Early cutaneous inflammatory response at different degree of burn and its significance for clinical diagnosis and management

Priyanka Shaw; Ajay Kumar Sharma; Aman Kalonia; Amit Shukla; Rishav Kumar; Kirti; Sandeep Kumar Shukla

doi:10.1016/j.jtv.2023.06.011

Early cutaneous inflammatory response at different degree of burn and its significance for clinical diagnosis and management

J Tissue Viability. 2023 Nov;32(4):550-563. doi: 10.1016/j.jtv.2023.06.011. Epub 2023 Jul 1.

Authors

Priyanka Shaw¹, Ajay Kumar Sharma¹, Aman Kalonia¹, Amit Shukla², Rishav Kumar¹, Kirti¹, Sandeep Kumar Shukla³

Affiliations

¹ Molecular and Radiation Biosciences, Institute of Nuclear Medicine & Allied Sciences, Defence Research and Development Organization, Lucknow Road, Timarpur, New Delhi, 110054, India.
² Department of Pharmacology and Toxicology, College of Veterinary Science and Animal Husbandry, UP Pandit Deen Dayal Upadhyaya Pashu Chikitsa Vigyan Vishwavidyalaya Evam Go-Anusandhan Sansthan (DUVASU), Mathura, 281001, India.
³ Molecular and Radiation Biosciences, Institute of Nuclear Medicine & Allied Sciences, Defence Research and Development Organization, Lucknow Road, Timarpur, New Delhi, 110054, India. Electronic address: sandeepshukla.inmas@gov.in.

PMID: 37414707
DOI: 10.1016/j.jtv.2023.06.011

Abstract

A complete characterization of the burn wound based on cutaneous architectural changes and inflammatory response is extremely important to provide evidence for progressive changes in the burn wound. Burn wounds are highly susceptible to conversion into deeper wounds, which need special care and attention; thereby, the complete characterization of burn wound type and their subsequent inflammatory status in the cutaneous system at the earliest is of paramount importance. Inflammatory markers at different degrees will help clinicians devise better and more specific treatment strategies for each burn type. The present study is carried out to profile pro-inflammatory gene expression along with immune cell quantification, vascular perfusion, and histopathological assessment in the cutaneous system of murine models. The study revealed that burn injury caused an immediate increase in vascular perfusion in superficial and partial-thickness burns, whereas there was a decrease in vascular perfusion in full-thickness burns. An influx of lymphocytes at the edges of burn wounds in each type of burn injury was well-orchestrated with the event of vascular perfusion. Further, pro-inflammatory gene expression profiling revealed significant upregulation vis-à-vis upregulation of TNF-α and MCP-1 genes, with an increase in the number of neutrophils following 72 h of injury that evidently cemented the conversion of superficial burn into partial-thickness burn. The molecular findings were profoundly supported by the histopathological changes. Thus, our foundational studies show distinct characteristic cutaneous changes correlated with the expression of key pro-inflammatory genes in three different types of burn injuries. Characterization of these cutaneous inflammatory responses provides a promising future for medical interventions involved with different degrees of burn injury, and it will also help in the pre-clinical testing of therapies for burn injury.

Keywords: Burn wound; Chemokines; Cytokines; Inflammatory markers; Vascular perfusion.

MeSH terms

Animals
Burns* / complications
Burns* / therapy
Humans
Mice
Neutrophils
Skin / pathology
Soft Tissue Injuries*
Tumor Necrosis Factor-alpha

Substances

Tumor Necrosis Factor-alpha