AI Article Synopsis

  • In April 2023, the National Comprehensive Cancer Network recommended neoadjuvant immunotherapy for certain patients with nonmetastatic mismatch repair deficient colon cancer, a subtype that comprises about 15% of colon cancers and responds well to immune treatments.
  • A review of the literature identified 8 relevant studies out of 7691, focusing on safety and efficacy of this treatment, which included diverse agents and treatment durations.
  • Results showed high rates of complete surgical resection (98%-100%) and significant pathological response rates (50%-91% achieving ypT0N0), with manageable safety profiles as most adverse events were mild to moderate.

Article Abstract

Background: In April 2023, the National Comprehensive Cancer Network endorsed neoadjuvant immunotherapy for select patients with nonmetastatic mismatch repair deficient colon cancer. Approximately 15% of incident colon cancers are mismatch repair deficient, resulting in a distinct molecular subtype with high microsatellite instability that is responsive to immune checkpoint inhibition.

Objective: To describe the existing evidence supporting neoadjuvant immunotherapy for mismatch repair deficient, microsatellite unstable nonmetastatic colon cancer.

Data Sources: A medical librarian performed PubMed, Embase, and Web of Science searches most recently on April 24, 2023. The PubMed search was re-run on September 26, 2023, to identify any additional studies published between April 24 and September 26, 2023.

Study Selection: Two authors screened titles and abstracts in the published studies. The inclusion criteria were 1) English language, 2) adults with primary cancer of the colon, 3) nonmetastatic disease, 4) neoadjuvant immunotherapy, and 5) reporting on 10 or more cases.

Intervention: Neoadjuvant immunotherapy.

Main Outcome Measures: Safety (grade 3+ treatment-related adverse events) and efficacy (complete pathologic responses).

Results: From 7691 studies identified, 6370 were screened and 8 were included. Various agents, dosing regimens, and treatment durations were used, with durations of immunotherapy ranging from 1 to 16 cycles. Complete R0 resections were consistently achieved in 98% to 100% of resections. Of patients who received neoadjuvant immunotherapy and underwent resection, 50% to 91% had ypT0N0 pathology. The safety profiles were generally favorable, with grade 1 to 2 treatment-related adverse events (mostly immune-related) during immunotherapy reported in 22.2% to 70% of patients. Postoperative complications after neoadjuvant immunotherapy were reassuring, with no severe complications reported.

Limitations: Small number of heterogeneous and uncontrolled studies precluding a meta-analysis.

Conclusions: Neoadjuvant immune checkpoint inhibition is associated with high rates of pathologic complete responses in locally advanced colon cancer. The literature is limited, particularly for postoperative outcomes, and more studies are needed to understand the safety and positioning of these regimens in the neoadjuvant context.

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Source
http://dx.doi.org/10.1097/DCR.0000000000003263DOI Listing

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