Risk of transmissibility from neurodegenerative disease-associated proteins: Experimental knowns and unknowns

David M. Asher; Ermias Belay; Eileen Bigio; Sebastian Brandner; Scott A. Brubaker; Byron Caughey; Brychan Clark; Inger Damon; Marc Diamond; Michelle Freund; Bradley T. Hyman; Mathias Jucker; C. Dirk Keene; Andrew P. Lieberman; Miroslaw MacKiewicz; Thomas J. Montine; Susan Morgello; Creighton Phelps; Jiri Safar; Julie A. Schneider; Lawrence B. Schonberger; Christina Sigurdson; Nina Silverberg; John Q. Trojanowski; Matthew P. Frosch

doi:10.1093/JNEN/NLAA109

Risk of transmissibility from neurodegenerative disease-associated proteins: Experimental knowns and unknowns

David M. Asher, Ermias Belay, Eileen Bigio, Sebastian Brandner, Scott A. Brubaker, Byron Caughey, Brychan Clark, Inger Damon, Marc Diamond, Michelle Freund, Bradley T. Hyman, Mathias Jucker, C. Dirk Keene, Andrew P. Lieberman, Miroslaw MacKiewicz, Thomas J. Montine, Susan Morgello, Creighton Phelps, Jiri Safar, Julie A. SchneiderLawrence B. Schonberger, Christina Sigurdson, Nina Silverberg, John Q. Trojanowski, Matthew P. Frosch

Research output: Contribution to journal › Review article › peer-review

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Abstract

Recent studies in animal models demonstrate that certain misfolded proteins associated with neurodegenerative diseases can support templated misfolding of cognate native proteins, to propagate across neural systems, and to therefore have some of the properties of classical prion diseases like Creutzfeldt-Jakob disease. The National Institute of Aging convened a meeting to discuss the implications of these observations for research priorities. A summary of the discussion is presented here, with a focus on limitations of current knowledge, highlighting areas that appear to require further investigation in order to guide scientific practice while minimizing potential exposure or risk in the laboratory setting. The committee concluded that, based on all currently available data, although neurodegenerative disease-associated aggregates of several different non-prion proteins can be propagated from humans to experimental animals, there is currently insufficient evidence to suggest more than a negligible risk, if any, of a direct infectious etiology for the human neurodegenerative disorders defined in part by these proteins. Given the importance of this question, the potential for noninvasive human transmission of proteopathic disorders is deserving of further investigation.

Original language	English (US)
Pages (from-to)	1141-1146
Number of pages	6
Journal	Journal of neuropathology and experimental neurology
Volume	79
Issue number	11
DOIs	https://doi.org/10.1093/JNEN/NLAA109
State	Published - 2021

ASJC Scopus subject areas

General Medicine

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Asher, D. M., Belay, E., Bigio, E., Brandner, S., Brubaker, S. A., Caughey, B., Clark, B., Damon, I., Diamond, M., Freund, M., Hyman, B. T., Jucker, M., Keene, C. D., Lieberman, A. P., MacKiewicz, M., Montine, T. J., Morgello, S., Phelps, C., Safar, J., ... Frosch, M. P. (2021). Risk of transmissibility from neurodegenerative disease-associated proteins: Experimental knowns and unknowns. Journal of neuropathology and experimental neurology, 79(11), 1141-1146. https://doi.org/10.1093/JNEN/NLAA109

Asher, DM, Belay, E, Bigio, E, Brandner, S, Brubaker, SA, Caughey, B, Clark, B, Damon, I, Diamond, M, Freund, M, Hyman, BT, Jucker, M, Keene, CD, Lieberman, AP, MacKiewicz, M, Montine, TJ, Morgello, S, Phelps, C, Safar, J, Schneider, JA, Schonberger, LB, Sigurdson, C, Silverberg, N, Trojanowski, JQ & Frosch, MP 2021, 'Risk of transmissibility from neurodegenerative disease-associated proteins: Experimental knowns and unknowns', Journal of neuropathology and experimental neurology, vol. 79, no. 11, pp. 1141-1146. https://doi.org/10.1093/JNEN/NLAA109

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title = "Risk of transmissibility from neurodegenerative disease-associated proteins: Experimental knowns and unknowns",

abstract = "Recent studies in animal models demonstrate that certain misfolded proteins associated with neurodegenerative diseases can support templated misfolding of cognate native proteins, to propagate across neural systems, and to therefore have some of the properties of classical prion diseases like Creutzfeldt-Jakob disease. The National Institute of Aging convened a meeting to discuss the implications of these observations for research priorities. A summary of the discussion is presented here, with a focus on limitations of current knowledge, highlighting areas that appear to require further investigation in order to guide scientific practice while minimizing potential exposure or risk in the laboratory setting. The committee concluded that, based on all currently available data, although neurodegenerative disease-associated aggregates of several different non-prion proteins can be propagated from humans to experimental animals, there is currently insufficient evidence to suggest more than a negligible risk, if any, of a direct infectious etiology for the human neurodegenerative disorders defined in part by these proteins. Given the importance of this question, the potential for noninvasive human transmission of proteopathic disorders is deserving of further investigation.",

author = "Asher, {David M.} and Ermias Belay and Eileen Bigio and Sebastian Brandner and Brubaker, {Scott A.} and Byron Caughey and Brychan Clark and Inger Damon and Marc Diamond and Michelle Freund and Hyman, {Bradley T.} and Mathias Jucker and Keene, {C. Dirk} and Lieberman, {Andrew P.} and Miroslaw MacKiewicz and Montine, {Thomas J.} and Susan Morgello and Creighton Phelps and Jiri Safar and Schneider, {Julie A.} and Schonberger, {Lawrence B.} and Christina Sigurdson and Nina Silverberg and Trojanowski, {John Q.} and Frosch, {Matthew P.}",

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doi = "10.1093/JNEN/NLAA109",

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AU - Asher, David M.

AU - Belay, Ermias

AU - Bigio, Eileen

AU - Brandner, Sebastian

AU - Brubaker, Scott A.

AU - Caughey, Byron

AU - Clark, Brychan

AU - Damon, Inger

AU - Diamond, Marc

AU - Freund, Michelle

AU - Hyman, Bradley T.

AU - Jucker, Mathias

AU - Keene, C. Dirk

AU - Lieberman, Andrew P.

AU - MacKiewicz, Miroslaw

AU - Montine, Thomas J.

AU - Morgello, Susan

AU - Phelps, Creighton

AU - Safar, Jiri

AU - Schneider, Julie A.

AU - Schonberger, Lawrence B.

AU - Sigurdson, Christina

AU - Silverberg, Nina

AU - Trojanowski, John Q.

AU - Frosch, Matthew P.

PY - 2021

Y1 - 2021

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AB - Recent studies in animal models demonstrate that certain misfolded proteins associated with neurodegenerative diseases can support templated misfolding of cognate native proteins, to propagate across neural systems, and to therefore have some of the properties of classical prion diseases like Creutzfeldt-Jakob disease. The National Institute of Aging convened a meeting to discuss the implications of these observations for research priorities. A summary of the discussion is presented here, with a focus on limitations of current knowledge, highlighting areas that appear to require further investigation in order to guide scientific practice while minimizing potential exposure or risk in the laboratory setting. The committee concluded that, based on all currently available data, although neurodegenerative disease-associated aggregates of several different non-prion proteins can be propagated from humans to experimental animals, there is currently insufficient evidence to suggest more than a negligible risk, if any, of a direct infectious etiology for the human neurodegenerative disorders defined in part by these proteins. Given the importance of this question, the potential for noninvasive human transmission of proteopathic disorders is deserving of further investigation.

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Risk of transmissibility from neurodegenerative disease-associated proteins: Experimental knowns and unknowns

Abstract

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