Lisa Naysmith scite author profile

Traditional clinical teaching emphasises the importance of a full clinical examination. In the clinical assessment of lesions that may be skin cancer, full examination allows detection of incidental lesions, as well as helping in the characterisation of the index lesion. Despite this, a total body skin examination is not always performed. Based on two prospective studies of over 1,800 sequential patients in two UK centres we show that over one third of melanomas detected in secondary care are found as incidental lesions, in patients referred for assessment of other potential skin cancers. The majority of these melanomas occurred in patients whose index lesion turned out to be benign. Alternative models of care--for instance some models of teledermatology in which a total body skin examination is not performed by a competent practitioner--cannot be considered equivalent to a traditional consultation and, if adopted uncritically, without system change, will likely lead to melanomas being missed.

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Physiological Variation in the Erythemal Response to Ultraviolet Radiation and Photoadaptation

Waterston

Naysmith

Rees

2004

Journal of Investigative Dermatology

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We have studied the cutaneous response to ultraviolet radiation, measured objectively as erythema in a sample of 12 body sites on 15 Northern European subjects with multiple doses of ultraviolet B (UVB). Skin pigmentation and the development of photoadaptation in response to five repeated doses of irradiation at three body sites was also measured. We report striking differences of up to 5-fold at different body sites to the same challenge dose (p < 0.001) and demonstrate that for this population, site variation is just as important as between-person variation. Skin color at each body site is a strong predictor of response (p < 0.001) and that this cannot be attributed to vascular differences, but instead we believe it reflects site-specific variations in melanin pigmentation. We also observed similar but smaller within-person effects for responses to another inflammatory agent, dithranol (p < 0.01). Despite this, we did not find evidence for differences in the development of photoadaptation by body site. These results have clear clinical implications for the practice of phototesting prior to commencing phototherapy, for therapeutic failure in sites such as the legs in patients with psoriasis, and perhaps for melanoma body-site distribution.

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Safety, complications and patients’ acceptance of Mohs micrographic surgery under local anaesthesia: results from the U.K. MAPS (Mohs Acceptance and Patient Safety) Collaboration Group

et al. 2017

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Mohs micrographic surgery (MMS) is recognized as the goldstandard treatment for high-risk nonmelanoma skin cancers (NMSC) of the head and neck. Given the rising incidence of skin cancer, the past two decades have seen a rapid increase in the number of centres providing this service in the U.K. However, data on the safety, complication rates and patient acceptance of MMS in the U.K. are lacking. Over a 3-month period (September to November 2012) eight regional MMS centres collected data that included tumour site, number of stages to clearance, method of reconstruction and intra-and postoperative complications. In addition to collecting basic demographic and medical information, patients were also asked to rate, on a 10-point Likert scale, (i) their perceived anxiety levels preoperatively, (ii) how well they tolerated the surgery on the day, and (iii) when followed up, their overall acceptance of having undergone MMS under local anaesthesia (LA). Data on 565 patients were analysed. There were 278 women and 287 men, with a median age of 67 years (range 28-93 years). The majority of lesions treated were NMSC (98%). The average number of stages to tumour clearance was 1Á3 (range 1-5). Overall, 60% of patients were clear of tumour within one stage and 34% in two stages, with 6% requiring three or more stages. On average, patients were able to leave the department a little over 4 h after commencing treatment. In total, 88% of all reconstructions (including large flaps and interpolated flaps) were performed on the day by the Mohs surgeon. No major peri-or postoperative complications occurred. Although trouble-

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The Relationship Between Constitutive Pigmentation and Sensitivity to Ultraviolet Radiation Induced Erythema is Dose–Dependent

Javedan

Waterston

et al. 2003

Pigment Cell Research

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The relationship between skin colour and experimental exposure to ultraviolet radiation (UVR) B, with response measured as erythema was studied. Two reflectance methods were used to measure skin colour--tristimulus colorimetry using a Minolta instrument (summarized as the alpha characteristic angle) and the melanin index based on the Diastron reflectance instrument. As expected both measures are highly correlated (0.91). A dose-dependent relationship between skin colour measured as the alpha characteristic angle and UVR was established, with the gradient increasing from 0.99 at 119 mJ to 2.7 at 300 mJ, with the relevant standard errors being 0.39 and 0.47, respectively. Similarly, for the melanin index (where the scale goes in the opposite direction) the gradient differs between -0.49 for 119 mJ and -0.91 for 300 mJ, with the standard errors being 0.14 and 0.17 respectively. The proportion of variation explained is also greater at higher UVR challenge doses. Studies relating UVR sensitivity and pigmentation need to take account of the dose of UVR administered.

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Quantitative Measures of the Effect of the Melanocortin 1 Receptor on Human Pigmentary Status11Presented in part at ESDR Geneva 2002, Naysmith L, Ha T, Waterston K, et al: Melanocortin 1 receptor accounts for 50% of variation in a Northern European dataset. J Invest Dermatol 119:758, 2002 (abstr).

Naysmith

Waterston

et al. 2004

Journal of Investigative Dermatology

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Variation in human hair and skin color is the most striking visible aspect of human genetic variation. The only gene known to exert an effect on pigmentary within the normal population is the melanocortin-1 receptor (MC1R). Previous studies have used a Mendelian framework to relate MC1R genotype to phenotype, by measuring pigmentary status using categorical scales. Such approaches are inadequate. We report results using direct measures of hair color using objective colorimetric dimensions and HPLC determined hair melanins. We have linked MC1R genotype with chemical measures of melanin quantity and type and objective phenotype measures of color. MC1R genotype was predictive of hair melanin expressed as the ratio of the loge of eumelanin to pheomelanin ratio, with a dosage effect evident: MC1R homozygote mean, 1.46; heterozygote, 4.44; and wild type, 5.81 (p<0.001). Approximately 67% of the variance in this model could be accounted for in terms of MC1R genotype. There was also a relation between MC1R status and hair color, most prominently for the b* axis (p<0.001), but also for the a* and L* scales (L*a*b*, CIE). We show for one of the most polymorphic human traits that it is possible to demonstrate meaningful relations between various physical characteristics: DNA sequence diversity, hair-wavelength-specific reflectance patterns, and chemical melanin assays.

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Lisa Naysmith

The Importance of a Full Clinical Examination: Assessment of Index Lesions Referred to a Skin Cancer Clinic Without a Total Body Skin Examination Would Miss One in Three Melanomas

Physiological Variation in the Erythemal Response to Ultraviolet Radiation and Photoadaptation

Safety, complications and patients’ acceptance of Mohs micrographic surgery under local anaesthesia: results from the U.K. MAPS (Mohs Acceptance and Patient Safety) Collaboration Group

The Relationship Between Constitutive Pigmentation and Sensitivity to Ultraviolet Radiation Induced Erythema is Dose–Dependent

Quantitative Measures of the Effect of the Melanocortin 1 Receptor on Human Pigmentary Status11Presented in part at ESDR Geneva 2002, Naysmith L, Ha T, Waterston K, et al: Melanocortin 1 receptor accounts for 50% of variation in a Northern European dataset. J Invest Dermatol 119:758, 2002 (abstr).

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