Five-Year Results With Patisiran for Hereditary Transthyretin Amyloidosis With Polyneuropathy: A Randomized Clinical Trial With Open-Label Extension

Global OLE study group

doi:10.1001/jamaneurol.2024.4631

Five-Year Results With Patisiran for Hereditary Transthyretin Amyloidosis With Polyneuropathy: A Randomized Clinical Trial With Open-Label Extension

Global OLE study group

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

18 Scopus citations

Abstract

Importance: There is a lack of long-term efficacy and safety data on hereditary transthyretin amyloidosis with polyneuropathy (hATTR-PN) and on RNA interference (RNAi) therapeutics in general. This study presents the longest-term data to date on patisiran for hATTR-PN. Objective: To present the long-term efficacy and safety of patisiran in adults with hATTR-PN. Design, Setting, and Participants: This global open-label extension (OLE) of the APOLLO randomized clinical trial and phase 2 OLE study enrolled patients from 43 hospitals or clinical centers across 19 countries between July 2015 and August 2017, with follow-up until November 2022. Of 212 eligible patients with hATTR who completed the phase 3 APOLLO or phase 2 OLE parent studies, 211 enrolled in and 138 completed the global OLE. Intervention: Patisiran, 0.3 mg/kg, intravenously once every 3 weeks for up to 5 years. Main Outcomes and Measures: Outcomes evaluated at year 5 of the global OLE included disability (polyneuropathy disability [PND] score); polyneuropathy severity (Neuropathy Impairment Score [NIS]), nutritional status (modified body mass index [mBMI]), quality of life (Norfolk Quality of Life-Diabetic Neuropathy [Norfolk QOL-DN]), and Rasch-Built Overall Disability Scale (R-ODS), with no statistical hierarchy. Safety, survival probability, and mortality were also assessed. Results: At the global OLE baseline, the mean (SD) age was 61.3 (12.3) years, and 156 patients (73.9%) were male. In 138 patients completing the study, PND scores remained stable or improved in 89 patients (65.0%), NISs showed a mean (SD) change of 10.9 (14.7), and mean (SD) mBMI (calculated as weight in kilograms divided by height in meters squared times serum albumin in grams per liter) increased by 46.4 (120.7) over 5 years from baseline. Norfolk QOL-DN and R-ODS scores showed mean (SD) changes of 4.1 (16.7) and -3.7 (6.2), respectively. Adverse events (AEs) leading to study withdrawal occurred in 47 patients (22.3%). Infusion-related reactions were the most common treatment-related AE (n = 34 [16.1%]). Overall, 41 patients (19.4%) died during the study. Patisiran treatment in the parent study and low familial amyloid polyneuropathy score at parent study baseline were associated with significantly improved survival. Conclusions and Relevance: In the longest study of an RNAi therapeutic for any disease, patisiran treatment resulted in modest changes for patients with hATTR-PN with an acceptable safety profile. These results highlight the importance of initiating early treatment for hATTR and the potential of RNAi therapeutics in medicine.

Original language	English
Pages (from-to)	228-236
Number of pages	9
Journal	JAMA Neurology
Volume	82
Issue number	3
DOIs	https://doi.org/10.1001/jamaneurol.2024.4631
State	Published - Mar 10 2025

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10.1001/jamaneurol.2024.4631

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@article{72a7a84151f4444496ec2efa393b28f6,

title = "Five-Year Results With Patisiran for Hereditary Transthyretin Amyloidosis With Polyneuropathy: A Randomized Clinical Trial With Open-Label Extension",

abstract = "Importance: There is a lack of long-term efficacy and safety data on hereditary transthyretin amyloidosis with polyneuropathy (hATTR-PN) and on RNA interference (RNAi) therapeutics in general. This study presents the longest-term data to date on patisiran for hATTR-PN. Objective: To present the long-term efficacy and safety of patisiran in adults with hATTR-PN. Design, Setting, and Participants: This global open-label extension (OLE) of the APOLLO randomized clinical trial and phase 2 OLE study enrolled patients from 43 hospitals or clinical centers across 19 countries between July 2015 and August 2017, with follow-up until November 2022. Of 212 eligible patients with hATTR who completed the phase 3 APOLLO or phase 2 OLE parent studies, 211 enrolled in and 138 completed the global OLE. Intervention: Patisiran, 0.3 mg/kg, intravenously once every 3 weeks for up to 5 years. Main Outcomes and Measures: Outcomes evaluated at year 5 of the global OLE included disability (polyneuropathy disability [PND] score); polyneuropathy severity (Neuropathy Impairment Score [NIS]), nutritional status (modified body mass index [mBMI]), quality of life (Norfolk Quality of Life-Diabetic Neuropathy [Norfolk QOL-DN]), and Rasch-Built Overall Disability Scale (R-ODS), with no statistical hierarchy. Safety, survival probability, and mortality were also assessed. Results: At the global OLE baseline, the mean (SD) age was 61.3 (12.3) years, and 156 patients (73.9\%) were male. In 138 patients completing the study, PND scores remained stable or improved in 89 patients (65.0\%), NISs showed a mean (SD) change of 10.9 (14.7), and mean (SD) mBMI (calculated as weight in kilograms divided by height in meters squared times serum albumin in grams per liter) increased by 46.4 (120.7) over 5 years from baseline. Norfolk QOL-DN and R-ODS scores showed mean (SD) changes of 4.1 (16.7) and -3.7 (6.2), respectively. Adverse events (AEs) leading to study withdrawal occurred in 47 patients (22.3\%). Infusion-related reactions were the most common treatment-related AE (n = 34 [16.1\%]). Overall, 41 patients (19.4\%) died during the study. Patisiran treatment in the parent study and low familial amyloid polyneuropathy score at parent study baseline were associated with significantly improved survival. Conclusions and Relevance: In the longest study of an RNAi therapeutic for any disease, patisiran treatment resulted in modest changes for patients with hATTR-PN with an acceptable safety profile. These results highlight the importance of initiating early treatment for hATTR and the potential of RNAi therapeutics in medicine.",

author = "\{Global OLE study group\} and David Adams and Jonas Wixner and Michael Polydefkis and Berk, \{John L.\} and Concei{\c c}{\~a}o, \{Isabel M.\} and Angela Dispenzieri and Amanda Peltier and Mitsuharu Ueda and Shaun Bender and Kelley Capocelli and Jay, \{Patrick Y.\} and Elena Yureneva and Laura Obici and Giuseppe Vita and Vincenzo Rizzo and Massimo Russo and Anna Mazzeo and Luca Gentile and Janice Wiesman and Michelle Kaku and Vincent Lau and Douglas DeLong and James Dalton and John May and Shahram Attarian and Emilien Delmont and Jean Pouget and Annie Verschueren and Grapperon, \{Aude Marie\} and Emmanuelle Campana-Salort and Carlos Neves and Santos, \{Miguel O.\} and \{de Azevedo Coutinho\}, Concei{\c c}{\~a}o and \{Falcao de Campos\}, Catarina and Teresa Coelho and Reis, \{Antonio H.\} and Nuno Correia and Perez, \{Javier M.\} and \{Martins da Silva\}, Ana and Cristina Alves and Marcio Cardoso and Katia Valdrez and Monte, \{Julia R.\} and Marta Nov{\'a}is and Nadia Guimaraes and Ines Cardoso and Monica Freitas and Joana Ramalho and Natalia Ferreira and Daisuke Kuzume and Masahiro Yamasaki and Yuko Morimoto and Celine Tard and Eric Hachulla and Clement Gauvain and Migaud-Chervy, \{Maria Claire\} and Dominique Deplanque and Elsa Jozefowicz and Loic Lebellec and Marie Th{\'e}audin-Saliou and C{\'e}cile Cauquil-Michon and Celine Labeyrie and Adeline Not and Abdallah Al-Salameh and Lecoq, \{Anne Lise\} and Maeva Stephant and Andoni Echaniz-Laguna and Laurent Becquemont and Guillemette Beaudonne and Vincent Algalarrondo and Ludivine Eliahou and Slama, \{Michel S.\} and Antoine Rousseau and Aissatou Signate and Paola Darche and Jerome Grimaud and Emeline Berthelot and Jocelyn Inamo and Violaine Plant{\'e}-Bordeneuve and Thierry Gendre and Raphaele Arrouasse and Ayache, \{Samar S.\} and Laura Ernande and \{Le Corvoisier\}, Philippe and Hayet Salhi and Ariane Choumert and Cyril Charlin and Thomas Megelin and Brannagan, \{Thomas H.\} and Steven Tsang and Fernanda Wajnsztajn and Jeffrey Shije and Christina Ulane and Inna Kleyman and Louis Weimer and Comana Cioroiu and Kleopas Kleopa and Eleni Zamba-Papanicolaou and Satoshi Tada and Masahiro Nagai and Rina Ando and Yuki Yamanishi and Overcash, \{J. Scott\} and Sinikka Green and Michael Waters and Coskun, \{Derya J.\} and Paul Manos and Zepeda, \{Karla A.\} and William O'Riordan and Andrea Cortese and Alessandro Lozza and Giampaolo Merlini and Vittorio Rosti and Mario Sabatelli and Giulia Bisogni and Daniela Bernardo and Marco Luigetti and \{Di Paolantonio\}, Andrea and Valeria Guglielmino and Angela Romano and Hans Nienhuis and Kristen, \{Arnt V.\} and Christian Nagel and \{aus dem Siepen\}, Fabian and Selina Hein and Shuichiro Neshige and Campistol, \{Josep M.\} and \{Rodas Marin\}, \{Lida Maria\} and \{Blasco Pelicano\}, \{Josep Miquel\} and \{Gal{\'a}n D{\'a}vila\}, Luc{\'i}a and \{Pytel Cordoba\}, \{Vanesa H.\} and Sola, \{Antonio Guerrero\} and \{Garc{\'i}a Feijoo\}, \{Juli{\'a}n H.\} and \{Perez de Isla\}, \{Leopoldo W.\} and Marques, \{Wilson J.\} and \{Lavigne Moreira\}, \{Carolina M.\} and \{Daccach Marques\}, \{Vanessa M.\} and \{Munoz Beamud\}, \{Francisco H.\} and Cristina Borrachero and L{\'o}pez, \{In{\'e}s A.L.\} and Monica Sanz and \{Rigo Oliver\}, \{Elena J.\} and \{Gonz{\'a}lez Moreno\}, \{Juan B.\} and \{Gamez Martinez\}, \{Jose M.\} and Cristina Descals and Mercedes Uson and Vega, \{Francisco Jose\} and Antoni Figuerola and Carles Montala and M{\'a}rcia Waddington-Cruz and \{Souza de Abreu\}, Aline and \{Dias da Silva\}, Moises and \{Gervais de Santa Rosa\}, \{Renata M.\} and Pinto, \{Marcus Vinicius\} and Berensztejn, \{Amanda Cardoso\} and \{Felipe Pinto\}, Luiz and \{de Andrade Guedes\}, \{Mariana M.\} and Fabio Barroso and Andrea Lautre and Orellana, \{Lucas G.\} and \{Gonz{\'a}lez-Duarte Brise{\~n}o\}, \{Maria Alejandra\} and Karla C{\'a}rdenas-Soto and \{Cant{\'u} Brito\}, \{Carlos Gerardo\} and \{Rivera de la Parra\}, David and \{Hernandez Reyes\}, \{Jose Pablo\} and \{Saniger Alba\}, \{Maria del Mar\} and Yesim Parman and Erdi Sahin and Serbest, \{Nail G.\} and Hacer Durmus and Arman Cakar and Sacit Karamursel and Ali Elitok and \{Sirin Inan\}, \{Nermin G.\} and Emre Altinkurt and Allen, \{Adriane C.\} and Vinay Chaudhry and Raquel Jarrett and Neil Bressler and Mandeep Singh and Mohammad Khoshnoodi and Judge, \{Daniel P.\} and Lui, \{Alvin T.\} and Chung, \{Tae Hwan\} and Geno Vista and Shah, \{Syed Mahmood\} and Hirotoshi Hamaguchi and Tetsuya Oda and Masahiro Shimomura and Christof Scheid and Udo Holtick and Jeeyoung Oh and Kim, \{Hee Jin\} and Shin, \{Hyun Jin\} and Kyomin Choi and Yohei Misumi and Toshiya Nomura and Glenn Lopate and Stephanie Geisler and Julaine Florence",

note = "Publisher Copyright: Copyright {\textcopyright} 2025 Adams D et al.",

year = "2025",

month = mar,

day = "10",

doi = "10.1001/jamaneurol.2024.4631",

language = "English",

volume = "82",

pages = "228--236",

journal = "JAMA Neurology",

issn = "2168-6149",

number = "3",

}

TY - JOUR

T1 - Five-Year Results With Patisiran for Hereditary Transthyretin Amyloidosis With Polyneuropathy

T2 - A Randomized Clinical Trial With Open-Label Extension

AU - Global OLE study group

AU - Adams, David

AU - Wixner, Jonas

AU - Polydefkis, Michael

AU - Berk, John L.

AU - Conceição, Isabel M.

AU - Dispenzieri, Angela

AU - Peltier, Amanda

AU - Ueda, Mitsuharu

AU - Bender, Shaun

AU - Capocelli, Kelley

AU - Jay, Patrick Y.

AU - Yureneva, Elena

AU - Obici, Laura

AU - Vita, Giuseppe

AU - Rizzo, Vincenzo

AU - Russo, Massimo

AU - Mazzeo, Anna

AU - Gentile, Luca

AU - Wiesman, Janice

AU - Kaku, Michelle

AU - Lau, Vincent

AU - DeLong, Douglas

AU - Dalton, James

AU - May, John

AU - Attarian, Shahram

AU - Delmont, Emilien

AU - Pouget, Jean

AU - Verschueren, Annie

AU - Grapperon, Aude Marie

AU - Campana-Salort, Emmanuelle

AU - Neves, Carlos

AU - Santos, Miguel O.

AU - de Azevedo Coutinho, Conceição

AU - Falcao de Campos, Catarina

AU - Coelho, Teresa

AU - Reis, Antonio H.

AU - Correia, Nuno

AU - Perez, Javier M.

AU - Martins da Silva, Ana

AU - Alves, Cristina

AU - Cardoso, Marcio

AU - Valdrez, Katia

AU - Monte, Julia R.

AU - Nováis, Marta

AU - Guimaraes, Nadia

AU - Cardoso, Ines

AU - Freitas, Monica

AU - Ramalho, Joana

AU - Ferreira, Natalia

AU - Kuzume, Daisuke

AU - Yamasaki, Masahiro

AU - Morimoto, Yuko

AU - Tard, Celine

AU - Hachulla, Eric

AU - Gauvain, Clement

AU - Migaud-Chervy, Maria Claire

AU - Deplanque, Dominique

AU - Jozefowicz, Elsa

AU - Lebellec, Loic

AU - Théaudin-Saliou, Marie

AU - Cauquil-Michon, Cécile

AU - Labeyrie, Celine

AU - Not, Adeline

AU - Al-Salameh, Abdallah

AU - Lecoq, Anne Lise

AU - Stephant, Maeva

AU - Echaniz-Laguna, Andoni

AU - Becquemont, Laurent

AU - Beaudonne, Guillemette

AU - Algalarrondo, Vincent

AU - Eliahou, Ludivine

AU - Slama, Michel S.

AU - Rousseau, Antoine

AU - Signate, Aissatou

AU - Darche, Paola

AU - Grimaud, Jerome

AU - Berthelot, Emeline

AU - Inamo, Jocelyn

AU - Planté-Bordeneuve, Violaine

AU - Gendre, Thierry

AU - Arrouasse, Raphaele

AU - Ayache, Samar S.

AU - Ernande, Laura

AU - Le Corvoisier, Philippe

AU - Salhi, Hayet

AU - Choumert, Ariane

AU - Charlin, Cyril

AU - Megelin, Thomas

AU - Brannagan, Thomas H.

AU - Tsang, Steven

AU - Wajnsztajn, Fernanda

AU - Shije, Jeffrey

AU - Ulane, Christina

AU - Kleyman, Inna

AU - Weimer, Louis

AU - Cioroiu, Comana

AU - Kleopa, Kleopas

AU - Zamba-Papanicolaou, Eleni

AU - Tada, Satoshi

AU - Nagai, Masahiro

AU - Ando, Rina

AU - Yamanishi, Yuki

AU - Overcash, J. Scott

AU - Green, Sinikka

AU - Waters, Michael

AU - Coskun, Derya J.

AU - Manos, Paul

AU - Zepeda, Karla A.

AU - O'Riordan, William

AU - Cortese, Andrea

AU - Lozza, Alessandro

AU - Merlini, Giampaolo

AU - Rosti, Vittorio

AU - Sabatelli, Mario

AU - Bisogni, Giulia

AU - Bernardo, Daniela

AU - Luigetti, Marco

AU - Di Paolantonio, Andrea

AU - Guglielmino, Valeria

AU - Romano, Angela

AU - Nienhuis, Hans

AU - Kristen, Arnt V.

AU - Nagel, Christian

AU - aus dem Siepen, Fabian

AU - Hein, Selina

AU - Neshige, Shuichiro

AU - Campistol, Josep M.

AU - Rodas Marin, Lida Maria

AU - Blasco Pelicano, Josep Miquel

AU - Galán Dávila, Lucía

AU - Pytel Cordoba, Vanesa H.

AU - Sola, Antonio Guerrero

AU - García Feijoo, Julián H.

AU - Perez de Isla, Leopoldo W.

AU - Marques, Wilson J.

AU - Lavigne Moreira, Carolina M.

AU - Daccach Marques, Vanessa M.

AU - Munoz Beamud, Francisco H.

AU - Borrachero, Cristina

AU - López, Inés A.L.

AU - Sanz, Monica

AU - Rigo Oliver, Elena J.

AU - González Moreno, Juan B.

AU - Gamez Martinez, Jose M.

AU - Descals, Cristina

AU - Uson, Mercedes

AU - Vega, Francisco Jose

AU - Figuerola, Antoni

AU - Montala, Carles

AU - Waddington-Cruz, Márcia

AU - Souza de Abreu, Aline

AU - Dias da Silva, Moises

AU - Gervais de Santa Rosa, Renata M.

AU - Pinto, Marcus Vinicius

AU - Berensztejn, Amanda Cardoso

AU - Felipe Pinto, Luiz

AU - de Andrade Guedes, Mariana M.

AU - Barroso, Fabio

AU - Lautre, Andrea

AU - Orellana, Lucas G.

AU - González-Duarte Briseño, Maria Alejandra

AU - Cárdenas-Soto, Karla

AU - Cantú Brito, Carlos Gerardo

AU - Rivera de la Parra, David

AU - Hernandez Reyes, Jose Pablo

AU - Saniger Alba, Maria del Mar

AU - Parman, Yesim

AU - Sahin, Erdi

AU - Serbest, Nail G.

AU - Durmus, Hacer

AU - Cakar, Arman

AU - Karamursel, Sacit

AU - Elitok, Ali

AU - Sirin Inan, Nermin G.

AU - Altinkurt, Emre

AU - Allen, Adriane C.

AU - Chaudhry, Vinay

AU - Jarrett, Raquel

AU - Bressler, Neil

AU - Singh, Mandeep

AU - Khoshnoodi, Mohammad

AU - Judge, Daniel P.

AU - Lui, Alvin T.

AU - Chung, Tae Hwan

AU - Vista, Geno

AU - Shah, Syed Mahmood

AU - Hamaguchi, Hirotoshi

AU - Oda, Tetsuya

AU - Shimomura, Masahiro

AU - Scheid, Christof

AU - Holtick, Udo

AU - Oh, Jeeyoung

AU - Kim, Hee Jin

AU - Shin, Hyun Jin

AU - Choi, Kyomin

AU - Misumi, Yohei

AU - Nomura, Toshiya

AU - Lopate, Glenn

AU - Geisler, Stephanie

AU - Florence, Julaine

PY - 2025/3/10

Y1 - 2025/3/10

N2 - Importance: There is a lack of long-term efficacy and safety data on hereditary transthyretin amyloidosis with polyneuropathy (hATTR-PN) and on RNA interference (RNAi) therapeutics in general. This study presents the longest-term data to date on patisiran for hATTR-PN. Objective: To present the long-term efficacy and safety of patisiran in adults with hATTR-PN. Design, Setting, and Participants: This global open-label extension (OLE) of the APOLLO randomized clinical trial and phase 2 OLE study enrolled patients from 43 hospitals or clinical centers across 19 countries between July 2015 and August 2017, with follow-up until November 2022. Of 212 eligible patients with hATTR who completed the phase 3 APOLLO or phase 2 OLE parent studies, 211 enrolled in and 138 completed the global OLE. Intervention: Patisiran, 0.3 mg/kg, intravenously once every 3 weeks for up to 5 years. Main Outcomes and Measures: Outcomes evaluated at year 5 of the global OLE included disability (polyneuropathy disability [PND] score); polyneuropathy severity (Neuropathy Impairment Score [NIS]), nutritional status (modified body mass index [mBMI]), quality of life (Norfolk Quality of Life-Diabetic Neuropathy [Norfolk QOL-DN]), and Rasch-Built Overall Disability Scale (R-ODS), with no statistical hierarchy. Safety, survival probability, and mortality were also assessed. Results: At the global OLE baseline, the mean (SD) age was 61.3 (12.3) years, and 156 patients (73.9%) were male. In 138 patients completing the study, PND scores remained stable or improved in 89 patients (65.0%), NISs showed a mean (SD) change of 10.9 (14.7), and mean (SD) mBMI (calculated as weight in kilograms divided by height in meters squared times serum albumin in grams per liter) increased by 46.4 (120.7) over 5 years from baseline. Norfolk QOL-DN and R-ODS scores showed mean (SD) changes of 4.1 (16.7) and -3.7 (6.2), respectively. Adverse events (AEs) leading to study withdrawal occurred in 47 patients (22.3%). Infusion-related reactions were the most common treatment-related AE (n = 34 [16.1%]). Overall, 41 patients (19.4%) died during the study. Patisiran treatment in the parent study and low familial amyloid polyneuropathy score at parent study baseline were associated with significantly improved survival. Conclusions and Relevance: In the longest study of an RNAi therapeutic for any disease, patisiran treatment resulted in modest changes for patients with hATTR-PN with an acceptable safety profile. These results highlight the importance of initiating early treatment for hATTR and the potential of RNAi therapeutics in medicine.

AB - Importance: There is a lack of long-term efficacy and safety data on hereditary transthyretin amyloidosis with polyneuropathy (hATTR-PN) and on RNA interference (RNAi) therapeutics in general. This study presents the longest-term data to date on patisiran for hATTR-PN. Objective: To present the long-term efficacy and safety of patisiran in adults with hATTR-PN. Design, Setting, and Participants: This global open-label extension (OLE) of the APOLLO randomized clinical trial and phase 2 OLE study enrolled patients from 43 hospitals or clinical centers across 19 countries between July 2015 and August 2017, with follow-up until November 2022. Of 212 eligible patients with hATTR who completed the phase 3 APOLLO or phase 2 OLE parent studies, 211 enrolled in and 138 completed the global OLE. Intervention: Patisiran, 0.3 mg/kg, intravenously once every 3 weeks for up to 5 years. Main Outcomes and Measures: Outcomes evaluated at year 5 of the global OLE included disability (polyneuropathy disability [PND] score); polyneuropathy severity (Neuropathy Impairment Score [NIS]), nutritional status (modified body mass index [mBMI]), quality of life (Norfolk Quality of Life-Diabetic Neuropathy [Norfolk QOL-DN]), and Rasch-Built Overall Disability Scale (R-ODS), with no statistical hierarchy. Safety, survival probability, and mortality were also assessed. Results: At the global OLE baseline, the mean (SD) age was 61.3 (12.3) years, and 156 patients (73.9%) were male. In 138 patients completing the study, PND scores remained stable or improved in 89 patients (65.0%), NISs showed a mean (SD) change of 10.9 (14.7), and mean (SD) mBMI (calculated as weight in kilograms divided by height in meters squared times serum albumin in grams per liter) increased by 46.4 (120.7) over 5 years from baseline. Norfolk QOL-DN and R-ODS scores showed mean (SD) changes of 4.1 (16.7) and -3.7 (6.2), respectively. Adverse events (AEs) leading to study withdrawal occurred in 47 patients (22.3%). Infusion-related reactions were the most common treatment-related AE (n = 34 [16.1%]). Overall, 41 patients (19.4%) died during the study. Patisiran treatment in the parent study and low familial amyloid polyneuropathy score at parent study baseline were associated with significantly improved survival. Conclusions and Relevance: In the longest study of an RNAi therapeutic for any disease, patisiran treatment resulted in modest changes for patients with hATTR-PN with an acceptable safety profile. These results highlight the importance of initiating early treatment for hATTR and the potential of RNAi therapeutics in medicine.

UR - https://www.scopus.com/pages/publications/85216938826

U2 - 10.1001/jamaneurol.2024.4631

DO - 10.1001/jamaneurol.2024.4631

M3 - Article

C2 - 39804640

AN - SCOPUS:85216938826

SN - 2168-6149

VL - 82

SP - 228

EP - 236

JO - JAMA Neurology

JF - JAMA Neurology

IS - 3

ER -

Five-Year Results With Patisiran for Hereditary Transthyretin Amyloidosis With Polyneuropathy: A Randomized Clinical Trial With Open-Label Extension

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