Hypopigmentation in burns is associated with alterations in the architecture of the skin and the dendricity of the melanocytes

Hypopigmentation in burns is associated with alterations in the architecture of the skin and the dendricity of the melanocytes

•Hypopigmentation is a major problem in deep dermal burns.•There is a scarcity of standard treatment for post burn hypopigmentation disorder.•Understanding of the pathophysiology is prerequisite for futuristic therapeutic intervention.•This is the first study understanding the preliminary cause of H...

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Veröffentlicht in:Burns 2020-06, Vol.46 (4), p.906-917
Hauptverfasser: Dutta, Shruti, Panda, Sangita, Singh, Prashant, Tawde, Sumit, Mishra, Mamata, Andhale, Vikas, Athavale, Angira, Keswani, Sunil Manohar
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Burns
Hypopigmentation
Keratinocyte
Melanin
Melanocyte
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container_end_page 917
container_issue 4
container_start_page 906
container_title Burns
container_volume 46
creator Dutta, Shruti
Panda, Sangita
Singh, Prashant
Tawde, Sumit
Mishra, Mamata
Andhale, Vikas
Athavale, Angira
Keswani, Sunil Manohar
description •Hypopigmentation is a major problem in deep dermal burns.•There is a scarcity of standard treatment for post burn hypopigmentation disorder.•Understanding of the pathophysiology is prerequisite for futuristic therapeutic intervention.•This is the first study understanding the preliminary cause of Hypopigmentation in post burn patients. Hypopigmentation is a major problem in deep dermal burns. To date, no standard treatment is available for the post burn hypopigmentation disorder. Therefore, understanding the molecular and cellular events are of benefit for therapeutic intervention. Hematoxylin and Eosin (H&E) and Fontana Masson (FM) staining of post burn hypopigmented skin (PBHS) showed an altered architectural pattern in cellular organization, cornified layer and melanin pigment as compared to the normal skin. This was confirmed by immunohistochemistry (IHC) analysis of PBHS samples using specific marker cytokeratin 5 (CK5) for keratinocytes and melanocortin 1 receptor (MCIR) for melanocytes. Validation of these observations was performed by IHC using proliferation and differentiation markers, Ki67 and Loricrin respectively and the melanocyte specific marker tyrosinase related protein 1 (TRP1). Taking a cue from the IHC study, the interaction of keratinocytes and melanocytes was studied by developing a co-culture model from PBHS and normal skin. Culture data exhibited a change of dendritic structure, reduced proliferation rate, faulty melanin synthesis and transfer of melanin from melanocytes to keratinocytes in PBHS samples. To the best of our knowledge, this is the first study showing structural and functional aberrations of melanocytes and keratinocytes, as a potential cause of hypopigmentation in burned patients. Our study, therefore, provides valuable insight for the basis of hypopigmentation in post burn patients, which may pave the way for clinical intervention in the future.
doi_str_mv 10.1016/j.burns.2019.10.003
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subjects Burns
Hypopigmentation
Keratinocyte
Melanin
Melanocyte
title Hypopigmentation in burns is associated with alterations in the architecture of the skin and the dendricity of the melanocytes
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