Amelanotic acral melanomas: Clinicopathological, BRAF mutation, and KIT aberration analyses
Amelanotic acral melanoma (AAM) is very rare and difficult to diagnose both clinically and pathologically. Complete-type AAM shows no black to brown pigmentation in the lesion, whereas incomplete-type AAM shows focal or subtle pigmentation. AAM has been the subject of few investigations. We analyzed...
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| Published in | Journal of the American Academy of Dermatology Vol. 69; no. 5; pp. 700 - 707 |
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| Main Authors | , , , , |
| Format | Journal Article |
| Language | English |
| Published |
United States
Elsevier Inc
01.11.2013
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| Subjects | |
| Online Access | Get full text |
| ISSN | 0190-9622 1097-6787 1097-6787 |
| DOI | 10.1016/j.jaad.2013.06.035 |
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| Abstract | Amelanotic acral melanoma (AAM) is very rare and difficult to diagnose both clinically and pathologically. Complete-type AAM shows no black to brown pigmentation in the lesion, whereas incomplete-type AAM shows focal or subtle pigmentation. AAM has been the subject of few investigations.
We analyzed the clinicopathological features, BRAF mutations, and KIT aberrations in 35 Korean AAM cases.
We included 28 cases of complete-type and 7 cases of incomplete-type AAM.
In all, 26 AAMs (45.7%) were located on the feet of patients, 21 of which (82.9%) showed ulceration. Sixteen cases developed in subungual areas. Nodular melanoma was the most common histopathological subtype (63.6%). The most frequent cell types affected were epithelioid and spindled. HMB-45 staining was strongly positive in 66.7% of AAMs; 4 (12.1%) were negative for HMB-45, and 3 of these were complete-type AAMs. Of 33 total patients, BRAF mutations were detected in 2 AAM cases, and KIT aberrations were present in 11 cases (33.3%). Four cases (12.1%), all of which were complete-type AAMs, had KIT mutations. KIT aberrations were weakly correlated with c-kit staining. Twenty patients were TNM stage I or II, and mean survival was 30.14 ± 4.54 months.
The study is limited by the small number of patients.
Physicians should be aware of rare and hard-to-diagnose AAMs. We expect that tyrosine kinase inhibitors would be effective for KIT-mutated patients with complete-type AAMs. |
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| AbstractList | Background Amelanotic acral melanoma (AAM) is very rare and difficult to diagnose both clinically and pathologically. Complete-type AAM shows no black to brown pigmentation in the lesion, whereas incomplete-type AAM shows focal or subtle pigmentation. AAM has been the subject of few investigations. Objectives We analyzed the clinicopathological features, BRAF mutations, and KIT aberrations in 35 Korean AAM cases. Methods We included 28 cases of complete-type and 7 cases of incomplete-type AAM. Results In all, 26 AAMs (45.7%) were located on the feet of patients, 21 of which (82.9%) showed ulceration. Sixteen cases developed in subungual areas. Nodular melanoma was the most common histopathological subtype (63.6%). The most frequent cell types affected were epithelioid and spindled. HMB-45 staining was strongly positive in 66.7% of AAMs; 4 (12.1%) were negative for HMB-45, and 3 of these were complete-type AAMs. Of 33 total patients, BRAF mutations were detected in 2 AAM cases, and KIT aberrations were present in 11 cases (33.3%). Four cases (12.1%), all of which were complete-type AAMs, had KIT mutations. KIT aberrations were weakly correlated with c-kit staining. Twenty patients were TNM stage I or II, and mean survival was 30.14 ± 4.54 months. Limitations The study is limited by the small number of patients. Conclusion Physicians should be aware of rare and hard-to-diagnose AAMs. We expect that tyrosine kinase inhibitors would be effective for KIT -mutated patients with complete-type AAMs. Amelanotic acral melanoma (AAM) is very rare and difficult to diagnose both clinically and pathologically. Complete-type AAM shows no black to brown pigmentation in the lesion, whereas incomplete-type AAM shows focal or subtle pigmentation. AAM has been the subject of few investigations. We analyzed the clinicopathological features, BRAF mutations, and KIT aberrations in 35 Korean AAM cases. We included 28 cases of complete-type and 7 cases of incomplete-type AAM. In all, 26 AAMs (45.7%) were located on the feet of patients, 21 of which (82.9%) showed ulceration. Sixteen cases developed in subungual areas. Nodular melanoma was the most common histopathological subtype (63.6%). The most frequent cell types affected were epithelioid and spindled. HMB-45 staining was strongly positive in 66.7% of AAMs; 4 (12.1%) were negative for HMB-45, and 3 of these were complete-type AAMs. Of 33 total patients, BRAF mutations were detected in 2 AAM cases, and KIT aberrations were present in 11 cases (33.3%). Four cases (12.1%), all of which were complete-type AAMs, had KIT mutations. KIT aberrations were weakly correlated with c-kit staining. Twenty patients were TNM stage I or II, and mean survival was 30.14 ± 4.54 months. The study is limited by the small number of patients. Physicians should be aware of rare and hard-to-diagnose AAMs. We expect that tyrosine kinase inhibitors would be effective for KIT-mutated patients with complete-type AAMs. Amelanotic acral melanoma (AAM) is very rare and difficult to diagnose both clinically and pathologically. Complete-type AAM shows no black to brown pigmentation in the lesion, whereas incomplete-type AAM shows focal or subtle pigmentation. AAM has been the subject of few investigations.BACKGROUNDAmelanotic acral melanoma (AAM) is very rare and difficult to diagnose both clinically and pathologically. Complete-type AAM shows no black to brown pigmentation in the lesion, whereas incomplete-type AAM shows focal or subtle pigmentation. AAM has been the subject of few investigations.We analyzed the clinicopathological features, BRAF mutations, and KIT aberrations in 35 Korean AAM cases.OBJECTIVESWe analyzed the clinicopathological features, BRAF mutations, and KIT aberrations in 35 Korean AAM cases.We included 28 cases of complete-type and 7 cases of incomplete-type AAM.METHODSWe included 28 cases of complete-type and 7 cases of incomplete-type AAM.In all, 26 AAMs (45.7%) were located on the feet of patients, 21 of which (82.9%) showed ulceration. Sixteen cases developed in subungual areas. Nodular melanoma was the most common histopathological subtype (63.6%). The most frequent cell types affected were epithelioid and spindled. HMB-45 staining was strongly positive in 66.7% of AAMs; 4 (12.1%) were negative for HMB-45, and 3 of these were complete-type AAMs. Of 33 total patients, BRAF mutations were detected in 2 AAM cases, and KIT aberrations were present in 11 cases (33.3%). Four cases (12.1%), all of which were complete-type AAMs, had KIT mutations. KIT aberrations were weakly correlated with c-kit staining. Twenty patients were TNM stage I or II, and mean survival was 30.14 ± 4.54 months.RESULTSIn all, 26 AAMs (45.7%) were located on the feet of patients, 21 of which (82.9%) showed ulceration. Sixteen cases developed in subungual areas. Nodular melanoma was the most common histopathological subtype (63.6%). The most frequent cell types affected were epithelioid and spindled. HMB-45 staining was strongly positive in 66.7% of AAMs; 4 (12.1%) were negative for HMB-45, and 3 of these were complete-type AAMs. Of 33 total patients, BRAF mutations were detected in 2 AAM cases, and KIT aberrations were present in 11 cases (33.3%). Four cases (12.1%), all of which were complete-type AAMs, had KIT mutations. KIT aberrations were weakly correlated with c-kit staining. Twenty patients were TNM stage I or II, and mean survival was 30.14 ± 4.54 months.The study is limited by the small number of patients.LIMITATIONSThe study is limited by the small number of patients.Physicians should be aware of rare and hard-to-diagnose AAMs. We expect that tyrosine kinase inhibitors would be effective for KIT-mutated patients with complete-type AAMs.CONCLUSIONPhysicians should be aware of rare and hard-to-diagnose AAMs. We expect that tyrosine kinase inhibitors would be effective for KIT-mutated patients with complete-type AAMs. |
| Author | Lee, Jee-Bum Yun, Sook Jung Chun, Seung Min Choi, Yoo Duk Jin, Sun A. |
| Author_xml | – sequence: 1 givenname: Yoo Duk surname: Choi fullname: Choi, Yoo Duk organization: Department of Pathology, Chonnam National University Medical School, Gwangju, Korea – sequence: 2 givenname: Seung Min surname: Chun fullname: Chun, Seung Min organization: Department of Dermatology, Chonnam National University Medical School, Gwangju, Korea – sequence: 3 givenname: Sun A. surname: Jin fullname: Jin, Sun A. organization: Department of Dermatology, Chonnam National University Medical School, Gwangju, Korea – sequence: 4 givenname: Jee-Bum surname: Lee fullname: Lee, Jee-Bum organization: Department of Dermatology, Chonnam National University Medical School, Gwangju, Korea – sequence: 5 givenname: Sook Jung surname: Yun fullname: Yun, Sook Jung email: sjyun@chonnam.ac.kr organization: Department of Dermatology, Chonnam National University Medical School, Gwangju, Korea |
| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/23972510$$D View this record in MEDLINE/PubMed |
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| Copyright | 2013 American Academy of Dermatology, Inc. American Academy of Dermatology, Inc. Copyright © 2013 American Academy of Dermatology, Inc. Published by Mosby, Inc. All rights reserved. |
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| Keywords | KIT mutation amelanotic acral melanoma amelanotic melanoma AJCC HMB-45 acral melanoma prognosis AAM PCR BRAF mutation American Joint Committee on Cancer polymerase chain reaction |
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| Snippet | Amelanotic acral melanoma (AAM) is very rare and difficult to diagnose both clinically and pathologically. Complete-type AAM shows no black to brown... Background Amelanotic acral melanoma (AAM) is very rare and difficult to diagnose both clinically and pathologically. Complete-type AAM shows no black to brown... |
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| SubjectTerms | acral melanoma Aged amelanotic acral melanoma amelanotic melanoma BRAF mutation Dermatology Female HMB-45 Humans KIT mutation Male Melanoma, Amelanotic - genetics Melanoma, Amelanotic - pathology Mutation prognosis Proto-Oncogene Proteins B-raf - genetics Proto-Oncogene Proteins c-kit - genetics |
| Title | Amelanotic acral melanomas: Clinicopathological, BRAF mutation, and KIT aberration analyses |
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