Melbourne Law School - Research Publications

Permanent URI for this collection

http://hdl.handle.net/11343/382

Search Results

Now showing 1 - 10 of 34

From single biobanks to international networks: developing e-governance

Kaye, J (SPRINGER, 2011-09)

The future holds the possibility to link and network biobanks, existing biorepositories and reference databases for research purposes in ways that have not been possible before. There is the potential to develop 'research portals' that will enable researchers to access these research resources that are located around the globe with the click of a mouse. In this paper, I will argue that our current governance system for research is unable to provide all of the oversight and accountability mechanisms that are required for this new way of doing research that is based upon flows of data across international borders. For example, our current governance framework for research is nationally based, with a complex system of laws, policies and practice that can be unique to a jurisdiction. It is also evident that many of the nationally based governance bodies in this field do not have the legal powers or expertise to adjudicate on the complex issues, such as privacy and disclosure risks that are raised by cross-border data sharing. In addition, the conceptual underpinning of this research governance structure is based on the "one researcher, one project, one jurisdiction" model. In the conclusion of this paper, I lay out some preliminary ideas as to how this system has to change to accommodate research that is based on networks. I suggest that a move to digital governance mechanisms might be a start to making research governance systems more appropriate for the 21st century.
A P3G generic access agreement for population genomic studies

Knoppers, BM ; Chisholm, RL ; Kaye, J ; Cox, D ; Thorogood, A ; Burton, P ; Brookes, AJ ; Fortier, I ; Goodwin, P ; Harris, JR ; Hveem, K ; Kent, A ; Little, J ; Riegman, PHJ ; Ripatti, S ; Stolk, RP (NATURE PUBLISHING GROUP, 2013-05)
Implementing a successful data-management framework: the UK10K managed access model

Muddyman, D ; Smee, C ; Griffin, H ; Kaye, J (BIOMED CENTRAL LTD, 2013-11-15)

This paper outlines the history behind open access principles and describes the development of a managed access data-sharing process for the UK10K Project, currently Britain's largest genomic sequencing consortium (2010 to 2013). Funded by the Wellcome Trust, the purpose of UK10K was two-fold: to investigate how low-frequency and rare genetic variants contribute to human disease, and to provide an enduring data resource for future research into human genetics. In this paper, we discuss the challenge of reconciling data-sharing principles with the practicalities of delivering a sequencing project of UK10K's scope and magnitude. We describe the development of a sustainable, easy-to-use managed access system that allowed rapid access to UK10K data, while protecting the interests of participants and data generators alike. Specifically, we focus in depth on the three key issues that emerge in the data pipeline: study recruitment, data release and data access.
Towards a data sharing Code of Conduct for international genomic research

Knoppers, BM ; Harris, JR ; Tasse, AM ; Budin-Ljosne, I ; Kaye, J ; Deschenes, M ; Zawati, MH (BMC, 2011)

Data sharing is increasingly regarded as an ethical and scientific imperative that advances knowledge and thereby respects the contributions of the participants. Because of this and the ever-increasing amount of data access requests currently filed around the world, three groups have decided to develop data sharing principles specific to the context of collaborative international genomics research. These groups are: the international Public Population Project in Genomics (P3G), an international consortium of projects partaking in large-scale genetic epidemiological studies and biobanks; the European Network for Genetic and Genomic Epidemiology (ENGAGE), a research project aiming to translate data from large-scale epidemiological research initiatives into relevant clinical information; and the Centre for Health, Law and Emerging Technologies (HeLEX). We propose seven different principles and a preliminary international data sharing Code of Conduct for ongoing discussion.
Direct-to-consumer genetic testing for predicting sports performance and talent identification: Consensus statement

Webborn, N ; Williams, A ; McNamee, M ; Bouchard, C ; Pitsiladis, Y ; Ahmetov, I ; Ashley, E ; Byrne, N ; Camporesi, S ; Collins, M ; Dijkstra, P ; Eynon, N ; Fuku, N ; Garton, FC ; Hoppe, N ; Holm, S ; Kaye, J ; Klissouras, V ; Lucia, A ; Maase, K ; Moran, C ; North, KN ; Pigozzi, F ; Wang, G (BMJ PUBLISHING GROUP, 2015-12)

The general consensus among sport and exercise genetics researchers is that genetic tests have no role to play in talent identification or the individualised prescription of training to maximise performance. Despite the lack of evidence, recent years have witnessed the rise of an emerging market of direct-to-consumer marketing (DTC) tests that claim to be able to identify children's athletic talents. Targeted consumers include mainly coaches and parents. There is concern among the scientific community that the current level of knowledge is being misrepresented for commercial purposes. There remains a lack of universally accepted guidelines and legislation for DTC testing in relation to all forms of genetic testing and not just for talent identification. There is concern over the lack of clarity of information over which specific genes or variants are being tested and the almost universal lack of appropriate genetic counselling for the interpretation of the genetic data to consumers. Furthermore independent studies have identified issues relating to quality control by DTC laboratories with different results being reported from samples from the same individual. Consequently, in the current state of knowledge, no child or young athlete should be exposed to DTC genetic testing to define or alter training or for talent identification aimed at selecting gifted children or adolescents. Large scale collaborative projects, may help to develop a stronger scientific foundation on these issues in the future.
A global reference for human genetic variation

Altshuler, DM ; Durbin, RM ; Abecasis, GR ; Bentley, DR ; Chakravarti, A ; Clark, AG ; Donnelly, P ; Eichler, EE ; Flicek, P ; Gabriel, SB ; Gibbs, RA ; Green, ED ; Hurles, ME ; Knoppers, BM ; Korbel, JO ; Lander, ES ; Lee, C ; Lehrach, H ; Mardis, ER ; Marth, GT ; McVean, GA ; Nickerson, DA ; Schmidt, JP ; Sherry, ST ; Wang, J ; Wilson, RK ; Gibbs, RA ; Boerwinkle, E ; Doddapaneni, H ; Han, Y ; Korchina, V ; Kovar, C ; Lee, S ; Muzny, D ; Reid, JG ; Zhu, Y ; Wang, J ; Chang, Y ; Feng, Q ; Fang, X ; Guo, X ; Jian, M ; Jiang, H ; Jin, X ; Lan, T ; Li, G ; Li, J ; Li, Y ; Liu, S ; Liu, X ; Lu, Y ; Ma, X ; Tang, M ; Wang, B ; Wang, G ; Wu, H ; Wu, R ; Xu, X ; Yin, Y ; Zhang, D ; Zhang, W ; Zhao, J ; Zhao, M ; Zheng, X ; Lander, ES ; Altshuler, DM ; Gabriel, SB ; Gupta, N ; Gharani, N ; Toji, LH ; Gerry, NP ; Resch, AM ; Flicek, P ; Barker, J ; Clarke, L ; Gil, L ; Hunt, SE ; Kelman, G ; Kulesha, E ; Leinonen, R ; McLaren, WM ; Radhakrishnan, R ; Roa, A ; Smirnov, D ; Smith, RE ; Streeter, I ; Thormann, A ; Toneva, I ; Vaughan, B ; Zheng-Bradley, X ; Bentley, DR ; Grocock, R ; Humphray, S ; James, T ; Kingsbury, Z ; Lehrach, H ; Sudbrak, R ; Albrecht, MW ; Amstislavskiy, VS ; Borodina, TA ; Lienhard, M ; Mertes, F ; Sultan, M ; Timmermann, B ; Yaspo, M-L ; Mardis, ER ; Wilson, RK ; Fulton, L ; Fulton, R ; Sherry, ST ; Ananiev, V ; Belaia, Z ; Beloslyudtsev, D ; Bouk, N ; Chen, C ; Church, D ; Cohen, R ; Cook, C ; Garner, J ; Hefferon, T ; Kimelman, M ; Liu, C ; Lopez, J ; Meric, P ; O'Sullivan, C ; Ostapchuk, Y ; Phan, L ; Ponomarov, S ; Schneider, V ; Shekhtman, E ; Sirotkin, K ; Slotta, D ; Zhang, H ; McVean, GA ; Durbin, RM ; Balasubramaniam, S ; Burton, J ; Danecek, P ; Keane, TM ; Kolb-Kokocinski, A ; McCarthy, S ; Stalker, J ; Quail, M ; Schmidt, JP ; Davies, CJ ; Gollub, J ; Webster, T ; Wong, B ; Zhan, Y ; Auton, A ; Campbell, CL ; Kong, Y ; Marcketta, A ; Gibbs, RA ; Yu, F ; Antunes, L ; Bainbridge, M ; Muzny, D ; Sabo, A ; Huang, Z ; Wang, J ; Coin, LJM ; Fang, L ; Guo, X ; Jin, X ; Li, G ; Li, Q ; Li, Y ; Li, Z ; Lin, H ; Liu, B ; Luo, R ; Shao, H ; Xie, Y ; Ye, C ; Yu, C ; Zhang, F ; Zheng, H ; Zhu, H ; Alkan, C ; Dal, E ; Kahveci, F ; Marth, GT ; Garrison, EP ; Kural, D ; Lee, W-P ; Leong, WF ; Stromberg, M ; Ward, AN ; Wu, J ; Zhang, M ; Daly, MJ ; DePristo, MA ; Handsaker, RE ; Altshuler, DM ; Banks, E ; Bhatia, G ; del Angel, G ; Gabriel, SB ; Genovese, G ; Gupta, N ; Li, H ; Kashin, S ; Lander, ES ; McCarroll, SA ; Nemesh, JC ; Poplin, RE ; Yoon, SC ; Lihm, J ; Makarov, V ; Clark, AG ; Gottipati, S ; Keinan, A ; Rodriguez-Flores, JL ; Korbel, JO ; Rausch, T ; Fritz, MH ; Stuetz, AM ; Flicek, P ; Beal, K ; Clarke, L ; Datta, A ; Herrero, J ; McLaren, WM ; Ritchie, GRS ; Smith, RE ; Zerbino, D ; Zheng-Bradley, X ; Sabeti, PC ; Shlyakhter, I ; Schaffner, SF ; Vitti, J ; Cooper, DN ; Ball, EV ; Stenson, PD ; Bentley, DR ; Barnes, B ; Bauer, M ; Cheetham, RK ; Cox, A ; Eberle, M ; Humphray, S ; Kahn, S ; Murray, L ; Peden, J ; Shaw, R ; Kenny, EE ; Batzer, MA ; Konkel, MK ; Walker, JA ; MacArthur, DG ; Lek, M ; Sudbrak, R ; Amstislavskiy, VS ; Herwig, R ; Mardis, ER ; Ding, L ; Koboldt, DC ; Larson, D ; Ye, K ; Gravel, S ; Swaroop, A ; Chew, E ; Lappalainen, T ; Erlich, Y ; Gymrek, M ; Willems, TF ; Simpson, JT ; Shriver, MD ; Rosenfeld, JA ; Bustamante, CD ; Montgomery, SB ; De La Vega, FM ; Byrnes, JK ; Carroll, AW ; DeGorter, MK ; Lacroute, P ; Maples, BK ; Martin, AR ; Moreno-Estrada, A ; Shringarpure, SS ; Zakharia, F ; Halperin, E ; Baran, Y ; Lee, C ; Cerveira, E ; Hwang, J ; Malhotra, A ; Plewczynski, D ; Radew, K ; Romanovitch, M ; Zhang, C ; Hyland, FCL ; Craig, DW ; Christoforides, A ; Homer, N ; Izatt, T ; Kurdoglu, AA ; Sinari, SA ; Squire, K ; Sherry, ST ; Xiao, C ; Sebat, J ; Antaki, D ; Gujral, M ; Noor, A ; Ye, K ; Burchard, EG ; Hernandez, RD ; Gignoux, CR ; Haussler, D ; Katzman, SJ ; Kent, WJ ; Howie, B ; Ruiz-Linares, A ; Dermitzakis, ET ; Devine, SE ; Goncalo, RA ; Kang, HM ; Kidd, JM ; Blackwell, T ; Caron, S ; Chen, W ; Emery, S ; Fritsche, L ; Fuchsberger, C ; Jun, G ; Li, B ; Lyons, R ; Scheller, C ; Sidore, C ; Song, S ; Sliwerska, E ; Taliun, D ; Tan, A ; Welch, R ; Wing, MK ; Zhan, X ; Awadalla, P ; Hodgkinson, A ; Li, Y ; Shi, X ; Quitadamo, A ; Lunter, G ; McVean, GA ; Marchini, JL ; Myers, S ; Churchhouse, C ; Delaneau, O ; Gupta-Hinch, A ; Kretzschmar, W ; Iqbal, Z ; Mathieson, I ; Menelaou, A ; Rimmer, A ; Xifara, DK ; Oleksyk, TK ; Fu, Y ; Liu, X ; Xiong, M ; Jorde, L ; Witherspoon, D ; Xing, J ; Eichler, EE ; Browning, BL ; Browning, SR ; Hormozdiari, F ; Sudmant, PH ; Khurana, E ; Durbin, RM ; Hurles, ME ; Tyler-Smith, C ; Albers, CA ; Ayub, Q ; Balasubramaniam, S ; Chen, Y ; Colonna, V ; Danecek, P ; Jostins, L ; Keane, TM ; McCarthy, S ; Walter, K ; Xue, Y ; Gerstein, MB ; Abyzov, A ; Balasubramanian, S ; Chen, J ; Clarke, D ; Fu, Y ; Harmanci, AO ; Jin, M ; Lee, D ; Liu, J ; Mu, XJ ; Zhang, J ; Zhang, Y ; Li, Y ; Luo, R ; Zhu, H ; Alkan, C ; Dal, E ; Kahveci, F ; Marth, GT ; Garrison, EP ; Kural, D ; Lee, W-P ; Ward, AN ; Wu, J ; Zhang, M ; McCarroll, SA ; Handsaker, RE ; Altshuler, DM ; Banks, E ; Del Angel, G ; Genovese, G ; Hartl, C ; Li, H ; Kashin, S ; Nemesh, JC ; Shakir, K ; Yoon, SC ; Lihm, J ; Makarov, V ; Degenhardt, J ; Korbel, JO ; Fritz, MH ; Meiers, S ; Raeder, B ; Rausch, T ; Stuetz, AM ; Flicek, P ; Casale, FP ; Clarke, L ; Smith, RE ; Stegle, O ; Zheng-Bradley, X ; Bentley, DR ; Barnes, B ; Cheetham, RK ; Eberle, M ; Humphray, S ; Kahn, S ; Murray, L ; Shaw, R ; Lameijer, E-W ; Batzer, MA ; Konkel, MK ; Walker, JA ; Ding, L ; Hall, I ; Ye, K ; Lacroute, P ; Lee, C ; Cerveira, E ; Malhotra, A ; Hwang, J ; Plewczynski, D ; Radew, K ; Romanovitch, M ; Zhang, C ; Craig, DW ; Homer, N ; Church, D ; Xiao, C ; Sebat, J ; Antaki, D ; Bafna, V ; Michaelson, J ; Ye, K ; Devine, SE ; Gardner, EJ ; Abecasis, GR ; Kidd, JM ; Mills, RE ; Dayama, G ; Emery, S ; Jun, G ; Shi, X ; Quitadamo, A ; Lunter, G ; McVean, GA ; Chen, K ; Fan, X ; Chong, Z ; Chen, T ; Witherspoon, D ; Xing, J ; Eichler, EE ; Chaisson, MJ ; Hormozdiari, F ; Huddleston, J ; Malig, M ; Nelson, BJ ; Sudmant, PH ; Parrish, NF ; Khurana, E ; Hurles, ME ; Blackburne, B ; Lindsay, SJ ; Ning, Z ; Walter, K ; Zhang, Y ; Gerstein, MB ; Abyzov, A ; Chen, J ; Clarke, D ; Lam, H ; Mu, XJ ; Sisu, C ; Zhang, J ; Zhang, Y ; Gibbs, RA ; Yu, F ; Bainbridge, M ; Challis, D ; Evani, US ; Kovar, C ; Lu, J ; Muzny, D ; Nagaswamy, U ; Reid, JG ; Sabo, A ; Yu, J ; Guo, X ; Li, W ; Li, Y ; Wu, R ; Marth, GT ; Garrison, EP ; Leong, WF ; Ward, AN ; del Angel, G ; DePristo, MA ; Gabriel, SB ; Gupta, N ; Hartl, C ; Poplin, RE ; Clark, AG ; Rodriguez-Flores, JL ; Flicek, P ; Clarke, L ; Smith, RE ; Zheng-Bradley, X ; MacArthur, DG ; Mardis, ER ; Fulton, R ; Koboldt, DC ; Gravel, S ; Bustamante, CD ; Craig, DW ; Christoforides, A ; Homer, N ; Izatt, T ; Sherry, ST ; Xiao, C ; Dermitzakis, ET ; Abecasis, GR ; Kang, HM ; McVean, GA ; Gerstein, MB ; Balasubramanian, S ; Habegger, L ; Yu, H ; Flicek, P ; Clarke, L ; Cunningham, F ; Dunham, I ; Zerbino, D ; Zheng-Bradley, X ; Lage, K ; Jespersen, JB ; Horn, H ; Montgomery, SB ; DeGorter, MK ; Khurana, E ; Tyler-Smith, C ; Chen, Y ; Colonna, V ; Xue, Y ; Gerstein, MB ; Balasubramanian, S ; Fu, Y ; Kim, D ; Auton, A ; Marcketta, A ; Desalle, R ; Narechania, A ; Sayres, MAW ; Garrison, EP ; Handsaker, RE ; Kashin, S ; McCarroll, SA ; Rodriguez-Flores, JL ; Flicek, P ; Clarke, L ; Zheng-Bradley, X ; Erlich, Y ; Gymrek, M ; Willems, TF ; Bustamante, CD ; Mendez, FL ; Poznik, GD ; Underhill, PA ; Lee, C ; Cerveira, E ; Malhotra, A ; Romanovitch, M ; Zhang, C ; Abecasis, GR ; Coin, L ; Shao, H ; Mittelman, D ; Tyler-Smith, C ; Ayub, Q ; Banerjee, R ; Cerezo, M ; Chen, Y ; Fitzgerald, T ; Louzada, S ; Massaia, A ; McCarthy, S ; Ritchie, GR ; Xue, Y ; Yang, F ; Gibbs, RA ; Kovar, C ; Kalra, D ; Hale, W ; Muzny, D ; Reid, JG ; Wang, J ; Dan, X ; Guo, X ; Li, G ; Li, Y ; Ye, C ; Zheng, X ; Altshuler, DM ; Flicek, P ; Clarke, L ; Zheng-Bradley, X ; Bentley, DR ; Cox, A ; Humphray, S ; Kahn, S ; Sudbrak, R ; Albrecht, MW ; Lienhard, M ; Larson, D ; Craig, DW ; Izatt, T ; Kurdoglu, AA ; Sherry, ST ; Xiao, C ; Haussler, D ; Abecasis, GR ; McVean, GA ; Durbin, RM ; Balasubramaniam, S ; Keane, TM ; McCarthy, S ; Stalker, J ; Chakravarti, A ; Knoppers, BM ; Abecasis, GR ; Barnes, KC ; Beiswanger, C ; Burchard, EG ; Bustamante, CD ; Cai, H ; Cao, H ; Durbin, RM ; Gerry, NP ; Gharani, N ; Gibbs, RA ; Gignoux, CR ; Gravel, S ; Henn, B ; Jones, D ; Jorde, L ; Kaye, JS ; Keinan, A ; Kent, A ; Kerasidou, A ; Li, Y ; Mathias, R ; McVean, GA ; Moreno-Estrada, A ; Ossorio, PN ; Parker, M ; Resch, AM ; Rotimi, CN ; Royal, CD ; Sandoval, K ; Su, Y ; Sudbrak, R ; Tian, Z ; Tishkoff, S ; Toji, LH ; Tyler-Smith, C ; Via, M ; Wang, Y ; Yang, H ; Yang, L ; Zhu, J ; Bodmer, W ; Bedoya, G ; Ruiz-Linares, A ; Cai, Z ; Gao, Y ; Chu, J ; Peltonen, L ; Garcia-Montero, A ; Orfao, A ; Dutil, J ; Martinez-Cruzado, JC ; Oleksyk, TK ; Barnes, KC ; Mathias, RA ; Hennis, A ; Watson, H ; McKenzie, C ; Qadri, F ; LaRocque, R ; Sabeti, PC ; Zhu, J ; Deng, X ; Sabeti, PC ; Asogun, D ; Folarin, O ; Happi, C ; Omoniwa, O ; Stremlau, M ; Tariyal, R ; Jallow, M ; Joof, FS ; Corrah, T ; Rockett, K ; Kwiatkowski, D ; Kooner, J ; Tran, TH ; Dunstan, SJ ; Nguyen, TH ; Fonnie, R ; Garry, R ; Kanneh, L ; Moses, L ; Sabeti, PC ; Schieffelin, J ; Grant, DS ; Gallo, C ; Poletti, G ; Saleheen, D ; Rasheed, A ; Brook, LD ; Felsenfeld, A ; McEwen, JE ; Vaydylevich, Y ; Green, ED ; Duncanson, A ; Dunn, M ; Schloss, JA ; Wang, J ; Yang, H ; Auton, A ; Brooks, LD ; Durbin, RM ; Garrison, EP ; Kang, HM ; Korbel, JO ; Marchini, JL ; McCarthy, S ; McVean, GA ; Abecasis, GR (NATURE PUBLISHING GROUP, 2015-10-01)

The 1000 Genomes Project set out to provide a comprehensive description of common human genetic variation by applying whole-genome sequencing to a diverse set of individuals from multiple populations. Here we report completion of the project, having reconstructed the genomes of 2,504 individuals from 26 populations using a combination of low-coverage whole-genome sequencing, deep exome sequencing, and dense microarray genotyping. We characterized a broad spectrum of genetic variation, in total over 88 million variants (84.7 million single nucleotide polymorphisms (SNPs), 3.6 million short insertions/deletions (indels), and 60,000 structural variants), all phased onto high-quality haplotypes. This resource includes >99% of SNP variants with a frequency of >1% for a variety of ancestries. We describe the distribution of genetic variation across the global sample, and discuss the implications for common disease studies.
Assessing the Privacy Risks of Data Sharing in Genomics

Heeney, C ; Hawkins, N ; de Vries, J ; Boddington, P ; Kaye, J (KARGER, 2011)

The protection of identity of participants in medical research has traditionally been guaranteed by the maintenance of the confidentiality of health information through mechanisms such as only releasing data in an aggregated form or after identifying variables have been removed. This protection of privacy is regarded as a fundamental principle of research ethics, through which the support of research participants and the public is maintained. Whilst this traditional model was adopted for genetics and genomics research, and was generally considered broadly fit for purpose, we argue that this approach is increasingly untenable in genomics. Privacy risk assessments need to have regard to the whole data environment, not merely the quality of the dataset to be released in isolation. As sources of data proliferate, issues of privacy protection are increasingly problematic in relation to the release of genomic data. However, we conclude that, by paying careful attention to potential pitfalls, scientific funders and researchers can take an important part in attempts to safeguard the public and ensure the continuation of potentially important scientific research.
Using digital technologies to engage with medical research: views of myotonic dystrophy patients in Japan

Coathup, V ; Teare, HJA ; Minari, J ; Yoshizawa, G ; Kaye, J ; Takahashi, MP ; Kato, K (BMC, 2016-08-24)

BACKGROUND: As in other countries, the traditional doctor-patient relationship in the Japanese healthcare system has often been characterised as being of a paternalistic nature. However, in recent years there has been a gradual shift towards a more participatory-patient model in Japan. With advances in technology, the possibility to use digital technologies to improve patient interactions is growing and is in line with changing attitudes in the medical profession and society within Japan and elsewhere. The implementation of an online patient engagement platform is being considered by the Myotonic Dystrophy Registry of Japan. The aim of this exploratory study was to understand patients' views and attitudes to using digital tools in patient registries and engagement with medical research in Japan, prior to implementation of the digital platform. METHODS: We conducted an exploratory, cross-sectional, self-completed questionnaire with a sample of myotonic dystrophy (MD) patients attending an Open Day at Osaka University, Japan. Patients were eligible for inclusion if they were 18 years or older, and were diagnosed with MD. RESULTS: A total of 68 patients and family members attended the Open Day and were invited to participate in the survey. Of those, 59 % submitted a completed questionnaire (n = 40). The survey showed that the majority of patients felt that they were not receiving the information they wanted from their clinicians, which included recent medical research findings and opportunities to participate in clinical trials, and 88 % of patients indicated they would be willing to engage with digital technologies to receive relevant medical information. Patients also expressed an interest in having control over when and how they received this information, as well as being informed of how their data is used and shared with other researchers. CONCLUSION: Overall, the findings from this study suggest that there is scope to develop a digital platform to engage with patients so that they can receive information about medical care and research opportunities. While this study group is a small, self-selecting population, who suffer from a particular condition, the results suggest that there are interested populations within Japan that would appreciate enhanced communication and interaction with healthcare teams.
Data sharing policy design for consortia: challenges for sustainability

Kaye, J ; Hawkins, N (BMC, 2014-01-29)

The field of human genomics has led advances in the sharing of data with a view to facilitating translation of research into innovations for human health. This change in scientific practice has been implemented through new policy developed by many principal investigators, project managers and funders, which has ultimately led to new forms of practice and innovative governance models for data sharing. Here, we examine the development of the governance of data sharing in genomics, and explore some of the key challenges associated with the design and implementation of these policies. We examine how the incremental nature of policy design, the perennial problem of consent, the gridlock caused by multiple and overlapping access systems, the administrative burden and the problems with incentives and acknowledgment all have an impact on the potential for data sharing to be maximized. We conclude by proposing ways in which the scientific community can address these problems, to improve the sustainability of data sharing into the future.
Health-related quality of life and a cost-utility simulation of adults in the UK with osteogenesis imperfecta, X-linked hypophosphatemia and fibrous dysplasia

Forestier-Zhang, L ; Watts, L ; Turner, A ; Teare, H ; Kaye, J ; Barrett, J ; Cooper, C ; Eastell, R ; Wordsworth, P ; Javaid, MK ; Pinedo-Villanueva, R (BMC, 2016-11-28)

BACKGROUND: Health-related quality of life of adults with osteogenesis imperfecta (OI), fibrous dysplasia (FD) and X-linked hypophosphatemia (XLH) remains poorly described. The aim of this study was to describe the HRQoL of adults with osteogenesis imperfecta, fibrous dysplasia and X-linked hypophophataemia and perform a cost-utility simulation to calculate the maximum cost that a health care system would be willing to pay for a hypothetical treatment of a rare bone disease. RESULTS: Participants completed the EQ-5D-5 L questionnaire between September 2014 and March 2016. For the economic simulation, we considered a hypothetical treatment that would be applied to OI participants in the lower tertile of the health utility score. A total of 109 study participants fully completed the EQ-5D-5 L questionnaire (response rate 63%). Pain/discomfort was the most problematic domain for participants with all three diseases (FD 31%, XLH 25%, OI 16%). The economic simulation identified an expected treatment impact of +2.5 QALYs gained per person during the 10-year period, which led to a willing to pay of £14,355 annually for a health care system willing to pay up to £50,000 for each additional QALY gained by an intervention. CONCLUSIONS: This is the first study to quantitatively measure and compare the HRQoL of adults with OI, FD and XLH and the first to use such data to conduct an economic simulation leading to healthcare system willingness-to-pay estimates for treatment of musculoskeletal rare diseases at various cost-effectiveness thresholds.

Melbourne Law School - Research Publications

Permanent URI for this collection

Filters

Date

Author

Type

Settings

Sort By

Results per page

Statistics

Citations

Search Results