The Central Memory CD4+ T Cell Population Generated during<i>Leishmania major</i>Infection Requires IL-12 to Produce IFN-γ

Pakpour, Nazzy; Zaph, Colby; Scott, Phillip

doi:10.4049/jimmunol.180.12.8299

Cited by 58 publications

(54 citation statements)

References 45 publications

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“…Central memory CD4 + T cell population generated during L. major infection is capable of developing into either Th1 or Th2 effectors. Under the influence of IL-12, Leishmania specific central memory CD4 + T cells get differentiated into IFN-producing Th1 cells (Pakpour et al, 2008). Low dose L. major promotes a transient Th2 response that is downregulated by IFN-producing CD8 + T cells which may contribute to rapid resolution of secondary lesions (Uzonna et al, 2004;Wang et al, 1993).…”

Section: Central Versus Effector Memory Cellsmentioning

confidence: 99%

Dynamicity of Immune Regulation during Visceral Leishmaniasis

Asad¹,

Ali²

2014

Proceedings of the Indian National Science Academy

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Section: Central Versus Effector Memory Cellsmentioning

confidence: 99%

Dynamicity of Immune Regulation during Visceral Leishmaniasis

Asad¹,

Ali²

2014

Proceedings of the Indian National Science Academy

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“…IL 12 promotes a T H 1 response in a mouse of model of CL for long-term immunity. 85,86 Consistent with this concept, inclusion of IL-12 as part of a DNA vaccine cocktail improved protection against L major challenge. [87][88][89] However, administration of IL-12 in humans is toxic; thus, this strategy is not suitable for human vaccination.…”

mentioning

confidence: 50%

“…Adjuvants improve the efficacy of Leishmania vaccine candidates by triggering high levels of IL-12 and IFN-γ expression, both of which play vital roles in long-term immunological memory. 85,86,96 The TLR7 agonist Aldara and TLR9 agonist CpG DNA exhibited therapeutic antileishmanial properties (reviewed in the study by Raman et al 97 ). In contrast, TLR2 agonist Pam3CSK4 led to conflicting results depending on the mouse model used.…”

Section: Targeting Tlrs For Vaccine Developmentmentioning

confidence: 99%

Cutaneous Leishmaniasis: Update on Vaccine Development

Zufferey¹,

Whyte²

2017

HPD

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ABSTRACT:Leishmaniasis is an important disease mediated by the protozoan parasite Leishmania via the bite of the female sandfly insect vector. Leishmaniasis is endemic in the tropical and subtropical regions. The most common form of the disease is cutaneous leishmaniasis, which affects more than 10 million people worldwide and includes at least 1.5 million new cases every year. So far, treatment of the disease relies on unsatisfactory chemotherapy that can be complicated by the rising appearance of drug-resistant parasites. Furthermore, it is challenging to achieve solid control of the insect vector and animal reservoir. Therefore, the development of a safe and effective vaccine is urgently needed for the treatment and prevention of leishmaniasis. This review focuses on the recent advances in the development of a safe vaccine that could be used for prevention and treatment of cutaneous leishmaniasis. A short outlook for future research efforts is also presented.

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“…IL-10 auto-regulates Th1 cell production of IFNc directly or indirectly through modulation of macrophage function effector cytokine production from both Th1 and Th2 effector cells by enhancing T-cell expression of the costimulatory molecule ICOS [33]. More recently, IL-12 has been implicated in driving IFNc production from central memory T cells [34], a subset of memory cells that can confer long-term immunity to L. major in the absence of persistent parasites [35]. For Th2 cells, continued expression of GATA3 expression appears critical for high-level cytokine production by Th2 effectors [36].…”

Section: Signals For Cd4 Effector Functionmentioning

confidence: 98%

Regulation of immunity at tissue sites of inflammation

et al. 2009

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The acquisition and execution of CD4 effector function are tightly regulated and spatially compartmentalized. In the lymph node (LN), naïve CD4+ T cells acquire specialized functions by means of expression of distinct cytokines and acquire distinct homing properties. Therefore, both the function and subsequent localization of effector cells appears to be predetermined during differentiation in the LN. Our studies with the protozoa Leishmania major suggest that this centrally (LN) generated effector repertoire can be further edited at the infected tissue site. Cytokine production in the inflamed tissue can be modulated at a number of levels including chemokine-driven differential recruitment of effector cells, the provision of signals for effector cell function and suppression by regulatory T cells (Tregs). The concept that tissue resident pathogens may subvert the centrally generated cytokine repertoire has important therapeutic implications. Novel therapies that focus on manipulating the local infection site to encourage appropriate recruitment or activation of effectors may be particularly beneficial.

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The Central Memory CD4+ T Cell Population Generated duringLeishmania majorInfection Requires IL-12 to Produce IFN-γ

Cited by 58 publications

References 45 publications

Dynamicity of Immune Regulation during Visceral Leishmaniasis

Dynamicity of Immune Regulation during Visceral Leishmaniasis

Cutaneous Leishmaniasis: Update on Vaccine Development

Regulation of immunity at tissue sites of inflammation

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