Cultured Human Melanocytes Respond to MSH Peptides and ACTH

Although the administration of melanocyte‐stimulating hormone (MSH) peptides results in skin darkening in man, cultured human melanocytes have been reported to be unresponsive to these peptides. This may be a consequence of the conditions under which the cells were maintained in vitro, particularly...

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Veröffentlicht in:Pigment cell research 1994-08, Vol.7 (4), p.217-221
Hauptverfasser: HUNT, GILLIAN, DONATIEN, PHILIPPE D., LUNEC, JOHN, TODD, CAROLE, KYNE, SYLVIA, THODY, ANTHONY J.
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container_issue 4
container_start_page 217
container_title Pigment cell research
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creator HUNT, GILLIAN
DONATIEN, PHILIPPE D.
LUNEC, JOHN
TODD, CAROLE
KYNE, SYLVIA
THODY, ANTHONY J.
description Although the administration of melanocyte‐stimulating hormone (MSH) peptides results in skin darkening in man, cultured human melanocytes have been reported to be unresponsive to these peptides. This may be a consequence of the conditions under which the cells were maintained in vitro, particularly the use of phorbol esters and cholera toxin as melanocyte mitogens. By culturing the cells in the absence of these additives, we demonstrate that α‐MSH and its synthetic analogue Nle4DPhe7α‐MSH (NDP‐MSH) induce dose‐related increases in melanin content and tyrosinase activity and affect cell morphology in the majority of human melanocyte cultures. In addition, NDP‐MSH induces increases in tyrosinase mRNA and tyrosinase‐related protein‐1 (TRP‐1) mRNA. The dose‐response curves for the MSH peptides are sigmoidal and the two peptides are equipotent in their effects on human melanocytes. Adrenocorticotropic hormone (ACTH) also affects morphology and stimulates melanogenesis and tyrosinase activity in human melanocytes. However, the dose‐response curves for ACTH are biphasic, and the melanocytes respond to lower concentrations of ACTH than MSH peptides, similar to those normally present in human plasma. These findings may be important in understanding the role of these pro‐opiomelanocortin peptides in human skin pigmentation.
doi_str_mv 10.1111/j.1600-0749.1994.tb00052.x
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This may be a consequence of the conditions under which the cells were maintained in vitro, particularly the use of phorbol esters and cholera toxin as melanocyte mitogens. By culturing the cells in the absence of these additives, we demonstrate that α‐MSH and its synthetic analogue Nle4DPhe7α‐MSH (NDP‐MSH) induce dose‐related increases in melanin content and tyrosinase activity and affect cell morphology in the majority of human melanocyte cultures. In addition, NDP‐MSH induces increases in tyrosinase mRNA and tyrosinase‐related protein‐1 (TRP‐1) mRNA. The dose‐response curves for the MSH peptides are sigmoidal and the two peptides are equipotent in their effects on human melanocytes. Adrenocorticotropic hormone (ACTH) also affects morphology and stimulates melanogenesis and tyrosinase activity in human melanocytes. However, the dose‐response curves for ACTH are biphasic, and the melanocytes respond to lower concentrations of ACTH than MSH peptides, similar to those normally present in human plasma. 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This may be a consequence of the conditions under which the cells were maintained in vitro, particularly the use of phorbol esters and cholera toxin as melanocyte mitogens. By culturing the cells in the absence of these additives, we demonstrate that α‐MSH and its synthetic analogue Nle4DPhe7α‐MSH (NDP‐MSH) induce dose‐related increases in melanin content and tyrosinase activity and affect cell morphology in the majority of human melanocyte cultures. In addition, NDP‐MSH induces increases in tyrosinase mRNA and tyrosinase‐related protein‐1 (TRP‐1) mRNA. The dose‐response curves for the MSH peptides are sigmoidal and the two peptides are equipotent in their effects on human melanocytes. Adrenocorticotropic hormone (ACTH) also affects morphology and stimulates melanogenesis and tyrosinase activity in human melanocytes. However, the dose‐response curves for ACTH are biphasic, and the melanocytes respond to lower concentrations of ACTH than MSH peptides, similar to those normally present in human plasma. 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This may be a consequence of the conditions under which the cells were maintained in vitro, particularly the use of phorbol esters and cholera toxin as melanocyte mitogens. By culturing the cells in the absence of these additives, we demonstrate that α‐MSH and its synthetic analogue Nle4DPhe7α‐MSH (NDP‐MSH) induce dose‐related increases in melanin content and tyrosinase activity and affect cell morphology in the majority of human melanocyte cultures. In addition, NDP‐MSH induces increases in tyrosinase mRNA and tyrosinase‐related protein‐1 (TRP‐1) mRNA. The dose‐response curves for the MSH peptides are sigmoidal and the two peptides are equipotent in their effects on human melanocytes. Adrenocorticotropic hormone (ACTH) also affects morphology and stimulates melanogenesis and tyrosinase activity in human melanocytes. 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identifier ISSN: 0893-5785
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subjects ACTH
Adrenocorticotropic Hormone - pharmacology
alpha-MSH - analogs & derivatives
alpha-MSH - pharmacology
Cells, Cultured
Cyclic AMP - pharmacology
Female
Humans
Male
Melanins - metabolism
Melanocyte-Stimulating Hormones - pharmacology
Melanocytes
Melanocytes - cytology
Melanocytes - drug effects
Melanocytes - metabolism
Melanogenesis
Membrane Glycoproteins
Monophenol Monooxygenase - genetics
Monophenol Monooxygenase - metabolism
Morphology
MSH
Oxidoreductases
Proteins - genetics
RNA, Messenger - metabolism
TRP-1
Tyrosinase
title Cultured Human Melanocytes Respond to MSH Peptides and ACTH
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