IL12Rβ1ΔTM Is a Secreted Product of<i>il12rb1</i>That Promotes Control of Extrapulmonary Tuberculosis

Ray, Aurélie; Fountain, Jeffrey J.; Miller, Halli E.; Cooper, Andrea M.; Robinson, Richard

doi:10.1128/iai.01230-13

Cited by 8 publications

(22 citation statements)

References 72 publications

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“…We have recently turned our attention to whether IL12Rβ1ΔTM also enhances IL12p40-dependent responses of T H cells, as T H cells must express il12rb1 to limit experimental tuberculosis (117). The results of these experiments are forthcoming, but are consistent with a model wherein IL12Rβ1ΔTM expression serves to potentiate mouse leukocytes’ responses to IL12 (163). …”

Section: Introductionsupporting

confidence: 75%

IL12Rβ1: The cytokine receptor that we used to know

Robinson

2015

Cytokine

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Human IL12RB1 encodes IL12Rβ1, a type I transmembrane receptor that is an essential component of the IL12- and IL23-signaling complex. IL12RB1 is well-established as being a promoter of delayed type hypersensitivity (DTH), the immunological reaction that limits tuberculosis. However, recent data demonstrate that in addition to promoting DTH, IL12RB1 also promotes autoimmunity. The contradictory roles of IL12RB1 in human health raises the question, what are the factors governing IL12RB1 function in a given individual, and how is inter-individual variability inIL12RB1 function introduced? Here we review recent data that demonstrate individual variability in IL12RB1 function is introduced at the epigenetic, genomic polymorphism, and mRNA splicing levels. Where and how these differences contribute to disease susceptibility and outcome are also reviewed. Collectively, recent data support a model whereinIL12RB1 sequence variability – whether introduced at the genomic or post-transcriptional level - contributes to disease, and that human IL12RB1 is not as simple agene as we once believed.

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Section: Introductionsupporting

confidence: 75%

IL12Rβ1: The cytokine receptor that we used to know

Robinson

2015

Cytokine

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“…Recently, it was shown that IL-12Rβ1ΔTM is a secreted product that promotes resistance to M. tuberculosis infection by potentiating T H cells response to IL-12 [50]. Ray and colleagues generated transgenic mice which do not express IL-12Rβ1ΔTM.…”

Section: Page 11 Of 36mentioning

confidence: 97%

“…Furthermore, the IL-12Rβ1ΔTM deficient mice had decreased numbers of M. tuberculosis induced T H 1 cells. The authors proposed a model where secreted IL-12Rβ1ΔTM enhances the stability and/or bioavailability of IL-12 [50]. In humans, IL-12Rβ1 deficiency is a rare autosomal recessive disorder characterized by predisposition to recurrent and/or severe infections caused by poorly pathogenic mycobacteria and salmonella [47,51].…”

Section: Page 11 Of 36mentioning

confidence: 99%

Insights into IL-23 biology: From structure to function

Floß

Schröder

Franke

et al. 2015

Cytokine & Growth Factor Reviews

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“…Dendritic cells in the lungs of Mtb-exposed mice produce not only IL-12p40 but also an alternative splice variant of IL-12Rβ1 which lacks the transmembrane domain and which we have called ΔTM-IL-12Rβ1 8 . This splice variant was identified when the receptor was first described 14 however its function was not appreciated until our studies in Mtb 8, 15 . The ΔTM-IL-12Rβ1 locates to the endoplasmic reticulum 16 and can be secreted by transfected cells and mitogen-activated T cells blasts 15 .…”

Section: Introductionmentioning

confidence: 99%

“…This splice variant was identified when the receptor was first described 14 however its function was not appreciated until our studies in Mtb 8, 15 . The ΔTM-IL-12Rβ1 locates to the endoplasmic reticulum 16 and can be secreted by transfected cells and mitogen-activated T cells blasts 15 . Human cells produce a similar splice variant of the IL12RB1 gene in response to Mtb exposure and this is referred to as isoform 2 8, 17 and has been shown to augment human T cell responsiveness to IL-12p70 18 .…”

Section: Introductionmentioning

confidence: 99%

Differential expression of an alternative splice variant of IL-12Rβ1 impacts early dissemination in the mouse and associates with disease outcome in both mouse and humans exposed to tuberculosis

Das

Cai

et al. 2018

Preprint

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Experimental mouse models of TB suggest that early events in the lung impact immunity. Early events in the human lung in response to TB are difficult to probe and their impact on disease outcome is unknown. We have shown in mouse that a secreted alternatively-spliced variant of IL-12Rβ1, lacking the transmembrane domain and termed ΔTM-IL-12Rβ1, promotes dendritic cell migration to the draining lymph node, augments T cell activation and limits dissemination of M. tuberculosis (Mtb). We show here that CBA/J and C3H/HeJ mice (both highly susceptible to Mtb) express higher levels of ΔTM-IL-12Rβ1 than resistant C57BL6 mice and limit early dissemination of Mtb from the lungs. Both CD11c+ cells and T cells express ΔTM-IL-12Rβ1 in humans, and mice unable to make ΔTM-IL-12Rβ1 in either CD4 or CD11c expressing cells permit early dissemination from the lung. Analysis of publically available blood transcriptomes indicates that pulmonary TB is associated with high ΔTM-IL-12Rβ1 expression and that of all IL-12 related signals, the ΔTM-IL-12Rβ1 signal best predicts active disease. ΔTM-IL-12Rβ1 expression reflects the heterogeneity of latent TB infection and has the capacity to discriminate between latent and active disease. In a new Chinese TB patient cohort, ΔTM-IL-12Rβ1 effectively differentiates TB from latent TB, healthy controls and pneumonia patients. Finally, ΔTM-IL-12Rβ1 expression drops in drug-treated individuals in the UK and China where infection pressure is low. We propose that ΔTM-IL-12Rβ1 regulates early dissemination from the lung and that it has diagnostic potential and provides mechanistic insights into human TB.

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IL12Rβ1ΔTM Is a Secreted Product ofil12rb1That Promotes Control of Extrapulmonary Tuberculosis

Cited by 8 publications

References 72 publications

IL12Rβ1: The cytokine receptor that we used to know

IL12Rβ1: The cytokine receptor that we used to know

Insights into IL-23 biology: From structure to function

Differential expression of an alternative splice variant of IL-12Rβ1 impacts early dissemination in the mouse and associates with disease outcome in both mouse and humans exposed to tuberculosis

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