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The Molecular Tumor Board of the Regina Elena National Cancer Institute: from accrual to treatment in real-world.
Giacomini, Patrizio; Valenti, Fabio; Allegretti, Matteo; Pallocca, Matteo; De Nicola, Francesca; Ciuffreda, Ludovica; Fanciulli, Maurizio; Scalera, Stefano; Buglioni, Simonetta; Melucci, Elisa; Casini, Beatrice; Carosi, Mariantonia; Pescarmona, Edoardo; Giordani, Elena; Sperati, Francesca; Jannitti, Nicoletta; Betti, Martina; Maugeri-Saccà, Marcello; Cecere, Fabiana Letizia; Villani, Veronica; Pace, Andrea; Appetecchia, Marialuisa; Vici, Patrizia; Savarese, Antonella; Krasniqi, Eriseld; Ferraresi, Virginia; Russillo, Michelangelo; Fabi, Alessandra; Landi, Lorenza; Minuti, Gabriele; Cappuzzo, Federico; Zeuli, Massimo; Ciliberto, Gennaro.
Affiliation
  • Giacomini P; Clinical Trial Center, Biostatistics and Bioinformatics, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy. patrizio.giacomini@ifo.it.
  • Valenti F; UOC Translational Oncology Research, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Allegretti M; UOC Translational Oncology Research, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Pallocca M; Clinical Trial Center, Biostatistics and Bioinformatics, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • De Nicola F; SAFU, Department of Research, Advanced Diagnostics, and Technological Innovation, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Ciuffreda L; SAFU, Department of Research, Advanced Diagnostics, and Technological Innovation, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Fanciulli M; SAFU, Department of Research, Advanced Diagnostics, and Technological Innovation, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Scalera S; Clinical Trial Center, Biostatistics and Bioinformatics, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Buglioni S; Department of Pathology, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Melucci E; Department of Pathology, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Casini B; Department of Pathology, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Carosi M; Department of Pathology, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Pescarmona E; Department of Pathology, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Giordani E; UOC Translational Oncology Research, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Sperati F; Clinical Trial Center, Biostatistics and Bioinformatics, San Gallicano Dermatological Institute IRCCS, 00144, Rome, Italy.
  • Jannitti N; Pharmacy Unit, Medical Direction, IRCCS-Regina Elena National Cancer Institute and San Gallicano Institute, 00144, Rome, Italy.
  • Betti M; Clinical Trial Center, Biostatistics and Bioinformatics, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Maugeri-Saccà M; Clinical Trial Center, Biostatistics and Bioinformatics, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Cecere FL; Medical Oncology 2, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Villani V; Medical Oncology 2, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Pace A; Neuro-Oncology Unit, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Appetecchia M; Neuro-Oncology Unit, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Vici P; Oncological Endocrinology Unit, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Savarese A; Phase IV Studies, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Krasniqi E; Medical Oncology 1, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Ferraresi V; Phase IV Studies, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Russillo M; Sarcomas and Rare Tumors Departmental Unit, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Fabi A; Sarcomas and Rare Tumors Departmental Unit, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Landi L; Precision Medicine Unit in Senology, Fondazione Policlinico Universitario A. Gemelli IRCCS, 00168, Rome, Italy.
  • Minuti G; Clinical Trial Center: Phase 1 and Precision Medicine, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Cappuzzo F; Clinical Trial Center: Phase 1 and Precision Medicine, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Zeuli M; Medical Oncology 2, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
  • Ciliberto G; Clinical Trial Center, Biostatistics and Bioinformatics, IRCCS-Regina Elena National Cancer Institute, 00144, Rome, Italy.
J Transl Med ; 21(1): 725, 2023 10 16.
Article in En | MEDLINE | ID: mdl-37845764
ABSTRACT

BACKGROUND:

Molecular Tumor Boards (MTB) operating in real-world have generated limited consensus on good practices for accrual, actionable alteration mapping, and outcome metrics. These topics are addressed herein in 124 MTB patients, all real-world accrued at progression, and lacking approved therapy options.

METHODS:

Actionable genomic alterations identified by tumor DNA (tDNA) and circulating tumor DNA (ctDNA) profiling were mapped by customized OncoKB criteria to reflect diagnostic/therapeutic indications as approved in Europe. Alterations were considered non-SoC when mapped at either OncoKB level 3, regardless of tDNA/ctDNA origin, or at OncoKB levels 1/2, provided they were undetectable in matched tDNA, and had not been exploited in previous therapy lines.

RESULTS:

Altogether, actionable alterations were detected in 54/124 (43.5%) MTB patients, but only in 39 cases (31%) were these alterations (25 from tDNA, 14 from ctDNA) actionable/unexploited, e.g. they had not resulted in the assignment of pre-MTB treatments. Interestingly, actionable and actionable/unexploited alterations both decreased (37.5% and 22.7% respectively) in a subset of 88 MTB patients profiled by tDNA-only, but increased considerably (77.7% and 66.7%) in 18 distinct patients undergoing combined tDNA/ctDNA testing, approaching the potential treatment opportunities (76.9%) in 147 treatment-naïve patients undergoing routine tDNA profiling for the first time. Non-SoC therapy was MTB-recommended to all 39 patients with actionable/unexploited alterations, but only 22 (56%) accessed the applicable drug, mainly due to clinical deterioration, lengthy drug-gathering procedures, and geographical distance from recruiting clinical trials. Partial response and stable disease were recorded in 8 and 7 of 19 evaluable patients, respectively. The time to progression (TTP) ratio (MTB-recommended treatment vs last pre-MTB treatment) exceeded the conventional Von Hoff 1.3 cut-off in 9/19 cases, high absolute TTP and Von Hoff values coinciding in 3 cases. Retrospectively, 8 patients receiving post-MTB treatment(s) as per physician's choice were noted to have a much longer overall survival from MTB accrual than 11 patients who had received no further treatment (35.09 vs 6.67 months, p = 0.006).

CONCLUSIONS:

MTB-recommended/non-SoC treatments are effective, including those assigned by ctDNA-only alterations. However, real-world MTBs may inadvertently recruit patients electively susceptible to diverse and/or multiple treatments.
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Full text: 1 Database: MEDLINE Main subject: Neoplasms Limits: Humans Country/Region as subject: America do norte Language: En Journal: J Transl Med Year: 2023 Type: Article Affiliation country: Italy
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Full text: 1 Database: MEDLINE Main subject: Neoplasms Limits: Humans Country/Region as subject: America do norte Language: En Journal: J Transl Med Year: 2023 Type: Article Affiliation country: Italy