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      Inclusion and exclusion in the globalisation of genomics; the case of rare genetic disease in Brazil

      1 , 2
      Anthropology & Medicine
      Informa UK Limited

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          Abstract

          ABSTRACT Within the context of a globalising agenda for genetic research where ‘global health’ is increasingly seen as necessarily informed by and having to account for genomics, the focus on rare genetic diseases is becoming prominent. Drawing from ethnographic research carried out separately by both authors in Brazil, this paper examines how an emerging focus on two different arenas of rare genetic disease, cancer genetics and a class of degenerative neurological diseases known as Ataxias, is subject to and a product of the dynamics of inclusion and exclusion as this concerns participation in research and access to health care. It examines how in these different cases ‘rarenesss’ has been diversely situated and differently politicised and how clinicians, patients and their families grapple with the slippery boundaries between research, rights to health and the limits of care, therapy or prevention. It illustrates how attention to rare genetic disease in Brazil emerges at the intersection of a particular history of genetic research and public health infrastructure, densely complicated feedback loops between clinical care and research, patient mobilisation around the ‘judicialisation’ of health and recent state legislation regarding rare disease in Brazil. It highlights the relevance of local configurations in the way rare genetic disease is being made relevant for and by different communities.

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          Genomics for the world.

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            Germ line p53 mutations in a familial syndrome of breast cancer, sarcomas, and other neoplasms.

            Familial cancer syndromes have helped to define the role of tumor suppressor genes in the development of cancer. The dominantly inherited Li-Fraumeni syndrome (LFS) is of particular interest because of the diversity of childhood and adult tumors that occur in affected individuals. The rarity and high mortality of LFS precluded formal linkage analysis. The alternative approach was to select the most plausible candidate gene. The tumor suppressor gene, p53, was studied because of previous indications that this gene is inactivated in the sporadic (nonfamilial) forms of most cancers that are associated with LFS. Germ line p53 mutations have been detected in all five LFS families analyzed. These mutations do not produce amounts of mutant p53 protein expected to exert a trans-dominant loss of function effect on wild-type p53 protein. The frequency of germ line p53 mutations can now be examined in additional families with LFS, and in other cancer patients and families with clinical features that might be attributed to the mutation.
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                Author and article information

                Contributors
                (View ORCID Profile)
                Journal
                Anthropology & Medicine
                Anthropology & Medicine
                Informa UK Limited
                1364-8470
                1469-2910
                March 13 2018
                January 02 2018
                March 13 2018
                January 02 2018
                : 25
                : 1
                : 11-29
                Affiliations
                [1 ] Department of Anthropology, University College London, London, UK
                [2 ] Department of Anthropology, Universidade do Estado do Rio de Janeiro, Rio de Janeiro, Brazil
                Article
                10.1080/13648470.2017.1381230
                98d6683a-567d-4a6a-a781-0cdc093d54dd
                © 2018

                http://creativecommons.org/licenses/by/4.0

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