Cell type-specific targeting dissociates the therapeutic from the adverse effects of protein kinase inhibition in allergic skin disease

Ritprajak, Patcharee; Hayakawa, Morisada; Sano, Yasuyo; Otsu, Kinya; Park, Jin Mo

doi:10.1073/pnas.1202984109

Cited by 22 publications

(27 citation statements)

References 28 publications

(22 reference statements)

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“…Importantly, despite the diversity of cell types where p38 MAPK plays a role, its effects in all of the cell types studied to date in EAE are unidirectionally propathogenic. This is in contrast to other immune-mediated models of inflammation, where emerging evidence points to potential anti-inflammatory roles for this kinase (62)(63)(64), which may explain the lack of efficacy of p38 MAPK inhibitors in treating rheumatoid arthritis (RA) and Crohn's disease (see below).…”

Section: Conclusion and Potential Therapeutic Perspectivesmentioning

confidence: 74%

The Emerging Role of p38 Mitogen-Activated Protein Kinase in Multiple Sclerosis and Its Models

Krementsov

Thornton

Teuscher

et al. 2013

Molecular and Cellular Biology

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Multiple sclerosis (MS), the most common disabling neurologic disease of young adults, is considered a classical T cell-mediated disease and is characterized by demyelination, axonal damage, and progressive neurological dysfunction. The currently available disease-modifying therapies are limited in their efficacy, and improved understanding of new pathways contributing to disease pathogenesis could reveal additional novel therapeutic targets. The p38 mitogen-activated protein kinase (MAPK) signaling pathway is known to be triggered by stress stimuli and to contribute to inflammatory responses. Importantly, a number of recent studies have identified this signaling pathway as a central player in MS and its principal animal model, experimental allergic encephalomyelitis. Here, we review the evidence from mouse and human studies supporting the role of p38 MAPK in regulating key immunopathogenic mechanisms underlying autoimmune inflammatory disease of the central nervous system and the potential of targeting this pathway as a disease-modifying therapy in MS. PATHOGENESIS OF MULTIPLE SCLEROSIS

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Section: Conclusion and Potential Therapeutic Perspectivesmentioning

confidence: 74%

The Emerging Role of p38 Mitogen-Activated Protein Kinase in Multiple Sclerosis and Its Models

Krementsov

Thornton

Teuscher

et al. 2013

Molecular and Cellular Biology

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“…Nevertheless, the involvement of the non‐epithelial cell‐derived p38δ in skin tumorigenesis cannot be excluded, since p38δ is expressed in many cell types, including immune, endothelial, and mesenchymal cells (reviewed in ), interplay of which with epithelial cells is known to be of key importance for tumor development and progression . Importantly, studies targeting p38α isoform in distinct cell types have revealed cell type‐specific effects of p38α loss on inflammatory and allergic responses in skin, and on inflammatory bowel disease . The effects of keratinocyte‐specific and myeloid cell‐specific p38δ loss on distinct stages of chemical skin carcinogenesis are under investigation in our laboratory.…”

Section: Discussionmentioning

confidence: 99%

Keratinocyte p38δ loss inhibits Ras-induced tumor formation, while systemic p38δ loss enhances skin inflammation in the early phase of chemical carcinogenesis in mouse skin

et al. 2015

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p38δ expression and/or activity are increased in human cutaneous malignancies, including invasive squamous cell carcinoma (SCC) and head and neck SCC, but the role of p38δ in cutaneous carcinogenesis has not been well-defined. We have reported that mice with germline loss of p38δ exhibited a reduced susceptibility to skin tumor development compared with wild-type mice in the two-stage 7,12-dimethylbenz(a)anthracene (DMBA)/12-O-tetradecanoylphorbol-13-acetate (TPA) chemical skin carcinogenesis model. Here, we report that p38δ gene ablation inhibited the growth of tumors generated from v-ras(Ha) -transformed keratinocytes in skin orthografts to nude mice, indicating that keratinocyte-intrinsic p38δ is required for Ras-induced tumorigenesis. Gene expression profiling of v-ras(Ha) -transformed p38δ-null keratinocytes revealed transcriptional changes associated with cellular responses linked to tumor suppression, such as reduced proliferation and increased differentiation, cell adhesion, and cell communications. Notably, a short-term DMBA/TPA challenge, modeling the initial stages of chemical skin carcinogenesis treatment, elicited an enhanced inflammation in p38δ-null skin compared with skin of wild-type mice, as assessed by measuring the expression of pro-inflammatory cytokines, including IL-1β, IL-6, IL-17, and TNFα. Additionally, p38δ-null skin and p38δ-null keratinocytes exhibited increased p38α activation and signaling in response to acute inflammatory challenges, suggesting a role for p38α in stimulating the elevated inflammatory response in p38δ-null skin during the initial phases of the DMBA/TPA treatment compared with similarly treated p38δ(+/+) skin. Altogether, our results indicate that p38δ signaling regulates skin carcinogenesis not only by keratinocyte cell-autonomous mechanisms, but also by influencing the interaction between between the epithelial compartment of the developing skin tumor and its stromal microenvironment.

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“…Moreover, CKO studies have shown that deletion of p38a in different cell types can have opposing effects on inflammation and disease outcome [17,[19][20][21]. In fact, deletion of p38a in macrophages/ myeloid cells aggravated skin inflammation [17,20] and experimental arthritis [18]. Moreover, we have shown in a mouse model of MS, an autoimmune inflammatory disease of the CNS-that deletion of p38a in myeloid cells can either exacerbate or ameliorate disease in a sex-specific fashion [22].…”

Section: Introductionmentioning

confidence: 86%

“…Taken together, these results suggest that cell-specific targeting of p38a in myeloid cells may have therapeutic potential in treating colitis and possibly other inflammatory diseases, particularly if combined with restoration of IL-10 levels. In contrast, deletion of p38a in myeloid cells can aggravate skin inflammation [17,20], experimental arthritis [18], and autoimmune CNS inflammation [22], suggesting that perhaps protective functions of myeloid p38a are colitis specific. This notion is supported by the exquisite sensitivity of colitis to the absence of IL-10 and the critical requirement for IL-10 to maintain normal intestinal homeostasis [50,53,54].…”

Section: Deletion Of Myeloid P38a In the Absence Of Il-10 Is Protectimentioning

confidence: 99%

“…Emerging studies describe a noncanonical role for p38a in dampening, rather than promoting inflammation, potentially via induction of autoinhibitory-feedback mechanisms involving dualspecificity phosphatase 1 and/or immune-suppressive cytokines, such as IL-10 [15][16][17][18], although the functional contribution of these pathways has not been formally demonstrated. Moreover, CKO studies have shown that deletion of p38a in different cell types can have opposing effects on inflammation and disease outcome [17,[19][20][21]. In fact, deletion of p38a in macrophages/ myeloid cells aggravated skin inflammation [17,20] and experimental arthritis [18].…”

Section: Introductionmentioning

confidence: 99%

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Anti-inflammatory roles of p38α MAPK in macrophages are context dependent and require IL-10

Raza

Crothers

McGill

et al. 2017

Journal of Leukocyte Biology

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The p38 MAPK pathway was originally identified as a master regulator of proinflammatory cytokine production by myeloid cells. Numerous drugs targeting this kinase showed promise in preclinical models of inflammatory disease, but so far, none have shown efficacy in clinical trials. The reasons behind this are unclear, but may, in part, be explained by emerging anti-inflammatory functions of this kinase or overly refined selectivity of second-generation pharmacologic inhibitors. Here, we show that p38α signaling in macrophages plays pro- and anti-inflammatory functions in vivo and in vitro, with the outcome depending on the stimulus, output, kinetics, or mode of kinase inhibition (genetic vs. pharmacologic). Different pharmacologic inhibitors of p38 exhibit opposing effects, with second-generation inhibitors acting more specifically but inhibiting anti-inflammatory functions. Functionally, we show that the anti-inflammatory functions of p38α in macrophages are critically dependent on production of IL-10. Accordingly, in the absence of IL-10, inhibition of p38α signaling in macrophages is protective in a spontaneous model of colitis. Taken together, our results shed light on the limited clinical efficacy of drugs targeting p38 and suggest that their therapeutic efficacy can be significantly enhanced by simultaneous modulation of p38-dependent anti-inflammatory mediators, such as IL-10.

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Cell type-specific targeting dissociates the therapeutic from the adverse effects of protein kinase inhibition in allergic skin disease

Cited by 22 publications

References 28 publications

The Emerging Role of p38 Mitogen-Activated Protein Kinase in Multiple Sclerosis and Its Models

The Emerging Role of p38 Mitogen-Activated Protein Kinase in Multiple Sclerosis and Its Models

Keratinocyte p38δ loss inhibits Ras-induced tumor formation, while systemic p38δ loss enhances skin inflammation in the early phase of chemical carcinogenesis in mouse skin

Anti-inflammatory roles of p38α MAPK in macrophages are context dependent and require IL-10

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