A deep dive into UV-based phototherapy: Mechanisms of action and emerging molecular targets in inflammation and cancer

UV-based phototherapy (including psoralen plus UVA (PUVA), UVB and UVA1) has a long, successful history in the management of numerous cutaneous disorders. Photoresponsive diseases are etiologically diverse, but most involve disturbances in local (and occasionally systemic) inflammatory cells and/or...

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Published inPharmacology & therapeutics (Oxford) Vol. 222; p. 107784
Main Authors Vieyra-Garcia, Pablo A., Wolf, Peter
Format Journal Article
LanguageEnglish
Published England Elsevier Inc 01.06.2021
Subjects
Humans
Inflammation - radiotherapy
Neoplasms - radiotherapy
Ultraviolet Therapy
MPD
CTCL
TCDD
β-EP
CHS
TRP
SSBR
mTOR
MF
cPAF
GvL
HSCT
IFNγ
UV
AD
IL
AMP
MED
bFGF
LD50
ET-1
ROS
PAFr
DTH
Treg cells
BMMC
HDAC
CRP
COX-2
HDC
PLE
SRC3
MCHR1
5-HTr
EGFR
LPS
FLG-null
cis-UCA
PUVA
5-MOP
DMD
FICZ
IGFBP7
TLR
PGE2
MSH
VDR
GvHD
AhR
8-oxoG
PAGPC
BER
POMC
STAT
8-MOP
ECP
APC
PAF
TNF-α
JAK
CPD
TMP
LC
6–4PP
CLA
NB-UVB
NER
DAMP
DC
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Summary:UV-based phototherapy (including psoralen plus UVA (PUVA), UVB and UVA1) has a long, successful history in the management of numerous cutaneous disorders. Photoresponsive diseases are etiologically diverse, but most involve disturbances in local (and occasionally systemic) inflammatory cells and/or abnormalities in keratinocytes that trigger inflammation. UV-based phototherapy works by regulating the inflammatory component and inducing apoptosis of pathogenic cells. This results in a fascinating and complex network of simultaneous events–immediate transcriptional changes in keratinocytes, immune cells, and pigment cells; the emergence of apoptotic bodies; and the trafficking of antigen-presenting cells in skin—that quickly transform the microenvironment of UV-exposed skin. Molecular elements in this system of UV recognition and response include chromophores, metabolic byproducts, innate immune receptors, neurotransmitters and mediators such as chemokines and cytokines, antimicrobial peptides, and platelet activating factor (PAF) and PAF-like molecules that simultaneously shape the immunomodulatory effects of UV and their interplay with the microbiota of the skin and beyond. Phototherapy's key effects—proapoptotic, immunomodulatory, antipruritic, antifibrotic, propigmentary, and pro-prebiotic—promote clinical improvement in various skin diseases such as psoriasis, atopic dermatitis (AD), graft-versus-host disease (GvHD), vitiligo, scleroderma, and cutaneous T-cell lymphoma (CTCL) as well as prevention of polymorphic light eruption (PLE). As understanding of phototherapy improves, new therapies (UV- and non-UV-based) are being developed that will modify regulatory T-cells (Treg), interact with (resident) memory T-cells and /or utilize agonists and antagonists as well as antibodies targeting soluble molecules such as cytokines and chemokines, transcription factors, and a variety of membrane-associated receptors.
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ISSN:0163-7258
1879-016X
DOI:10.1016/j.pharmthera.2020.107784