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{{CMG}} {{AE}} {{YD}}; {{SSK}}
 
{{CMG}} {{AE}} {{YD}}; {{SSK}}; {{S.M.}}
{{Melanoma}}
{{Melanoma}}


==Overview==
==Overview==
[[Malignant]] melanoma is the most common [[fatal]] [[skin cancer]] that arises from the [[Epidermis (skin)|epidermal]] [[Melanocyte|melanocytes]], which are [[Neural crest|neural crest cells]] involved in the synthesis of [[melanin]] (a brown pigment with photoprotective properties). The [[prevalence]] of melanoma is approximately 150 - 200 per 100,000 individuals. It may be caused by sporadic [[Mutation|genetic mutations]] (e.g. ''[[BRAF]]'' and/or ''[[Ras|N-RAS]]'') or may be part of familial syndromes (e.g. familial atypical multiple [[Melanocytic nevus|mole]] melanoma [[syndrome]]). Melanoma may be classified into either [[Skin|cutaneous]] or non-[[Skin|cutaneous]] melanomas. The most common 4 subtypes of [[Skin|cutaneous]] melanoma include superficial spreading melanoma, [[Nodule (medicine)|nodular]] melanoma, acral lentiginous melanoma, and [[lentigo]] maligna melanoma. Development of melanoma is the result of multiple [[Mutation|genetic mutations]] (multiple hits). The progression to melanoma usually involves the [[serine]]-[[threonine]] [[kinases]] of the [[MAPK/ERK pathway]] ([[mitogen]]-activated [[protein kinase]]) following [[mutation]] of either the ''[[Ras|N-RAS]]'' or ''[[BRAF]]'' [[oncogene]]. On [[gross pathology]], the majority of melanomas appear as [[Hyperkeratosis|hyperkeratotic]], black-brown, asymmetric [[nodule]]s with irregular borders, but the [[morphology]] of the [[lesion]] mostly depends on the subtype of melanoma and amelanotic (no pigmentation) melanomas are not uncommon. On [[microscopic]] [[Histopathology|histopathological]] analysis, each subtype of melanoma has unique characteristic features. The two most potent [[Risk factor|risk factors]] in the development of melanoma are light-colored [[skin]] and exposure to [[Ultraviolet|ultraviolet radiation]]. If left untreated, melanoma progression occurs both horizontally (radial growth plate) and vertically (vertical growth plate) and is then followed by [[Dermis|dermal]] invasion and distant [[metastasis]]. Common sites of [[metastasis]] include [[bone]]s, [[brain]], [[kidney]]s, [[lungs]], [[liver]], and [[skin]] (distant site). The 5-year relative survival of [[Patient|patients]] with melanoma is highly dependent on the stage at [[diagnosis]]. [[Cancer staging|Staging]] is based on the 2010 [[American Joint Committee on Cancer|AJCC]] [[TNM]] Classification and is divided into stage 0 or melanoma [[in situ]], stage I or invasive melanoma with good [[prognosis]], stage II or high-risk melanoma, stage III or melanoma with regional [[lymph node]] [[metastasis]], and stage IV or melanoma with distant [[metastasis]]. The predominant treatment for primary melanoma is wide excision of the [[lesion]] margins. The choice of clinical margins is based on the [[tumor]] thickness. When [[Lymph node|lymph nodes]] are involved, complete [[Dissection (medical)|dissection]] of the [[Lymph node|nodal]] basin is recommended. [[Chemotherapy]] is indicated for high risk melanomas (stages IIB-IV) as [[adjuvant therapy]] and for [[Metastasis|metastatic]] disease as first-line [[therapy]]. Once [[Diagnosis|diagnosed]], follow-up at regular intervals is recommended.
==Historical Perspective==
==Historical Perspective==
Melanoma was first described by Hippocrates in the 5th century BC. It was often described as the fatal black tumor. In 1838, the term ''melanoma'' was first proposed by Sir Robert Carswell, a British pathologist. In 1956, Henry Lancaster, an Australian mathematician, was the first to discover the association between UV radiation exposure and development of melanoma. In 2003, ''BRAF'' mutations were first identified in the pathogenesis of melanoma.
Melanoma was first described by Hippocrates in the 5th century BC. It was often described as the fatal black tumor. In 1838, the term ''melanoma'' was first proposed by Sir Robert Carswell, a British [[Pathology|pathologist]]. In 1956, Henry Lancaster, an Australian [[mathematician]], was the first to discover the association between [[Ultraviolet|UV radiation]] exposure and development of melanoma. In 2003, ''[[BRAF]]'' [[Mutation|mutations]] were first identified in the [[pathogenesis]] of melanoma.
==Classification==
==Classification==
Melanoma may be classified into either cutaneous or subcutaneous melanomas. The most common 4 subtypes of cutaneous melanoma include superficial spreading melanoma, nodular melanoma, acral lentiginous melanoma, and lentigo maligna melanoma. Less common subtypes of melanoma include desmoplastic/spindle cell melanoma, nevoid melanoma, spitzoid melanocytic melanoma, angiotropic melanoma, blue nevus-like melanoma, and composite melanoma.
Melanoma may be classified into either [[Skin|cutaneous]] or non-[[Skin|cutaneous]] melanomas. The most common 4 subtypes of [[Skin|cutaneous]] melanoma include superficial spreading melanoma, [[Nodule (medicine)|nodular]] melanoma, acral lentiginous melanoma, and lentigo maligna melanoma. Less common subtypes of melanoma include [[Desmoplasia|desmoplastic]]/spindle cell melanoma, nevoid melanoma, spitzoid melanocytic melanoma, angiotropic melanoma, blue nevus-like melanoma, and composite melanoma.
 
==Pathophysiology==
==Pathophysiology==
Development of melanoma is the result of multiple genetic mutations. The progression to melanoma usually involves the of serine-threonine kinases of the [[MAPK/ERK pathway]] (mitogen-activated protein kinase) following mutation of either the ''[[Ras|N-RAS]]'' or ''[[BRAF]]'' oncogene. On gross pathology, the majority of melanomas appear as hyperkeratotic, black-brown, asymmetric [[nodule]]s with irregular borders, but the morphology of the lesion mostly depends on the subtype of melanoma. On microscopic histopathological analysis, each subtype of melanoma has unique characteristic features.
[[Malignant]] melanoma arises from the [[Epidermis (skin)|epidermal]] [[Melanocyte|melanocytes]], which are [[Neural crest|neural crest cells]] involved in the synthesis of [[melanin]] (a brown pigment with photoprotective properties). Development of melanoma is the result of multiple [[Mutation|genetic mutations]]. The progression to melanoma usually involves the [[serine]]-[[threonine]] [[kinases]] of the [[MAPK/ERK pathway]] ([[mitogen]]-activated [[protein kinase]]) following [[mutation]] of either the ''[[Ras|N-RAS]]'' or ''[[BRAF]]'' [[oncogene]]. On [[gross pathology]], the majority of melanomas appear as [[Hyperkeratosis|hyperkeratotic]], black-brown, asymmetric [[nodule]]s with irregular borders, but the [[morphology]] of the [[lesion]] mostly depends on the subtype of melanoma. On [[microscopic]] [[Histopathology|histopathological]] analysis, each subtype of melanoma has unique characteristic features. All [[Patient|patients]] with suspected melanoma require [[biopsy]]. Findings on [[biopsy]] may distinguish the subtype and the [[Cancer staging|stage]] of melanoma.
 
==Causes==
==Causes==
Melanoma may be caused by sporadic genetic mutations (e.g. ''[[BRAF]]'' and/or ''[[Ras|N-RAS]]'') or may be part of familial syndromes (e.g. familial atypical multiple mole melanoma syndrome).
Melanoma may be caused by sporadic [[Mutation|genetic mutations]] (e.g. ''[[BRAF]]'' and/or ''[[Ras|N-RAS]]'') or may be part of familial [[Syndrome|syndromes]] (e.g. familial atypical multiple [[Melanocytic nevus|mole]] melanoma [[syndrome]]).
==Differential Diagnosis==
==Differential Diagnosis==
Melanoma must be differentiated from other causes of skin lesions, such as other skin cancers, premalignant skin tumors, and benign skin lesions.
Melanoma must be differentiated from other causes of [[Skin lesion|skin lesions]], such as other [[Skin cancer|skin cancers]], [[Premalignant condition|premalignant]] [[skin]] [[Tumor|tumors]], and [[benign]] [[Skin lesion|skin lesions]].
==Epidemiology and Demographics==
==Epidemiology and Demographics==
The prevalence of melanoma is approximately 150-200 per 100,000 individuals. The majority of patients are diagnosed after the age of 65 years. Melanoma is more common among males and individuals of Caucasian race.
The [[prevalence]] of melanoma is approximately 150 - 200 per 100,000 individuals. The majority of [[Patient|patients]] are [[Diagnosis|diagnosed]] after the age of 65 years. Melanoma is more common among males and individuals of Caucasian race.
==Risk Factors==
==Risk Factors==
The two most potent risk factors in the development of melanoma are light-colored skin and exposure to ultraviolet radiation. Other risk factors include old age, male gender, family history of melanoma, personal history of skin cancers, immunodeficiency, and certain hereditary disorders.
The two most potent [[Risk factor|risk factors]] in the development of melanoma are light-colored [[skin]] and exposure to [[Ultraviolet|ultraviolet radiation]]. Other [[risk factors]] include old age, male gender, family history of melanoma, personal history of [[Skin cancer|skin cancers]], [[immunodeficiency]], and certain [[Heredity|hereditary]] disorders.
==Screening==
==Screening==
According to the the U.S. Preventive Service Task Force (USPSTF), there is insufficient evidence to recommend routine screening for skin cancers, including melanoma.<ref name=USPSTF>{{cite web |url=http://www.uspreventiveservicestaskforce.org/Page/Document/RecommendationStatementFinal/skin-cancer-screening |title=USPSTF Skin Cancer Screening |access-date=20/8/2015}}</ref>
The 1992-1994 free [[American Academy of Dermatology|American Academy of Dermatology's]] National [[Skin]] [[Cancer (disease)|Cancer]] Early [[Detection theory|Detection]] and [[Screening (medicine)|Screening]] Program provided broad [[skin]] [[Cancer (disease)|cancer]] [[Education|educational]][[Information science|information]] to general [[Public health|public]] and enabled thousands of free [[Expert Patient Programme|expert]] [[skin]] [[Cancer (disease)|cancer]] [[Examination|examinations]]. The 2001-2005 [[American Academy of Dermatology]] National [[Melanoma]]/[[Skin]] [[Cancer (disease)|Cancer]] [[Screening (medicine)|Screening]] Program emphasized on the use of HARMM [[criteria]] to identify the higher-[[RiskMetrics|risk]] [[Subgroup analysis|subgroup]] of [[skin]] [[Cancer (disease)|cancer]] [[Screening (medicine)|screening]] [[Population (statistics)|population]] via [[Assessment and Plan|assessment]] of multiple [[risk factors]] for [[MM]] hence, both [[Reduced|reducing]] the [[Cost-effectiveness|cost]] & increasing the [[Yield (chemistry)|yields]] for suspected [[MM]] in [[Future interests (actuarial science)|future]] [[mass]] [[Screening (medicine)|screening]] [[Initiation (chemistry)|initiatives]]. [[Melanoma]][[Genetics]] Program identifies the [[genetic]] [[causes]] of [[skin]] [[Cancer (disease)|cancer]], and provides [[genetic counseling]] to the [[Individual growth|individuals]] with [[strong]] [[family history]] of [[melanoma]]. [[Dermoscopy]] [[Usage analysis|usage]] [[Improving agent|improves]] the [[Ability grouping|ability]] of [[Primary care physician|primary care physicians]] to [[triage]] [[lesions]] [[Suggestion|suggestive]] of [[skin]] [[Cancer (disease)|cancer,]] thus saving from [[Unnecessary Fuss|unnecessary]] [[Expert Patient Programme|expert]] [[Consultation|consultations]]. [[Combination therapy|Combination]] of [[dermoscopy]] and short-term [[Sequential analysis|sequential]] [[Digital dictation|digital]] [[dermoscopy]] [[imaging]] (SDDI) in a [[Primary care provider|primary care setting]] doubles the [[Sensitivity (tests)|sensitivity]] for [[melanoma]] [[diagnosis]]<nowiki/>and [[Lead|leads]] to >50% [[chance]] of [[reduction]] in [[excision]] or [[Reference|referral]] of [[benign]] [[pigmented lesions]].
 
==Natural History, Complications and Prognosis==
==Natural History, Complications and Prognosis==
If left untreated, melanoma progression occurs horizontally (radial growth plate) and vertically (vertical growth plate) and is then followed by dermal invasion and distant metastasis. Melanoma is an aggressive tumor characterized by early metastasis. Common sites of metastasis include [[bone]]s, [[brain]], [[kidney]]s, [[lungs]], [[liver]], and [[skin]] (distant site). Complications of melanoma are usually related to the site of metastasis. The 5-year relative survival of patients with melanoma is approximately 93%.<ref name="SEER">Howlader N, Noone AM, Krapcho M, Garshell J, Miller D, Altekruse SF, Kosary CL, Yu M, Ruhl J, Tatalovich Z,Mariotto A, Lewis DR, Chen HS, Feuer EJ, Cronin KA (eds). SEER Cancer Statistics Review, 1975-2011, National Cancer Institute. Bethesda, MD, http://seer.cancer.gov/csr/1975_2011/, based on November 2013 SEER data submission, posted to the SEER web site, April 2014.</ref> Features associated with worse [[prognosis]] are [[tumor]] thickness ([[Breslow's depth|Breslow thickness]]), depth related to skin structures (Clark level), type of melanoma, presence of ulceration, presence of lymphatic/perineural invasion, location of lesion, presence of satellite lesions, and presence of regional or distant metastasis.<ref>{{cite journal | author = Homsi J, Kashani-Sabet M, Messina J, Daud A | title = Cutaneous melanoma: prognostic factors. | journal = Cancer Control | volume = 12 | issue = 4 | pages = 223-9 | year = 2005 | id = PMID 16258493}}''[https://www.moffitt.usf.edu/pubs/ccj/v12n4/pdf/223.pdf Full text (PDF)]''</ref>
If left untreated, melanoma progression occurs horizontally (radial growth plate) and vertically (vertical growth plate) and is then followed by [[Dermis|dermal]] invasion and distant [[metastasis]]. Melanoma is an aggressive [[tumor]] characterized by early [[metastasis]]. Common sites of [[metastasis]] include [[bone]]s, [[brain]], [[kidney]]s, [[lungs]], [[liver]], and [[skin]] (distant site). [[Complication (medicine)|Complications]] of melanoma are usually related to the site of [[metastasis]]. The 5-year relative survival of [[Patient|patients]] with melanoma is approximately 93%. Features associated with worse [[prognosis]] are [[tumor]] thickness ([[Breslow's depth|Breslow thickness]]), depth related to [[skin]] structures (Clark level), type of melanoma, presence of [[Ulcer|ulceration]], presence of [[Lymphatic system|lymphatic]]/[[Perineurium|perineural]] invasion, location of [[lesion]], presence of satellite [[Lesion|lesions]], and presence of regional or distant [[metastasis]].


==Diagnosis==
==Diagnosis==
===History and Symptoms===
===History and Symptoms===
Symptoms of melanoma include a rapidly growing existing [[nevus]], [[Ulcer|non-healing skin ulcers]], [[pruritus]], or [[bone pain]].
[[Symptom|Symptoms]] of melanoma include a rapidly growing existing [[nevus]], [[Ulcer|non-healing skin ulcers]], [[pruritus]], or [[bone pain]].
===Physical Examination===
===Physical Examination===
Physical examination findings suggestive of malignant melanoma include ABCD: <u>A</u>symmetry of lesion, <u>B</u>order irregularity, <u>C</u>olor change, and large <u>D</u>iameter.
[[Physical examination]] findings suggestive of [[malignant]] melanoma include ABCDE: <u>A</u>symmetry of [[lesion]], <u>B</u>order irregularity, <u>C</u>olor change, large [[Diameter|<u>D</u>iameter]], and <u>E</u>volution over time.


===Laboratory Findings===
===Laboratory Findings===
There are no laboratory findings associated with the diagnosis of melanoma. Serum [[lactate dehydrogenase]] (LDH) may be elevated among patients with metastasis.
There are no [[Medical laboratory|laboratory]] findings associated with the [[diagnosis]] of melanoma. [[Serum]] [[lactate dehydrogenase|lactate dehydrogenase (LDH)]] may be elevated among [[Patient|patients]] with [[metastasis]].


===Biopsy===
===Biopsy===
All patients with suspected melanoma require biopsy. Findings on biopsy may distinguish the subtype and the stage of melanoma.
All [[Patient|patients]] with suspected melanoma require [[biopsy]]. Findings on [[biopsy]] may distinguish the subtype and the [[Cancer staging|stage]] of melanoma.
===Staging===
===Staging===
Staging of melanoma is essential to determine the prognosis. Staging is based on the 2010 AJCC TNM Classification<ref name="pmid19917835">{{cite journal| author=Balch CM, Gershenwald JE, Soong SJ, Thompson JF, Atkins MB, Byrd DR et al.| title=Final version of 2009 AJCC melanoma staging and classification. | journal=J Clin Oncol | year= 2009 | volume= 27 | issue= 36 | pages= 6199-206 | pmid=19917835 | doi=10.1200/JCO.2009.23.4799 | pmc=PMC2793035 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19917835  }} </ref> and is divided into stage 0 or melanoma in situ, stage I or invasive melanoma with good prognosis, stage II or high-risk melanoma, stage III or melanoma with regional lymph node metastasis, and stage IV or melanoma with distant metastasis.
[[Cancer staging|Staging]] of melanoma is essential to determine the [[prognosis]]. [[Cancer staging|Staging]] is based on the 2010 [[American Joint Committee on Cancer|AJCC]] [[TNM]] Classification and is divided into stage 0 or melanoma [[in situ]], stage I or invasive melanoma with good [[prognosis]], stage II or high-risk melanoma, stage III or melanoma with regional [[lymph node]] [[metastasis]], and stage IV or melanoma with distant [[metastasis]].


===Chest X Ray===
===Chest X Ray===
There are no chest x-ray findings associated with melanoma.
There are no [[Chest X-ray|chest x-ray]] findings associated with melanoma.
===CT===
===CT===
There are no CT scan findings associated with melanoma. Chest CT scan is recommended for diagnosis of metastatic lesions among patients who have been diagnosed with stage IA-IV melanoma and for secondary prevention of melanoma among patients who were previously diagnosed with Stage IIB-IV melanoma (annually for 5 years).<ref name="pmid23584343">{{cite journal| author=Coit DG, Andtbacka R, Anker CJ, Bichakjian CK, Carson WE, Daud A et al.| title=Melanoma, version 2.2013: featured updates to the NCCN guidelines. | journal=J Natl Compr Canc Netw | year= 2013 | volume= 11 | issue= 4 | pages= 395-407 | pmid=23584343 | doi= | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=23584343  }} </ref>
There are no [[Computed tomography|CT scan]] findings associated with melanoma. [[Chest]] [[Computed tomography|CT scan]] is recommended for [[diagnosis]] of [[Metastasis|metastatic]] [[Lesion|lesions]] among [[Patient|patients]] who have been [[Diagnosis|diagnosed]] with [[Cancer staging|stage]] IA-IV melanoma and for [[Prevention (medical)|secondary prevention]] of melanoma among [[Patient|patients]] who were previously [[Diagnosis|diagnosed]] with [[Cancer staging|stage]] IIB-IV melanoma (annually for 5 years).


===MRI===
===MRI===
There are no MRI scan findings associated with melanoma. Brain MRI may be considered for diagnosis of metastatic lesions among patients who have been diagnosed with stage IA-IV melanoma and for secondary prevention of melanoma among patients who were previously diagnosed with Stage IIB-IV melanoma (annually for 5 years).<ref name="pmid23584343">{{cite journal| author=Coit DG, Andtbacka R, Anker CJ, Bichakjian CK, Carson WE, Daud A et al.| title=Melanoma, version 2.2013: featured updates to the NCCN guidelines. | journal=J Natl Compr Canc Netw | year= 2013 | volume= 11 | issue= 4 | pages= 395-407 | pmid=23584343 | doi= | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=23584343  }} </ref>
There are no [[Magnetic resonance imaging|MRI scan]] findings associated with melanoma. [[Brain]] [[Magnetic resonance imaging|MRI]] may be considered for [[diagnosis]] of [[Metastasis|metastatic]] [[Lesion|lesions]] among [[Patient|patients]] who have been [[Diagnosis|diagnosed]] with [[Cancer staging|stage]] IA-IV melanoma and for [[Prevention (medical)|secondary prevention]] of melanoma among [[Patient|patients]] who were previously [[Diagnosis|diagnosed]] with [[Cancer staging|stage]] IIB-IV melanoma (annually for 5 years).
===Echocardiography or Ultrasound===
===Echocardiography or Ultrasound===
There are no ultrasound findings associated with melanoma.
There are no [[ultrasound]] findings associated with melanoma.
===Other Imaging Findings===
===Other Imaging Findings===
There are no PET scan findings associated with melanoma. Chest PET scan may be considered for diagnosis of metastatic lesions among patients who have been diagnosed with stage IA-IV melanoma and for secondary prevention of melanoma among patients who were previously diagnosed with Stage IIB-IV melanoma (annually for 5 years).<ref name="pmid23584343">{{cite journal| author=Coit DG, Andtbacka R, Anker CJ, Bichakjian CK, Carson WE, Daud A et al.| title=Melanoma, version 2.2013: featured updates to the NCCN guidelines. | journal=J Natl Compr Canc Netw | year= 2013 | volume= 11 | issue= 4 | pages= 395-407 | pmid=23584343 | doi= | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=23584343  }} </ref>
There are no [[Positron emission tomography|PET scan]] findings associated with melanoma. [[Chest]] [[Positron emission tomography|PET]] scan may be considered for [[diagnosis]] of [[Metastasis|metastatic]] [[Lesion|lesions]] among [[Patient|patients]] who have been [[Diagnosis|diagnosed]] with [[Cancer staging|stage]] IA-IV melanoma and for [[Prevention (medical)|secondary prevention]] of melanoma among [[Patient|patients]] who were previously [[Diagnosis|diagnosed]] with [[Cancer staging|stage]] IIB-IV melanoma (annually for 5 years).
===Other Diagnostic Studies===
===Other Diagnostic Studies===
No additional tests are recommended for the diagnosis of melanoma.
No additional tests are recommended for the [[diagnosis]] of melanoma.
==Treatment==
==Treatment==
===Medical Therapy===
===Medical Therapy===
Chemotherapy is indicated for high risk melanomas (stages IIB-IV) as adjuvant therapy and for metastatic disease as first-line therapy. Several single agent and combination regimens have been studied, all with modest impact on survival. All current guidelines still recommend enrollment in clinical trials over current available regimens for patients with metastatic disease. Interferon therapy is the only regimen recommended for adjuvant therapy.
[[Chemotherapy]] is indicated for high risk melanomas ([[Cancer staging|stages]] IIB-IV) as [[adjuvant therapy]] and for [[Metastasis|metastatic]] disease as first-line [[therapy]]. Several single agent and combination regimens have been studied, all with modest impact on survival. All current guidelines still recommend enrollment in [[Clinical trial|clinical trials]] over current available regimens for [[Patient|patients]] with [[Metastasis|metastatic]] disease. [[Interferon]] [[therapy]] is the only regimen recommended as [[adjuvant therapy]].
===Surgery===
===Surgery===
The predominant treatment for primary melanoma is wide excision of the lesion margins. The choice of clinical margins is based on the tumor thickness. When lymph nodes are involved, complete dissection of the nodal basin is recommended.
The predominant treatment for primary melanoma is wide [[excision]] of the [[lesion]] margins. The choice of clinical margins is based on the [[tumor]] thickness. When [[Lymph node|lymph nodes]] are involved, complete [[Dissection (medical)|dissection]] of the [[Lymph node|nodal]] basin is recommended.
===Primary Prevention===
===Primary Prevention===
Primary prevention of melanoma includes avoidance of sunlight/ultraviolet radiation exposure.<ref name="pmid11126854">{{cite journal| author=Edman RL, Wolfe JT| title=Prevention and early detection of malignant melanoma. | journal=Am Fam Physician | year= 2000 | volume= 62 | issue= 10 | pages= 2277-85 | pmid=11126854 | doi= | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=11126854  }} </ref>
[[Prevention (medical)|Primary prevention]] of melanoma includes avoidance of [[sunlight]]/[[Ultraviolet|ultraviolet radiation]] exposure.


===Secondary Prevention===
===Secondary Prevention===
The choice of work-up for secondary prevention of melanoma is based on the stage of melanoma at diagnosis. Secondary prevention includes monthly self-exams, routine dermatologic evaluations, and chest and brain imaging.
The choice of work-up for [[Prevention (medical)|secondary prevention]] of melanoma is based on the [[Cancer staging|stage]] of melanoma at [[diagnosis]]. [[Prevention (medical)|Secondary prevention]] includes monthly self-exams, routine [[Dermatology|dermatologic]] evaluations, and [[chest]] and [[brain]] [[imaging]].


==References==
==References==
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[[Category:Up-To-Date]]
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Latest revision as of 17:12, 16 July 2019


Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Yazan Daaboul, M.D.; Serge Korjian M.D.; Sara Mohsin, M.D.[2]

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Overview

Malignant melanoma is the most common fatal skin cancer that arises from the epidermal melanocytes, which are neural crest cells involved in the synthesis of melanin (a brown pigment with photoprotective properties). The prevalence of melanoma is approximately 150 - 200 per 100,000 individuals. It may be caused by sporadic genetic mutations (e.g. BRAF and/or N-RAS) or may be part of familial syndromes (e.g. familial atypical multiple mole melanoma syndrome). Melanoma may be classified into either cutaneous or non-cutaneous melanomas. The most common 4 subtypes of cutaneous melanoma include superficial spreading melanoma, nodular melanoma, acral lentiginous melanoma, and lentigo maligna melanoma. Development of melanoma is the result of multiple genetic mutations (multiple hits). The progression to melanoma usually involves the serine-threonine kinases of the MAPK/ERK pathway (mitogen-activated protein kinase) following mutation of either the N-RAS or BRAF oncogene. On gross pathology, the majority of melanomas appear as hyperkeratotic, black-brown, asymmetric nodules with irregular borders, but the morphology of the lesion mostly depends on the subtype of melanoma and amelanotic (no pigmentation) melanomas are not uncommon. On microscopic histopathological analysis, each subtype of melanoma has unique characteristic features. The two most potent risk factors in the development of melanoma are light-colored skin and exposure to ultraviolet radiation. If left untreated, melanoma progression occurs both horizontally (radial growth plate) and vertically (vertical growth plate) and is then followed by dermal invasion and distant metastasis. Common sites of metastasis include bones, brain, kidneys, lungs, liver, and skin (distant site). The 5-year relative survival of patients with melanoma is highly dependent on the stage at diagnosis. Staging is based on the 2010 AJCC TNM Classification and is divided into stage 0 or melanoma in situ, stage I or invasive melanoma with good prognosis, stage II or high-risk melanoma, stage III or melanoma with regional lymph node metastasis, and stage IV or melanoma with distant metastasis. The predominant treatment for primary melanoma is wide excision of the lesion margins. The choice of clinical margins is based on the tumor thickness. When lymph nodes are involved, complete dissection of the nodal basin is recommended. Chemotherapy is indicated for high risk melanomas (stages IIB-IV) as adjuvant therapy and for metastatic disease as first-line therapy. Once diagnosed, follow-up at regular intervals is recommended.

Historical Perspective

Melanoma was first described by Hippocrates in the 5th century BC. It was often described as the fatal black tumor. In 1838, the term melanoma was first proposed by Sir Robert Carswell, a British pathologist. In 1956, Henry Lancaster, an Australian mathematician, was the first to discover the association between UV radiation exposure and development of melanoma. In 2003, BRAF mutations were first identified in the pathogenesis of melanoma.

Classification

Melanoma may be classified into either cutaneous or non-cutaneous melanomas. The most common 4 subtypes of cutaneous melanoma include superficial spreading melanoma, nodular melanoma, acral lentiginous melanoma, and lentigo maligna melanoma. Less common subtypes of melanoma include desmoplastic/spindle cell melanoma, nevoid melanoma, spitzoid melanocytic melanoma, angiotropic melanoma, blue nevus-like melanoma, and composite melanoma.

Pathophysiology

Malignant melanoma arises from the epidermal melanocytes, which are neural crest cells involved in the synthesis of melanin (a brown pigment with photoprotective properties). Development of melanoma is the result of multiple genetic mutations. The progression to melanoma usually involves the serine-threonine kinases of the MAPK/ERK pathway (mitogen-activated protein kinase) following mutation of either the N-RAS or BRAF oncogene. On gross pathology, the majority of melanomas appear as hyperkeratotic, black-brown, asymmetric nodules with irregular borders, but the morphology of the lesion mostly depends on the subtype of melanoma. On microscopic histopathological analysis, each subtype of melanoma has unique characteristic features. All patients with suspected melanoma require biopsy. Findings on biopsy may distinguish the subtype and the stage of melanoma.

Causes

Melanoma may be caused by sporadic genetic mutations (e.g. BRAF and/or N-RAS) or may be part of familial syndromes (e.g. familial atypical multiple mole melanoma syndrome).

Differential Diagnosis

Melanoma must be differentiated from other causes of skin lesions, such as other skin cancers, premalignant skin tumors, and benign skin lesions.

Epidemiology and Demographics

The prevalence of melanoma is approximately 150 - 200 per 100,000 individuals. The majority of patients are diagnosed after the age of 65 years. Melanoma is more common among males and individuals of Caucasian race.

Risk Factors

The two most potent risk factors in the development of melanoma are light-colored skin and exposure to ultraviolet radiation. Other risk factors include old age, male gender, family history of melanoma, personal history of skin cancers, immunodeficiency, and certain hereditary disorders.

Screening

The 1992-1994 free American Academy of Dermatology's National Skin Cancer Early Detection and Screening Program provided broad skin cancer educationalinformation to general public and enabled thousands of free expert skin cancer examinations. The 2001-2005 American Academy of Dermatology National Melanoma/Skin Cancer Screening Program emphasized on the use of HARMM criteria to identify the higher-risk subgroup of skin cancer screening population via assessment of multiple risk factors for MM hence, both reducing the cost & increasing the yields for suspected MM in future mass screening initiatives. MelanomaGenetics Program identifies the genetic causes of skin cancer, and provides genetic counseling to the individuals with strong family history of melanoma. Dermoscopy usage improves the ability of primary care physicians to triage lesions suggestive of skin cancer, thus saving from unnecessary expert consultations. Combination of dermoscopy and short-term sequential digital dermoscopy imaging (SDDI) in a primary care setting doubles the sensitivity for melanoma diagnosisand leads to >50% chance of reduction in excision or referral of benign pigmented lesions.

Natural History, Complications and Prognosis

If left untreated, melanoma progression occurs horizontally (radial growth plate) and vertically (vertical growth plate) and is then followed by dermal invasion and distant metastasis. Melanoma is an aggressive tumor characterized by early metastasis. Common sites of metastasis include bones, brain, kidneys, lungs, liver, and skin (distant site). Complications of melanoma are usually related to the site of metastasis. The 5-year relative survival of patients with melanoma is approximately 93%. Features associated with worse prognosis are tumor thickness (Breslow thickness), depth related to skin structures (Clark level), type of melanoma, presence of ulceration, presence of lymphatic/perineural invasion, location of lesion, presence of satellite lesions, and presence of regional or distant metastasis.

Diagnosis

History and Symptoms

Symptoms of melanoma include a rapidly growing existing nevus, non-healing skin ulcers, pruritus, or bone pain.

Physical Examination

Physical examination findings suggestive of malignant melanoma include ABCDE: Asymmetry of lesion, Border irregularity, Color change, large Diameter, and Evolution over time.

Laboratory Findings

There are no laboratory findings associated with the diagnosis of melanoma. Serum lactate dehydrogenase (LDH) may be elevated among patients with metastasis.

Biopsy

All patients with suspected melanoma require biopsy. Findings on biopsy may distinguish the subtype and the stage of melanoma.

Staging

Staging of melanoma is essential to determine the prognosis. Staging is based on the 2010 AJCC TNM Classification and is divided into stage 0 or melanoma in situ, stage I or invasive melanoma with good prognosis, stage II or high-risk melanoma, stage III or melanoma with regional lymph node metastasis, and stage IV or melanoma with distant metastasis.

Chest X Ray

There are no chest x-ray findings associated with melanoma.

CT

There are no CT scan findings associated with melanoma. Chest CT scan is recommended for diagnosis of metastatic lesions among patients who have been diagnosed with stage IA-IV melanoma and for secondary prevention of melanoma among patients who were previously diagnosed with stage IIB-IV melanoma (annually for 5 years).

MRI

There are no MRI scan findings associated with melanoma. Brain MRI may be considered for diagnosis of metastatic lesions among patients who have been diagnosed with stage IA-IV melanoma and for secondary prevention of melanoma among patients who were previously diagnosed with stage IIB-IV melanoma (annually for 5 years).

Echocardiography or Ultrasound

There are no ultrasound findings associated with melanoma.

Other Imaging Findings

There are no PET scan findings associated with melanoma. Chest PET scan may be considered for diagnosis of metastatic lesions among patients who have been diagnosed with stage IA-IV melanoma and for secondary prevention of melanoma among patients who were previously diagnosed with stage IIB-IV melanoma (annually for 5 years).

Other Diagnostic Studies

No additional tests are recommended for the diagnosis of melanoma.

Treatment

Medical Therapy

Chemotherapy is indicated for high risk melanomas (stages IIB-IV) as adjuvant therapy and for metastatic disease as first-line therapy. Several single agent and combination regimens have been studied, all with modest impact on survival. All current guidelines still recommend enrollment in clinical trials over current available regimens for patients with metastatic disease. Interferon therapy is the only regimen recommended as adjuvant therapy.

Surgery

The predominant treatment for primary melanoma is wide excision of the lesion margins. The choice of clinical margins is based on the tumor thickness. When lymph nodes are involved, complete dissection of the nodal basin is recommended.

Primary Prevention

Primary prevention of melanoma includes avoidance of sunlight/ultraviolet radiation exposure.

Secondary Prevention

The choice of work-up for secondary prevention of melanoma is based on the stage of melanoma at diagnosis. Secondary prevention includes monthly self-exams, routine dermatologic evaluations, and chest and brain imaging.

References

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