Aberrations and clinical significance of BRAF in malignant melanoma: A series of 60 cases in Chinese Uyghur

Abstract

Malignant melanoma (MM) is a highly malignant melanocytic tumor, it occurs mostly in the skin, the mucous membrane close to the skin, but also in the tunicae rhagoides and the pia mater. The Uyghur is the largest ethnic group living in the Xinjiang Uyghur Autonomous Region of China, accounting for 46% of the total population of 20 million. Large-scale studies on MMs in Asian countries are limited. This study aimed to investigate BRAF mRNA expression and mutations in Chinese Uyghur patients with MMs and to identify the clinical features associated with these parameters.Formalin-fixed, paraffin wax-embedded tumor sections from 60 MMs were analyzed for BRAF expression using reverse transcription polymerase chain reaction (RT-PCR). Exons 11 and 15 of BRAF were analyzed for the presence of mutations using PCR and DNA sequencing. Sixty MMs were followed by mobile phone for survival analysis.BRAF mRNA expression was higher in MMs than in pigmented moles and normal skin tissues. Fourteen of 60 MMs had BRAF mutations. The frequency of BRAF mutations was significantly higher in patients younger than 60 years (10/28, 4/32, P = .02). A significant difference was observed in the frequency of BRAF mutations among specimens of mucosal, acral, chronic sun-induced damage (CSD), and non-CSD MMs (2/10, 3/19, 8/25, 1/6, P = .002). No significant association was found among BRAF mutations, sex, ulceration, or lymph node metastasis. MMs lymph node metastasis (hazard ratio 2.54 [95% confidence interval 1.062 - 6.066], P = .01) affected survival.This study indicated that BRAF mutations and expression might serve as independent adverse prognostic factors in melanoma.

Figure 1

Distribution of malignant melanomas in Uyghur patients. CSD = chronic sun-induced damage.

Figure 2

(A) Mutation corresponding to V600E. (B) Wild-type sequence of BRAF exon 15. (C) Mutation corresponding to G593C. (D) Wild-type sequence of BRAF exon 15. (E) Mutation corresponding to L597Q. (F) Wild-type sequence of BRAF exon 15. (G) Mutation corresponding to S465F. (H) Wild-type sequence of BRAF exon 11. (I) Mutation corresponding to P453H. (J) Wild-type sequence of BRAF exon 11.

Figure 3

Two groups were compared using the t test, and the single factor analysis of variance was used.