z’ in the word ‘randomised’. The full text of all 59 potentially relevant papers was examined in more detail, and 50 were consistent with the inclusion criteria for this review (Figure 2).

FIGURE 2 PRISMA diagram to illustrate the literature search process and the resulting number of reviewed articles found in the Medline, Psych INFO and EMBASE databases.

Trial Characteristics

Sample size and allocation of twins

The sample size varied greatly across the RCTs included in the review. Table 1 illustrates that 42% of RCTs had a sample size that fell within 10–100 twin pairs. Twenty four percent of the studies had a sample size smaller than 10 twin pairs as research participants. Therefore, the majority of studies had 100 twin pairs or fewer as participants.

TABLE 1 Characteristics of Randomized Controlled Trials With Twin Participants

Zygosity and twin assignment across the randomized controlled trials

As illustrated in Table 1, 13 RCTs assigned both twins in a pair to the same study arm, 10 of which included both MZ and DZ twins, two included only MZ twins, and one included only DZ twins. This is in contrast to 33 RCTs where twin pairs were assigned to different study arms, of which 6 included both MZ and DZ twins, 24 included only MZ twins, and 3 included only DZ twins. In most instances (33/50) the pair of twins had been assigned to different study arms, and most of these studies (24/33) had been with MZ twins.

Location of studies

The vast majority of the studies included in this review were conducted in the United States (21). The remaining studies were from Canada (5), Australia (3), United Kingdom (3), Finland (2), Germany (2), Greece (2), and one from each of the following countries; Bangladesh, Belgium, Dominican Republic, France, Hawaii, Hong Kong, India, Iran, Norway, Switzerland, Taiwan, and Thailand. A twin registry had been used to support recruitment in eight of the RCTs. These were the Australian Twin Registry (3), the Twin Research Registry, United Kingdom (3), the St. Thomas UK Adult Twin Registry (1), and the University of Washington Twin Registry (1). In the remaining 39 studies, there was no evidence of a twin registry being used to support recruitment. RCTs were diverse in nature, and areas included preterm birth nutrition, behavior, dental health, antiviral treatments, and co-bedding of twins (twin infants sleeping together).

Discussion

RCTs involving only twins as participants are limited, as shown by this review. Only 50 studies met our inclusion criteria after a comprehensive search in clinical trials and NHS library databases, even across a wide range of disciplines. Out of the 186,027 clinical trials registered in the U.S. clinical trial register, only six RCTs used twins as participants. While it is impossible to determine how many RCTs had been reported through PubMed and other databases in total, it is clear that the number of twin RCTs is disproportionate to the number involving singletons. Therefore, it can be concluded that specifically using twins in RCTs is not common compared to using singletons.

Randomization of Twins in a RCT

When twins participate in a clinical trial, they may be randomized to the same treatment group, independent of each other, or to different treatment groups as in the co-twin control design. Our review found that most clinical trials used the co-twin control design with MZ twins. Therefore, it could be concluded that in the majority of studies, MZ twins had been used for perfect control of genetic variation between the treatment groups. Recent work suggests that twins and their parents have a strong preference for assigning both twins to the same treatment group, rather than using the co-twin control design (Bernardo et al., Reference Bernardo, Nowacki, Martin, Fanaroff and Hibbs2015). This has important implications for future RCTs conducted in twins, since recruitment may be more successful if both twins in a pair will receive the same treatment, although the impact of different methods of randomizing twins on the sample size must also be considered.

The Impact of Twins on Sample Size and Power

The sample size of trials included in our review ranged from 2 to 1,162 (Table 1) and in the majority of trials (64%), the sample size was 100 or less. Although we did not attempt to assess whether the sample size was adequate for addressing the specific research question of each trial, this does raise the issue of whether small RCTs involving twins are adequately powered to detect meaningful treatment effects. One of the advantages of conducting RCTs in twins is that the sample sizes can be less compared to using non-twin RCTs (Carr et al., Reference Carr, Martin and Whitfield1981; Martin et al., Reference Martin, Carr, Oakeshott and Clark1982; Miller et al., Reference Miller, Mulvey, Martin, Miller, Mulvey and Martin1995). However, this will depend on how twins from the same pair are randomized. If the co-twin control design is used, such that one twin from each pair receives the intervention and the other acts as their control, the trial will have more power than a trial in singletons, and hence the sample size can be reduced. In contrast, if both twins are assigned to the same treatment group, the trial will have less power than a trial in singletons, thus requiring a larger sample size. This is due to the fact that comparisons of the intervention and control conditions must be made across twin pairs, rather than within twin pairs as in the co-twin control design. If twins from the same pair are randomized independently (ignoring that they are twins and treating as individuals), the trial will likely have similar power to a trial in singletons. Methods for calculating the sample size for trials involving twins only or a combination of singletons and twins have been discussed elsewhere (Yelland et al., Reference Yelland, Sullivan, Price and Lee2017).

International Collaborations Using Twin Registries

We found that only 11/50 (22%) of the studies used twin registries for recruitment. One option particularly for multi-center RCTs with a relatively large sample size is international collaboration, as currently utilized in non-RCT twin research (Buchwald et al., Reference Buchwald, Kaprio, Hopper, Sung, Goldberg, Fortier and Harris2014). The CODA Twins project was a classic example initiated in 2013 by identifying all twin projects in the world. It comprises 67 twin projects having data from both MZ and DZ twin pairs. The main sources used to identify the projects were a special issue of Twin Research and Human Genetics (Hur & Craig Reference Hur and Craig2013), and the participants of the INTR (Buchwald et al., Reference Buchwald, Kaprio, Hopper, Sung, Goldberg, Fortier and Harris2014; van Dongen et al., Reference van Dongen, Slagboom, Draisma, Martin and Boomsma2012). The INTR is a platform for international collaborations and would be an excellent resource for large-scale multicenter clinical trials.

Implications for Future Work and Directions

To understand the potential benefits of the co-twin control design, it would be useful to compare the sample sizes of twin RCTs and non-twin RCTs required to detect the same effect size. The advantages and disadvantages of inclusion of both MZ and DZ twins in RCTs needs more in-depth discussion and are areas for future methodological research. Contamination between intervention and control twin participants allocated to different treatment groups (particularly in psychological interventions), especially among twins living together, will be an important issue to address.

Limitation of the Review

In-depth analyses of the quality of individual 50 studies qualified for the review and methodological issues of these studies were not done. We did not include a meta-analysis for this review.

Conclusion

Both MZ and DZ twins have been used in RCTs. However, in a majority of instances they have been MZ twins randomized to opposite arms of a RCT.

The continuous development and implementation of innovative twin designs in intervention studies, especially RCTs, indicates that twin research can extend beyond the more widely recognized heritability estimates toward the possibility of inference on causation.

Acknowledgments

JMC is supported by grants from the Australian National Health and Medical Research Council (grant number 1079102), the Financial Markets Foundation for Children (grant number 2015-111), the Cerebral Palsy Alliance Research Foundation (grant number PG2316), and by the Victorian Government's Operational Infrastructure Support Program. LNY is supported by an Australian National Health and Medical Research Council Early Career Fellowship (ID 1052388).

Conflict of Interest

None.

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Figure 0

FIGURE 1 PRISMA diagram to illustrate the literature search process and the resulting number of reviewed articles from USA Clinical Trial database.

Figure 1

FIGURE 2 PRISMA diagram to illustrate the literature search process and the resulting number of reviewed articles found in the Medline, Psych INFO and EMBASE databases.

Figure 2

TABLE 1 Characteristics of Randomized Controlled Trials With Twin Participants