Frequent detection of BRAFV600E mutations in histiocytic and dendritic cell neoplasms

Author:

Go Heounjeong1,Jeon Yoon Kyung23,Huh Jooryung1,Choi Suk Jin4,Choi Yoo‐Duk5,Cha Hee Jeong6,Kim Hyun‐Jung7,Park Gyeongsin8,Min Sookee9,Kim Ji Eun210

Affiliation:

1. Department of Pathology Asan Medical Center University of Ulsan College of Medicine Seoul Korea

2. Department of Pathology Seoul National University College of Medicine Seoul Korea

3. Department of Pathology Seoul National University Hospital Seoul Korea

4. Department of Pathology Inha University Hospital Incheon Korea

5. Department of Pathology Chonnam National University Medical School Gwangju Korea

6. Department of Pathology University of Ulsan College of Medicine Ulsan Korea

7. Department of Pathology Inje University Sanggye Paik Hospital Seoul Korea

8. Department of Pathology Catholic University Seoul St. Mary Hospital Seoul Korea

9. Department of Pathology Hallym University Sacred Heart Hospital Anyang Korea

10. Department of Pathology Seoul National University Boramae Hospital Seoul Korea

Abstract

AimsIn this study, we examined BRAF mutation in a wide range of histiocytic and dendritic cell neoplasms and compared its detection rate in each disease group.Methods and resultsA total of 129 cases of histiocytic, dendritic cell and other related lesions were reviewed from the archives of 10 hospitals in Korea. The cases consisted of histiocytic sarcoma, follicular dendritic cell (FDC) sarcoma, interdigitating cell sarcoma, Langerhans cell histiocytosis (LCH), Langerhans cell sarcoma, blastic plasmacytoid dendritic cell neoplasm, acute monocytic leukaemia M5, giant cell tumour, xanthogranuloma, inflammatory myofibroblastic tumour and Rosai–Dorfman disease. BRAF mutation analysis was performed by Sanger sequencing and PNAcqPCR. All the detected mutations of BRAF were V600E. Histiocytic sarcoma exhibited the highest rate of BRAFV600E (62.5%, five of eight), followed by Langerhans cell tumours (25%, seven of 28), FDC sarcoma (18.5%, five of 27) and giant cell tumour (6.7%, two of 30). The other tumours did not harbour BRAF mutations. In histiocytic sarcoma, FDC sarcoma and LCH, there were no significant differences in clinical features between tumours containing BRAFV600E and those with BRAFwt.ConclusionsBRAFV600E was not limited to LCH and was detected more frequently in histiocytic sarcoma. Our findings suggest that the BRAF pathway may contribute to the pathogenesis or malignant transformation of histiocytic and dendritic cell neoplasms.

Funder

SK telecom health project

Publisher

Wiley

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