Pedro Andrade scite author profile

SummaryBackground. The fixed drug eruption is a common adverse drug reaction. Clear identification of the culprit drug is not always possible in the clinical setting, and oral rechallenge may induce new lesions or severe reactions. Objectives. The main purpose of this study was to evaluate the diagnostic value of patch testing in establishing an aetiological diagnosis in fixed drug eruptions. Method. A retrospective analysis was conducted evaluating 52 patients (17M/35F, mean age 53±17 years) with clinical diagnoses of fixed drug eruptions submitted to patch tests in a 20-year period in a Dermatology Department. Nonsteroidal anti-inflammatory drugs (NSAID) were clinically suspected in 90.4% of the cases, followed by antibiotics (28.9%) and paracetamol (15.4%). Results. Patch tests on pigmented lesions were reactive in 21 patients (40.4%), 20 of those to NSAID (nimesulide, piroxicam and etoricoxib) and 1 to an antihistamine (cetirizine). All patch tests using other drugs were negative, even under conditions of high clinical suspicion. Oral rechallenge allowed confirmation of drug imputability in 5 of 31 test-negative cases. Cross reactivity was frequently observed between piroxicam and other oxicams, and between different antihistamines. Conclusions. Patch testing was shown to be a simple and safe method to confirm drug imputabililty in fixed drug eruption, mainly when NSAID or multiple drugs are suspected. Persistent lack of reactivity to drug classes such as antibiotics and allopurinol represent an important limitation.

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Epidemiology of basal cell carcinomas and squamous cell carcinomas in a Department of Dermatology: a 5 year review

Andrade¹,

Brites²,

Vieira³

et al. 2012

An. Bras. Dermatol.

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BACKGROUND: Non-melanoma skin cancer, a common designation for both basal cell carcinomas and squamous cell carcinomas, is the most frequent malignant skin neoplasm. OBJECTIVE: Epidemiologic characterization of the population with Non-melanoma skin cancer. METHODS: Retrospective analysis of all patients diagnosed with Non-melanoma skin cancer based on histopathologic analysis of all incisional or excisional skin biopsies performed between 2004 and 2008 in a Department of Dermatology. RESULTS: A total of 3075 Non-melanoma skin cancers were identified, representing 88% of all malignant skin neoplasms (n=3493) diagnosed in the same period. Of those, 68,3% were basal cell carcinomas. Most Non-melanoma skin cancer patients were female and over 60 years old. Of all Non-melanoma skin cancer, 81,7% (n=1443) were located in sun-exposed skin, and represented 95,1% of malignant skin neoplasms in sun-exposed skin. Non-melanoma skin cancer was the most frequent malignant skin neoplasm in most topographic locations, except for abdomen and pelvis - over 95% of all malignant skin neoplasms in the face, neck and scalp were Non-melanoma skin cancer. Basal cell carcinomas were clearly predominant in all locations, except in upper and lower limbs, lower lip and genitals, where squamous cell carcinomas represented respectively 77,7%, 77,4%, 94,7% and 95,3% of the Non-melanoma skin cancers. CONCLUSION: Being the most common skin cancer, Non-melanoma skin cancer should be under constant surveillance, in order to monitor its epidemiologic dynamics, the efficiency of preventive measures and the adaptation of the healthcare resources.

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Extreme dentoalveolar compensation in the treatment of Class III malocclusion

Janson

Souza

Alves

et al. 2005

American Journal of Orthodontics and Dentofacial Orthopedics

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The UV Filter Tinosorb M, Containing Decyl Glucoside, Is a Frequent Cause of Allergic Contact Dermatitis

Pereira¹,

Coutinho²,

Andrade³

et al. 2013

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Allergic Contact Dermatitis to Decyl Glucoside in Tinosorb M^®

2010

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Pedro Andrade

Patch testing in fixed drug eruptions-a 20-year review

Epidemiology of basal cell carcinomas and squamous cell carcinomas in a Department of Dermatology: a 5 year review

Extreme dentoalveolar compensation in the treatment of Class III malocclusion

The UV Filter Tinosorb M, Containing Decyl Glucoside, Is a Frequent Cause of Allergic Contact Dermatitis

Allergic Contact Dermatitis to Decyl Glucoside in Tinosorb M^®

Contact Info

Product

Resources

About

Pedro Andrade

Patch testing in fixed drug eruptions-a 20-year review

Epidemiology of basal cell carcinomas and squamous cell carcinomas in a Department of Dermatology: a 5 year review

Extreme dentoalveolar compensation in the treatment of Class III malocclusion

The UV Filter Tinosorb M, Containing Decyl Glucoside, Is a Frequent Cause of Allergic Contact Dermatitis

Allergic Contact Dermatitis to Decyl Glucoside in Tinosorb M®

Contact Info

Product

Resources

About

Allergic Contact Dermatitis to Decyl Glucoside in Tinosorb M^®