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PERSPECTIVE article

Front. Public Health, 05 September 2018
Sec. Public Health Policy
This article is part of the Research Topic How can Genomic Biobanks Provide the Bridge for Implementation of Effective Clinical Therapy? View all 7 articles

Equitable Participation in Biobanks: The Risks and Benefits of a “Dynamic Consent” Approach

\r\nMegan Prictor*Megan Prictor1*Harriet J. A. Teare,Harriet J. A. Teare1,2Jane Kaye,Jane Kaye1,2
  • 1Melbourne Law School, The University of Melbourne, Carlton, VIC, Australia
  • 2Centre for Health, Law and Emerging Technologies, Nuffield Department of Population Health, University of Oxford, Oxford, United Kingdom

Participation in biobanks tends to favor certain groups—white, middle-class, more highly-educated—often to the exclusion of others, such as indigenous people, the socially-disadvantaged and the culturally and linguistically diverse. Barriers to participation, which include age, location, cultural sensitivities around human tissue, and issues of literacy and language, can influence the diversity of samples found in biobanks. This has implications for the generalizability of research findings from biobanks being able to be translated into the clinic. Dynamic Consent, which is a digital decision-support tool, could improve participants' recruitment to, and engagement with, biobanks over time and help to overcome some of the barriers to participation. However, there are also risks that it may deepen the “digital divide” by favoring those with knowledge and access to digital technologies, with the potential to decrease participant engagement in research. When applying a Dynamic Consent approach in biobanking, researchers should give particular attention to adaptations that can improve participant inclusivity, and evaluate the tool empirically, with a focus on equity-relevant outcome measures. This may help biobanks to fulfill their promise of enabling translational research that is relevant to all.

Introduction: The Importance of Inclusivity

Participation in health research has tended to be dominated by white, middle-class, higher-educated people in most Western countries, to the exclusion of indigenous groups, the socially-disadvantaged and the culturally and linguistically diverse. This is concerning both from a moral perspective, where equitable access and benefit sharing are valued, and from a scientific perspective that relies on the extrapolation of findings from individual studies to larger population groups to improve health. This bias is also evident in biobank recruitment and affects the wide range of research conducted using biobank samples and data. Biobanks have been used in translational research that seeks to “understand the impact of environmental and other risk exposures on health, understanding genetic risks for common disease, identification of biomarkers in disease progression and prognosis, and are central to the implementation of personalized medicine projects” (1). Therefore, it is important that this bias is recognized and addressed, so that it does not introduce bias in the consideration of new health policy, or perpetuate existing social inequalities. In this paper we will consider whether efforts to achieve representativeness in biobank samples, specifically in terms of the potential for improved recruitment and retention of participants through a “Dynamic Consent” platform (2), can address the known barriers to participation for specific populations.

Bias in Biobanking Recruitment

Biobanks, though diverse in size, funding, contents, infrastructure, regulatory and governance frameworks, access policies and purposes, often comprise samples that reflect the lack of diversity and representativeness common to other forms of precision medicine research. Empirical studies have confirmed this, with researchers recently reporting that participants in the UK Biobank—some half a million people aged 40–69 years—were more likely to be female, in better health and living in a less deprived area, than the general population (3). The Estonian Biobank, involving around 5% of the country's population by 2014, reported a bias toward women and younger people compared to the whole population; further, the minority ethnicity Russians in Estonia were underrepresented (4). Similar trends were reported in an analysis of the Dutch Lifelines Study (fewer people were elderly, immigrants, unemployed, had ever smoked, or had less education) (5) and a consortium of Nordic cancer biobanks (cancer rates were less than the general population) (6). While this tendency is not universal [e.g., (7)], the issues of inclusivity and representativeness in large population biobanks are of concern.

Despite the promise of universal benefit that was expected to flow from the Human Genome Project, genetic research has struggled with the same bias toward homogeneity of data sets as other forms of health research—demonstrating a preference for large, “well-characterized, well-powered, predominantly European ancestry cohorts” (8). For example, in genome-wide association studies, researchers reported in 2009 that only around 4% utilized samples with non-European ancestry (9). By 2016 the proportion had risen to almost 20%, but this shift largely reflected the addition of Asian cohorts, with other groups still not represented (10).

While there are many different types of biobanks, cohorts of six or seven figures are becoming increasingly commonplace, as well as associated large-scale longitudinal projects capturing related health and lifestyle data. Biobank managers and funders are increasingly aware of recruitment bias and commonly seek to bolster inclusivity to ensure the representativeness and applicability of their collections. Studies actively seeking to minimize bias include the US-based “All of Us” project, which is “focused especially on enrolling those who have been overlooked in past research studies, and who may represent communities that have inadequately benefited from previous findings” (11). The Gen V project in Victoria, Australia, incorporating newborn heel prick cards, DNA samples and multiple health and education data sets for a 2-year state-wide cohort, is similarly premised on inclusivity (12).

The Effect on Research

Diversity of biobank samples is not merely an aspiration for ethical research conduct, it is a scientific imperative. In a paper examining how representative biobanks are of their local populations (7), the authors assert that it is a “primary responsibility [for biobanks] to collect tissues that are a true reflection of their local population and thereby promote translational research, which is applicable to the community.” Oh et al. note that several different factors, including genomic profile and genetic ancestry, inform our comprehension of disease (13). Limiting inclusivity must therefore narrow our understanding of genomics, and stymie progress. Importantly, this selection bias may also be invisible to scientists using the samples–and hence “may be impossible to adjust for in subsequent laboratory or statistical analysis” (14).

If biobanks are not appropriately reflective of the wider population, nor will the research findings derived from them be representative. This raises the risk that research products reaching the clinic will only be relevant for certain sections of the population, which could further exacerbate inequity and health inequalities.

Recognized Barriers to Participation

To achieve their recruitment targets, biobank managers and researchers should consider the barriers to inclusion of hard-to-reach groups. This also requires a review of the “[p]olicies for enrolling participants, returning research results and obtaining samples and data [that] can have a far-reaching impact on the type of research that can be performed with each biobank” (1) as well as the research outcomes and results. Several barriers have been identified in the literature that limit the participation in biobanks by all citizens in society.

Location

Research infrastructures tend to be concentrated in large urban centers, and so distance and transportation (1517) may have an impact on willingness and capacity to participate in biobank research. However, this is not always the case; the Estonian Biobank has achieved accurate representation from both urban/rural populations (4). Novel solutions such as mobile laboratories might address this problem (18), although these are expensive.

Literacy and Language

People with low literacy, including low health or scientific literacy, or who are linguistically diverse, are sometimes specifically excluded from biobanks. For example, the LifeLines study excluded people who were unable to read Dutch (5). Even absent specific exclusion, they are harder to recruit (16). It may be difficult to find appropriate terminology to explain biobank-relevant concepts in some languages (17, 19). The readability of biobank consent materials can be challenging for the general population (20) and act as a real disincentive to some groups (21) including migrants, those with lower education levels, people with intellectual disability, and children and adolescents.

Age

There are challenges to the recruitment of both older adults and children to biobanks. For children, these challenges are ethical as well as practical. They are vulnerable subjects with limited but increasing capacity, as they grow older, to understand research and provide truly informed consent (22). Legally, only their parent or legal guardian can consent, but children may provide assent, and have a right to be given information at an appropriate reading level. When they reach adulthood, they can reconsent or withdraw consent for themselves, but re-contacting participants years after the original sample donation can be problematic (23, 24).

Older people are both excluded from, and under-recruited to, healthcare research (25). Age-related health conditions that may affect hearing, vision, cognition, and mobility can impede participation.

Cultural Difference

It is known that “non-White populations are less likely to participate in biobanks and more likely to express concerns about the storage, collection, and use of biospecimens” (26). The considerations driving this reluctance are multifaceted, springing both from cultural values and experiences of exploitation as research subjects.

Blood and Tissue

Different cultural perspectives around the meaning of blood and tissue samples may weigh heavily on decision-making by indigenous peoples, diverse cultural groups, and minorities around biomedical sample donation (2628). These include perceptions that samples remain intimately connected with both whole people and groups (29), and hence that the mistreatment of body parts can cause physical or mental harm (30).

Individual vs. Group Decision-Making

Some groups have different views as to who can appropriately provide consent, which may diverge from the Western individualist notion of autonomous decision-making. Collective (family or community) engagement, recruitment, and consent has been utilized in settings including some indigenous communities [e.g., Australia, New Zealand, and Alaska (29)], southern Africa (28), and East Asia (3133). Where research focuses on a specific community, the International Society for Biological and Environmental Repositories endorses community participation in planning for the study and consent processes, specimen use and dissemination of research findings (34). Yet engaging with the appropriate decision-makers in different contexts adds complexity to the biobank recruitment process that can increase costs and time.

Mistrust

Indigenous people and minorities have often been subjects of health and anthropological research without consent [with infamous examples including the Tuskegee Syphilis Study (35) and the Havasupai sample research (36)], creating mistrust—and more recently, deep caution on the part of researchers to avoid further harm—that is hard to overcome. In this context, efforts to expand genomic research to address the known lack of ancestral diversity have sometimes backfired. For example, the Human Genome Diversity Project, which arose in the mid-1990s to analyse genetic material to better understand genetic variation, migration and evolution (37), was characterized as the “Vampire Project” by some indigenous groups (38). There remains a clear association between minority status, mistrust, and reluctance to donate biomedical samples (39).

Online Tools to Facilitate Participation—the Example of Dynamic Consent

Given these challenges, online tools are being developed that might improve engagement, communication and participation with a range of communities. One such tool is Dynamic Consent, which allows research participants to access a digital record of their consent decisions, and to have greater control over how their data and samples are used. Participants can revisit previous decisions and change their mind in real-time via a secure, personal profile. This establishes a channel of communication allowing participants to receive information about the research endeavor, and news and updates as the project progresses. It also enables researchers to manage their communication and engagement strategies with participants and keep a record of interactions.

Potential Benefits of Dynamic Consent

Dynamic Consent has been discussed as a mechanism that may improve the informed consent process for biobanking (and more widely) by providing research participants with stronger oversight of the uses of their samples and data (2). While Dynamic Consent was originally developed in response to a legal question surrounding consent and decision-making, it has progressed as a mechanism bolstering communication and engagement. Focus groups found that some biobank participants wanted more information about the uses of their samples and data, and the development of the research (40). This emphasis on communication and engagement has led to further discussion around the opportunities offered by a digital patient interface for information delivery, broadening both the range of information provided, and the delivery mode. Several papers reference the potential benefits to be derived from the use of multi-media, and of providing information over time, to counteract the current need to deliver complex information in a single encounter, at the beginning of the research process using a traditional consent approach (2, 4143).

Given this emphasis on tailored engagement, it is appropriate to examine Dynamic Consent's capacity to enable inclusivity within research endeavors such as biobanks, to overcome some of the barriers outlined earlier. For instance, digital tools and applications have been developed to enable real-time language translation, enabling linguistically diverse communities to contribute on an equal footing. The accessibility of websites is also a significant area of progress; options to work with communities to develop videos, diagrams, and animations have been cited as opportunities for inclusivity and hence diversification of the sample population. This could advance the participation of children by using age-appropriate language and tailored communication techniques, as well as enhancing accessibility to indigenous communities. The animation developed to explain the historical samples held in the National Centre for Indigenous Genomics is an excellent example (44).

Alongside these specific tools for accessibility is the philosophy behind Dynamic Consent which emphasizes the importance of timing. This includes: the timing of recruitment, and allowing participants to reconsider their decisions at home; the timing of information provision, such that it can be cascaded at different points throughout the research endeavor; and recognition that biobanking often takes place over years, if not decades. Having a system that allows participants to check in at their own convenience, over time, and be reminded of their involvement in research, is itself inclusive. It can help to facilitate the informed decision-making of adults who contributed to biobanks as children about their continued participation, and might mean that fewer are lost to follow-up (24). This ongoing connection might also foster trust by promoting improved understanding of the biobank and its research outputs, and a stronger sense of collaboration between donors and researchers. It could thus help to overcome cultural concerns about the treatment of blood and tissue samples, through promoting greater transparency and accountability.

Potential Drawbacks and the Need for Further Evaluation

Notwithstanding these significant benefits, there are also concerns about the challenges such technology will create. The most obvious is its potential to exacerbate exclusion and disenfranchisement, if participants are not willing to engage using the technology. This is often cited as a “digital divide,” with focus (perhaps unfairly) on older generations. However, it could equally apply to communities, for instance in remote parts of Australia, that lack access to technology, or reliable infrastructure including Wifi networks to allow meaningful reliance on these tools (45, 46). Some research on the willingness of different populations to engage with health information electronically has had encouraging findings (47, 48). However, this needs to be examined more carefully and tested with a diverse range of people, before researchers can rely on solely on digital tools. The move toward whole population electronic health records, such as the My Health Record in Australia (49), offers an opportunity to apply empirical methods, including focus groups and qualitative interviews, to investigate the willingness and capacity of different groups to engage with digital health tools.

While several projects already use Dynamic Consent [e.g., RUDY (50), CHRIS (42), PEER (51)], further evaluation is needed to gather real-world data on its influence on the participant experience, people's understanding of the research endeavor, and their sense of oversight and control. Within Dynamic Consent, consent choices are carefully set out to allow granular decision-making and tailored involvement. This approach should mitigate the challenges commonly encountered with online terms and conditions for products and services, including software and applications, that discourage full consideration of long legal explanations, and instead allows an easy and informative tick-box agreement (52). However, this will need to be explored as the projects using Dynamic Consent reach maturity, and it becomes possible to examine its influence on consenting behavior. Any risk that Dynamic Consent might further discourage participants from carefully considering important aspects of the research, or might promote “consent fatigue,” would undermine the intentions of the approach. Dynamic Consent interfaces must be designed to support people to think through important aspects of biobank sample donation, while not overwhelming them or causing further disengagement. Solutions may be found in citizen-science programmes using gamification to maintain interest, for example the project Foldit (53), which encourages members of the public to help describe the structures of proteins (54).

Accessibility challenges have and can be addressed using information technology. Examples include providing larger text or audio tools for visually-impaired people, and deploying a keyboard or joystick for those with certain physical impairments. Nonetheless, there is still concern that digital consenting tools will not be appropriately tailorable for all needs, and that biobanks will lack the resources to finance the variety of tools necessary to support accessibility. The needs of specific populations must be carefully considered for each project, to balance what is needed against what is practical, and to enhance inclusivity. This will not only relate to the consenting tools, but to the wider requirements of the biobank, and will rely upon an ongoing conversation with the target population.

Researchers conducting medical research, including using biobanks, are increasingly concerned about managing results that could be of immediate significance for a participant's health, and may also be relevant for their family or wider community. This raises a question about how to support consent relating to communication of findings, for the participant, but also whether (and if so how) family or community consent needs to be developed (31). Within genomics and precision medicine, projects involving multiple family members, often over several generations, are vital in building a clearer picture of different diseases and conditions (55). These projects rely on agreement from all family members, and could be undermined if one person was to withdraw. This raises questions for diversity and inclusion, as it may lead to family groups with particular characteristics being supportive of research, and may exacerbate some of the issues experienced with individual participation. Dynamic Consent has not yet been developed to support “family consent,” however it should be possible to allow records to be linked and unlinked based on each family member's decisions.

Next Steps

Considering the implications of narrow participation for the generalizability of translational research arising from biobanks, further attention must be given to mechanisms that could overcome barriers to inclusivity. Dynamic Consent holds the potential to improve the engagement of different groups through its flexibility and adaptability, and its focus on participant empowerment over an extended period. Further to the examples of Dynamic Consent mentioned above, it will be important for biobank managers and researchers to experiment with applications of the approach that focus on addressing barriers and facilitating widespread involvement. These applications could, for instance, incorporate child-friendly language, multiple translations, and culturally-tailored explanations. The relevance of biobank-based research to family members and communities should be reflected in tools that can accommodate decision-making by groups as well as individuals, and multi-generational sample donation.

There is also a need for empirical research on the effects of Dynamic Consent tools on equity-oriented research participation outcomes. The approach should be tested in high-quality evaluations reporting on outcome measures that are able to show if there is a difference between more and less advantaged groups (56, 57). The PROGRESS-Plus characteristics (58, 59) provide a sound basis for the design of Dynamic Consent research applying an equity lens. Attending to these concerns will help to ensure that biobanks fulfill their promise as a driver of translational research having benefits for all patients, not just some. Dynamic Consent cannot overcome all challenges to inclusivity; the starting point is for researchers to consider which populations need better representation, and to work alongside communities to design methods for inclusion. Once recruitment strategies have been devised, however, Dynamic Consent can support participants, and ensure a partnership approach to research that might motivate future involvement, and for participants to encourage friends and relatives to participate too.

Author Contributions

MP and HT planned the manuscript with input from JK. All authors compiled the first draft of the manuscript. MP and HT revised the manuscript. MP finalized and submitted the manuscript after all authors had critically read, revised, and approved the final version.

Funding

MP and HT Melbourne Law School and University of Melbourne STEM funding. JK Wellcome Trust 096599/2/11/2.

Conflict of Interest Statement

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Acknowledgments

The authors gratefully acknowledge the assistance of Melbourne Law School Academic Research Service in formatting this paper for submission.

References

1. Smith ME, Aufox S. Biobanking: the melding of research with clinical care. Curr Genet Med Rep. (2013) 1:122–28. doi: 10.1007/s40142-013-0014-6

PubMed Abstract | CrossRef Full Text | Google Scholar

2. Kaye J, Whitley EA, Lund D, Morrison M, Teare H, Melham K. Dynamic consent: A patient interface for twenty-first century research networks. Eur J Hum Genet. (2015) 23:141–46. doi: 10.1038/ejhg.2014.71

PubMed Abstract | CrossRef Full Text | Google Scholar

3. Fry A, Littlejohns TJ, Sudlow C, Doherty N, Adamska L, Sprosen T, et al. Comparison of sociodemographic and health-related characteristics of UK Biobank participants with those of the general population. Am J Epidemiol. (2017) 186:1026–34. doi: 10.1093/aje/kwx246

PubMed Abstract | CrossRef Full Text | Google Scholar

4. Leitsalu L, Haller T, Esko T, Tammesoo M-L, Alavere H, Snieder H, et al. Cohort profile: Estonian Biobank of the Estonian Genome Center, University of Tartu. Int J Epidemiol. (2015) 44:1137–47. doi: 10.1093/ije/dyt268

PubMed Abstract | CrossRef Full Text | Google Scholar

5. Klijs B, Scholtens S, Mandemakers JJ, Snieder H, Stolk RP, Smidt N. Representativeness of the LifeLines Cohort Study. PLoS ONE (2015) 10:e0137203. doi: 10.1371/journal.pone.0137203

PubMed Abstract | CrossRef Full Text | Google Scholar

6. Pukkala E, Andersen A, Berglund G, Gislefoss R, Gudnason V, Hallmans G, et al. Nordic biological specimen banks as basis for studies of cancer causes and control—more than 2 million sample donors, 25 million person years and 100 000 prospective cancers. Acta Oncol. (2007) 46:286–307. doi: 10.1080/02841860701203545

CrossRef Full Text | Google Scholar

7. Kozlakidis Z, Mant C, Peters B, Post F, Fox J, Philpott-Howard J, et al. How representative are research tissue biobanks of the local populations? Experience of the Infectious Diseases Biobank at King's College, London, UK. Biopreserv. Biobanking (2011) 9:287–88. doi: 10.1089/bio.2011.0015

PubMed Abstract | CrossRef Full Text | Google Scholar

8. Bentley AR, Callier S, Rotimi CN. Diversity and inclusion in genomic research: why the uneven progress? J Community Genet. (2017) 8:255–66. doi: 10.1007/s12687-017-0316-6

PubMed Abstract | CrossRef Full Text | Google Scholar

9. Need AC, Goldstein DB. Next generation disparities in human genomics: concerns and remedies. Trends Genet. (2009) 25:489–94. doi: 10.1016/j.tig.2009.09.012

PubMed Abstract | CrossRef Full Text | Google Scholar

10. Popejoy AB, Fullerton SM. Genomics is failing on diversity. Nature (2016) 538:161–64. doi: 10.1038/538161a

PubMed Abstract | CrossRef Full Text | Google Scholar

11. Azar AM, Collins FS. Pay It Forward: Join With All of Us Research Program to Build a Healthier Future. USA Today [Internet]. Available online at: https://www.usatoday.com/story/opinion/2018/05/07/all-us-research-medical-issues-national-institutes-health-column/584949002/

12. Generation Victoria [Internet]. Murdoch Children's Research Institute. Available online at: https://www.mcri.edu.au/genv.

13. Oh SS, Galanter J, Thakur N, Pino-Yanes M, Barcelo NE, White MJ, et al. Diversity in clinical and biomedical research: A promise yet to be fulfilled. PLoS Med. (2015) 12:e1001918. doi: 10.1371/journal.pmed.1001918

PubMed Abstract | CrossRef Full Text | Google Scholar

14. Ransohoff DF, Gourlay ML. Sources of bias in specimens for research about molecular markers for cancer. J Clin Oncol. (2010) 28:698–704. doi: 10.1200/JCO.2009.25.6065

PubMed Abstract | CrossRef Full Text | Google Scholar

15. Morgan LL, Fahs PS, Klesh J. Barriers to research participation identified by rural people. J Agric Saf Health (2005) 11:407–14. doi: 10.13031/2013.19719

PubMed Abstract | CrossRef Full Text | Google Scholar

16. Bonevski B, Randell M, Paul C, Chapman K, Twyman L, Bryant J, et al. Reaching the hard-to-reach: A systematic review of strategies for improving health and medical research with socially disadvantaged groups. BMC Med Res Methodol. (2014) 14:42. doi: 10.1186/1471-2288-14-42

PubMed Abstract | CrossRef Full Text | Google Scholar

17. O'Connor MR, Adem A, Starks H. East African perceptions of barriers/facilitators for pediatric clinical research participation and development of the inclusive research model. J Pediatr Nurs. (2018). doi: 10.1016/j.pedn.2018.05.005. [Epub ahead of print].

PubMed Abstract | CrossRef Full Text | Google Scholar

18. Where's the ASPREE Biobus? [Internet]. ASPREE Australia (2014) Available online at: https://aspree.org/aus/wheres-the-aspree-biobus/

19. Munung FS, Marshall P, Campbell M, Littler K, Masiye F, Ouwe-Missi-Oukem-Boyer O, et al. Obtaining informed consent for genomics research in Africa: analysis of H3Africa consent documents. J Med Ethics (2016) 42:132–37. doi: 10.1136/medethics-2015-102796

PubMed Abstract | CrossRef Full Text | Google Scholar

20. McGraw SA, Wood-Nutter CA, Solomon MZ, Maschke KJ, Benson JT, Irwin DE. Clarity and appeal of a multimedia informed consent tool for biobanking. IRB Ethics Hum Res. (2012) 34:9–19.

PubMed Abstract | Google Scholar

21. Eisenhauer ER, Tait AR, Rieh SY, Arslanian-Engoren CM. Participants' understanding of informed consent for biobanking: a systematic review. Clin Nurs Res. (2017). [Epub ahead of print].doi: 10.1177/1054773817722690

PubMed Abstract | CrossRef Full Text | Google Scholar

22. Hein IM, De Vries MC, Troost PW, Meynen G, Van Goudoever JB, Lindauer RJL. Informed consent instead of assent is appropriate in children from the age of twelve: policy implications of new findings on children's competence to consent to clinical research. BMC Med Ethics (2015) 16:76. doi: 10.1186/s12910-015-0067-z

PubMed Abstract | CrossRef Full Text | Google Scholar

23. Hens K, Van El CE, Borry P, Cambon-Thomsen A, Cornel MC, Forzano F, et al. Developing a policy for paediatric biobanks: principles for good practice. Eur J Hum Genet. (2013) 21:2–7. doi: 10.1038/ejhg.2012.99

PubMed Abstract | CrossRef Full Text | Google Scholar

24. Rush A, Battisti R, Barton B, Catchpoole D. Opinions of young adults on re-consenting for biobanking. J Pediatr. (2015) 167:925–30. doi: 10.1016/j.jpeds.2015.07.005

PubMed Abstract | CrossRef Full Text | Google Scholar

25. McMurdo MET, Roberts H, Parker S, Wyatt N, May H, Goodman C, et al. Improving recruitment of older people to research through good practice. Age Ageing (2011) 40:659–65. doi: 10.1093/ageing/afr115

PubMed Abstract | CrossRef Full Text | Google Scholar

26. Kowal E, Greenwood A, McWhirter RE. All in the blood: A review of Aboriginal Australians' cultural beliefs about blood and implications for biospecimen research. J Empir Res Hum Res Ethics (2015) 10:347–59. doi: 10.1177/1556264615604521

PubMed Abstract | CrossRef Full Text | Google Scholar

27. The H3Africa Consortium, Matovu E, Bucheton B, Chisi J, Enyaru J, Hertz-Fowler C, et al. Enabling the genomic revolution in Africa. Science (2014) 344:1346–48. doi: 10.1126/science.1251546

CrossRef Full Text | Google Scholar

28. Moodley K, Singh S. “It's all about trust”: reflections of researchers on the complexity and controversy surrounding biobanking in South Africa. BMC Med Ethics (2016) 17:57. doi: 10.1186/s12910-016-0140-2

CrossRef Full Text | Google Scholar

29. Kowal E, Easteal S, Gooda M. Indigenous genomics. Australas Sci. (2016) 37:18–20.

Google Scholar

30. Durie M. Understanding health and illness: research at the interface between science and indigenous knowledge. Int J Epidemiol. (2004) 33:1138–43. doi: 10.1093/ije/dyh250

PubMed Abstract | CrossRef Full Text | Google Scholar

31. Minari J, Teare H, Mitchell C, Kaye J, Kato K. The emerging need for family-centric initiatives for obtaining consent in personal genome research. Genome Med. (2014) 6:118. doi: 10.1186/s13073-014-0118-y

PubMed Abstract | CrossRef Full Text | Google Scholar

32. Yoshizawa G, Ho CW-L, Zhu W, Hu C, Syukriani Y, Lee I, et al. ELSI practices in genomic research in East Asia: implications for research collaboration and public participation. Genome Med. (2014) 6:39. doi: 10.1186/gm556

PubMed Abstract | CrossRef Full Text | Google Scholar

33. Yoshizawa G, Sasongko TH, Ho C-H, Kato K. Social and communicative functions of informed consent forms in East Asia and beyond. Front Genet. (2017) 8:99. doi: 10.3389/fgene.2017.00099

PubMed Abstract | CrossRef Full Text | Google Scholar

34. ISBER. ISBER Best Practices: Recommendations for Repositories. 4th ed. Vancouver, BC: ISBER (2018).

35. Brandt AM Racism and research: the case of the Tuskegee Syphilis Study. Hastings Cent Rep. (1978) 8:21–29.

PubMed Abstract | Google Scholar

36. Garrison NA. Genomic justice for native Americans: impact of the Havasupai case on genetic research. Sci Technol Hum Values (2013) 38:201–23. doi: 10.1177/0162243912470009

PubMed Abstract | CrossRef Full Text | Google Scholar

37. Cavalli-Sforza LL. The Human Genome Diversity Project: past, present and future. Nat Rev Genet. (2005) 6:333–40. doi: 10.1038/nrg1596

PubMed Abstract | CrossRef Full Text | Google Scholar

38. Crigger B-J. The “vampire project.” Hastings Cent Rep. (1995) 25:2.

PubMed Abstract | Google Scholar

39. Bussey-Jones J, Garrett J, Henderson G, Moloney M, Blumenthal C, Corbie-Smith G. The role of race and trust in tissue/blood donation for genetic research. Genet Med. (2010) 12:116–21. doi: 10.1097/GIM.0b013e3181cd6689

PubMed Abstract | CrossRef Full Text | Google Scholar

40. Teare HJ, Morrison M, Whitley EA, Kaye J. Towards “Engagement 2.0”: insights from a study of dynamic consent with biobank participants. Digit Health (2015) 1:1–13. doi: 10.1177/2055207615605644

PubMed Abstract | CrossRef Full Text | Google Scholar

41. Budin-Ljøsne I, Teare HJA, Kaye J, Beck S, Bentzen HB, Caenazzo L, et al. Dynamic Consent: a potential solution to some of the challenges of modern biomedical research. BMC Med Ethics (2017) 18:4. doi: 10.1186/s12910-016-0162-9

PubMed Abstract | CrossRef Full Text | Google Scholar

42. Pattaro C, Gögele M, Mascalzoni D, Melotti R, Schwienbacher C, De Grandi A, et al. The Cooperative Health Research in South Tyrol (CHRIS) study: rationale, objectives, and preliminary results. J Transl Med. (2015) 13:348. doi: 10.1186/s12967-015-0704-9

PubMed Abstract | CrossRef Full Text | Google Scholar

43. Williams H, Spencer K, Sanders C, Lund D, Whitley EA, Kaye J, et al. Dynamic Consent: a possible solution to improve patient confidence and trust in how electronic patient records are used in medical research. JMIR Med Inform. (2015) 3:e3. doi: 10.2196/medinform.3525

PubMed Abstract | CrossRef Full Text | Google Scholar

44. About NCIG: An Introduction for Donor Communities [Internet]. National Centre for Indigenous Genomics (2018) Available online at: http://ncig.anu.edu.au/ncig-collection/current-projects/community-engagement/about-ncig-introduction-donor-communities

45. Rennie E, Hogan E, Gregory R, Crouch A, Wright A, Thomas J. Internet on the Outstation: The Digital Divide and Remote Aboriginal Communities. Amsterdam: Institute of Network Cultures. (2016)

Google Scholar

46. Rennie E. Policy experiments and the digital divide: understanding the context of internet adoption in remote Aboriginal communities. In: Dezuanni M, Foth M, Mallan K, Hughes H, Digital Participation through Social Living Labs: Valuing Local Knowledge, Enhancing Engagement. Cambridge, MA: Chandos Publishing. (2018) p. 299–313.

Google Scholar

47. Coathup V, Teare HJA, Minari J, Yoshizawa G, Kaye J, Takahashi MP, et al. Using digital technologies to engage with medical research: views of myotonic dystrophy patients in Japan. BMC Med Ethics (2016) 17:51. doi: 10.1186/s12910-016-0132-2

PubMed Abstract | CrossRef Full Text | Google Scholar

48. Coathup V, Finlay T, Teare HJ, Kaye J, South M, Watt FE, et al. Making the most of the waiting room: electronic patient engagement, a mixed methods study. Digit Health (2018) 4:1–134. doi: 10.1177/2055207617751304

PubMed Abstract | CrossRef Full Text | Google Scholar

49. My Health Record [Internet]. Australian Digital Health Agency. Available online at: https://www.myhealthrecord.gov.au/front.

50. Teare HJ, Hogg J, Kaye J, Luqmani R, Rush E, Turner A, et al. The RUDY study: using digital technologies to enable a research partnership. Eur J Hum Genet. (2017) 25:816–22. doi: 10.1038/ejhg.2017.57

PubMed Abstract | CrossRef Full Text | Google Scholar

51. Platform for Engaging Everyone Responsibly [Internet]. Genetic Alliance. Available online at: http://www.geneticalliance.org/programs/biotrust/peer.

52. Obar JA, Oeldorf-Hirsch A. The biggest lie on the Internet: ignoring the privacy policies and terms of service policies of social networking services. In: TPRC 44: The 44th Research Conference on Communication, Information and Internet Policy (2016). Available online at: https://ssrn.com/abstract=2757465

Google Scholar

53. Solve Puzzles for Science [Internet]. Foldit. Available online at: https://fold.it/portal/.

54. Cooper S, Khatib F, Treuille A, Barbero J, Lee J, Beenen M, et al. Predicting protein structures with a multiplayer online game. Nature (2010) 466:756–60. doi: 10.1038/nature09304

PubMed Abstract | CrossRef Full Text | Google Scholar

55. Engaging Australia's First Peoples in the Development of Ethics Protocols for a Family-Based Microbiome Study Social Health History Project [Internet]. The Lowitja Institute (2018) Available online at: https://www.lowitja.org.au/first-peoples-ethics-protocols

56. Petkovic J, Welch V, Jull J, Petticrew M, Kristjansson E, Rader T, et al. How health equity is reported and analyzed in randomized trials. Cochrane Database Syst Rev. (2017). doi: 10.1002/14651858.MR000046

CrossRef Full Text | Google Scholar

57. Welch V, Petticrew M, Tugwell P, Moher D, O'Neill J, Waters E, et al. PRISMA-Equity 2012 Extension: Reporting Guidelines for Systematic Reviews with a focus on health equity. PLoS Med. (2012) 9:e1001333. doi: 10.1371/journal.pmed.1001333

PubMed Abstract | CrossRef Full Text | Google Scholar

58. PROGRESS-Plus [Internet]. Cochrane Equity. Available online at: http://methods.cochrane.org/equity/projects/evidence-equity/progress-plus.

59. O'Neill J, Tabish H, Welch V, Petticrew M, Pottie K, Clarke M, et al. Applying an equity lens to interventions: using PROGRESS ensures consideration of socially stratifying factors to illuminate inequities in health. J Clin Epidemiol. (2014) 67:56–64. doi: 10.1016/j.jclinepi.2013.08.005

PubMed Abstract | CrossRef Full Text | Google Scholar

Keywords: biobanks, consent, equity, participation, translation, Dynamic Consent, inclusive, communication

Citation: Prictor M, Teare HJA and Kaye J (2018) Equitable Participation in Biobanks: The Risks and Benefits of a “Dynamic Consent” Approach. Front. Public Health 6:253. doi: 10.3389/fpubh.2018.00253

Received: 28 June 2018; Accepted: 15 August 2018;
Published: 05 September 2018.

Edited by:

Ronald Przygodzki, United States Department of Veterans Affairs, United States

Reviewed by:

Luret Albert Lar, Jos University Teaching Hospital, Nigeria
Jan Fizzell, New South Wales Department of Health, Australia

Copyright © 2018 Prictor, Teare and Kaye. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

*Correspondence: Megan Prictor, bWVnYW4ucHJpY3RvciYjeDAwMDQwO3VuaW1lbGIuZWR1LmF1

Disclaimer: All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article or claim that may be made by its manufacturer is not guaranteed or endorsed by the publisher.