Post on 12-Jan-2016
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Patient
64 yo caucasian woman noted to have elevated LFTs on annual P.E. Felt well.
US Liver: 9 cm mass in right lobe of liverBiopsy: Melanoma, high mitotic rate
PMH: Melanoma in situ removed from scalp 14 years earlier
Patient
PMH: Htn, osteoporosisFamHx: Fa had prostate cancer; died of
other causes at age 89; mother died of natural causes at age 84. Two healthy children. No other malignancies in family
SH: Married. Choir director, pianist. Rare EtOH. Remote, brief tobacco use.
Patient
ROS: Mild fatigue, mild dyspnea with exertion, dry cough, 3# wt loss
PE: Normal vital signs. Normal funduscopic exam. No adenopathy. Normal lung exam. Normal abdominal exam. Normal skin exam.
Labs: Alk Phos 160; AST 64; ALT 46
Patient
CT chest: 3 nodules, largest 7 cm in right lung base
CT abdomen: 4 liver mets, largest 9 cm; bilateral adrenal mets, 7 cm
MRI brain: Normal
Melanoma
54,000 new cases in 2003; 7600 deathsIncidence risingLifetime risk 1 in 82 for women; 1 in 58
for menNinth most common cancer; second in
terms of loss of years of potential lifeAt presentation, 84% localized; 12%
regional; 4% distant metastatic disease
Risk Factors for Melanoma
Fair complexion with red/blonde hairLiving in Australia (3X US incidence)>5 nevi >5mm or >50 nevi over 2mmDysplastic nevus syndrome Intense, intermittent sun exposure (ages 10-19)Family history of melanoma- 1/3 have mutation
in p16 (INK4a =CDKN2A cyclin dependent kinase) on chromosome 9p21
UV Light & Melanoma
Intense intermittent exposure does not give time for melanocytes to synthesize melanin to protect them from UV-B irradiation & subsequent DNA mutations
Melanocytes contain antiapoptotic proteins that inhibit cell death after intense UV exposure
Genetic Basis of Hereditary Melanoma
CDKN2A gene on 9p21: p16 protein that prevents phosphorylation of RB protein which regulates transcription factors and cell division
Mutations in this tumor suppressor gene can lead to unregulated cell growth
Associated with increased risk of pancreatic caAssociation of this mutation with atypical moles
is unclearGenetic testing is commercially available
Other proto-oncogene links
Mutation in B-raf protooncogene in 65% of melanomas
This gene product is similar to the tyrosine kinase targeted by Gleevec which has been very successful in treating CML and GIST
Inhibitors of this gene are undergoing testing (BAY 43-9006)
Melanoma Staging
Stage 0: melanoma in situ (95% cure rate)Stage IA: <1 mm, level II-III, no ulceration (88% IB: <1mm, level IV-V or 1-2 mm, no ulcer(79%) IIA: 1-2mm with ulcer; 2-4mm, no ulcer (64%) IIC: >4mm, with ulcer (45%) IIIA: Microscopic node met (55%) IIIB: Micro2 or 3 regional nodes (37%) IIIC: Macroscopic dz in 2 or 3 nodes (20%) IV: Distant metastases (<5%)
Melanoma
Breslow: thickness of the melanoma, most useful prognostic factor
Clark’s: level of penetration- (I)confined to epidermis, (II) into papillary dermis, (IV) into reticular dermis, (IV) into subcutaneous fat
Melanoma
Prognostic factors for localized disease: Breslow’s thickness, ulceration, Clark’s level (only for <1mm), primary tumor site, gender
Ulceration: absence of an intact epidermis overlying the melanoma (microscopic)
Likelihood of regional nodal involvement rises with increasing tumor thickness
Treatment of Melanoma
In situ: Excision< 1mm deep, 1 cm excision margin1-2 mm deep, 1 to 2 cm margin>2 mm deep, 2 cm marginConsider sentinel node evaluation if >1mm
deep with Clark level IV or ulcerated; node dissection only if positive
Adjuvant Therapy in Melanoma
Most pts with in situ or early stage disease are cured by excision alone
For node negative patients with <4mm without ulceration or <1mm with ulceration, no proven benefit
Clinical trial or high dose interferon adjuvant therapy appropriate for >4mm without ulceration & >1mm with ulceration
Improved relapse free survival but no improvement in overall survival in these node negative patients
Adjuvant Therapy in Melanoma
For node positive patients whose disease has been resected: Adjuvant high dose interferon prolongs survival (37% 5yr RFS vs 26% with no Rx)
20 million U/m2 IV 5 d/wk x 4 wks then 10 million U/m2 SQ 3 d/wk x 48 wks
Follow up after excision
Stage 0: skin exams for life IA: exam q3 to 12 mos IB-III: history, physical exam (attn to regional
node area), skin exam q3-6 mos x 3 yrs, q4-12 mos x 2 years, then annually. CXR, LDH, CBC “amy be considered”. CTs and PET scans not recommended.
Lifetime risk for developing second melanoma: 5%
Treatment of Metastatic Disease
Solitary site: resect (often wait 8 to 12 wks to be sure there are not many subclinical sites)
Multiple sites: clinical trial vs systemic therapy (Dacarbazine or Temazolamide or IL-2 or combination chemoimmunotherapy [Dacarbazine + Vinblastine+ cisPlatin + IL2 + Interferon)
Treatment of Metastatic Disease
BiochemotherapyCisplatinum 20mg/m2 daily x 4dVinblastine 1.6 mg/m2 daily x 4dDTIC 800 mg/m2 day 1 onlyInterleukin-2 9 million U/m2/d x 4d CIVInterferon alpha: 5 million U/m2 SQ qd x 5Repeat q3 wks
Treatment of Metastatic Disease
Biochemotherapy21% Complete response43% partial responseHalf of the patients with CR remained in
remission >5 years.This complete response rate is ~3X greater
than with single agent chemo
Other drugs
Thalidomide: active in myeloma, gliomas, renal cell cancer
Antiangiogenesis and anti-inflammatory properties; inhibits TNF
When given with temozolomide, 25% respond
Vaccine therapy in melanoma
Rare spontaneous regression of metastatic melanoma suggests host immunity plays important role in control
CancerVax: whole cell vaccine from 3 melanoma cell lines helpful in initial trial
Melacine: immunizes with 3 peptides present in/on melanoma cells; studies ongoing
No vaccine has thus far improved survival in adjuvant or metastatic setting
Patient Follow Up
3 cycles of chemoimmunotherapyLung nodule decreased from 7 to 5 cmNo change in liver masses but LFTs normalizedAdrenal metastases decreased from 7 to 5 cmMesenteric adenopathy improvedThalidomide + Temozolamide planned for 8
weeks
Lessons
Even in situ lesions can spreadDon’t allow kids to get sunburnsLook at your patients skin (everywhere)
during annual examUnderstanding the molecular biology may
lead to better treatments