Journal of Translational Medicine (Nov 2006)

In vivo migration of labeled autologous natural killer cells to liver metastases in patients with colon carcinoma

  • Satolli Maria A,
  • Stacchini Alessandra,
  • Castellano Giancarlo,
  • Chiappino Isabella,
  • Baiocco Cinzia,
  • Bello Marilena,
  • Galetto Alessandra,
  • Matera Lina,
  • Mele Michele,
  • Sandrucci Sergio,
  • Mussa Antonio,
  • Bisi Gianni,
  • Whiteside Theresa L

DOI
https://doi.org/10.1186/1479-5876-4-49
Journal volume & issue
Vol. 4, no. 1
p. 49

Abstract

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Abstract Background Besides being the effectors of native anti-tumor cytotoxicity, NK cells participate in T-lymphocyte responses by promoting the maturation of dendritic cells (DC). Adherent NK (A-NK) cells constitute a subset of IL-2-stimulated NK cells which show increased expression of integrins and the ability to adhere to solid surface and to migrate, infiltrate, and destroy cancer. A critical issue in therapy of metastatic disease is the optimization of NK cell migration to tumor tissues and their persistence therein. This study compares localization to liver metastases of autologous A-NK cells administered via the systemic (intravenous, i.v.) versus locoregional (intraarterial, i.a.) routes. Patients and methods A-NK cells expanded ex-vivo with IL-2 and labeled with 111In-oxine were injected i.a. in the liver of three colon carcinoma patients. After 30 days, each patient had a new preparation of 111In-A-NK cells injected i.v. Migration of these cells to various organs was evaluated by SPET and their differential localization to normal and neoplastic liver was demonstrated after i.v. injection of 99mTc-phytate. Results A-NK cells expressed a donor-dependent CD56+CD16+CD3- (NK) or CD56+CD16+CD3+ (NKT) phenotype. When injected i.v., these cells localized to the lung before being visible in the spleen and liver. By contrast, localization of i.a. injected A-NK cells was virtually confined to the spleen and liver. Binding of A-NK cells to liver neoplastic tissues was observed only after i.a. injections. Conclusion This unique study design demonstrates that A-NK cells adoptively transferred to the liver via the intraarterial route have preferential access and substantial accumulation to the tumor site.