Abstract

The overall objective of this grant has been the development of new approaches to the surgical treatment of melanoma and other solid neoplasms, utilizing a multidisciplinary approach of pathologic, immunologic and molecular techniques to achieve a more precise """"""""ultra- staging"""""""" for melanoma and solid neoplasms, utilizing a multidisciplinary approach of pathologic, immunologic and molecular techniques to achieve a more precise """"""""ultra-staging"""""""" for melanoma and solid neoplasms. We are hopeful that the use of these multidisciplinary techniques will reduce the extent of surgery and post-operative adjuvant therapy by differentiating those patients who are curable by surgery alone from those who have residual occult metastases and need post-operative adjuvant therapy. The advent of effect post-surgical adjuvant therapy for AJCC Stages III and IIA/B melanoma in the form of high dose intron-A and intermediate dose Roferon has increased the urgency of achieving this aim. The toxicity and expense of such therapy make it essential to avoid these adjuvant therapies in those patients who are unlikely to recur. The primary Aim of this proposal is to determine whether the innovate technique of lymphatic mapping and sentinel node biopsy, with selective lymphadenectomy, conveys a survival benefit for patients with clinical stage I melanoma with Breslow Thickness greater than 1.0 mm. This technique accurately identifies patients with early stage melanoma who have nodal metastases and are likely to benefit from radical lymphadenectomy. Furthermore, it avoids unnecessary lymph node dissection in those patients whose melanoma failed to metastasize to regional nodes. This new approach has been extended to a multi-center trial, the Multi- center Selective Lymphadenectomy Trial (MSLT), comparing wide excision alone or combined with selective lymphadenectomy. This multi-center trial, which involves 16 melanoma centers, must accrue 800 more patients to answer this important question. Secondary Aims include: (a) development of new pathologic methods to more accurately identify micrometastases in the sentinel node and predict prognosis for individual patients; (b) development of new molecular, immunological and genetic markers to more accurately measure the presence of subclinical micrometastases in the blood and sentinel nodes which provide more precise """"""""ultra-staging"""""""" of occult melanoma metastases. The above techniques are applied retrospectively to archival specimens collected in the JWCI and prospectively to patients in the MSLT.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
2P01CA029605-17
Application #
2686757
Study Section
Subcommittee G - Education (NCI)
Program Officer
Wu, Roy S
Project Start
1981-04-01
Project End
2002-11-30
Budget Start
1998-09-10
Budget End
1998-11-30
Support Year
17
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
John Wayne Cancer Institute
Department
Type
DUNS #
556074458
City
Santa Monica
State
CA
Country
United States
Zip Code
90404

  Publications

Jones, Maris S; Lee, Jihey; Stern, Stacey L et al. (2017) Is Pregnancy-Associated Melanoma Associated with Adverse Outcomes? J Am Coll Surg 225:149-158
Faries, Mark B; Thompson, John F; Cochran, Alistair J et al. (2017) Completion Dissection or Observation for Sentinel-Node Metastasis in Melanoma. N Engl J Med 376:2211-2222
Ozao-Choy, Junko; Nelson, Daniel W; Hiles, Jason et al. (2017) The prognostic importance of scalp location in primary head and neck melanoma. J Surg Oncol 116:337-343
Karakousis, Giorgos; Gimotty, Phyllis A; Bartlett, Edmund K et al. (2017) Thin Melanoma with Nodal Involvement: Analysis of Demographic, Pathologic, and Treatment Factors with Regard to Prognosis. Ann Surg Oncol 24:952-959
Jones, Maris S; Torisu-Itakura, Hitoe; Flaherty, Devin C et al. (2016) Second Primary Melanoma: Risk Factors, Histopathologic Features, Survival, and Implications for Follow-Up. Am Surg 82:1009-1013
Faries, Mark B (2016) Intralesional Immunotherapy for Metastatic Melanoma: The Oldest and Newest Treatment in Oncology. Crit Rev Oncog 21:65-73
Marzese, Diego M; Liu, Michelle; Huynh, Jamie L et al. (2015) Brain metastasis is predetermined in early stages of cutaneous melanoma by CD44v6 expression through epigenetic regulation of the spliceosome. Pigment Cell Melanoma Res 28:82-93
Wang, Jinhua; Hua, Wei; Huang, Sharon K et al. (2015) RASSF8 regulates progression of cutaneous melanoma through nuclear factor-?b. Oncotarget 6:30165-77
Faries, Mark B (2015) From the guest editor: The sentinel node: evolution of the revolution. Introduction. Cancer J 21:1-2
Ono, Shigeshi; Oyama, Takashi; Lam, Stella et al. (2015) A direct plasma assay of circulating microRNA-210 of hypoxia can identify early systemic metastasis recurrence in melanoma patients. Oncotarget 6:7053-64

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