Title: Newly Diagnosed with MelanomaNow What
1- Newly Diagnosed with MelanomaNow What?
- Bret Taback, MD
- Division of Surgical Oncology
- Columbia University Medical Center
- May 10, 2008
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4Obtain a Second Opinion
- Ask your
- Internist
- Family members
- Friends
- Colleagues
- Others who may have had melanoma
- Search online
5What to do Before Visiting the Doctors Office
- Make a list of questions before you arrive none
are foolish - Bring all records, i.e. path reports and slides,
any x-ray films/disks and reports, (prior
surgical records especially operative reports) - Come with a friend, family member, colleague
and/or physician - Bring a pencil and paper take notes (record if
necessary) - Ask for their business and call them if you have
future questions or concerns
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7 8First Description of Melanoma
- 1787
- John Hunter first published account of patient
with melanoma (recurrence) removal of tumor
behind the jaw, cancerous fungous excrescence - 1806
- Laennec first to describe melanoma as a disease
entity before the Faculty of Medicine in Paris as
la melanose melanosis
9Historical Aspects
- 1892
- Herbert Snow (1847-1930) Royal Marsden Hospital
- He rejects treatment of the primary tumor
with irritants i.e. ligature or silver
nitrate/caustics. - He recognizes death is due to metastasis
which he states first involves the nearest lymph
glands and radical removal of such organs is
indicated before enlargement takes place ELND -
10Handley Presents to The Royal College of Surgeons
- 1907
- William Sampson Handley (1872-1962)
- Senior Surgeon Middlesex Hospital gives two
Hunterian Lectures to the Royal College of
Surgeons (Feb 25 and Feb 27) - The first lecture was pathology of melanoma
- It was based on a single autopsy study - 34 y.o.
female with advanced metastasis - Suggested melanoma spread centrifugally through
the lymphatics first and then through the blood
(similar to breast cancer)
11- And thus radical primary tumor excision with
ELND survived for over half a century until the
1960s
12Primary Tumor
- Wallace H. Clark, Jr.
- 1969 defined anatomic levels of invasion
- Radial and vertical growth phase
- Alexander Breslow
- 1969 recognized tumor thickness as an important
prognostic factor - 1975 correlated thickness with survival
- Breslow Thickness (millimeters) 5-Year
Survival () - less than 0.76 97
- 0.76-1.50 92
- 1.51-2.50 762.51-4.0 624.1-8.0 52
- gt 8.0 32
13Melanoma Diagnosis
14Biopsy -gt Diagnosis
- Punch
- Incision
- Excision
- Shave
- Goals
- Make a diagnosis
- Rule out lesions with potentially similar
features - Determine depth and level of invasion, ulceration
15Surgical Treatment of Primary Melanoma
16 17Prognostic Factors for Primary MelanomaClinically
or Pathologically Staged Patients
Variable P Risk Ratio 95 CI Thickness lt.0000
1 1.558 1.473-1.647 Ulceration lt.00001 1.901 1.73
5-2.083 Age lt.00001 1.101 1.071-1.132 Site lt.000
01 1.338 1.224-1.463 Level of invasion
lt.00001 1.214 1.136-1.297 Sex .001 0.836 0.764-
0.915
J Clin Oncol. 2001193622-3634.
18Wide Excision Prospective Randomized Trials
Surgical Trial
n
Tumor Thickness
Arms
19Surgical Excision for Localized Cutaneous
MelanomaRecommended Margins
Melanoma Thickness
Margin
Melanoma in situ lt1 mm 14 mm gt4 mm
5 mm 1 cm 2 cm gt2 cm
NCCN Practice Guidelines Melanoma.
20Treatment of Primary Lesion Avoid Local
Recurrence
21US Intergroup Trial Results Surgical Margin
- n740 (486 randomized)
- Melanoma 1-4 mm
- 2 cm vs. 4 cm margin
- Median follow up gt10 years
- No difference in local recurrence
- 2.6 (4 cm) vs. 2.1 (2 cm)
- Skin grafts rates
- 46 (4 cm) vs. 11 (2 cm)
- Survival rates
- 77 (4 cm) vs 70 (2 cm) gt PNS
- Risk of LR based on primary tumor not margin
22Margins Matter
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26Prognostic Factors for Primary Melanoma Patients
Staged after Node Dissection
Variable P Risk Ratio 95 CI Nodal status
lt.00001 2.239 1.913-2.621 Thickness lt.00001
1.583 1.433-1.749 Ulceration
lt.00001 1.938 1.674-2.242 Site
lt.00001 1.483 1.281-1.716 Age
.0002 1.095 1.044-1.147 Sex .1705
0.900 0.774-1.046 Level of invasion .9082 1.007
0.896-1.131
J Clin Oncol. 2001193622-3634.
27- Lymph node status is the single most important
prognostic factor in patients diagnosed with
melanoma
28- Elective Lymph Node Dissection
29Elective Lymph Node Dissection (ELND)
Prospective Randomized Trials
Surgical Trial
n
Criteria Survival
Issues
30Disadvantage of Routine ELND
- 80 of patients do not have lymph node metastasis
at the time of melanoma diagnosis - No survival advantage
- Complete lymphadenectomy is associated with
considerable morbidity1
Complication No () Lymphedema 32
(29) Seroma 11 (13) Wound Flap
Prob 7 (6) Hematoma 1 (1)
1Sim et al Cancer 1978, 41948-956-630
31- Sentinel Lymph Node Biopsy
32Sentinel Lymph Node (SLN)Mapping and Biopsy
- Lymphatic metastases from tumor spread first
through afferent channels - Lymph node spread occurs in an orderly
progression - SLN is first node along those channels
Ann Surg. 1999230453465.
33Sentinel Lymph Node Studies
34Prognostic Implications of SLN Status on
Disease-Specific Survival
Disease-Specific Survival
Prognostic Factor
HR
95 CI
P value
- 6.53 3.39 12.58 lt.00001
- 1.23 1.10 1.38 .0004
- 2.32 1.03 5.23 .04
- 1.62 0.85 3.08 .14
- 1.72 0.85 3.45 .13
- 1.01 0.98 1.01 .57
- 1.11 0.45 1.82 .78
SLN status Tumor thickness Clark level
gtIII Ulceration Axial location Age Sex
HR Hazard ratio CI Confidence interval
J Clin Oncol. 199917976983.
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36MSLT Results
- Randomized trial WLE SLNB (w/ LND if ) vs.
WLE Observation - Inclusion Intermediate Thickness (1.2-3.5 mm),
no clinical LAD - Accrual 1994-2002, 1269 patients, analysis w/
median 60 mo follow-up - LN evaluated by HE and IHC for S100, HMB45,
(later MART-1 or Melan-A) - 16 SLN
- False negative rate (recurrence in same bed)
5-10, decreased w/ center volume and surgeon
experience
Morton et al 2006 3351307-1317
37Disease-free Survival and Melanoma-Specific
Survival, According to the Type of Treatment and
the Tumor Status of the Sentinel Node
Morton D et al. N Engl J Med 20063551307-1317
Morton et al 2006 3351307-1317
38Baseline Characteristics of MSLT Patients
39Rationale for Lymphadenectomy
- Improve regional disease control
- Enhance accuracy of staging
- Improve odds of survival ?
40Surgical Management of Clinical Stage I and II
Melanoma
SLN identified
Evaluate by hematoxylin/eosin
immunohistochemistry, stepped sections
Node negative
Node positive
Observation
En bloc dissection
Adjuvant therapy
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44Follow-up Staging Studies
- CXR
- CBC/Chem/LFTs (LDH)
- Stage III/IV
- CT scan chest/abdomen/pelvis (oral and IV
contrast) - PET scan
- MRI brain
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46Summary
- Prevention
- Avoid sun burning, protective clothing, sun block
- Detection
- Skin checks, Dermatology exam, Mole mapping
- Surgical treatment
- Biopsy -gt Melanoma Center appropriate surgery
(WLE, LM, SLNB, CLND) - Adjuvant therapy (stage III)
- Interferon
- Therapy for stage IV
- IL-2, Chemotherapy, Biochemotherapy, Surgery,
- Clinical trials
- Peptides
- Protein
- DNA/RNA
- Ganglioside
- Lysate
- Shed antigen
- Whole cells IFA
- Dendritic Cells