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 in | Cancer research (Chicago, Ill.) Vol. 50; no. 12; pp. 3743 - 3747 |
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Main Authors | , , |
Format | Journal Article |
Language | English |
Published |
Philadelphia, PA
American Association for Cancer Research
15.06.1990
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Subjects | |
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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. |
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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 |
Author_xml | – sequence: 1 givenname: F surname: ALENA fullname: ALENA, F organization: Univ. Alberta, div. dermatology cutaneous sci., Edmonton AB T6G 2C2, Canada – sequence: 2 givenname: K surname: JIMBOW fullname: JIMBOW, K organization: Univ. Alberta, div. dermatology cutaneous sci., Edmonton AB T6G 2C2, Canada – sequence: 3 givenname: S surname: ITO fullname: ITO, S organization: Univ. Alberta, div. dermatology cutaneous sci., Edmonton AB T6G 2C2, Canada |
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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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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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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 |
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