Efficacy and Safety of Zilucoplan in Amyotrophic Lateral Sclerosis: A Randomized Clinical Trial

HEALEY ALS Platform Trial Study Group

doi:10.1001/jamanetworkopen.2024.59058

Efficacy and Safety of Zilucoplan in Amyotrophic Lateral Sclerosis: A Randomized Clinical Trial

HEALEY ALS Platform Trial Study Group

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

15 Scopus citations

Abstract

IMPORTANCE The etiology of amyotrophic lateral sclerosis (ALS), a fatal neurodegenerative disease, is unknown. However, neuroinflammation and complement activation may play a role in disease progression. OBJECTIVE To determine the effects of zilucoplan, an inhibitor of complement C5, in individuals with ALS. DESIGN, SETTING, AND PARTICIPANTS Zilucoplan was tested as regimen A of the HEALEY ALS Platform Trial, a phase 2 to 3 multicenter, randomized, double-blind, placebo-controlled perpetual platform clinical trial with sharing of trial infrastructure and placebo data across multiple regimens. Regimen A was conducted from August 17, 2020, to May 4, 2022. A total of 162 participants were randomized to receive zilucoplan (122 [75.3%]) or regimen-specific placebo (40 [24.7%]). An additional 124 concurrently randomized participants were randomized to receive placebo in other regimens. INTERVENTIONS Eligible participants were randomized in a 3:1 ratio to receive zilucoplan or matching placebo within strata of edaravone and/or riluzole use for a planned duration of 24 weeks. Active drug (zilucoplan, 0.3mg/kg) and placebo were provided for daily subcutaneous dosing. MAIN OUTCOMES AND MEASURES The primary end point was change in disease severity from baseline through 24 weeks as measured by the Amyotrophic Lateral Sclerosis Functional Rating Scale-Revised (ALSFRS-R) total score and survival, analyzed using a bayesian shared-parameter model and reported as disease rate ratio (DRR; <1 indicating treatment benefit). The study included prespecified rules for early stopping for futility. Outcome analyses were performed in the full analysis set comparing the zilucoplan group with the total shared placebo group (n = 164). RESULTS Among the 162 participants who were randomized (mean [SD] age, 59.6 [11.3]; 99 [61.1%] male), 115 (71.0%) completed the trial. The estimated DRR common to ALSFRS-R and survival was 1.08 (95%credible interval, 0.87-1.31; posterior probability of superiority, 0.24). The trial was stopped early for futility. No unexpected treatment-related risks were identified. CONCLUSIONS AND RELEVANCE In this randomized clinical trial of zilucoplan in ALS, treatment did not alter disease progression. The adaptive platform design of the HEALEY ALS Platform Trial made it possible to test a new investigational product with efficient use of time and resources.

Original language	English
Article number	e2459058
Journal	JAMA Network Open
Volume	8
Issue number	2
DOIs	https://doi.org/10.1001/jamanetworkopen.2024.59058
State	Published - 2025

Access to Document

10.1001/jamanetworkopen.2024.59058

Cite this

@article{91e24d6b9c7d45ebad64fe0ab14b403c,

title = "Efficacy and Safety of Zilucoplan in Amyotrophic Lateral Sclerosis: A Randomized Clinical Trial",

abstract = "IMPORTANCE The etiology of amyotrophic lateral sclerosis (ALS), a fatal neurodegenerative disease, is unknown. However, neuroinflammation and complement activation may play a role in disease progression. OBJECTIVE To determine the effects of zilucoplan, an inhibitor of complement C5, in individuals with ALS. DESIGN, SETTING, AND PARTICIPANTS Zilucoplan was tested as regimen A of the HEALEY ALS Platform Trial, a phase 2 to 3 multicenter, randomized, double-blind, placebo-controlled perpetual platform clinical trial with sharing of trial infrastructure and placebo data across multiple regimens. Regimen A was conducted from August 17, 2020, to May 4, 2022. A total of 162 participants were randomized to receive zilucoplan (122 [75.3\%]) or regimen-specific placebo (40 [24.7\%]). An additional 124 concurrently randomized participants were randomized to receive placebo in other regimens. INTERVENTIONS Eligible participants were randomized in a 3:1 ratio to receive zilucoplan or matching placebo within strata of edaravone and/or riluzole use for a planned duration of 24 weeks. Active drug (zilucoplan, 0.3mg/kg) and placebo were provided for daily subcutaneous dosing. MAIN OUTCOMES AND MEASURES The primary end point was change in disease severity from baseline through 24 weeks as measured by the Amyotrophic Lateral Sclerosis Functional Rating Scale-Revised (ALSFRS-R) total score and survival, analyzed using a bayesian shared-parameter model and reported as disease rate ratio (DRR; <1 indicating treatment benefit). The study included prespecified rules for early stopping for futility. Outcome analyses were performed in the full analysis set comparing the zilucoplan group with the total shared placebo group (n = 164). RESULTS Among the 162 participants who were randomized (mean [SD] age, 59.6 [11.3]; 99 [61.1\%] male), 115 (71.0\%) completed the trial. The estimated DRR common to ALSFRS-R and survival was 1.08 (95\%credible interval, 0.87-1.31; posterior probability of superiority, 0.24). The trial was stopped early for futility. No unexpected treatment-related risks were identified. CONCLUSIONS AND RELEVANCE In this randomized clinical trial of zilucoplan in ALS, treatment did not alter disease progression. The adaptive platform design of the HEALEY ALS Platform Trial made it possible to test a new investigational product with efficient use of time and resources.",

author = "\{HEALEY ALS Platform Trial Study Group\} and Sabrina Paganoni and Fournier, \{Christina N.\} and MacKlin, \{Eric A.\} and Chibnik, \{Lori B.\} and Melanie Quintana and Saville, \{Benjamin R.\} and Detry, \{Michelle A.\} and Matteo Vestrucci and Joe Marion and Anna McGlothlin and Senda Ajroud-Driss and Marianne Chase and Lindsay Pothier and Harkey, \{Brittney A.\} and Hong Yu and Sherman, \{Alexander A.\} and Shefner, \{Jeremy M.\} and Meghan Hall and Gale Kittle and Berry, \{James D.\} and Suma Babu and Jinsy Andrews and Derek Dagostino and Eric Tustison and Elisa Giacomelli and Erica Scirocco and Gustavo Alameda and Eduardo Locatelli and Doreen Ho and Adam Quick and Jonathan Katz and Daragh Heitzman and Appel, \{Stanley H.\} and Sheetal Shroff and Kevin Felice and Maragakis, \{Nicholas J.\} and Zachary Simmons and Miller, \{Timothy M.\} and Nicholas Olney and Weiss, \{Michael D.\} and Goutman, \{Stephen A.\} and Fernandes, \{Joseph A.\} and Omar Jawdat and Owegi, \{Margaret A.\} and Foster, \{Laura A.\} and Tuan Vu and Hristelina Ilieva and Newman, \{Daniel S.\} and Ximena Arcila-Londono and Jackson, \{Carlayne E.\} and Shafeeq Ladha and Terry Heiman-Patterson and Caress, \{James B.\} and Andrea Swenson and Amanda Peltier and Richard Lewis and Dominic Fee and Matthew Elliott and Richard Bedlack and Kasarskis, \{Edward J.\} and Lauren Elman and Jeffrey Rosenfeld and David Walk and Courtney McIlduff and Paul Twydell and Eufrosina Young and Kristin Johnson and Kourosh Rezania and Goyal, \{Namita A.\} and Cohen, \{Jeffrey A.\} and Michael Benatar and Vovanti Jones and Jonathan Glass and Jaimin Shah and Beydoun, \{Said R.\} and Wymer, \{James P.\} and Zilliox, \{Lindsay L.\} and Shakti Nayar and Pattee, \{Gary L.\} and Jennifer Martinez-Thompson and Brittany Harvey and Shital Patel and Paul Mahoney and Duda, \{Petra W.\} and Cudkowicz, \{Merit E.\} and Douglas Hayden and Lai, \{Po Ying\} and Donahue, \{Rachel A.\} and Chen, \{Hao Wun\} and Jianing Wang and Nithya Mathai and Gabriela Lopes and Alexandra McCaffrey and Jennifer Scalia and Sarah Luppino and Clotilde Lagier-Tourenne and Ghazaleh Sadri-Vakili and Stephen Kolb and Sarah Heintzman and Robert Sufit and April Szymanski and Liberty Jenkins and Alan Martin and Ericka Greene and Thonhoff, \{Jason R.\} and Bing Liao and Charles Whitaker and Clawson, \{Lora L.\} and Alpa Uchil and Riley, \{Kristen M.\} and Arneklev, \{Jin Ae\} and James Grogan and Xiaowei Su and Mansoureh Mamarabadi and Amber Malcolm and Tracy Bazan and Nassim Rad and Wang, \{Leo H.\} and Feldman, \{Eva L.\} and Ezequiel Piccione and Pariwat Thaisetthawatkul and Constantine Farmakidis and Duaa Jabari and Jeffrey Statland and Mamatha Pasnoor and Mazen Dimachkie and Brown, \{Robert H.\} and Mehdi Ghasemi and Hajar Houmani and Catherine Douthwright and Kate Daniello and Niraja Suresh and Jerrica Farias and Chen, \{I. Hweii A.\} and Piera Pasinelli and Kara Steijlen and Ratna Bhavaraju-Sanka and Bill Jacobsen and Jourdan Milliard and Robert Bowser and Anahita Deboo and Cartwright, \{Michael S.\} and Christopher Nance and Ludwig Gutmann and Julia Yasek and Matthew Harms and Matthew Burford and Frank Diaz and David Shrilla and Goran Rakocevic and Sarah Jones and Guillermo Solorzano and Xiaoyan Li and Zabeen Mahuwala and Mathur, \{Vishakhadatta (Vish) Mathur\} and Colin Quinn and Michael Baer and David Borg and Karthikeyan Bhuvaneswaran and Jasdeep Kaur and Sam Maiser and Rutkove, \{Seward B.\} and Andrew Mundwiler and Meyer, \{Jenny A.\} and Pooja Rao and Betty Soliven and Raymond Roos and Habib, \{Ali A.\} and Tahseen Mozaffar and Korb, \{Manisha Kak\} and Jeffrey Mullen and Elijah Stommel and Robbins, \{Nathaniel M.\} and Nathan Carberry and Volkan Granit and Raghav Govindarajan and Bjorn Oskarsson and Leila Darki and Rodrigo Rodriguez and Miguel Chuquilin and Whitney McNeely and Montserrat Diaz-Abad and Jin, \{Peter H.\} and Chandana Chauhan and James Bobenhouse and Staff, \{Nathan P.\} and Ghazala Hayat and Luisa Arroyave and Abbey Bailey and Jesse Bailey and Victoria Barlow and Allison Bulat and Genevive Changkuon and Melissa Cirino and Cristina Deignan and Emma Deirmendjian and \{De Mattos\}, Annette and Sofia DiStefano and Kristin Drake and Michaela Estes",

year = "2025",

doi = "10.1001/jamanetworkopen.2024.59058",

language = "English",

volume = "8",

journal = "JAMA Network Open",

issn = "2574-3805",

number = "2",

}

TY - JOUR

T1 - Efficacy and Safety of Zilucoplan in Amyotrophic Lateral Sclerosis

T2 - A Randomized Clinical Trial

AU - HEALEY ALS Platform Trial Study Group

AU - Paganoni, Sabrina

AU - Fournier, Christina N.

AU - MacKlin, Eric A.

AU - Chibnik, Lori B.

AU - Quintana, Melanie

AU - Saville, Benjamin R.

AU - Detry, Michelle A.

AU - Vestrucci, Matteo

AU - Marion, Joe

AU - McGlothlin, Anna

AU - Ajroud-Driss, Senda

AU - Chase, Marianne

AU - Pothier, Lindsay

AU - Harkey, Brittney A.

AU - Yu, Hong

AU - Sherman, Alexander A.

AU - Shefner, Jeremy M.

AU - Hall, Meghan

AU - Kittle, Gale

AU - Berry, James D.

AU - Babu, Suma

AU - Andrews, Jinsy

AU - Dagostino, Derek

AU - Tustison, Eric

AU - Giacomelli, Elisa

AU - Scirocco, Erica

AU - Alameda, Gustavo

AU - Locatelli, Eduardo

AU - Ho, Doreen

AU - Quick, Adam

AU - Katz, Jonathan

AU - Heitzman, Daragh

AU - Appel, Stanley H.

AU - Shroff, Sheetal

AU - Felice, Kevin

AU - Maragakis, Nicholas J.

AU - Simmons, Zachary

AU - Miller, Timothy M.

AU - Olney, Nicholas

AU - Weiss, Michael D.

AU - Goutman, Stephen A.

AU - Fernandes, Joseph A.

AU - Jawdat, Omar

AU - Owegi, Margaret A.

AU - Foster, Laura A.

AU - Vu, Tuan

AU - Ilieva, Hristelina

AU - Newman, Daniel S.

AU - Arcila-Londono, Ximena

AU - Jackson, Carlayne E.

AU - Ladha, Shafeeq

AU - Heiman-Patterson, Terry

AU - Caress, James B.

AU - Swenson, Andrea

AU - Peltier, Amanda

AU - Lewis, Richard

AU - Fee, Dominic

AU - Elliott, Matthew

AU - Bedlack, Richard

AU - Kasarskis, Edward J.

AU - Elman, Lauren

AU - Rosenfeld, Jeffrey

AU - Walk, David

AU - McIlduff, Courtney

AU - Twydell, Paul

AU - Young, Eufrosina

AU - Johnson, Kristin

AU - Rezania, Kourosh

AU - Goyal, Namita A.

AU - Cohen, Jeffrey A.

AU - Benatar, Michael

AU - Jones, Vovanti

AU - Glass, Jonathan

AU - Shah, Jaimin

AU - Beydoun, Said R.

AU - Wymer, James P.

AU - Zilliox, Lindsay L.

AU - Nayar, Shakti

AU - Pattee, Gary L.

AU - Martinez-Thompson, Jennifer

AU - Harvey, Brittany

AU - Patel, Shital

AU - Mahoney, Paul

AU - Duda, Petra W.

AU - Cudkowicz, Merit E.

AU - Hayden, Douglas

AU - Lai, Po Ying

AU - Donahue, Rachel A.

AU - Chen, Hao Wun

AU - Wang, Jianing

AU - Mathai, Nithya

AU - Lopes, Gabriela

AU - McCaffrey, Alexandra

AU - Scalia, Jennifer

AU - Luppino, Sarah

AU - Lagier-Tourenne, Clotilde

AU - Sadri-Vakili, Ghazaleh

AU - Kolb, Stephen

AU - Heintzman, Sarah

AU - Sufit, Robert

AU - Szymanski, April

AU - Jenkins, Liberty

AU - Martin, Alan

AU - Greene, Ericka

AU - Thonhoff, Jason R.

AU - Liao, Bing

AU - Whitaker, Charles

AU - Clawson, Lora L.

AU - Uchil, Alpa

AU - Riley, Kristen M.

AU - Arneklev, Jin Ae

AU - Grogan, James

AU - Su, Xiaowei

AU - Mamarabadi, Mansoureh

AU - Malcolm, Amber

AU - Bazan, Tracy

AU - Rad, Nassim

AU - Wang, Leo H.

AU - Feldman, Eva L.

AU - Piccione, Ezequiel

AU - Thaisetthawatkul, Pariwat

AU - Farmakidis, Constantine

AU - Jabari, Duaa

AU - Statland, Jeffrey

AU - Pasnoor, Mamatha

AU - Dimachkie, Mazen

AU - Brown, Robert H.

AU - Ghasemi, Mehdi

AU - Houmani, Hajar

AU - Douthwright, Catherine

AU - Daniello, Kate

AU - Suresh, Niraja

AU - Farias, Jerrica

AU - Chen, I. Hweii A.

AU - Pasinelli, Piera

AU - Steijlen, Kara

AU - Bhavaraju-Sanka, Ratna

AU - Jacobsen, Bill

AU - Milliard, Jourdan

AU - Bowser, Robert

AU - Deboo, Anahita

AU - Cartwright, Michael S.

AU - Nance, Christopher

AU - Gutmann, Ludwig

AU - Yasek, Julia

AU - Harms, Matthew

AU - Burford, Matthew

AU - Diaz, Frank

AU - Shrilla, David

AU - Rakocevic, Goran

AU - Jones, Sarah

AU - Solorzano, Guillermo

AU - Li, Xiaoyan

AU - Mahuwala, Zabeen

AU - Mathur, Vishakhadatta (Vish) Mathur

AU - Quinn, Colin

AU - Baer, Michael

AU - Borg, David

AU - Bhuvaneswaran, Karthikeyan

AU - Kaur, Jasdeep

AU - Maiser, Sam

AU - Rutkove, Seward B.

AU - Mundwiler, Andrew

AU - Meyer, Jenny A.

AU - Rao, Pooja

AU - Soliven, Betty

AU - Roos, Raymond

AU - Habib, Ali A.

AU - Mozaffar, Tahseen

AU - Korb, Manisha Kak

AU - Mullen, Jeffrey

AU - Stommel, Elijah

AU - Robbins, Nathaniel M.

AU - Carberry, Nathan

AU - Granit, Volkan

AU - Govindarajan, Raghav

AU - Oskarsson, Bjorn

AU - Darki, Leila

AU - Rodriguez, Rodrigo

AU - Chuquilin, Miguel

AU - McNeely, Whitney

AU - Diaz-Abad, Montserrat

AU - Jin, Peter H.

AU - Chauhan, Chandana

AU - Bobenhouse, James

AU - Staff, Nathan P.

AU - Hayat, Ghazala

AU - Arroyave, Luisa

AU - Bailey, Abbey

AU - Bailey, Jesse

AU - Barlow, Victoria

AU - Bulat, Allison

AU - Changkuon, Genevive

AU - Cirino, Melissa

AU - Deignan, Cristina

AU - Deirmendjian, Emma

AU - De Mattos, Annette

AU - DiStefano, Sofia

AU - Drake, Kristin

AU - Estes, Michaela

PY - 2025

Y1 - 2025

N2 - IMPORTANCE The etiology of amyotrophic lateral sclerosis (ALS), a fatal neurodegenerative disease, is unknown. However, neuroinflammation and complement activation may play a role in disease progression. OBJECTIVE To determine the effects of zilucoplan, an inhibitor of complement C5, in individuals with ALS. DESIGN, SETTING, AND PARTICIPANTS Zilucoplan was tested as regimen A of the HEALEY ALS Platform Trial, a phase 2 to 3 multicenter, randomized, double-blind, placebo-controlled perpetual platform clinical trial with sharing of trial infrastructure and placebo data across multiple regimens. Regimen A was conducted from August 17, 2020, to May 4, 2022. A total of 162 participants were randomized to receive zilucoplan (122 [75.3%]) or regimen-specific placebo (40 [24.7%]). An additional 124 concurrently randomized participants were randomized to receive placebo in other regimens. INTERVENTIONS Eligible participants were randomized in a 3:1 ratio to receive zilucoplan or matching placebo within strata of edaravone and/or riluzole use for a planned duration of 24 weeks. Active drug (zilucoplan, 0.3mg/kg) and placebo were provided for daily subcutaneous dosing. MAIN OUTCOMES AND MEASURES The primary end point was change in disease severity from baseline through 24 weeks as measured by the Amyotrophic Lateral Sclerosis Functional Rating Scale-Revised (ALSFRS-R) total score and survival, analyzed using a bayesian shared-parameter model and reported as disease rate ratio (DRR; <1 indicating treatment benefit). The study included prespecified rules for early stopping for futility. Outcome analyses were performed in the full analysis set comparing the zilucoplan group with the total shared placebo group (n = 164). RESULTS Among the 162 participants who were randomized (mean [SD] age, 59.6 [11.3]; 99 [61.1%] male), 115 (71.0%) completed the trial. The estimated DRR common to ALSFRS-R and survival was 1.08 (95%credible interval, 0.87-1.31; posterior probability of superiority, 0.24). The trial was stopped early for futility. No unexpected treatment-related risks were identified. CONCLUSIONS AND RELEVANCE In this randomized clinical trial of zilucoplan in ALS, treatment did not alter disease progression. The adaptive platform design of the HEALEY ALS Platform Trial made it possible to test a new investigational product with efficient use of time and resources.

AB - IMPORTANCE The etiology of amyotrophic lateral sclerosis (ALS), a fatal neurodegenerative disease, is unknown. However, neuroinflammation and complement activation may play a role in disease progression. OBJECTIVE To determine the effects of zilucoplan, an inhibitor of complement C5, in individuals with ALS. DESIGN, SETTING, AND PARTICIPANTS Zilucoplan was tested as regimen A of the HEALEY ALS Platform Trial, a phase 2 to 3 multicenter, randomized, double-blind, placebo-controlled perpetual platform clinical trial with sharing of trial infrastructure and placebo data across multiple regimens. Regimen A was conducted from August 17, 2020, to May 4, 2022. A total of 162 participants were randomized to receive zilucoplan (122 [75.3%]) or regimen-specific placebo (40 [24.7%]). An additional 124 concurrently randomized participants were randomized to receive placebo in other regimens. INTERVENTIONS Eligible participants were randomized in a 3:1 ratio to receive zilucoplan or matching placebo within strata of edaravone and/or riluzole use for a planned duration of 24 weeks. Active drug (zilucoplan, 0.3mg/kg) and placebo were provided for daily subcutaneous dosing. MAIN OUTCOMES AND MEASURES The primary end point was change in disease severity from baseline through 24 weeks as measured by the Amyotrophic Lateral Sclerosis Functional Rating Scale-Revised (ALSFRS-R) total score and survival, analyzed using a bayesian shared-parameter model and reported as disease rate ratio (DRR; <1 indicating treatment benefit). The study included prespecified rules for early stopping for futility. Outcome analyses were performed in the full analysis set comparing the zilucoplan group with the total shared placebo group (n = 164). RESULTS Among the 162 participants who were randomized (mean [SD] age, 59.6 [11.3]; 99 [61.1%] male), 115 (71.0%) completed the trial. The estimated DRR common to ALSFRS-R and survival was 1.08 (95%credible interval, 0.87-1.31; posterior probability of superiority, 0.24). The trial was stopped early for futility. No unexpected treatment-related risks were identified. CONCLUSIONS AND RELEVANCE In this randomized clinical trial of zilucoplan in ALS, treatment did not alter disease progression. The adaptive platform design of the HEALEY ALS Platform Trial made it possible to test a new investigational product with efficient use of time and resources.

UR - https://www.scopus.com/pages/publications/85218953640

U2 - 10.1001/jamanetworkopen.2024.59058

DO - 10.1001/jamanetworkopen.2024.59058

M3 - Article

C2 - 39960672

AN - SCOPUS:85218953640

SN - 2574-3805

VL - 8

JO - JAMA Network Open

JF - JAMA Network Open

IS - 2

M1 - e2459058

ER -

Efficacy and Safety of Zilucoplan in Amyotrophic Lateral Sclerosis: A Randomized Clinical Trial

Abstract

Access to Document

Other files and links

Fingerprint

Cite this