Disease modification and biomarker development in Parkinson disease: Revision or reconstruction?

Alberto J. Espay; Lorraine V. Kalia; Ziv Gan-Or; Caroline H. Williams-Gray; Philippe L. Bedard; Steven M. Rowe; Francesca Morgante; Alfonso Fasano; Benjamin Stecher; Marcelo A. Kauffman; Matthew J. Farrer; Chris S. Coffey; Michael A. Schwarzschild; Todd Sherer; Ronald B. Postuma; Antonio P. Strafella; Andrew B. Singleton; Roger A. Barker; Karl Kieburtz; C. Warren Olanow; Andres Lozano; Jeffrey H. Kordower; Jesse M. Cedarbaum; Patrik Brundin; David G. Standaert; Anthony E. Lang

doi:10.1212/WNL.0000000000009107

Disease modification and biomarker development in Parkinson disease: Revision or reconstruction?

Alberto J. Espay, Lorraine V. Kalia, Ziv Gan-Or, Caroline H. Williams-Gray, Philippe L. Bedard, Steven M. Rowe, Francesca Morgante, Alfonso Fasano, Benjamin Stecher, Marcelo A. Kauffman, Matthew J. Farrer, Chris S. Coffey, Michael A. Schwarzschild, Todd Sherer, Ronald B. Postuma, Antonio P. Strafella, Andrew B. Singleton, Roger A. Barker, Karl Kieburtz, C. Warren OlanowAndres Lozano, Jeffrey H. Kordower, Jesse M. Cedarbaum, Patrik Brundin, David G. Standaert, Anthony E. Lang

Research output: Contribution to journal › Article › peer-review

83 Scopus citations

Abstract

A fundamental question in advancing Parkinson disease (PD) research is whether it represents one disorder or many. Does each genetic PD inform a common pathobiology or represent a unique entity? Do the similarities between genetic and idiopathic forms of PD outweigh the differences? If aggregates of a-synuclein in Lewy bodies and Lewy neurites are present in most (a-synucleinopathies), are they also etiopathogenically significant in each (a-synuclein pathogenesis)? Does it matter that postmortem studies in PD have demonstrated that mixed protein-aggregate pathology is the rule and pure a-synucleinopathy the exception? Should we continue to pursue convergent biomarkers that are representative of the diverse whole of PD or subtype-specific, divergent biomarkers, present in some but absent in most? Have clinical trials that failed to demonstrate efficacy of putative disease-modifying interventions been true failures (shortcomings of the hypotheses, which should be rejected) or false failures (shortcomings of the trials; hypotheses should be preserved)? Each of these questions reflects a nosologic struggle between the lumper's clinicopathologic model that embraces heterogeneity of one disease and the splitter's focus on a pathobiology-specific set of diseases. Most important, even if PD is not a single disorder, can advances in biomarkers and disease modification be revised to concentrate on pathologic commonalities in large, clinically defined populations? Or should our efforts be reconstructed to focus on smaller subgroups of patients, distinguished by well-defined molecular characteristics, regardless of their phenotypic classification? Will our clinical trial constructs be revised to target larger and earlier, possibly even prodromal, cohorts? Or should our trials efforts be reconstructed to target smaller but molecularly defined presymptomatic or postsymptomatic cohorts? At the Krembil Knowledge Gaps in Parkinson's Disease Symposium, the tentative answers to these questions were discussed, informed by the failures and successes of the fields of breast cancer and cystic fibrosis.

Original language	English (US)
Pages (from-to)	481-494
Number of pages	14
Journal	Neurology
Volume	94
Issue number	11
DOIs	https://doi.org/10.1212/WNL.0000000000009107
State	Published - Mar 17 2020
Externally published	Yes

ASJC Scopus subject areas

Clinical Neurology

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10.1212/WNL.0000000000009107

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Espay, A. J., Kalia, L. V., Gan-Or, Z., Williams-Gray, C. H., Bedard, P. L., Rowe, S. M., Morgante, F., Fasano, A., Stecher, B., Kauffman, M. A., Farrer, M. J., Coffey, C. S., Schwarzschild, M. A., Sherer, T., Postuma, R. B., Strafella, A. P., Singleton, A. B., Barker, R. A., Kieburtz, K., ... Lang, A. E. (2020). Disease modification and biomarker development in Parkinson disease: Revision or reconstruction? Neurology, 94(11), 481-494. https://doi.org/10.1212/WNL.0000000000009107

Espay, AJ, Kalia, LV, Gan-Or, Z, Williams-Gray, CH, Bedard, PL, Rowe, SM, Morgante, F, Fasano, A, Stecher, B, Kauffman, MA, Farrer, MJ, Coffey, CS, Schwarzschild, MA, Sherer, T, Postuma, RB, Strafella, AP, Singleton, AB, Barker, RA, Kieburtz, K, Olanow, CW, Lozano, A, Kordower, JH, Cedarbaum, JM, Brundin, P, Standaert, DG & Lang, AE 2020, 'Disease modification and biomarker development in Parkinson disease: Revision or reconstruction?', Neurology, vol. 94, no. 11, pp. 481-494. https://doi.org/10.1212/WNL.0000000000009107

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title = "Disease modification and biomarker development in Parkinson disease: Revision or reconstruction?",

abstract = "A fundamental question in advancing Parkinson disease (PD) research is whether it represents one disorder or many. Does each genetic PD inform a common pathobiology or represent a unique entity? Do the similarities between genetic and idiopathic forms of PD outweigh the differences? If aggregates of a-synuclein in Lewy bodies and Lewy neurites are present in most (a-synucleinopathies), are they also etiopathogenically significant in each (a-synuclein pathogenesis)? Does it matter that postmortem studies in PD have demonstrated that mixed protein-aggregate pathology is the rule and pure a-synucleinopathy the exception? Should we continue to pursue convergent biomarkers that are representative of the diverse whole of PD or subtype-specific, divergent biomarkers, present in some but absent in most? Have clinical trials that failed to demonstrate efficacy of putative disease-modifying interventions been true failures (shortcomings of the hypotheses, which should be rejected) or false failures (shortcomings of the trials; hypotheses should be preserved)? Each of these questions reflects a nosologic struggle between the lumper's clinicopathologic model that embraces heterogeneity of one disease and the splitter's focus on a pathobiology-specific set of diseases. Most important, even if PD is not a single disorder, can advances in biomarkers and disease modification be revised to concentrate on pathologic commonalities in large, clinically defined populations? Or should our efforts be reconstructed to focus on smaller subgroups of patients, distinguished by well-defined molecular characteristics, regardless of their phenotypic classification? Will our clinical trial constructs be revised to target larger and earlier, possibly even prodromal, cohorts? Or should our trials efforts be reconstructed to target smaller but molecularly defined presymptomatic or postsymptomatic cohorts? At the Krembil Knowledge Gaps in Parkinson's Disease Symposium, the tentative answers to these questions were discussed, informed by the failures and successes of the fields of breast cancer and cystic fibrosis.",

author = "Espay, {Alberto J.} and Kalia, {Lorraine V.} and Ziv Gan-Or and Williams-Gray, {Caroline H.} and Bedard, {Philippe L.} and Rowe, {Steven M.} and Francesca Morgante and Alfonso Fasano and Benjamin Stecher and Kauffman, {Marcelo A.} and Farrer, {Matthew J.} and Coffey, {Chris S.} and Schwarzschild, {Michael A.} and Todd Sherer and Postuma, {Ronald B.} and Strafella, {Antonio P.} and Singleton, {Andrew B.} and Barker, {Roger A.} and Karl Kieburtz and Olanow, {C. Warren} and Andres Lozano and Kordower, {Jeffrey H.} and Cedarbaum, {Jesse M.} and Patrik Brundin and Standaert, {David G.} and Lang, {Anthony E.}",

note = "Funding Information: Major support for the Revision vs Reconstruction meeting leading to this manuscript was provided by The Krembil Foundation, the Ronald Kimel Foundation Trust, the Parkinson{\textquoteright}s Foundation, the International Parkinson and Movement Disorder Society, and the American Parkinson Disease Association. Additional support was provided by the International Parkinson and Movement Disorders Society, the Parkinson Foundation, and the following pharmaceutical companies: Sunovion, UCB, Valeo Pharma, Acadia Pharma-ceuXcals Inc, Medtronic of Canada Ltd, ProtoKinetics, Theravance Biopharma US, Inc, and Neurocrine Bioscience. The Revision vs Reconstruction meeting was endorsed by the Michael J. Fox Foundation and the American Parkinson Disease Association. C.H. Williams-Gray holds a Research Councils UK/UK Research Innovation Research Innovation Fellowship awarded by the Medical Research Council (MR/R007446/1); R.A. Barker is supported by the Wellcome Trust/Medical Research Council Stem Cell Institute (203151/Z/16/Z). Publisher Copyright: {\textcopyright} American Academy of Neurology.",

year = "2020",

month = mar,

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doi = "10.1212/WNL.0000000000009107",

language = "English (US)",

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T1 - Disease modification and biomarker development in Parkinson disease

T2 - Revision or reconstruction?

AU - Espay, Alberto J.

AU - Kalia, Lorraine V.

AU - Gan-Or, Ziv

AU - Williams-Gray, Caroline H.

AU - Bedard, Philippe L.

AU - Rowe, Steven M.

AU - Morgante, Francesca

AU - Fasano, Alfonso

AU - Stecher, Benjamin

AU - Kauffman, Marcelo A.

AU - Farrer, Matthew J.

AU - Coffey, Chris S.

AU - Schwarzschild, Michael A.

AU - Sherer, Todd

AU - Postuma, Ronald B.

AU - Strafella, Antonio P.

AU - Singleton, Andrew B.

AU - Barker, Roger A.

AU - Kieburtz, Karl

AU - Olanow, C. Warren

AU - Lozano, Andres

AU - Kordower, Jeffrey H.

AU - Cedarbaum, Jesse M.

AU - Brundin, Patrik

AU - Standaert, David G.

AU - Lang, Anthony E.

N1 - Funding Information: Major support for the Revision vs Reconstruction meeting leading to this manuscript was provided by The Krembil Foundation, the Ronald Kimel Foundation Trust, the Parkinson’s Foundation, the International Parkinson and Movement Disorder Society, and the American Parkinson Disease Association. Additional support was provided by the International Parkinson and Movement Disorders Society, the Parkinson Foundation, and the following pharmaceutical companies: Sunovion, UCB, Valeo Pharma, Acadia Pharma-ceuXcals Inc, Medtronic of Canada Ltd, ProtoKinetics, Theravance Biopharma US, Inc, and Neurocrine Bioscience. The Revision vs Reconstruction meeting was endorsed by the Michael J. Fox Foundation and the American Parkinson Disease Association. C.H. Williams-Gray holds a Research Councils UK/UK Research Innovation Research Innovation Fellowship awarded by the Medical Research Council (MR/R007446/1); R.A. Barker is supported by the Wellcome Trust/Medical Research Council Stem Cell Institute (203151/Z/16/Z). Publisher Copyright: © American Academy of Neurology.

PY - 2020/3/17

Y1 - 2020/3/17

N2 - A fundamental question in advancing Parkinson disease (PD) research is whether it represents one disorder or many. Does each genetic PD inform a common pathobiology or represent a unique entity? Do the similarities between genetic and idiopathic forms of PD outweigh the differences? If aggregates of a-synuclein in Lewy bodies and Lewy neurites are present in most (a-synucleinopathies), are they also etiopathogenically significant in each (a-synuclein pathogenesis)? Does it matter that postmortem studies in PD have demonstrated that mixed protein-aggregate pathology is the rule and pure a-synucleinopathy the exception? Should we continue to pursue convergent biomarkers that are representative of the diverse whole of PD or subtype-specific, divergent biomarkers, present in some but absent in most? Have clinical trials that failed to demonstrate efficacy of putative disease-modifying interventions been true failures (shortcomings of the hypotheses, which should be rejected) or false failures (shortcomings of the trials; hypotheses should be preserved)? Each of these questions reflects a nosologic struggle between the lumper's clinicopathologic model that embraces heterogeneity of one disease and the splitter's focus on a pathobiology-specific set of diseases. Most important, even if PD is not a single disorder, can advances in biomarkers and disease modification be revised to concentrate on pathologic commonalities in large, clinically defined populations? Or should our efforts be reconstructed to focus on smaller subgroups of patients, distinguished by well-defined molecular characteristics, regardless of their phenotypic classification? Will our clinical trial constructs be revised to target larger and earlier, possibly even prodromal, cohorts? Or should our trials efforts be reconstructed to target smaller but molecularly defined presymptomatic or postsymptomatic cohorts? At the Krembil Knowledge Gaps in Parkinson's Disease Symposium, the tentative answers to these questions were discussed, informed by the failures and successes of the fields of breast cancer and cystic fibrosis.

AB - A fundamental question in advancing Parkinson disease (PD) research is whether it represents one disorder or many. Does each genetic PD inform a common pathobiology or represent a unique entity? Do the similarities between genetic and idiopathic forms of PD outweigh the differences? If aggregates of a-synuclein in Lewy bodies and Lewy neurites are present in most (a-synucleinopathies), are they also etiopathogenically significant in each (a-synuclein pathogenesis)? Does it matter that postmortem studies in PD have demonstrated that mixed protein-aggregate pathology is the rule and pure a-synucleinopathy the exception? Should we continue to pursue convergent biomarkers that are representative of the diverse whole of PD or subtype-specific, divergent biomarkers, present in some but absent in most? Have clinical trials that failed to demonstrate efficacy of putative disease-modifying interventions been true failures (shortcomings of the hypotheses, which should be rejected) or false failures (shortcomings of the trials; hypotheses should be preserved)? Each of these questions reflects a nosologic struggle between the lumper's clinicopathologic model that embraces heterogeneity of one disease and the splitter's focus on a pathobiology-specific set of diseases. Most important, even if PD is not a single disorder, can advances in biomarkers and disease modification be revised to concentrate on pathologic commonalities in large, clinically defined populations? Or should our efforts be reconstructed to focus on smaller subgroups of patients, distinguished by well-defined molecular characteristics, regardless of their phenotypic classification? Will our clinical trial constructs be revised to target larger and earlier, possibly even prodromal, cohorts? Or should our trials efforts be reconstructed to target smaller but molecularly defined presymptomatic or postsymptomatic cohorts? At the Krembil Knowledge Gaps in Parkinson's Disease Symposium, the tentative answers to these questions were discussed, informed by the failures and successes of the fields of breast cancer and cystic fibrosis.

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Disease modification and biomarker development in Parkinson disease: Revision or reconstruction?

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