Stage I Melanoma
Current Clinical Trials
Note: Some citations in the text of this section are followed by a level of
evidence. The PDQ editorial boards use a formal ranking system to help the
reader judge the strength of evidence linked to the reported results of a
therapeutic strategy. (Refer to the PDQ summary on Levels of Evidence for more
information.)
Stage I melanoma is defined by the following clinical stage groupings:
- T1a, N0, M0
- T1b, N0, M0
- T2a, N0, M0
Standard treatment options:
- Current evidence suggests that lesions 2 mm or less in thickness may be treated conservatively with radial excision margins of 1
cm. A randomized trial compared narrow margins (1 cm) with wide margins (at least 3 cm) in patients with melanomas no thicker than 2 mm.[1,2] No difference was observed between the two groups in respect to the development of metastatic disease, disease-free survival, or overall survival (OS). Two other randomized trials have compared 2
cm margins with wider margins (i.e., 4 cm or 5 cm), and found no
statistically significant difference in local recurrence, distant
metastasis, or OS, with a median follow-up of 10 years or more
for both trials.[3-5][Level of evidence:1iiA] In the Intergroup Melanoma Surgical Trial, the reduction in margins from 4 cm to 2 cm
was associated with a statistically significant reduction in the need for skin
grafting (from 46% to 11%, P < .001) and a reduction in the length of the
hospital stay.[5] Depending on the location of the melanoma, most patients can
now have this procedure performed on an outpatient basis.
Elective regional lymph node dissection is of no proven benefit for patients
with stage I melanoma. Lymphatic mapping and sentinel lymph node
biopsy for patients who have tumors of intermediate thickness and/or ulcerated tumors, however, may allow the identification of individuals with occult nodal disease
who might benefit from regional lymphadenectomy and adjuvant therapy.[6-9] The International Multicenter Selective Lymphadenectomy Trial (MSLT-1) included 1,269 patients with intermediate-thickness (defined as 1.2 mm-3.5 mm in this study) primary melanomas.[10] There was no melanoma-specific survival advantage (the primary endpoint) for those patients randomly assigned to wide excision plus sentinel lymph node biopsy followed by immediate completion lymphadenectomy for node positivity versus patients randomly assigned to nodal observation and delayed lymphadenectomy for subsequent nodal recurrence at a median of 59.8 months.[10][Level of evidence: 1iiB] This trial was not designed to detect a difference in the impact of lymphadenectomy in patients with microscopic lymph node involvement.[10]
Treatment options under clinical evaluation:
- Because of the higher rate of treatment failure in the subset of clinical stage
I patients with occult nodal disease, clinical trials are evaluating new
techniques to detect submicroscopic sentinel lymph node metastasis to
identify those patients who may benefit from regional lymphadenectomy with or
without adjuvant therapy. One of the objectives of the currently ongoing phase
III Sunbelt Melanoma Trial (UAB-9735) is to determine the effects of lymphadenectomy
with or without adjuvant high-dose interferon-alpha-2b versus observation on
disease-free survival and OS in patients with submicroscopic sentinel
lymph node metastasis detected only by the polymerase chain reaction (PCR)
(i.e., sentinel lymph node negative by histology and immunohistochemistry).
No survival data have been reported from this study. An ongoing diagnostic
study (UCCRC-9308) is testing the combination of reverse transcription and PCR in
the detection of melanoma tumor antigen transcripts in lymph nodes and
peripheral blood samples.
Current Clinical Trials
Check for U.S. clinical trials from NCI's PDQ Cancer Clinical Trials Registry that are now accepting patients with stage I melanoma. The list of clinical trials can be further narrowed by location, drug, intervention, and other criteria.
General information about clinical trials is also available from the NCI Web site.
References
-
Veronesi U, Cascinelli N: Narrow excision (1-cm margin). A safe procedure for thin cutaneous melanoma. Arch Surg 126 (4): 438-41, 1991.
[PUBMED Abstract]
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Veronesi U, Cascinelli N, Adamus J, et al.: Thin stage I primary cutaneous malignant melanoma. Comparison of excision with margins of 1 or 3 cm. N Engl J Med 318 (18): 1159-62, 1988.
[PUBMED Abstract]
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Cohn-Cedermark G, Rutqvist LE, Andersson R, et al.: Long term results of a randomized study by the Swedish Melanoma Study Group on 2-cm versus 5-cm resection margins for patients with cutaneous melanoma with a tumor thickness of 0.8-2.0 mm. Cancer 89 (7): 1495-501, 2000.
[PUBMED Abstract]
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Balch CM, Soong SJ, Smith T, et al.: Long-term results of a prospective surgical trial comparing 2 cm vs. 4 cm excision margins for 740 patients with 1-4 mm melanomas. Ann Surg Oncol 8 (2): 101-8, 2001.
[PUBMED Abstract]
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Balch CM, Urist MM, Karakousis CP, et al.: Efficacy of 2-cm surgical margins for intermediate-thickness melanomas (1 to 4 mm). Results of a multi-institutional randomized surgical trial. Ann Surg 218 (3): 262-7; discussion 267-9, 1993.
[PUBMED Abstract]
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Hochwald SN, Coit DG: Role of elective lymph node dissection in melanoma. Semin Surg Oncol 14 (4): 276-82, 1998.
[PUBMED Abstract]
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Essner R, Conforti A, Kelley MC, et al.: Efficacy of lymphatic mapping, sentinel lymphadenectomy, and selective complete lymph node dissection as a therapeutic procedure for early-stage melanoma. Ann Surg Oncol 6 (5): 442-9, 1999 Jul-Aug.
[PUBMED Abstract]
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Gershenwald JE, Thompson W, Mansfield PF, et al.: Multi-institutional melanoma lymphatic mapping experience: the prognostic value of sentinel lymph node status in 612 stage I or II melanoma patients. J Clin Oncol 17 (3): 976-83, 1999.
[PUBMED Abstract]
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Mraz-Gernhard S, Sagebiel RW, Kashani-Sabet M, et al.: Prediction of sentinel lymph node micrometastasis by histological features in primary cutaneous malignant melanoma. Arch Dermatol 134 (8): 983-7, 1998.
[PUBMED Abstract]
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Morton DL, Thompson JF, Cochran AJ, et al.: Sentinel-node biopsy or nodal observation in melanoma. N Engl J Med 355 (13): 1307-17, 2006.
[PUBMED Abstract]
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