methimazole and Facial-Dermatoses

methimazole has been researched along with Facial-Dermatoses* in 2 studies

Other Studies

2 other study(ies) available for methimazole and Facial-Dermatoses

Article	Year
Limited cutaneous systemic sclerosis arising in a patient with Graves' disease. BMJ case reports, 2017, Jan-27, Volume: 2017 Although Graves' disease and systemic sclerosis are both autoimmune disorders, their relationship is rarely reported. We present the case of a Filipino woman with goitre and thyrotoxic signs and symptoms. Diagnosed with Graves' disease at the outpatient clinic, she took antithyroid medications and underwent radioactive iodine ablation with resultant hypothyroidism after 6 months, during which she began to experience skin tightness over the face, neck and fingers. Workup revealed limited cutaneous systemic sclerosis, and the patient improved with methotrexate. This case highlights the increased prevalence of coincident autoimmune disorders in Graves' disease. Topics: Adult; Antithyroid Agents; Facial Dermatoses; Female; Graves Disease; Hormone Replacement Therapy; Humans; Hypothyroidism; Immunosuppressive Agents; Iodine Radioisotopes; Methimazole; Methotrexate; Neck; Scleroderma, Limited; Thyroxine	2017
Topical methimazole as a new treatment for postinflammatory hyperpigmentation: report of the first case. Dermatology (Basel, Switzerland), 2005, Volume: 211, Issue:4 We have previously shown that the peroxidase inhibitor methimazole (1-methyl-2-mercapto imidazole; MMI) is a noncytotoxic inhibitor of melanin production in cultured B16 melanocytes. It was further demonstrated that the topical application of 5% MMI on brown guinea pig skin for 6 weeks causes a significant reduction in the amount of epidermal melanin, resulting in visually recognizable cutaneous depigmentation. Herein, we report a 27-year-old male with postinflammatory hyperpigmentation (due to acid burn), successfully treated with topical MMI as a new skin depigmenting agent. Topical 5% MMI caused a moderate to marked improvement of the hyperpigmented lesions within 6 weeks of once-daily application. Topical MMI was well tolerated by the patient and did not affect the level of serum thyroid hormones (free thyroxin, free triiodothyronine and the thyroid-stimulating hormone). Unlike most known depigmenting agents, such as hydroquinone and kojic acid, MMI is a noncytotoxic, nonmutagenic compound, and it is possible that MMI could serve as a novel agent for the treatment of hyperpigmentary disorders in human. Topics: Administration, Cutaneous; Adult; Burns, Chemical; Dermatologic Agents; Facial Dermatoses; Humans; Hyperpigmentation; Male; Melanins; Methimazole; Occupational Diseases; Peroxidase; Thyrotropin; Thyroxine; Triiodothyronine	2005

Article

Year

Limited cutaneous systemic sclerosis arising in a patient with Graves' disease.

BMJ case reports, 2017, Jan-27, Volume: 2017

Although Graves' disease and systemic sclerosis are both autoimmune disorders, their relationship is rarely reported. We present the case of a Filipino woman with goitre and thyrotoxic signs and symptoms. Diagnosed with Graves' disease at the outpatient clinic, she took antithyroid medications and underwent radioactive iodine ablation with resultant hypothyroidism after 6 months, during which she began to experience skin tightness over the face, neck and fingers. Workup revealed limited cutaneous systemic sclerosis, and the patient improved with methotrexate. This case highlights the increased prevalence of coincident autoimmune disorders in Graves' disease.

Topics: Adult; Antithyroid Agents; Facial Dermatoses; Female; Graves Disease; Hormone Replacement Therapy; Humans; Hypothyroidism; Immunosuppressive Agents; Iodine Radioisotopes; Methimazole; Methotrexate; Neck; Scleroderma, Limited; Thyroxine

2017

Topical methimazole as a new treatment for postinflammatory hyperpigmentation: report of the first case.

Dermatology (Basel, Switzerland), 2005, Volume: 211, Issue:4

We have previously shown that the peroxidase inhibitor methimazole (1-methyl-2-mercapto imidazole; MMI) is a noncytotoxic inhibitor of melanin production in cultured B16 melanocytes. It was further demonstrated that the topical application of 5% MMI on brown guinea pig skin for 6 weeks causes a significant reduction in the amount of epidermal melanin, resulting in visually recognizable cutaneous depigmentation. Herein, we report a 27-year-old male with postinflammatory hyperpigmentation (due to acid burn), successfully treated with topical MMI as a new skin depigmenting agent. Topical 5% MMI caused a moderate to marked improvement of the hyperpigmented lesions within 6 weeks of once-daily application. Topical MMI was well tolerated by the patient and did not affect the level of serum thyroid hormones (free thyroxin, free triiodothyronine and the thyroid-stimulating hormone). Unlike most known depigmenting agents, such as hydroquinone and kojic acid, MMI is a noncytotoxic, nonmutagenic compound, and it is possible that MMI could serve as a novel agent for the treatment of hyperpigmentary disorders in human.

Topics: Administration, Cutaneous; Adult; Burns, Chemical; Dermatologic Agents; Facial Dermatoses; Humans; Hyperpigmentation; Male; Melanins; Methimazole; Occupational Diseases; Peroxidase; Thyrotropin; Thyroxine; Triiodothyronine

2005