Temporal order of clinical and biomarker changes in familial frontotemporal dementia

Frontotemporal Dementia Prevention Initiative (FPI) Investigators; ALLFTD Investigators; GENFI investigators; Carolina Maruta; Frederico Simões do Couto; Maria Rosario Almeida

doi:10.1038/s41591-022-01942-9

Temporal order of clinical and biomarker changes in familial frontotemporal dementia

Frontotemporal Dementia Prevention Initiative (FPI) Investigators, ALLFTD Investigators, GENFI investigators, Carolina Maruta, Frederico Simões do Couto, Maria Rosario Almeida

Resultado de pesquisa › revisão de pares

60 Citações (Scopus)

7 Transferências (Pure)

Resumo

Unlike familial Alzheimer’s disease, we have been unable to accurately predict symptom onset in presymptomatic familial frontotemporal dementia (f-FTD) mutation carriers, which is a major hurdle to designing disease prevention trials. We developed multimodal models for f-FTD disease progression and estimated clinical trial sample sizes in C9orf72, GRN and MAPT mutation carriers. Models included longitudinal clinical and neuropsychological scores, regional brain volumes and plasma neurofilament light chain (NfL) in 796 carriers and 412 noncarrier controls. We found that the temporal ordering of clinical and biomarker progression differed by genotype. In prevention-trial simulations using model-based patient selection, atrophy and NfL were the best endpoints, whereas clinical measures were potential endpoints in early symptomatic trials. f-FTD prevention trials are feasible but will likely require global recruitment efforts. These disease progression models will facilitate the planning of f-FTD clinical trials, including the selection of optimal endpoints and enrollment criteria to maximize power to detect treatment effects.

Idioma original	English
Páginas (de-até)	2194-2206
Número de páginas	13
Revista	Nature Medicine
Volume	28
Número de emissão	10
DOIs	https://doi.org/10.1038/s41591-022-01942-9
Estado da publicação	Publicado - out. 2022

Acesso ao documento

10.1038/s41591-022-01942-9

69358952Accepted author manuscript, 14,4 MBLicença:

http://hdl.handle.net/10400.14/41156Licença:

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CIIS: Centro de Investigação Interdisciplinar em Saúde
Barros, M. (PI), Rosa, N. (Investigador), Correia, M. J. (Investigador), Caldas, A. C. (Investigador), Amado, J. C. (Investigador), Figueiredo, A. S. (Investigador), Esteves, A. C. (Investigador), Mineiro, A. (Investigador), Abreu, A. M. (Investigador), Duarte, A. S. (Investigador), Almeida, S. F. (Investigador), Correia, A. (Investigador), Moura, A. (Investigador), Almeida, A. (Investigador), Araújo, B. (Investigador), Moura-Netto, C. (Investigador), Ferrito, C. (Investigador), Pais-Vieira, C. (Investigador), Festas, C. (Investigador), Marques-Vieira, C. (Investigador), Catré, D. (Investigador), Nunes, E. (Investigador), Jesus, É. (Investigador), Ribeiro, F. (Investigador), Rosário, F. (Investigador), Fernandes, G. (Investigador), Rato, J. R. (Bolseiro), Salgado, J. R. (Investigador), Neves-Amado, J. (Investigador), Amendoeira, J. (Investigador), Sá, L. (Investigador), Capelas, M. L. (Investigador), Vieira, M. M. (Investigador), Nunes, M. V. S. (Investigador), Cardoso, M. (Investigador), Veiga, N. J. (Investigador), Fonseca, P. (Investigador), Correia, P. N. (Investigador), Couto, P. (Investigador), Pontífice-Sousa, P. (Investigador), Ravasco, P. (Investigador), Carvalho, P. V. D. (Investigador), Alves, P. (Investigador), Melo, P. (Investigador), Silva, R. (Investigador), Canaipa, R. (Investigador), Noites, R. (Investigador), Rio, R. (Investigador), Almeida, S. (Investigador), Deodato, S. (Investigador), Caldeira, S. (Investigador), Silva, S. (Investigador), Borges, T. (Investigador), Silva, V. (Investigador), Charepe, Z. (Investigador), Rodrigues-Pires, F. (Voluntário), Veludo, F. (Investigador), Carmo, H. (Bolseiro), Romeiro, J. (Estudante), Melo, M. (Investigador), Braga, M. (Investigador), Amaral, T. (Investigador), Moreira, M. A. (Investigador), Guerra, N. (Estudante), Santos, P. (Investigador), Paço, S. (Estudante), Lynce, S. (Bolseiro), Miguel, S. (Estudante), Costa, T. (Investigador), Silva-Neves, V. (Investigador), Silva, A. (Investigador), Carvalho, A. R. (Investigador), Almeida, B. (Investigador), Figueiredo, C. (Investigador), Esteves, E. (Bolseiro), Araújo, F. M. (Investigador), Garcia, J. G. (Investigador), Santos, L. (Investigador), Santos, N. M. D. (Investigador), Lopes, P. (Investigador), Bornes, R. (Investigador), Silva, R. (Investigador), Costa, S. (Investigador), Silva, S. M. (Investigador), Marques, T. (Investigador), Almeida, A. (Investigador), Santos, M. (Bolseiro), Santos, P. (Investigador), Miguel, S. (Investigador), Mendes, K. (Investigador), Gomes, A. P. (Investigador), Henriques, J. M. P. (Investigador), Costa, H. A. F. P. (Investigador) & Ribeiro, P. (Investigador)
Fundação para a Ciência e a Tecnologia
1/01/20 → 31/12/24
Projeto

Citação

@article{314dd221402a4dd3bee7980ab65aa06d,

title = "Temporal order of clinical and biomarker changes in familial frontotemporal dementia",

abstract = "Unlike familial Alzheimer{\textquoteright}s disease, we have been unable to accurately predict symptom onset in presymptomatic familial frontotemporal dementia (f-FTD) mutation carriers, which is a major hurdle to designing disease prevention trials. We developed multimodal models for f-FTD disease progression and estimated clinical trial sample sizes in C9orf72, GRN and MAPT mutation carriers. Models included longitudinal clinical and neuropsychological scores, regional brain volumes and plasma neurofilament light chain (NfL) in 796 carriers and 412 noncarrier controls. We found that the temporal ordering of clinical and biomarker progression differed by genotype. In prevention-trial simulations using model-based patient selection, atrophy and NfL were the best endpoints, whereas clinical measures were potential endpoints in early symptomatic trials. f-FTD prevention trials are feasible but will likely require global recruitment efforts. These disease progression models will facilitate the planning of f-FTD clinical trials, including the selection of optimal endpoints and enrollment criteria to maximize power to detect treatment effects.",

author = "{Frontotemporal Dementia Prevention Initiative (FPI) Investigators} and {ALLFTD Investigators} and {GENFI investigators} and Staffaroni, {Adam M.} and Melanie Quintana and Barbara Wendelberger and Heuer, {Hilary W.} and Russell, {Lucy L.} and Yann Cobigo and Amy Wolf and Goh, {Sheng Yang Matt} and Leonard Petrucelli and Gendron, {Tania F.} and Carolin Heller and Clark, {Annie L.} and Taylor, {Jack Carson} and Amy Wise and Elise Ong and Leah Forsberg and Danielle Brushaber and Rojas, {Julio C.} and Lawren VandeVrede and Peter Ljubenkov and Joel Kramer and Casaletto, {Kaitlin B.} and Brian Appleby and Yvette Bordelon and Hugo Botha and Dickerson, {Bradford C.} and Kimiko Domoto-Reilly and Fields, {Julie A.} and Tatiana Foroud and Ralitza Gavrilova and Daniel Geschwind and Nupur Ghoshal and Jill Goldman and Jonathon Graff-Radford and Neill Graff-Radford and Murray Grossman and Hall, {Matthew G.H.} and Hsiung, {Ging Yuek} and Huey, {Edward D.} and David Irwin and Jones, {David T.} and Kejal Kantarci and Daniel Kaufer and David Knopman and Walter Kremers and Lago, {Argentina Lario} and Lapid, {Maria I.} and Carolina Maruta and Couto, {Frederico Sim{\~o}es do} and Almeida, {Maria Rosario}",

note = "Publisher Copyright: {\textcopyright} 2022, The Author(s), under exclusive licence to Springer Nature America, Inc.",

year = "2022",

month = oct,

doi = "10.1038/s41591-022-01942-9",

language = "English",

volume = "28",

pages = "2194--2206",

journal = "Nature Medicine",

issn = "1078-8956",

publisher = "Nature Research",

number = "10",

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T1 - Temporal order of clinical and biomarker changes in familial frontotemporal dementia

AU - Frontotemporal Dementia Prevention Initiative (FPI) Investigators

AU - ALLFTD Investigators

AU - GENFI investigators

AU - Staffaroni, Adam M.

AU - Quintana, Melanie

AU - Wendelberger, Barbara

AU - Heuer, Hilary W.

AU - Russell, Lucy L.

AU - Cobigo, Yann

AU - Wolf, Amy

AU - Goh, Sheng Yang Matt

AU - Petrucelli, Leonard

AU - Gendron, Tania F.

AU - Heller, Carolin

AU - Clark, Annie L.

AU - Taylor, Jack Carson

AU - Wise, Amy

AU - Ong, Elise

AU - Forsberg, Leah

AU - Brushaber, Danielle

AU - Rojas, Julio C.

AU - VandeVrede, Lawren

AU - Ljubenkov, Peter

AU - Kramer, Joel

AU - Casaletto, Kaitlin B.

AU - Appleby, Brian

AU - Bordelon, Yvette

AU - Botha, Hugo

AU - Dickerson, Bradford C.

AU - Domoto-Reilly, Kimiko

AU - Fields, Julie A.

AU - Foroud, Tatiana

AU - Gavrilova, Ralitza

AU - Geschwind, Daniel

AU - Ghoshal, Nupur

AU - Goldman, Jill

AU - Graff-Radford, Jonathon

AU - Graff-Radford, Neill

AU - Grossman, Murray

AU - Hall, Matthew G.H.

AU - Hsiung, Ging Yuek

AU - Huey, Edward D.

AU - Irwin, David

AU - Jones, David T.

AU - Kantarci, Kejal

AU - Kaufer, Daniel

AU - Knopman, David

AU - Kremers, Walter

AU - Lago, Argentina Lario

AU - Lapid, Maria I.

AU - Maruta, Carolina

AU - Couto, Frederico Simões do

AU - Almeida, Maria Rosario

PY - 2022/10

Y1 - 2022/10

N2 - Unlike familial Alzheimer’s disease, we have been unable to accurately predict symptom onset in presymptomatic familial frontotemporal dementia (f-FTD) mutation carriers, which is a major hurdle to designing disease prevention trials. We developed multimodal models for f-FTD disease progression and estimated clinical trial sample sizes in C9orf72, GRN and MAPT mutation carriers. Models included longitudinal clinical and neuropsychological scores, regional brain volumes and plasma neurofilament light chain (NfL) in 796 carriers and 412 noncarrier controls. We found that the temporal ordering of clinical and biomarker progression differed by genotype. In prevention-trial simulations using model-based patient selection, atrophy and NfL were the best endpoints, whereas clinical measures were potential endpoints in early symptomatic trials. f-FTD prevention trials are feasible but will likely require global recruitment efforts. These disease progression models will facilitate the planning of f-FTD clinical trials, including the selection of optimal endpoints and enrollment criteria to maximize power to detect treatment effects.

AB - Unlike familial Alzheimer’s disease, we have been unable to accurately predict symptom onset in presymptomatic familial frontotemporal dementia (f-FTD) mutation carriers, which is a major hurdle to designing disease prevention trials. We developed multimodal models for f-FTD disease progression and estimated clinical trial sample sizes in C9orf72, GRN and MAPT mutation carriers. Models included longitudinal clinical and neuropsychological scores, regional brain volumes and plasma neurofilament light chain (NfL) in 796 carriers and 412 noncarrier controls. We found that the temporal ordering of clinical and biomarker progression differed by genotype. In prevention-trial simulations using model-based patient selection, atrophy and NfL were the best endpoints, whereas clinical measures were potential endpoints in early symptomatic trials. f-FTD prevention trials are feasible but will likely require global recruitment efforts. These disease progression models will facilitate the planning of f-FTD clinical trials, including the selection of optimal endpoints and enrollment criteria to maximize power to detect treatment effects.

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DO - 10.1038/s41591-022-01942-9

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AN - SCOPUS:85139804219

SN - 1078-8956

VL - 28

SP - 2194

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JO - Nature Medicine

JF - Nature Medicine

IS - 10

ER -

Temporal order of clinical and biomarker changes in familial frontotemporal dementia

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CIIS: Centro de Investigação Interdisciplinar em Saúde

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