Secondary Response to Listeria Infection Requires IFN-gamma but is Partially Independent of IL-12

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 1995 Oct 1

PMID 7561037

Citations 20

Authors

C S Tripp

O Kanagawa

E R UNANUE

Affiliations

Soon will be listed here.

Abstract

During a secondary immune response to Listeria monocytogenes (LM), the production of IFN-gamma was still required for resistance, but it was considerably less dependent on IL-12 production. When IL-12 was neutralized in vivo using specific hamster antimurine IL-12 mAbs, there was a dramatically increased susceptibility to infection during primary listeriosis but much less during a secondary infection. However, neutralization of IFN-gamma in vivo resulted in a similar increased susceptibility during both primary and secondary listeriosis. In culture, splenocytes isolated from unimmunized mice produced IFN-gamma in response to heat-killed L. monocytogenes (hk-LM) that was absolutely dependent upon IL-12 production. However, directly stimulating the TCR with anti-CD3-epsilon mAbs resulted in IFN-gamma production that was unaffected by neutralizing IL-12 in vitro. In contrast, splenocytes isolated from LM-immune mice produced IFN-gamma in response to hk-LM, part of which was independent on IL-12 production. However, anti-CD3-epsilon Ab-stimulated IFN-gamma production remained independent of IL-12 production. The source of hk-LM-induced, IL-12-independent IFN-gamma production was the T cell because anti-Thy1.2 Ab plus complement treatment in vitro completely abolished it. Together, these data support a model of memory T cells being produced during the primary infection with LM that can be stimulated to produce IFN-gamma during the secondary response to LM, partially independent of macrophage IL-12 production.

Citing Articles

Intestinal cDC1s provide cues required for CD4+ T cell-mediated resistance to Cryptosporidium.

Cohn I, Wallbank B, Haskins B, ODea K, Pardy R, Shaw S J Exp Med. 2024; 221(7).

PMID: 38829369 PMC: 11148471. DOI: 10.1084/jem.20232067.

Intestinal cDC1s provide IL-12 dependent and independent functions required for CD4 T cell-mediated resistance to .

Cohn I, Wallbank B, Haskins B, ODea K, Pardy R, Shaw S bioRxiv. 2023; .

PMID: 38014026 PMC: 10680586. DOI: 10.1101/2023.11.11.566669.

IFN-Gamma-Dependent and Independent Mechanisms of CD4⁺ Memory T Cell-Mediated Protection from Listeria Infection.

Meek S, Williams M Pathogens. 2018; 7(1).

PMID: 29438281 PMC: 5874748. DOI: 10.3390/pathogens7010022.

Ikaros imposes a barrier to CD8+ T cell differentiation by restricting autocrine IL-2 production.

OBrien S, Thomas R, Wertheim G, Zhang F, Shen H, Wells A J Immunol. 2014; 192(11):5118-29.

PMID: 24778448 PMC: 4042307. DOI: 10.4049/jimmunol.1301992.

Distinct subunit pairing criteria within the heterodimeric IL-12 cytokine family.

Jones L, Chaturvedi V, Uyttenhove C, Van Snick J, Vignali D Mol Immunol. 2012; 51(2):234-44.

PMID: 22487722 PMC: 3341524. DOI: 10.1016/j.molimm.2012.03.025.