Differential microRNA profile underlies the divergent healing responses in skin and oral mucosal wounds

Simões, Alyne; Chen, Lin; Chen, Zujian; Zhao, Yan; Gao, Shang; Marucha, Phillip T.; Dai, Yang; DiPietro, Luisa A.; Zhou, Xiaofeng

doi:10.1038/s41598-019-43682-w

Cited by 32 publications

(61 citation statements)

References 48 publications

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“…One of our important observations is that more piRNA genes were differentially expressed in skin wounds than in oral mucosal wounds. This is in agreement with our previous observations showing that nearly twice as many protein-coding genes and six times as many microRNA genes are differentially expressed in the skin wounds than in mucosal wounds [2,3]. Collectively, these observations imply that, as compared to the skin, the oral mucosa has an intrinsic genetic/epigenetic controlling program that makes it be highly adaptable to the accelerated healing upon injury.…”

Section: Discussionsupporting

confidence: 92%

“…In this study, we present the first tissue-specific piRNA profiles in corresponding skin and oral mucosal wounds. Together with our previous study that established the tissue-specific transcriptome and microRNAome of matching skin and mucosal wounds [2,3], we demonstrated striking differences in the transcribed genome (transcriptome, microRNAome, and piRNAome) of oral mucosal and skin wounds. Along with studies by others [4,29], our results suggest that the intrinsic differences in the genetic and epigenetic responses to injury in the skin and mucosa contribute to the divergent wound healing outcomes.…”

Section: Discussionsupporting

confidence: 76%

“…The expression of piRNA genes in the normal murine uninjured skin and oral mucosal epithelium (baseline) was explored by re-analyzing of our previous small-RNA seq data [3], and mapping to the piRNA database. A total of 20,862,850 and 3,769,588 sequence reads were mapped to 1084 and 1103 unique piRNAs for skin and oral mucosa, respectively.…”

Section: High Levels Of Pirna Presented In Skin and Oral Mucosa Epithmentioning

confidence: 99%

“…Oral mucosal wound healing has long been considered an optimal wound resolution and is characterized by rapid and scarless healing. Recent comparative studies focusing on differential molecular characterization of the skin and oral mucosa have revealed that the intrinsic molecular differences in skin and oral mucosa contribute to the divergent wound healing outcomes [2][3][4]. This novel approach defines critical molecular regulators involved in accelerated wound healing and allows the harnessing of regenerative healing capabilities in oral mucosa to treat deficient healing processes.…”

Section: Introductionmentioning

confidence: 99%

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Site-Specific Expression Pattern of PIWI-Interacting RNA in Skin and Oral Mucosal Wound Healing

Lin

Chen

Simões

et al. 2020

IJMS

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The oral mucosa exhibits exceptional healing capability when compared to skin. Recent studies suggest that intrinsic differences in coding genes and regulatory small non-coding RNA (sncRNA) genes (e.g., microRNAs) may underlie the exceptional healing that occurs in the oral mucosa. Here, we investigate the role of a novel class of sncRNA—Piwi-interacting RNA (piRNA)—in the tissue-specific differential response to injury. An abundance of piRNAs was detected in both skin and oral mucosal epithelium during wound healing. The expression of PIWI genes (the obligate binding partners of piRNAs) was also detected in skin and oral wound healing. This data suggested that PIWI-piRNA machinery may serve an unknown function in the highly orchestrated wound healing process. Furthermore, unique tissue-specific piRNA profiles were obtained in the skin and oral mucosal epithelium, and substantially more changes in piRNA expression were observed during skin wound healing than oral mucosal wound healing. Thus, we present the first clue suggesting a role of piRNA in wound healing, and provide the first site-specific piRNA profile of skin and oral mucosal wound healing. These results serve as a foundation for the future investigation of the functional contribution(s) of piRNA in wound repair and tissue regeneration.

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Section: Discussionsupporting

confidence: 92%

Section: Discussionsupporting

confidence: 76%

Section: High Levels Of Pirna Presented In Skin and Oral Mucosa Epithmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Site-Specific Expression Pattern of PIWI-Interacting RNA in Skin and Oral Mucosal Wound Healing

Lin

Chen

Simões

et al. 2020

IJMS

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“…The skin and oral mucosa share some histological similarities, yet oral mucosal wounds heal with faster re-epithelialization, decreased inflammation, a refined angiogenic response, and minimal scarring [3][4][5][6][7]. Our most recent studies demonstrate that microRNA 10a/b, 21, and 31 may be partially responsible for the different outcomes observed in skin and oral wound healing [27,28]. Although these findings have been well characterized, the precise mechanisms behind the more regenerative response to injury in the oral cavity is still being elucidated.…”

Section: Discussionmentioning

confidence: 90%

Differential Expression and Function of Bicellular Tight Junctions in Skin and Oral Wound Healing

Leonardo

Shi

Chen

et al. 2020

IJMS

Self Cite

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Bicellular tight junctions are multiprotein complexes that are required for maintenance of barrier function and fence function in epithelial tissues. Wound healing in the oral cavity leads to minimal scar formation compared to the skin, and the precise mechanisms for this regenerative response remain to be elucidated. We hypothesized that oral and skin tissues express a different tight junction repertoire both at baseline and during the wound healing response, and that these molecules may be critical to the differential repair between the two tissues. We re-analyzed a mouse skin and palate epithelium microarray dataset to identify the tight junction repertoire of these tissue types. We then re-analyzed a skin and tongue wound healing microarray dataset to see how expression levels of tight junction genes change over time in response to injury. We performed in vitro scratch assays on human oral and skin keratinocyte cell lines to assay for tight junction expression over time, tight junction expression in response to lipopolysaccharide and histamine treatment, and the effects of siRNA knockdown of claudin 1 or occludin on migration and proliferation. Our data showed that oral and skin epithelium expressed different tight junction genes at baseline and during the wound healing response. Knockdown of claudin 1 or occludin led to changes in proliferation and migration in human skin keratinocytes but not oral keratinocytes. Furthermore, we also showed that skin keratinocytes were more permeable than oral keratinocytes upon histamine treatment. In conclusion, this study highlights a specific subset of functional tight junction genes that are differentially expressed between the oral and skin tissues, which may contribute to the mechanisms leading to distinct healing phenotypes in response to injury in the two tissues.

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Effects of Mesenchymal Stem Cell‐Derived Paracrine Signals and Their Delivery Strategies

Chang

Yan

Yao

et al. 2021

Adv Healthcare Materials

114

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Mesenchymal stem cells (MSCs) have been widely studied as a versatile cell source for tissue regeneration and remodeling due to their potent bioactivity, which includes modulation of inflammation response, macrophage polarization toward proregenerative lineage, promotion of angiogenesis, and reduction in fibrosis. This review focuses on profiling the effects of paracrine signals of MSCs, commonly referred to as the secretome, and highlighting the various engineering approaches to tune the MSC secretome. Recent advances in biomaterials‐based therapeutic strategies for delivery of MSCs and MSC‐derived secretome in the form of extracellular vesicles are discussed, along with their advantages and challenges.

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Differential microRNA profile underlies the divergent healing responses in skin and oral mucosal wounds

Cited by 32 publications

References 48 publications

Site-Specific Expression Pattern of PIWI-Interacting RNA in Skin and Oral Mucosal Wound Healing

Site-Specific Expression Pattern of PIWI-Interacting RNA in Skin and Oral Mucosal Wound Healing

Differential Expression and Function of Bicellular Tight Junctions in Skin and Oral Wound Healing

Effects of Mesenchymal Stem Cell‐Derived Paracrine Signals and Their Delivery Strategies

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