Abstract
Human skin cells recognize the presence of the skin microbiome through pathogen recognition receptors. Epidermal keratinocytes are known to activate toll-like receptors (TLRs) 2 and 4 in response to the commensal Cutibacterium acnes (C. acnes, formerly known as Propionibacterium acnes) bacterium and subsequently to induce innate immune and inflammatory events. These events may lead to the appearance of macroscopic inflammatory acne lesions in puberty: comedos, papules and, pustules. Healthy skin does not exhibit inflammation or skin lesions, even in the continuous presence of the same microbes. As the molecular mechanism for this duality is still unclear, we aimed to identify factors and mechanisms that control the innate immune response to C. acnes in keratinocytes using a human immortalized keratinocyte cell line, HPV-KER, normal human keratinocytes (NHEK) and an organotypic skin model (OSM). TNIP1, a negative regulator of the NF-κB signaling pathway, was found to be expressed in HPV-KER cells, and its expression was rapidly induced in response to C. acnes treatment, which was confirmed in NHEK cells and OSMs. Expression changes were not dependent on the C. acnes strain. However, we found that the extent of expression was dependent on C. acnes dose. Bacterial-induced changes in TNIP1 expression were regulated by signaling pathways involving NF-κB, p38, MAPKK and JNK. Experimental modification of TNIP1 levels affected constitutive and C. acnes-induced NF-κB promoter activities and subsequent inflammatory cytokine and chemokine mRNA and protein levels. These results suggest an important role for this negative regulator in the control of bacterially induced TLR signaling pathways in keratinocytes. We showed that all-trans retinoic acid (ATRA) induced elevated TNIP1 expression in HPV-KER cells and also in OSMs, where TNIP1 levels increased throughout the epidermis. ATRA also reduced constitutive and bacterium-induced levels of TNFα, CCL5 and TLR2, while simultaneously increasing CXCL8 and TLR4 expression. Based on these findings, we propose that ATRA may exhibit dual effects in acne therapy by both affecting the expression of the negative regulator TNIP1 and attenuating TLR2-induced inflammation. Overall, TNIP1, as a possible regulator of C. acnes-induced innate immune and inflammatory events in keratinocytes, may play important roles in the maintenance of epidermal homeostasis.
Highlights
The human skin harbors a specialized microbiome, which plays an important role in the regulation and maintenance of epidermal homeostasis
We found that TNIP1 is expressed in HPV-KER cells and that mRNA expression rapidly and significantly increased after C. acnes 889 treatment (MOI = 100), reaching the maximum at 12– 24 h (Figure 1A)
These findings suggest that these cells recognize the presence of C. acnes bacterium
Summary
The human skin harbors a specialized microbiome, which plays an important role in the regulation and maintenance of epidermal homeostasis. Various members of the microbiome are important in the pathogenesis of several skin diseases, most of which lead to exaggerated innate immune and inflammatory events. Adaptive immune events are induced, leading to the activation of the Th1/Th17 pathway [11, 12] Overall, these events contribute to the induction of the characteristic inflammatory symptoms during disease pathogenesis in adolescents. The bacterium does not usually provoke immune activation and inflammation in keratinocytes and/or other immune cells This age-dependent response to C. acnes indicates different mechanisms controlling the downstream events induced by the bacterium
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