Mismatch repair deficiency predicts response of solid tumors to PD-1 blockade.
Dung T LeJennifer N DurhamKellie N SmitHao WangBjarne R BartlettLaveet K AulakhSteve LuHolly KemberlingCara WiltBrandon S LuberFay WongNilofer S AzadAgnieszka A RuckiDan LaheruRoss DonehowerAtif ZaheerGeorge A FisherTodd S CrocenziJames J LeeTim F GretenAustin G DuffyKristen K CiomborAleksandra D EyringBao H LamAndrew JoeS Peter KangMatthias HoldhoffLudmila V DanilovaLeslie CopeChristian F MeyerShibin ZhouRichard M GoldbergDeborah K ArmstrongKatherine M BeverAmanda N FaderJanis TaubeFranck HousseauDavid SpetzlerNianqing XiaoDrew M PardollNickolas PapadopoulosKenneth W KinzlerJames R EshlemanBert VogelsteinRobert A AndersLuis A DiazPublished in: Science (New York, N.Y.) (2017)
The genomes of cancers deficient in mismatch repair contain exceptionally high numbers of somatic mutations. In a proof-of-concept study, we previously showed that colorectal cancers with mismatch repair deficiency were sensitive to immune checkpoint blockade with antibodies to programmed death receptor-1 (PD-1). We have now expanded this study to evaluate the efficacy of PD-1 blockade in patients with advanced mismatch repair-deficient cancers across 12 different tumor types. Objective radiographic responses were observed in 53% of patients, and complete responses were achieved in 21% of patients. Responses were durable, with median progression-free survival and overall survival still not reached. Functional analysis in a responding patient demonstrated rapid in vivo expansion of neoantigen-specific T cell clones that were reactive to mutant neopeptides found in the tumor. These data support the hypothesis that the large proportion of mutant neoantigens in mismatch repair-deficient cancers make them sensitive to immune checkpoint blockade, regardless of the cancers' tissue of origin.