ReNeu: A Pivotal, Phase IIb Trial of Mirdametinib in Adults and Children With Symptomatic Neurofibromatosis Type 1-Associated Plexiform Neurofibroma

Christopher L. Moertel; Angela C. Hirbe; Hans Shuhaiber; Kevin Bielamowicz; Alpa Sidhu; David Viskochil; Michael Weber; Armend Lokku; L. Mary Smith; Nicholas K. Foreman; Fouad Hajjar; Rene McNall‐Knapp; Lauren Weintraub; Reuben Antony; Andrea Franson; Julia Meade; David Schiff; Tobias Walbert; Prakash Ambady; Daniela A. Bota; Cynthia Campen; Gurcharanjeet Kaur; Laura J. Klesse; Stefania Maraka; Paul L. Moots; Kathryn Nevel; Miriam Bornhorst; Ana Aguilar-Bonilla; Sarah Chagnon; Nagma Dalvi; Punita Gupta; Ziad Khatib; Laura K. Metrock; Phioanh L. Nghiemphu; Ryan D. Roberts; Nathan Robison; Zsila Sadighi; Stacie Stapleton; Dusica Babovic‐Vuksanovic; Timothy R. Gershon; for the ReNeu Trial Investigators; Ahmed M. Raslan; Alpa Sidhu; Ana Aguilar-Bonilla; Andrea T. Franson; Andrew Walter; Angela C. Hirbe; Brian A. Van Tine; Carl Koschmann; Christopher L. Moertel; Cynthia Campen; Daniela A. Bota; David Schiff; David Viskochil; Dusica Babovic‐Vuksanovic; Fouad M. Hajjar; Gurcharanjeet Kaur; Hans Shuhaiber; Jamie K. Capal; John M. Slopis; Jonathan Gill; Julia Meade; Kathryn Nevel; Laura K. Metrock; Kevin Bielamowicz; Laura J. Klesse; Lauren Weintraub; Leia Nghiemphu; Lindsay Kilburn; Maciej M. Mrugała; Mary Lou Schmidt; Miriam Bornhorst; Nagma Dalvi; Nathan Robison; Nick K. Foreman; Paul L. Moots; Prakash Ambady; Punita Gupta; Radhika Dhamija; Rene McNall‐Knapp; Rueben Antony; Ryan D. Roberts; Ryan Merrell; Sarah Chagnon; Stacie Stapleton; Stefania Maraka; Timothy R. Gershon; Tobias Walbert; Ziad Khatib; Zsila Sadighi

doi:10.1200/jco.24.01034

ReNeu: A Pivotal, Phase IIb Trial of Mirdametinib in Adults and Children With Symptomatic Neurofibromatosis Type 1-Associated Plexiform Neurofibroma

Christopher L. Moertel(University of Minnesota), Angela C. Hirbe(Washington University in St. Louis), Hans Shuhaiber(University of Florida), Kevin Bielamowicz(Arkansas Children's Hospital), Alpa Sidhu(University of Iowa Hospitals and Clinics), David Viskochil(University of Utah), Michael Weber, Armend Lokku, L. Mary Smith, Nicholas K. Foreman(Children's Hospital Colorado), Fouad Hajjar(AdventHealth for Children), Rene McNall‐Knapp(University of Oklahoma Health Sciences Center), Lauren Weintraub(Albany Medical Center Hospital), Reuben Antony(University of California, Davis), Andrea Franson(University of Michigan), Julia Meade(University of Pittsburgh), David Schiff(University of Virginia Medical Center), Tobias Walbert(Wayne State University), Prakash Ambady(Oregon Health & Science University), Daniela A. Bota(University of California, Irvine), Cynthia Campen(Lucile Packard Children's Hospital), Gurcharanjeet Kaur(Morgan Stanley Children's Hospital), Laura J. Klesse(The University of Texas Southwestern Medical Center), Stefania Maraka(University of Illinois Chicago), Paul L. Moots(Vanderbilt University Medical Center), Kathryn Nevel(Indiana University Health), Miriam Bornhorst(Children's National), Ana Aguilar-Bonilla(Orlando Health), Sarah Chagnon(Children's Hospital of The King's Daughters), Nagma Dalvi(Montefiore Medical Center), Punita Gupta(St. Joseph’s University Medical Center), Ziad Khatib(Miami Children's Hospital), Laura K. Metrock(University of Alabama at Birmingham), Phioanh L. Nghiemphu(University of California, Los Angeles), Ryan D. Roberts(Nationwide Children's Hospital), Nathan Robison(Children's Hospital of Los Angeles), Zsila Sadighi(The University of Texas MD Anderson Cancer Center), Stacie Stapleton(Johns Hopkins University), Dusica Babovic‐Vuksanovic(Mayo Clinic in Arizona), Timothy R. Gershon(Emory University), for the ReNeu Trial Investigators, Ahmed M. Raslan, Alpa Sidhu(University of Iowa Hospitals and Clinics), Ana Aguilar-Bonilla(Orlando Health), Andrea T. Franson(University of Michigan), Andrew Walter, Angela C. Hirbe(Washington University in St. Louis), Brian A. Van Tine, Carl Koschmann, Christopher L. Moertel(University of Minnesota), Cynthia Campen(Lucile Packard Children's Hospital), Daniela A. Bota(University of California, Irvine), David Schiff(University of Virginia Medical Center), David Viskochil(University of Utah), Dusica Babovic‐Vuksanovic(Mayo Clinic in Arizona), Fouad M. Hajjar(AdventHealth for Children), Gurcharanjeet Kaur(Morgan Stanley Children's Hospital), Hans Shuhaiber(University of Florida), Jamie K. Capal, John M. Slopis, Jonathan Gill, Julia Meade(University of Pittsburgh), Kathryn Nevel(Indiana University Health), Laura K. Metrock(University of Alabama at Birmingham), Kevin Bielamowicz(Arkansas Children's Hospital), Laura J. Klesse(The University of Texas Southwestern Medical Center), Lauren Weintraub(Albany Medical Center Hospital), Leia Nghiemphu, Lindsay Kilburn, Maciej M. Mrugała, Mary Lou Schmidt, Miriam Bornhorst(Children's National), Nagma Dalvi(Montefiore Medical Center), Nathan Robison(Children's Hospital of Los Angeles), Nick K. Foreman(Children's Hospital Colorado), Paul L. Moots(Vanderbilt University Medical Center), Prakash Ambady(Oregon Health & Science University), Punita Gupta(St. Joseph’s University Medical Center), Radhika Dhamija, Rene McNall‐Knapp(University of Oklahoma Health Sciences Center), Rueben Antony(University of California, Davis), Ryan D. Roberts(Nationwide Children's Hospital), Ryan Merrell, Sarah Chagnon(Children's Hospital of The King's Daughters), Stacie Stapleton(Johns Hopkins University), Stefania Maraka(University of Illinois Chicago), Timothy R. Gershon(Emory University), Tobias Walbert(Wayne State University), Ziad Khatib(Miami Children's Hospital), Zsila Sadighi(The University of Texas MD Anderson Cancer Center)

Journal of Clinical Oncology

November 8, 2024

10.1200/jco.24.01034

Cited by 85Open Access

Full Text

Abstract

PURPOSE: Pharmacologic therapies for neurofibromatosis type 1-associated plexiform neurofibromas (NF1-PNs) are limited; currently, none are US Food and Drug Administration-approved for adults. METHODS: twice daily, maximum 4 mg twice daily), regardless of food intake, in 3 weeks on/1 week off 28-day cycles. The primary end point was confirmed objective response rate (ORR; proportion of patients with a ≥20% reduction of target PN volume from baseline on consecutive scans during the 24-cycle treatment phase) assessed by blinded independent central review (BICR) of volumetric magnetic resonance imaging. RESULTS: Twenty-four of 58 adults (41%) and 29 of 56 children (52%) had a BICR-confirmed objective response during the 24-cycle treatment phase; in addition, two adults and one child had confirmed responses during long-term follow-up. Median (range) target PN volumetric best response was -41% (-90 to 13) in adults and -42% (-91 to 48) in children. Both cohorts reported significant and clinically meaningful improvement in patient- or parent proxy-reported outcome measures of worst tumor pain severity, pain interference, and health-related quality of life (HRQOL) that began early and were sustained during treatment. The most commonly reported treatment-related adverse events were dermatitis acneiform, diarrhea, and nausea in adults and dermatitis acneiform, diarrhea, and paronychia in children. CONCLUSION: In ReNeu, the largest multicenter NF1-PN trial reported to date, mirdametinib treatment demonstrated significant confirmed ORRs by BICR, deep and durable PN volume reductions, and early, sustained, and clinically meaningful improvement in pain and HRQOL. Mirdametinib was well-tolerated in adults and children.

Related Papers

No related papers found

Powered by citation graph analysis