Membrane-bound p35 Subunit of IL-12 on Tumor Cells is Functionally Equivalent to Membrane-bound Heterodimeric Single Chain IL-12 for Induction of Anti-tumor Immunity

Hyun-Jin Kim; Sang Min Park; Hayyoung Lee; Young Sang Kim

doi:10.4110/in.2016.16.5.305

Membrane-bound p35 Subunit of IL-12 on Tumor Cells is Functionally Equivalent to Membrane-bound Heterodimeric Single Chain IL-12 for Induction of Anti-tumor Immunity

Immune Netw. 2016 Oct;16(5):305-310. doi: 10.4110/in.2016.16.5.305. Epub 2016 Oct 25.

Authors

Hyun-Jin Kim¹, Sang Min Park¹, Hayyoung Lee², Young Sang Kim¹

Affiliations

¹ Department of Biochemistry, College of Natural Sciences, Chungnam National University, Daejeon 34134, Korea.
² Institute of Biotechnology, Chungnam National University, Daejeon 34134, Korea.

Abstract

In this study, we compared two different tumor cell vaccines for their induction of anti-tumor immunity; one was a tumor cell clone expressing a membrane-bound form of IL-12 p35 subunit (mbIL-12 p35 tumor clone), and the other was a tumor clone expressing heterodimeric IL-12 as a single chain (mb-scIL-12 tumor clone). The stimulatory effect of mb-scIL-12 on the proliferation of ConA-activated splenocytes was higher than that of mbIL-12 p35 in vitro. However, the stimulatory effect of mbIL-12 p35 was equivalent to that of recombinant soluble IL-12 (3 ng/ml). Interestingly, both tumor clones (mbIL-12 p35 and mb-scIL-12) showed similar tumorigenicity and induction of systemic anti-tumor immunity in vivo, suggesting that tumor cell expression of the membrane-bound p35 subunit is sufficient to induce anti-tumor immunity in our tumor vaccine model.

Keywords: Anti-tumor immunity; Cytokine gene therapy; Interleukin-12; Membrane-bound form.