Recent insights into the role of dipeptidyl aminopeptidase IV (DPIV) and aminopeptidase N (APN) families in immune functions

Ansorge, Siegfried; Bank, Ute; Heimburg, Anke; Helmuth, Martin; G, Koch; Tadje, Janine; Lendeckel, Uwe; Wolke, Carmen; Neubert, Klaus; Faust, Jürgen; Fuchs, Petra; Reinhold, Dirk; Thielitz, Anja; Täger, Michael

doi:10.1515/cclm.2009.063

Cited by 66 publications

(43 citation statements)

References 29 publications

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“…Considering that DPP IV/CD26 is a member of a large S9b family of structurally homologous serine proteases that possess a unique catalytic activity, and since two recent studies have demonstrated a broad tissue distribution of DPP IV-like enzyme activity in both wild type and CD26 -/-, a possible explanation of results obtained in our study could be that other DPP IV-like protease are involved in the activation of the inflammatory response in animal model of colitis (Ansorge et al, 2009;Yu et al, 2009). Furthermore, it was recently demonstrated by Yazbeck and its coworkers (Yazbeck et al, 2008) that inhibition of DPP-like activity ameliorates the severity of inflammation in experimental colitis in mice.…”

Section: Dpp Iv/cd26 and Dpp Iv/cd26-like Activity In Dss-colitissupporting

confidence: 62%

Role of Dipeptidyl Peptidase IV/CD26 in Inflammatory Bowel Disease

Detel¹,

Pučar²,

Pugel³

et al. 2012

Inflammatory Bowel Disease - Advances in Pathogenesis and Management

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Section: Dpp Iv/cd26 and Dpp Iv/cd26-like Activity In Dss-colitissupporting

confidence: 62%

Role of Dipeptidyl Peptidase IV/CD26 in Inflammatory Bowel Disease

Detel¹,

Pučar²,

Pugel³

et al. 2012

Inflammatory Bowel Disease - Advances in Pathogenesis and Management

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“…It was reported in 2009 that a new inhibitor for both CD26 and APN was developed for the treatment of inflammatory skin diseases and recruited to a clinical phase II study [8]. On the other hand, the effects of DPP-IV inhibitors on the immune system have not been extensively investigated.…”

Section: Introductionmentioning

confidence: 99%

Sitagliptin, a Dipeptidyl Peptidase-IV Inhibitor, Improves Psoriasis

Nishioka¹,

Shinohara²,

Tanimoto³

et al. 2011

Dermatology

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A patient with a 17-year history of plaque psoriasis accompanied by type 2 diabetes mellitus discontinued cyclosporine and steroid ointment given for treatment of psoriasis because she was dissatisfied with the effects of the drugs. After sitagliptin, a dipeptidyl peptidase-IV (DPP-IV) inhibitor, was administered for control of blood glucose, psoriatic skin lesions were gradually diminished, although HbA1c did not improve. Three months after the administration of sitagliptin, infiltration, scales and erythema on all psoriatic plaques disappeared, leaving pigmentation on flat skin. DPP-IV in serum degrades the incretin hormones which stimulate β-cell insulin secretion. DPP-IV inhibitors, as incretin enhancers, cause an increase in glucose-dependent insulin secretion, and are applied for the treatment of diabetes mellitus. DPP-IV is also expressed on T cells as CD26, a surface antigen which plays an important role in activating T cells. As helper T cells are involved in the pathogenesis of psoriasis, it is possible that DPP-IV inhibitors improve psoriatic skin lesions by inhibiting T cell activation, independently of glycemic control. DPP-IV inhibitors could be an alternative for the treatment of psoriasis.

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“…CD26 is proposed to function as a keratinocyte activation antigen (Novelli et al, 1996). Moreover, CD26 inhibitors, currently used to manage type-2 diabetes, are being evaluated as treatments for psoriasis (Ansorge et al, 2009). CD26 is expressed in the differentiating epidermal layers and thus the upregulation in InvEE transgenic mice is correlated with the increased number of differentiated cell layers.…”

Section: Discussionmentioning

confidence: 99%

Upregulation of CD26 expression in epithelial cells and stromal cells during wound-induced skin tumour formation

et al. 2011

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We have previously described InvEE transgenic mice in which non-dividing, differentiating epidermal cells express oncogenically activated MAPK kinase 1 (MEK1). Skin wounding triggers tumour formation in InvEE mice via a mechanism that involves epidermal release of IL-1a and attraction of a pro-tumorigenic inflammatory infiltrate. To look for potential effects on the underlying connective tissue, we screened InvEE and wild-type epidermis for differential expression of cytokines and immune modulators. We identified a single protein, CD26 (dipeptidyl peptidase-4). CD26 serum levels were not increased in InvEE mice. In contrast, CD26 was upregulated in keratinocytes expressing mutant MEK1 and in the epithelial compartment of InvEE tumours, where it accumulated at cell-cell borders. CD26 expression was increased in dermal fibroblasts following skin wounding but was downregulated in tumour stroma. CD26 activity was stimulated by calcium-induced intercellular adhesion in keratinocytes, suggesting that the upregulation of CD26 in InvEE epidermis is due to expansion of the differentiated cell layers. IL-1a treatment of dermal fibroblasts stimulated CD26 activity, and therefore epidermal IL-1a release may contribute to the upregulation of CD26 expression in wounded dermis. Pharmacological blockade of CD26, via Sitagliptin, reduced growth of InvEE tumours, while combined inhibition of IL-1a and CD26 delayed tumour onset and reduced tumour incidence. Our results demonstrate that inappropriate activation of MEK1 in the epidermis leads to changes in dermal fibroblasts that, like the skin inflammatory infiltrate, contribute to tumour formation.

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Recent insights into the role of dipeptidyl aminopeptidase IV (DPIV) and aminopeptidase N (APN) families in immune functions

Cited by 66 publications

References 29 publications

Role of Dipeptidyl Peptidase IV/CD26 in Inflammatory Bowel Disease

Role of Dipeptidyl Peptidase IV/CD26 in Inflammatory Bowel Disease

Sitagliptin, a Dipeptidyl Peptidase-IV Inhibitor, Improves Psoriasis

Upregulation of CD26 expression in epithelial cells and stromal cells during wound-induced skin tumour formation

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