Melanocytotoxicity and antimelanoma effects of phenolic amine compounds in mice in vivo

A phenolic amine compound, 4-S-cysteaminylphenol (4-S-CAP), is a potent depigmenting agent. To develop more efficacious antimelanoma agents, we synthesized four homologues of 4-S-CAP: N-acetyl-4-S-CAP (N-Ac-4-S-CAP), alpha-methyl-4-S-CAP, 4-S-homo-CAP, and N,N'-dimethyl-4-S-CAP. We tested these...

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Published inCancer research (Chicago, Ill.) Vol. 50; no. 12; pp. 3743 - 3747
Main Authors ALENA, F, JIMBOW, K, ITO, S
Format Journal Article
LanguageEnglish
Published Philadelphia, PA American Association for Cancer Research 15.06.1990
Subjects
550600 > Medicine
ANIMAL CELLS
ANIMALS
Antineoplastic agents
ANTINEOPLASTIC DRUGS
AROMATICS
Biological and medical sciences
BIOLOGICAL EFFECTS
CHEMICAL PREPARATION
CHEMOTHERAPY
COLONY FORMATION
Cysteamine - administration & dosage
Cysteamine - pharmacology
DISEASES
DRUGS
EXPERIMENTAL NEOPLASMS
Female
Hair - analysis
Hair Color - drug effects
HYDROXY COMPOUNDS
IN VIVO
INHIBITION
INJECTION
Injections, Intraperitoneal
Injections, Subcutaneous
INTAKE
INTRAPERITONEAL INJECTION
MAMMALS
Medical sciences
MELANIN
Melanins - analysis
Melanocytes - drug effects
Melanocytes - ultrastructure
Melanoma, Experimental - drug therapy
MELANOMAS
MICE
Mice, Inbred C57BL
NEOPLASMS
ORGANIC COMPOUNDS
ORGANIC NITROGEN COMPOUNDS
Pharmacology. Drug treatments
PHENOLS
Phenols - administration & dosage
Phenols - pharmacology
Pigmentation - drug effects
PIGMENTS
RADIATION, THERMAL, AND OTHER ENVIRON. POLLUTANT EFFECTS ON LIVING ORGS. AND BIOL. MAT
RADIOLOGY AND NUCLEAR MEDICINE
RODENTS
SUBCUTANEOUS INJECTION
SYNTHESIS
THERAPY
TUMOR CELLS
VERTEBRATES 560300 > Chemicals Metabolism & Toxicology
Therapeutic efficiency
Hypomelanosis
Rodentia
Electron microscopy
Organic sulfide
Pathology
Vertebrata
Chemotherapy
Experimental disease
Mammalia
Amine
Structure activity relation
Mouse
Animal
B16-Melanoma
Malignant melanoma
Aromatic compound
Melanin
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Abstract A phenolic amine compound, 4-S-cysteaminylphenol (4-S-CAP), is a potent depigmenting agent. To develop more efficacious antimelanoma agents, we synthesized four homologues of 4-S-CAP: N-acetyl-4-S-CAP (N-Ac-4-S-CAP), alpha-methyl-4-S-CAP, 4-S-homo-CAP, and N,N'-dimethyl-4-S-CAP. We tested these five compounds in mice in vivo. After s.c. or i.p. injection of saline solution (in control groups) or one of the compounds, follicular melanocytes were examined by light and electron microscopy to assess the degree of melanocytotoxicity; N-Ac-4-S-CAP induced the most depigmentation (98%), whether given i.p. or s.c. After injection of 4-S-CAP or N-Ac-4-S-CAP, the number of murine B16F10 melanoma colonies formed in the lungs was determined; 4-S-CAP and N-Ac-4-S-CAP were almost equally effective, reducing the colonies to 32 and 25% of mean control, respectively. Metabolic studies of the urine showed 9% of 4-S-CAP and 20% of N-Ac-4-S-CAP injected i.p. were excreted unchanged in 24 h; 1.3% of the N-Ac-4-S-CAP was excreted as 4-S-CAP, indicating some conversion. We conclude that N-Ac-4-S-CAP is a suitable model for developing chemotherapy to treat melanoma characterized by high tyrosinase activity and melanin synthesis.
AbstractList A phenolic amine compound, 4-S-cysteaminylphenol (4-S-CAP), is a potent depigmenting agent. To develop more efficacious antimelanoma agents, we synthesized four homologues of 4-S-CAP: N-acetyl-4-S-CAP (N-Ac-4-S-CAP), alpha-methyl-4-S-CAP, 4-S-homo-CAP, and N,N'-dimethyl-4-S-CAP. We tested these five compounds in mice in vivo. After s.c. or i.p. injection of saline solution (in control groups) or one of the compounds, follicular melanocytes were examined by light and electron microscopy to assess the degree of melanocytotoxicity; N-Ac-4-S-CAP induced the most depigmentation (98%), whether given i.p. or s.c. After injection of 4-S-CAP or N-Ac-4-S-CAP, the number of murine B16F10 melanoma colonies formed in the lungs was determined; 4-S-CAP and N-Ac-4-S-CAP were almost equally effective, reducing the colonies to 32 and 25% of mean control, respectively. Metabolic studies of the urine showed 9% of 4-S-CAP and 20% of N-Ac-4-S-CAP injected i.p. were excreted unchanged in 24 h; 1.3% of the N-Ac-4-S-CAP was excreted as 4-S-CAP, indicating some conversion. We conclude that N-Ac-4-S-CAP is a suitable model for developing chemotherapy to treat melanoma characterized by high tyrosinase activity and melanin synthesis.
Author JIMBOW, K
ALENA, F
ITO, S
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Issue 12
Keywords Therapeutic efficiency
Hypomelanosis
Rodentia
Electron microscopy
Organic sulfide
Pathology
Vertebrata
Chemotherapy
Experimental disease
Mammalia
Amine
Structure activity relation
Mouse
Animal
B16-Melanoma
Malignant melanoma
Aromatic compound
Melanin
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PublicationTitle Cancer research (Chicago, Ill.)
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Snippet A phenolic amine compound, 4-S-cysteaminylphenol (4-S-CAP), is a potent depigmenting agent. To develop more efficacious antimelanoma agents, we synthesized...
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StartPage 3743
SubjectTerms 550600 -- Medicine
ANIMAL CELLS
ANIMALS
Antineoplastic agents
ANTINEOPLASTIC DRUGS
AROMATICS
Biological and medical sciences
BIOLOGICAL EFFECTS
CHEMICAL PREPARATION
CHEMOTHERAPY
COLONY FORMATION
Cysteamine - administration & dosage
Cysteamine - pharmacology
DISEASES
DRUGS
EXPERIMENTAL NEOPLASMS
Female
Hair - analysis
Hair Color - drug effects
HYDROXY COMPOUNDS
IN VIVO
INHIBITION
INJECTION
Injections, Intraperitoneal
Injections, Subcutaneous
INTAKE
INTRAPERITONEAL INJECTION
MAMMALS
Medical sciences
MELANIN
Melanins - analysis
Melanocytes - drug effects
Melanocytes - ultrastructure
Melanoma, Experimental - drug therapy
MELANOMAS
MICE
Mice, Inbred C57BL
NEOPLASMS
ORGANIC COMPOUNDS
ORGANIC NITROGEN COMPOUNDS
Pharmacology. Drug treatments
PHENOLS
Phenols - administration & dosage
Phenols - pharmacology
Pigmentation - drug effects
PIGMENTS
RADIATION, THERMAL, AND OTHER ENVIRON. POLLUTANT EFFECTS ON LIVING ORGS. AND BIOL. MAT
RADIOLOGY AND NUCLEAR MEDICINE
RODENTS
SUBCUTANEOUS INJECTION
SYNTHESIS
THERAPY
TUMOR CELLS
VERTEBRATES 560300 -- Chemicals Metabolism & Toxicology
Title Melanocytotoxicity and antimelanoma effects of phenolic amine compounds in mice in vivo
URI https://www.ncbi.nlm.nih.gov/pubmed/2340520
https://search.proquest.com/docview/79776549
https://www.osti.gov/biblio/6742404
Volume 50
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