B7.2-Ig fusion proteins enhance IL-4-dependent differentiation of tumor-sensitized CD8+ cytotoxic T lymphocyte precursors

doi:10.1093/intimm/dxh288

International Immunology Advance Access originally published online on July 18, 2005
International Immunology 2005 17(8):1071-1079; doi:10.1093/intimm/dxh288

This Article

	Full Text
	FREE Full Text (PDF)
	All Versions of this Article: 17/8/1071 most recent dxh288v1
	Alert me when this article is cited
	Alert me if a correction is posted

Services

	Email this article to a friend
	Similar articles in this journal
	Similar articles in ISI Web of Science
	Similar articles in PubMed
	Alert me to new issues of the journal
	Add to My Personal Archive
	Download to citation manager
	Request Permissions

Google Scholar

	Articles by Hiraoka, S.-i.
	Articles by Fujiwara, H.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Hiraoka, S.-i.
	Articles by Fujiwara, H.

Social Bookmarking

	What's this?

B7.2-Ig fusion proteins enhance IL-4-dependent differentiation of tumor-sensitized CD8⁺ cytotoxic T lymphocyte precursors

Shin-ichiro Hiraoka¹, Noritami Takeuchi¹, Yang Bian¹, Hirokazu Nakahara², Mikihiko Kogo², Kyriaki Dunussi-Joannopoulos³, Stanley Wolf³, Shiro Ono¹ and Hiromi Fujiwara¹

¹ Department of Oncology (C6), Graduate School of Medicine and ² First Department of Oral and Maxillo-facial surgery, Faculty of Dentistry, Osaka University, 2-2, Yamada-oka, Suita, Osaka 565-0871, Japan
³ Department of Inflammation, Wyeth Research, Cambridge, MA 02140, USA

Correspondence to: S. Ono; E-mail: sono{at}ongene.med.osaka-u.ac.jp

The B7/CD28 co-stimulatory pathway plays a critical role inT cell activation and differentiation. Our previous study demonstratedthat administration of B7.2-Ig fusion proteins to tumor-bearingmice elicits IL-4-dependent, CD8⁺ T cell-mediated tumor regression.Here, we investigated whether B7.2-Ig stimulation of tumor-sensitizedCD8⁺ CTL precursors during in vitro antigen re-sensitizationactually results in their differentiation into mature CTLs andif so, whether such a process depends on IL-4 signals. Splenocytesfrom tumor-sensitized (tumor-bearing or tumor-immunized) miceexhibited low levels of anti-tumor CTL responses upon culturingalone, but induced strikingly enhanced CTL responses when stimulatedin vitro with B7.2-Ig fusion proteins. Because CTLs were notgenerated from normal splenocytes even by B7.2-Ig stimulation,the expression of the B7.2-Ig effect required the in vivo tumorsensitization of CD8⁺ CTL precursors. Administration of anti-CD4or anti-CD40 ligand (CD40L) to mice before tumor sensitizationresulted in almost complete inhibition of CTL responses generatedin the subsequent culture containing B7.2-Ig. In contrast, anti-IL-4did not influence in vivo tumor sensitization required for CTLinduction. However, B7.2-Ig stimulation of tumor-sensitizedsplenocytes enhanced IL-4 production and neutralization of thisIL-4 with anti-IL-4 potently down-regulated CTL responses. Theseresults indicate that B7.2-Ig enhances IL-4-dependent differentiationof anti-tumor CD8⁺ CTL precursors that can be sensitized invivo depending on collaboration with CD4⁺ T cells involvingCD40L function.

Keywords: costimulation, Th1/Tc2, Th2/Tc2, tumor immunity, CD40L

Transmitting editor: A. Singer

Add to CiteULike CiteULike Add to Connotea Connotea Add to Del.icio.us Del.icio.us What's this?