Melanoma
Classification and external resources
A melanoma
ICD-10	C43
ICD-9	172.9
ICD-O:	M8720/3
OMIM	155600
DiseasesDB	7947
MedlinePlus	000850
eMedicine	derm/257 med/1386 ent/27 plastic/456
MeSH	D008545

Melanoma ⁱ/ˌmɛləˈnoʊmə/ (from Greek μέλας — melas, "dark"^[1]) is a malignant tumor of melanocytes. Melanocytes are cells that produce the dark pigment, melanin, which is responsible for the color of skin. They predominantly occur in skin, but are also found in other parts of the body, including the bowel and the eye (see uveal melanoma). Melanoma can originate in any part of the body that contains melanocytes.

Melanoma is less common than other skin cancers. However, it is much more dangerous if it is not found early. It causes the majority (75%) of deaths related to skin cancer.^[2] Worldwide, doctors diagnose about 160,000 new cases of melanoma yearly. It is more common in women than in men. In women, the most common site is the legs and melanomas in men are most common on the back. ^[3] It is particularly common among Caucasians, especially northern Europeans living in sunny climates. There are high rates of incidence in Australia, New Zealand, North America (especially Texas and Florida), Latin America, and Northern Europe,^[4] with a paradoxical decrease in southern Italy and Sicily.^[5] This geographic pattern reflects the primary cause, ultraviolet light (UV) exposure ^[6] crossed with the amount of skin pigmentation in the population ^[7][8]

According to a WHO report, about 48,000 melanoma related deaths occur worldwide per year.^[9]

Signs and symptoms[link]

Early signs of melanoma are changes to the shape or color of existing moles or, in the case of nodular melanoma, the appearance of a new lump anywhere on the skin (such lesions should be referred without delay to a dermatologist). At later stages, the mole may itch, ulcerate or bleed.^[10] Early signs of melanoma are summarized by the mnemonic "ABCDE":

• Asymmetry
• Borders (irregular)
• Color (variegated), and
• Diameter (greater than 6 mm (0.24 in), about the size of a pencil eraser)
• Evolving over time

These classifications do not, however, apply to the most dangerous form of melanoma, nodular melanoma, which has its own classifications:

• Elevated above the skin surface
• Firm to the touch
• Growing

Metastatic melanoma may cause nonspecific paraneoplastic symptoms, including loss of appetite, nausea, vomiting and fatigue.Metastasis of early melanoma is possible, but relatively rare: less than a fifth of melanomas diagnosed early become metastatic. Brain metastases are particularly common in patients with metastatic melanoma.^[11] It can also spread to the liver, bones, abdomen or distant lymph nodes.

Cause[link]

All cancers are caused by damage to the DNA inside cells. This damage can be inherited in the form of genetic mutations, but in most cases, it builds up over a person's lifetime and is caused by factors in their environment. DNA damage causes the cell to grow out of control, leading to a tumor. Melanoma is usually caused by damage from UV light from the sun, but UV light from sunbeds can also contribute to the disease.^[12]

Natural history [link]

The earliest stage of melanoma starts when the melanocytes begin to grow out of control. Melanocytes are found between the outer layer of the skin (the epidermis) and the next layer (the dermis). This early stage of the disease is called the radial growth phase, and the tumour is less than 1mm thick. Because the cancer cells have not yet reached the blood vessels lower down in the skin, it is very unlikely that this early-stage cancer will spread to other parts of the body. If the melanoma is detected at this stage, then it can usually be completely removed with surgery.

When the tumour cells start to move in a different direction — vertically up into the epidermis and into the papillary dermis — the behaviour of the cells changes dramatically.^[13]

The next step in the evolution is the invasive radial growth phase, which is a confusing term; however, it explains the next step in the process of the radial growth, when individual cells start to acquire invasive potential. This step is important – from this point on the melanoma is capable of spreading. The Breslow's depth of the lesion is usually less than1 mm (0.04 in), the Clark level is usually 2.

The following step in the process is the invasive melanoma — the vertical growth phase (VGP). The tumour attains invasive potential, meaning it can grow into the surrounding tissue and can spread around the body through blood or lymph vessels. The tumour thickness is usually more than 1 mm (0.04 in), and the tumour involves the deeper parts of the dermis.

The host elicits an immunological reaction against the tumour (during the VGP),^[14] which is judged by the presence and activity of the tumour infiltrating lymphocytes (TILs). These cells sometimes completely destroy the primary tumour; this is called regression, which is the latest stage of the melanoma development. In certain cases, the primary tumour is completely destroyed and only the metastatic tumour is discovered.

Genetics[link]

A number of rare mutations, which often run in families, are known to greatly increase one’s susceptibility to melanoma. Several different genes have been identified as increasing the risk of developing melanoma. Some rare genes have a relatively high risk of causing melanoma; some more common genes, such as a gene called MC1R that causes red hair, have a relatively low risk. Genetic testing can be used to determine whether a person has one of the currently known mutations.

One class of mutations affects the gene CDKN2A. An alternative reading frame mutation in this gene leads to the destabilization of p53, a transcription factor involved in apoptosis and in fifty percent of human cancers. Another mutation in the same gene results in a nonfunctional inhibitor of CDK4, a [cyclin-dependent kinase] that promotes cell division. Mutations that cause the skin condition xeroderma pigmentosum (XP) also seriously predispose one to melanoma. Scattered throughout the genome, these mutations reduce a cell’s ability to repair DNA. Both CDKN2A and XP mutations are highly penetrant^{[clarification needed]}.

Familial melanoma is genetically heterogeneous,^[15] and loci for familial melanoma have been identified on the chromosome arms 1p, 9p and 12q. Multiple genetic events have been related to the pathogenesis (disease development) of melanoma.^[16] The multiple tumor suppressor 1 (CDKN2A/MTS1) gene encodes p16INK4a — a low-molecular weight protein inhibitor of cyclin-dependent protein kinases (CDKs) — which has been localised to the p21 region of human chromosome 9.^[17]

Other mutations confer lower risk, but are more prevalent in the population. People with mutations in the MC1R gene, for example, are two to four times more likely to develop melanoma than those with two wild-type (typical unaffected type) copies of the gene. MC1R mutations are very common; in fact, all people with red hair have a mutated copy of the gene.

Two-gene models of melanoma risk have already been created,^{[citation needed]} and in the future, researchers hope to create genome-scale models that will allow them to predict a patient’s risk of developing melanoma based on his or her genotype.

In addition to identifying high-risk patients, researchers want to identify high-risk lesions (abnormal area of tissue) within a given patient. Many new technologies, such as optical coherence tomography(OCT), are being developed to accomplish this. OCT allows pathologists to view three-dimensional reconstructions of the skin and offers more resolution than past techniques could provide. In vivo confocal microscopy and fluorescently tagged antibodies are also proving to be valuable diagnostic tools.

Mutation of the MDM2 SNP309 gene is associated with increased risk of melanoma in younger women.^[18]

UV radiation[link]

In July 2009, the IARC released a report that categorized tanning beds as “carcinogenic to humans”. The agency, which is part of the World Health Organization (WHO), previously classified tanning beds as “probably carcinogenic”. The change comes after an analysis of more than 20 epidemiological studies indicating that people who begin using tanning devices before age 30 are 75% more likely to develop melanoma.^[19]

In December 2009, Julie Morgan, Labour MP for Cardiff North, introduced a Private Member's Bill before Parliament aimed at preventing under-18s using sunbeds. MPs considered the evidence, including research from a UK cancer charity.^[20] The research found that a quarter of a million children in England between the ages of 11 and 17 regularly used sunbeds. The bill was passed in April 2010; the Sunbed (Regulation) Bill restricts the use of sunbeds to over-18s in England and Wales (Scotland already had this legislation). All sunbed salons will have to be staffed and provide accurate health information on the dangers of sunbeds.^[21]

Diagnosis[link]

ABCD rule illustration: On the left side from top to bottom: melanomas showing (A) Asymmetry, (B) a border that is uneven, ragged, or notched, (C) coloring of different shades of brown, black, or tan and (D) diameter that had changed in size. The normal moles on the right side do not have abnormal characteristics (no asymmetry, even border, even color, no change in diameter).

A dermatoscope

Melanoma in skin biopsy with H&E stain — this case may represent superficial spreading melanoma.

There is no blood test for detecting melanomas. Visual diagnosis of melanomas is still the most common method employed by health professionals.^[22] To detect melanomas (and increase survival rates), it is recommended to learn what they look like (see "ABCDE" mnemonic below), to be aware of moles and check for changes (shape, size, color, itching or bleeding) and to show any suspicious moles to a doctor with an interest and skills in skin malignancy.^[23][24]

A popular method for remembering the signs and symptoms of melanoma is the mnemonic "ABCDE":

• Asymmetrical skin lesion.
• Border of the lesion is irregular.
• Color: melanomas usually have multiple colors.
• Diameter: moles greater than 6 mm are more likely to be melanomas than smaller moles.
• Enlarging: Enlarging or evolving

A weakness in this system is the diameter. Many melanomas present themselves as lesions smaller than 6 mm in diameter; and all melanomas were malignant on day 1 of growth, which is merely a dot. An astute physician will examine all abnormal moles, including ones less than 6 mm in diameter. Seborrheic keratosis may meet some or all of the ABCD criteria, and can lead to false alarms among laypeople and sometimes even physicians. An experienced doctor can generally distinguish seborrheic keratosis from melanoma upon examination, or with dermatoscopy.

Some will advocate the system "ABCDE",^[25] with E for evolution. Certainly moles which change and evolve will be a concern. Alternatively, some will refer to E as elevation. Elevation can help identify a melanoma, but lack of elevation does not mean that the lesion is not a melanoma. Most melanomas are detected in the very early stage, or in-situ stage, before they become elevated. By the time elevation is visible, they may have progressed to the more dangerous invasive stage.

However, nodular melanomas do not fulfill these criteria, having their own mnemonic "EFG":

• Elevated: the lesion is raised above the surrounding skin.
• Firm: the nodule is solid to the touch.
• Growing: the nodule is increasing in size.

A recent and novel method of melanoma detection is the "ugly duckling sign"^[26][27] It is simple, easy to teach, and highly effective in detecting melanoma. Simply, correlation of common characteristics of a person's skin lesion is made. Lesions which greatly deviate from the common characteristics are labeled as an "Ugly Duckling", and further professional exam is required. The "Little Red Riding Hood" sign^[27] suggests that individuals with fair skin and light-colored hair might have difficult-to-diagnose amelanotic melanomas. Extra care and caution should be rendered when examining such individuals, as they might have multiple melanomas and severely dysplastic nevi. A dermatoscope must be used to detect "ugly ducklings", as many melanomas in these individuals resemble non-melanomas or are considered to be "wolves in sheep clothing".^[28] These fair-skinned individuals often have lightly pigmented or amelanotic melanomas which will not present easy-to-observe color changes and variation in colors. The borders of these amelanotic melanomas are often indistinct, making visual identification without a dermatoscope (dermatoscopy) very difficult.

People with a personal or family history of skin cancer or of dysplastic nevus syndrome (multiple atypical moles) should see a dermatologist at least once a year to be sure they are not developing melanoma.

Moles that are irregular in color or shape are often treated as candidates of melanoma. Following a visual examination and a dermatoscopic exam,^[28] or in vivo diagnostic tools such as a confocal microscope, the doctor may biopsy the suspicious mole. If the mole is malignant, the mole and an area around it need excision.

The diagnosis of melanoma requires experience, as early stages may look identical to harmless moles or not have any color at all. A skin biopsy performed under local anesthesia is often required to assist in making or confirming the diagnosis and in defining the severity of the melanoma. Amelanotic melanomas and melanomas arising in fair-skinned individuals (see the "Little Red Riding Hood" sign) are very difficult to detect, as they fail to show many of the characteristics in the ABCD rule, break the "Ugly Duckling" sign, and are very hard to distinguish from acne scarring, insect bites, dermatofibromas, or lentigines.

Total body photography, which involves photographic documentation of as much body surface as possible, is often used during follow-up of high-risk patients. The technique has been reported to enable early detection and provides a cost-effective approach (being possible with the use of any digital camera), but its efficacy has been questioned due to its inability to detect macroscopic changes.^[22] The diagnosis method should be used in conjunction with (and not as a replacement for) dermoscopic imaging, with a combination of both methods appearing to give extremely high rates of detection.

Classification[link]

Melanoma is divided into the following types:^[29]

• Lentigo maligna
• Lentigo maligna melanoma
• Superficial spreading melanoma
• Acral lentiginous melanoma
• Mucosal melanoma
• Nodular melanoma
• Polypoid melanoma
• Desmoplastic melanoma
• Amelanotic melanoma
• Soft-tissue melanoma

See also:^[30]

• Melanoma with small nevus-like cells
• Melanoma with features of a Spitz nevus
• Uveal melanoma

Laboratory[link]

Lactate dehydrogenase (LDH) tests are often used to screen for metastases, although many patients with metastases (even end-stage) have a normal LDH; extraordinarily high LDH often indicates metastatic spread of the disease to the liver. It is common for patients diagnosed with melanoma to have chest X-rays and an LDH test, and in some cases CT, MRI, PET and/or PET/CT scans. Although controversial, sentinel lymph node biopsies and examination of the lymph nodes are also performed in patients to assess spread to the lymph nodes. A diagnosis of melanoma is supported by the presence of the S-100 protein marker.

Staging[link]

Further context on cancer staging is available at TNM.

Also of importance are the "Clark level" and "Breslow's depth", which refer to the microscopic depth of tumor invasion.^[31]

Melanoma stages:^[32] 5 year survival rates:

Stage 0: Melanoma in situ (Clark Level I), 99.9% survival

Stage I/II: Invasive melanoma, 85–99% survival

• T1a: Less than 1.00 mm primary tumor thickness, without ulceration, and mitosis < 1/mm2
• T1b: Less than 1.00 mm primary tumor thickness, with ulceration or mitoses ≥ 1/mm2
• T2a: 1.00–2.00 mm primary tumor thickness, without ulceration

Stage II: High risk melanoma, 40–85% survival

• T2b: 1.00–2.00 mm primary tumor thickness, with ulceration
• T3a: 2.00–4.00 mm primary tumor thickness, without ulceration
• T3b: 2.00–4.00 mm primary tumor thickness, with ulceration
• T4a: 4.00 mm or greater primary tumor thickness without ulceration
• T4b: 4.00 mm or greater primary tumor thickness with ulceration

Stage III: Regional metastasis, 25–60% survival

• N1: Single positive lymph node
• N2: Two to three positive lymph nodes OR regional skin/in-transit metastasis
• N3: Four positive lymph nodes OR one lymph node and regional skin/in-transit metastases

Stage IV: Distant metastasis, 9–15% survival

• M1a: Distant skin metastasis, normal LDH
• M1b: Lung metastasis, normal LDH
• M1c: Other distant metastasis OR any distant metastasis with elevated LDH

Based upon AJCC five-year survival with proper treatment

Prevention[link]

Minimizing exposure to sources of ultraviolet radiation (the sun and sunbeds),^[33] following sun protection measures and wearing sun protective clothing (long-sleeved shirts, long trousers, and broad-brimmed hats) can offer protection. In the past, use of sunscreens with a sun protection factor (SPF) rating of 50 or higher on exposed areas were recommended, as older sunscreens more effectively blocked UVA with higher SPF.^[34] Currently, newer sunscreen ingredients (avobenzone, zinc, and titanium) effectively block both UVA and UVB even at lower SPFs. However, there are questions about the ability of sunscreen to prevent melanoma.^[35] This controversy is well discussed in numerous review articles, and is rejected by most dermatologists.^[36] This correlation might be due to the confounding variable that individuals who used sunscreen to prevent burn might have a higher lifetime exposure to either UVA or UVB. See Sunscreen controversy for further references and discussions. Tanning, once believed to help prevent skin cancers, actually can lead to an increased incidence of melanomas.^[37] Even though tanning beds emit mostly UVA, which causes tanning, it by itself might be enough to induce melanomas.

A good rule of thumb for decreasing ultraviolet light exposure is to avoid the sun between the hours of 9 a.m. and 3 p.m. or avoid the sun when one's shadow is shorter than one's height. These are rough rules, however, and can vary depending on locality and individual skin cancer risk.

Almost all melanomas start with altering the color and appearance of normal-looking skin. This area may be a dark spot or an abnormal new mole. Other melanomas form from a mole or freckle that is already present in the skin. It can be difficult to distinguish between a melanoma and a normal mole. When looking for danger signs in pigmented lesions of the skin, a few simple rules are often used.

Treatment[link]

Extensive malignant melanoma on a patient's chest

Confirmation of the clinical diagnosis is either done with an excisional skin biopsy or a small, full-thickness sampling with a punch skin biopsy. This is usually followed up with a wider excision of the scar or tumor. Depending on the stage, a sentinel lymph node biopsy is done, as well, although controversy exists around trial evidence for this procedure.^[38] Treatment of advanced malignant melanoma is performed from a multidisciplinary approach.

Surgery[link]

Elliptical excisional biopsies are performed to excise (followed by histological analysis and Breslow scoring, and in some cases may indeed actually remove) the tumor, but further surgery is often necessary to reduce the risk of recurrence. Punch biopsies are contraindicated in suspected melanomas, for fear of seeding tumour cells and hastening the spread of the malignant cells.

Complete surgical excision with adequate surgical margins and assessment for the presence of detectable metastatic disease along with short- and long-term followup is standard. Often this is done by a wide local excision (WLE) with 1 to 2 cm margins. Melanoma-in-situ and lentigo malignas are treated with narrower surgical margins, usually 0.2 to 0.5 cm.^[39] Many surgeons consider 0.5 cm the standard of care for standard excision of melanoma-in-situ,^[40] but 0.2 cm margin might be acceptable for margin controlled surgery (Mohs surgery, or the double-bladed technique with margin control). The wide excision aims to reduce the rate of tumour recurrence at the site of the original lesion. This is a common pattern of treatment failure in melanoma. Considerable research has aimed to elucidate appropriate margins for excision with a general trend toward less aggressive treatment during the last decades.^[41]

Mohs surgery has been reported with cure rate as low as 77%^[42] and as high as 98% for melanoma-in-situ.^[43] CCPDMA and the "double scalpel" peripheral margin controlled surgery is equivalent to Mohs surgery in effectiveness on this "intra-epithelial" type of melanoma.

Melanomas which spread usually do so to the lymph nodes in the area of the tumor before spreading elsewhere. Attempts to improve survival by removing lymph nodes surgically (lymphadenectomy) were associated with many complications, but unfortunately, no overall survival benefit. Recently, the technique of sentinel lymph node biopsy has been developed to reduce the complications of lymph node surgery while allowing assessment of the involvement of nodes with tumor.^[44]

Although controversial and without prolonging survival, sentinel lymph node biopsy is often performed, especially for T1b/T2+ tumors, mucosal tumors, ocular melanoma and tumors of the limbs. A process called lymphoscintigraphy is performed in which a radioactive tracer is injected at the tumor site to localize the sentinel node(s). Further precision is provided using a blue tracer dye, and surgery is performed to biopsy the node(s). Routine H&E staining, and immunoperoxidase staining will be adequate to rule out node involvement. PCR tests on nodes, usually performed to test for entry into clinical trials, now demonstrate that many patients with a negative SLN actually had a small number of positive cells in their nodes. Alternatively, a fine-needle aspiration may be performed and is often used to test masses.

If a lymph node is positive, depending on the extent of lymph node spread, a radical lymph node dissection will often be performed. If the disease is completely resected, the patient will be considered for adjuvant therapy. Excisional skin biopsy is the management of choice. Here, the suspect lesion is totally removed with an adequate (but minimal, usually 1 or 2 mm) ellipse of surrounding skin and tissue.^[45] To avoid disruption of the local lymphatic drainage, the preferred surgical margin for the initial biopsy should be narrow (1 mm). The biopsy should include the epidermal, dermal, and subcutaneous layers of the skin. This enables the histopathologist to determine the thickness of the melanoma by microscopic examination. This is described by Breslow's thickness (measured in millimeters). However, for large lesions, such as suspected lentigo maligna, or for lesions in surgically difficult areas (face, toes, fingers, eyelids), a small punch biopsy in representative areas will give adequate information and will not disrupt the final staging or depth determination. In no circumstances should the initial biopsy include the final surgical margin (0.5 cm, 1.0 cm, or 2 cm), as a misdiagnosis can result in excessive scarring and morbidity from the procedure. A large initial excision will disrupt the local lymphatic drainage and can affect further lymphangiogram-directed lymphnode dissection. A small punch biopsy can be used at any time where for logistical and personal reasons a patient refuses more invasive excisional biopsy. Small punch biopsies are minimally invasive and heal quickly, usually without noticeable scarring.

Adjuvant treatment[link]

High-risk melanomas may require adjuvant treatment, although attitudes to this vary in different countries. In the United States, most patients in otherwise good health will begin up to a year of high-dose interferon treatment, which has severe side effects, but may improve the patient's prognosis slightly.^[46] However British Association of Dermatologist guidelines on melanoma state that interferon is not recommended as a standard adjuvant treatment for melanoma. ^[47] A 2011 meta-analysis showed that interferon could lengthen the time before a melanoma comes back but increased survival by only 3% at 5 years. The unpleasant side effects also greatly decrease quality of life.^[48]

In Europe, interferon is usually not used outside the scope of clinical trials.^[49][50]

Metastatic melanomas can be detected by X-rays, CT scans, MRIs, PET and PET/CTs, ultrasound, LDH testing and photoacoustic detection.^[51]

Chemotherapy and immunotherapy[link]

Various chemotherapy agents are used, including dacarbazine (also termed DTIC), immunotherapy (with interleukin-2 (IL-2) or interferon (IFN)), as well as local perfusion, are used by different centers. The overall success in metastatic melanoma is quite limited.^[52] IL-2 (Proleukin) is the first new therapy approved for the treatment of metastatic melanoma in 20 years. Studies have demonstrated that IL-2 offers the possibility of a complete and long-lasting remission in this disease, although only in a small percentage of patients.^[53] A number of new agents and novel approaches are under evaluation and show promise.^[54] Clinical trial participation should be considered the standard of care for metastatic melanoma.^[55]

Lentigo maligna treatment[link]

Standard excision is still being done by most surgeons. Unfortunately, the recurrence rate is exceedingly high (up to 50%). This is due to the ill-defined visible surgical margin, and the facial location of the lesions (often forcing the surgeon to use a narrow surgical margin). The narrow surgical margin used, combined with the limitation of the standard "bread-loafing" technique of fixed tissue histology — result in a high "false negative" error rate, and frequent recurrences. Margin control (peripheral margins) is necessary to eliminate the false negative errors. If bread loafing is used, distances from sections should approach 0.1 mm to assure that the method approaches complete margin control.

Mohs surgery has been done with cure rate reported to be as low as 77%,^[42] and as high as 95% by another author.^[43] The "double scalpel" peripheral margin controlled excision method approximates the Mohs method in margin control, but requires a pathologist intimately familiar with the complexity of managing the vertical margin on the thin peripheral sections and staining methods.^[56]

Some melanocytic nevi, and melanoma-in-situ (lentigo maligna) have resolved with an experimental treatment, imiquimod (Aldara) topical cream, an immune enhancing agent. Some dermasurgeons are combining the 2 methods: surgically excising the cancer and then treating the area with Aldara cream postoperatively for three months.

Radiation therapy[link]

Radiation therapy is often used after surgical resection for patients with locally or regionally advanced melanoma or for patients with unresectable distant metastases. It may reduce the rate of local recurrence but does not prolong survival.^[57] Radioimmunotherapy of metastatic melanoma is currently under investigation. Radiotherapy has a role in the palliation of metastatic melanoma.^[58]

Prognosis[link]

Features that affect prognosis are tumor thickness in millimeters (Breslow's depth), depth related to skin structures (Clark level), type of melanoma, presence of ulceration, presence of lymphatic/perineural invasion, presence of tumor-infiltrating lymphocytes (if present, prognosis is better), location of lesion, presence of satellite lesions, and presence of regional or distant metastasis.^[59] Certain types of melanoma have worse prognoses but this is explained by their thickness. Interestingly, less invasive melanomas even with lymph node metastases carry a better prognosis than deep melanomas without regional metastasis at time of staging. Local recurrences tend to behave similarly to a primary unless they are at the site of a wide local excision (as opposed to a staged excision or punch/shave excision) since these recurrences tend to indicate lymphatic invasion.

When melanomas have spread to the lymph nodes, one of the most important factors is the number of nodes with malignancy. Extent of malignancy within a node is also important; micrometastases in which malignancy is only microscopic have a more favorable prognosis than macrometastases. In some cases micrometastases may only be detected by special staining, and if malignancy is only detectable by a rarely employed test known as the polymerase chain reaction (PCR), the prognosis is better. Macrometastases in which malignancy is clinically apparent (in some cases cancer completely replaces a node) have a far worse prognosis, and if nodes are matted or if there is extracapsular extension, the prognosis is still worse.

When there is distant metastasis, the cancer is generally considered incurable. The five year survival rate is less than 10%.^[32] The median survival is 6 to 12 months. Treatment is palliative, focusing on life-extension and quality of life. In some cases, patients may live many months or even years with metastatic melanoma (depending on the aggressiveness of the treatment). Metastases to skin and lungs have a better prognosis. Metastases to brain, bone and liver are associated with a worse prognosis.

There is not enough definitive evidence to adequately stage, and thus give a prognosis for ocular melanoma and melanoma of soft parts, or mucosal melanoma (e.g. rectal melanoma), although these tend to metastasize more easily. Even though regression may increase survival, when a melanoma has regressed, it is impossible to know its original size and thus the original tumor is often worse than a pathology report might indicate.

Epidemiology[link]

Age-standardized death from melanoma and other skin cancers per 100,000 inhabitants in 2004.^[61]

  no data

  less than 0.7

  0.7–1.4

  1.4–2.1

  2.1–2.8

  2.8–3.5

  3.5–4.2

  4.2–4.9

  4.9–5.6

  5.6–6.3

  6.3–7

  7–7.7

  more than 7.7

Generally, an individual's risk for developing melanoma depends on two groups of factors: intrinsic and environmental.^[62] "Intrinsic" factors are generally an individual's family history and inherited genotype, while the most relevant environmental factor is sun exposure.

Epidemiologic studies suggest that exposure to ultraviolet radiation (UVA^[63] and UVB) is one of the major contributors to the development of melanoma. UV radiation causes damage to the DNA of cells, typically thymine dimerization, which when unrepaired can create mutations in the cell's genes. When the cell divides, these mutations are propagated to new generations of cells. If the mutations occur in protooncogenes or tumor suppressor genes, the rate of mitosis in the mutation-bearing cells can become uncontrolled, leading to the formation of a tumor. Data from patients suggest that aberrant levels of Activating Transcription Factor in the nucleus of melanoma cells are associated with increased metastatic activity of melanoma cells;^[64][65][66] studies from mice on skin cancer tend to confirm a role for Activating Transcription Factor-2 in cancer progression.^[67][68] Occasional extreme sun exposure (resulting in "sunburn") is causally related to melanoma.^[69] Melanoma is most common on the back in men and on legs in women (areas of intermittent sun exposure). The risk appears to be strongly influenced by socio-economic conditions rather than indoor versus outdoor occupations; it is more common in professional and administrative workers than unskilled workers.^[70][71] Other factors are mutations in or total loss of tumor suppressor genes. Use of sunbeds (with deeply penetrating UVA rays) has been linked to the development of skin cancers, including melanoma.^[72]

Possible significant elements in determining risk include the intensity and duration of sun exposure, the age at which sun exposure occurs, and the degree of skin pigmentation. Exposure during childhood is a more important risk factor than exposure in adulthood. This is seen in migration studies in Australia^[73] where people tend to retain the risk profile of their country of birth if they migrate to Australia as an adult. Individuals with blistering or peeling sunburns (especially in the first twenty years of life) have a significantly greater risk for melanoma. This does not mean that sunburn is the cause of melanoma. Instead it is merely statistically correlated. The cause is the exaggerated UV-exposure. It has been shown that sunscreen — while preventing the sunburn — does not protect mice, injected with melanoma cells a day after UV exposure, from developing melanoma.^[74]

Fair and red-headed people, persons with multiple atypical nevi or dysplastic nevi and persons born with giant congenital melanocytic nevi are at increased risk.^[75]

A family history of melanoma greatly increases a person's risk because mutations in CDKN2A^{[disambiguation needed ]}, CDK4 and several other genes have been found in melanoma-prone families.^[76] Patients with a history of one melanoma are at increased risk of developing a second primary tumour.^[77]

The incidence of melanoma has increased in the recent years, but it is not clear to what extent changes in behavior, in the environment, or in early detection are involved.^[78]

To understand how sunscreen can reduce sunburn and at the same time cause melanoma it is necessary to distinguish between direct DNA damage and indirect DNA damage. Genetic analysis has shown that 92% of all melanoma are caused by the indirect DNA damage.^[79] Although some people believe that dark-skinned people such as those of African descent cannot get sunburns, they are in fact susceptible, and should use sunscreen accordingly, as sunscreen has been proven to protect against other cancers such as squamous cell carcinoma and basal cell carcinoma.^[80]

History[link]

Although melanoma is not a new disease, evidence for its occurrence in antiquity is rather scarce. However, one example lies in a 1960s examination of nine Peruvian mummies, radiocarbon dated to be approximately 2400 years old, which showed apparent signs of melanoma: melanotic masses in the skin and diffuse metastases to the bones.^[81]

John Hunter is reported to be the first to operate on metastatic melanoma in 1787. Although not knowing precisely what it was, he described it as a "cancerous fungous excrescence". The excised tumor was preserved in the Hunterian Museum of the Royal College of Surgeons of England. It was not until 1968 that microscopic examination of the specimen revealed it to be an example of metastatic melanoma.^[82]

The French physician René Laennec was the first to describe melanoma as a disease entity. His report was initially presented during a lecture for the Faculté de Médecine de Paris in 1804 and then published as a bulletin in 1806.^[83] The first English language report of melanoma was presented by an English general practitioner from Stourbridge, William Norris in 1820.^[84] In his later work in 1857 he remarked that there is a familial predisposition for development of melanoma (Eight Cases of Melanosis with Pathological and Therapeutical Remarks on That Disease).

The first formal acknowledgment of advanced melanoma as untreatable came from Samuel Cooper in 1840. He stated that the only chance for benefit depends upon the early removal of the disease ...'^[85] More than one and a half centuries later this situation remains largely unchanged.

Research[link]

One important pathway in melanin synthesis involves the transcription factor MITF. The MITF gene is highly conserved and is found in people, mice, birds, and even fish. MITF production is regulated via a fairly straightforward pathway. UV radiation causes increased expression of transcription factor p53 in keratinocytes, and p53 causes these cells to produce melanocyte-stimulating hormone (MSH), which binds to melanocortin 1 receptors (MC1R) on melanocytes. Ligand-binding at MC1R receptors activates adenylate cyclases, which produce cAMP, which activates CREB, which promote MITF expression. The targets of MITF include p16 (a CDK inhibitor) and Bcl2, a gene essential to melanocyte survival. It is often difficult to design drugs that interfere with transcription factors, but perhaps new drugs will be discovered that can impede some reaction in the pathway upstream of MITF.

Studies of chromatin structure also promise to shed light on transcriptional regulation in melanoma cells. It has long been assumed that nucleosomes are positioned randomly on DNA, but murine studies of genes involved in melanin production now suggest that nucleosomes are stereotypically positioned on DNA. When a gene is undergoing transcription, its transcription start site is almost always nucleosome-free. When the gene is silent, however, nucleosomes often block the transcriptional start site, suggesting that nucleosome position may play a role in gene regulation.

Finally, given the fact that melanin helps protect skin cells from UV-induced damage, new melanoma prevention strategies could involve attempts to induce melanin synthesis in individuals who would otherwise get sunburns. Redheads, for example, do not tan because they have MC1R mutations. In mice, it has been shown that the melanin production pathway can be rescued downstream of MC1R.^{[citation needed]}

A study published on January 27, 2011, by M. Raza Zaidi et al. shows that interferon-γ links ultraviolet radiation to melanomagenesis in mice. Using a mouse model that allowed the visual tracking and purification of melanocytes using a green fluorescent dye, data showed that UVB-induced, macrophage-enhanced interferon-γ release results in melanoma growth, proliferation and immunoevasion. Based on these results, the interferon-γ pathway can potentially serve as part of new therapeutic measures to treat patients suffering from malignant melanoma, as well as a potential preventive strategy against UV-induced radiation.^[86]

BRAF[link]

About 60% of melanomas contain a mutation in the B-Raf gene. Early clinical trials suggested that B-Raf inhibitors including Plexxicon(R)'s vemurafenib could lead to substantial tumor regression in a majority of patients if their tumor contain the B-Raf mutation.^[87] In June 2011, a large clinical trial confirmed the positive findings from those earlier trials.^[88][89]

Ipilimumab[link]

At the American Society of Clinical Oncology Conference in June 2010, the Bristol-Myers Squibb pharmaceutical company reported the clinical findings of their drug ipilimumab. The study found an increase in median survival from 6.4 to 10 months in patients with advanced melanomas treated with the monoclonal ipilimumab, versus an experimental vaccine. It also found a one year survival rate of 25% in the control group using the vaccine, 44% in the vaccine and ipilimumab group, and 46% in the group treated with ipilimumab alone.^[90] However, some have raised concerns about this study for its use of the unconventional control arm, rather than comparing the drug against a placebo or standard treatment.^[91][92][93] Meaning that the drug performed better than the vaccine, although the vaccine has not been tested before and may be causing toxicity — making the drug appear better by comparison.

In June 2011, a clinical trial of ipilimumab plus dacarbazine combined this immune system booster with the standard chemotherapy drug that targets cell division. It showed an increase in median survival for these late stage patients to 11 months instead of the 9 months normally seen. Researchers were also hopeful that perhaps 10–20% of patients could live a long time. Some serious side-effects of revving up the immune system were seen in some patients. A course of treatment costs $120,000. The drug's brandname is Yervoy.^[88][94]

Targeted therapies [link]

In clinical research setting other therapies, such as Adoptive Cell Therapy or gene therapy, may be tested.^[95] Two kinds of experimental treatments developed at the National Cancer Institute (NCI), part of the National Institutes of Health (NIH) in the US have been used in advanced (metastatic) melanoma with high success rates in terms of melanoma treatments.^[13] The first treatment involves Adoptive Cell Therapy (ACT) using TILs immune cells (Tumor Infiltrating Lymphocytes) isolated from a patient's own melanoma tumor. These cells are grown in large numbers in a laboratory and returned to the patient after a treatment that temporarily reduces normal T cells in the patient's body. TIL Therapy following lymphodepletion can result in durable complete response in a variety of setups.^[96][97] Up to date, the only medical center outside the USA managed to successfully implement this technology is Sheba Medical Center through "Ella Institute of Melanoma", found in Israel (objective response rates of 50%).^[97] The second treatment, adoptive transfer of genetically altered autologous lymphocytes, depends on delivering genes that encode so called T cell receptors (TCRs), into patient's lymphocytes. After that manipulation lymphocytes recognize and bind to certain molecules found on the surface of melanoma cells and kill them.^[98]

A new treatment that trains the immune system to fight cancer has shown modest benefit in late-stage testing against melanoma.^[99] Sutent may be effective for patients with metastatic melanoma.^[100]

Surveillance methods [link]

Advances in high resolution ultrasound scanning have enabled surveillance of metastatic burden to the sentinel lymph nodes.^[101] The Screening and Surveillance of Ultrasound in Melanoma trial (SUNMEL) is evaluating ultrasound as an alternative to invasive surgical methods.^[102]

See also[link]

• List of cutaneous conditions
• Seborrheic keratosis looks like melanoma but is benign
• Spitz nevus
• Melanotropin receptor
• Slip-Slop-Slap An Australian health campaign
• Basal cell carcinoma type of non-melanoma skin cancer
• Squamous cell carcinoma type of non-melanoma skin cancer

Notes[link]

External links[link]

Wikimedia Commons has media related to: Melanoma

• Melanoma at the Open Directory Project
• Melanomas and melanocytic hyperplasias in: Atlas histopatologii guzów skóry (pl.wikibooks.org)

This article has multiple issues. Please help improve it or discuss these issues on the talk page. It includes a list of references, related reading or external links, but its sources remain unclear because it lacks inline citations. Tagged since August 2008.</li> It is written like an advertisement and needs to be rewritten from a neutral point of view. Tagged since November 2010.</li> Very few or no other articles link to it. Please help introduce links to this page from other articles related to it. Tagged since February 2009.</li>

Shonda Schilling (born November 23, 1967 in Dundalk, Maryland) is founder of the Shade Foundation of America. She is married to professional baseball player Curt Schilling.

Biography [link]

Personal life[link]

Shonda graduated from Towson State College majoring in journalism, member of the Iota Delta chapter of Zeta Tau Alpha. She worked in television production for Home Team Sports in Baltimore until marrying Curt Schilling in 1992. They have four children: Gehrig (5/27/95); Gabriella (5/22/97); Grant (10/13/99); and Garrison (6/27/02). The family resides in Medfield, Massachusetts.^{[citation needed]}

Skin Cancer[link]

Schilling was diagnosed with stage 2 malignant melanoma in February 2001. A total of five surgeries left 25 scars crisscrossing her back, arms, legs and chest.^{[citation needed]} The media picked up on her skin cancer scare during the 2001 World Series, when her husband Curt won the World Series co-MVP honor for the Arizona Diamondbacks. Her story was featured in People Magazine, Glamour, Family Circle, Pregnancy, Good Housekeeping and ABC's "The View." Shonda invited Good Morning America into the operating room to witness her fifth and final surgery in order to inspire others to have their skin checked and to alter their sun habits. In 2002, she accepted the Melanoma Monday national spokeswoman role with the American Academy of Dermatology (AAD). An overwhelming response from fellow melanoma survivors^{[citation needed]} resulted in Shonda creating the Shade Foundation of America.

Shade Foundation of America[link]

Shonda Schilling founded the Shade Foundation of America in 2002 with the goal of changing society's attitude towards sun exposure. The wife of major league baseball pitcher Curt Schilling, she has traveled all over the United States promoting sun-safety awareness.

Schilling’s dedication to promote sun safety has been expressed through many partnerships and appearances. In 2003, the Shade Foundation joined with the Environmental Protection Agency (EPA) to launch the annual SunWise Poster Contest in conjunction with the Arizona Diamondbacks and the Arizona Department of Health to implement sun-safety curriculum in schools. Schilling testified before the Arizona state legislatures in an effort to help pass the current law requiring schools to teach the SunWise curriculum in the state of Arizona. The launch of this partnership was heard by 20 million people through media exposure and hundreds of school principals across the country signed up to teach the SunWise program in their classrooms. Thousands of kids have learned skin cancer prevention techniques through the program by drawing a SunWise poster for the contest. When the Schillings were relocated to Boston, Shonda partnered the program with the Dana Faber Cancer Institute in Massachusetts where it continues to result in overwhelming success.^{[citation needed]}

Schilling aligned the Shade Foundation with Major League Baseball and the Play it Smart When it Comes to the Sun Program in 2005, generating awareness in MLB Parks around the country and at the MLB All-Star Game in Detroit. The program continues to reach millions of Americans with a sun-safety message through media appearances with Geraldo At Large, Women's World Magazine among other local channels across the country.

Since 2005, Schilling has participated in running the Boston Marathon every year to raise money for the Shade Foundation. She also ran the PF Chang's Rock N Roll Marathon in 2005 on behalf of the Shade Foundation.

Schilling’s involvement with the Shade Foundation has garnered intense media attention since its inception. The Schilling family appeared in a public service print advertisement promoting sun-safety in Sports Illustrated's popular swimsuit issue as well as a television PSA that aired in New England and around the country. Through all of Schilling’s hard work, she has been recognized for her commitment to the community and promoting sun safety numerous times. Shade’s partnership with the EPA earned Shonda and the Shade Foundation the "Excellence in Cancer Awareness" award in 2003 from the Congressional Families Program of the Cancer Research and Prevention Foundation in Washington, DC. That same year, she was presented with the Girl Scout World of Humanity Award by the Arizona Cactus- Pine Girl Scout Council and in her honor they created the Shade Badge for scouts to earn. Also in 2003, Shonda accepted the Outstanding Fundraiser Award by the Association of Professional Fundraisers.^{[citation needed]}

She was recognized nationally with the Speaker Thomas J. "Tip" O'Neill, Jr. Award for Public Service by the Greater Boston Federal Executive Board in 2004.^{[citation needed]} That same year, the American Academy of Dermatology acknowledged Shonda's awareness efforts with an individual achievement Gold Triangle Award. She was also given the Alumni of the Year Award from Zeta Tau Alpha Sorority. In 2005, Schilling picked up an honorary doctorate degree in public service from Framingham State College. She was also presented with the exceptional women's award for community service by Boston radio station Magic 106.7. Merrimack College gave Shonda an honorary Doctor of Humane Letters degree in 2006 and that same year she was awarded the Lady Baden Powell Good Scout Award by the Boston Minuteman Council. Schilling continues to serve as a commencement speaker at high school and college graduations.

The Wellness Community-Greater Boston recognized Schilling with the 2007 Gilda Radner Award as an individual who demonstrated courage, determination and hope in the face of cancer. She was named host of Facing Cancer Together, a television program produced by the Wellness Community which aired on cable stations around the country. The Massachusetts Interscholastic Athletic Association presented her with the 2007 Partners in Prevention "Making a Difference" Award during the 11th Annual MIAA Wellness Summit held in Milford, MA.^{[citation needed]}

Work with the ALS Association[link]

Shonda and Curt have been active with the [ALS Association] since 1992 in developing public awareness and fundraising campaigns to improve the services of the ALS Association. Both have appeared in numerous public service announcements featuring Curt's Pitch'n to Win campaign that joins the ALS Association and Shaw's Supermarkets in which people can donate $1.38 or $3.38 to benefit the ALS Association. Together they have donated and raised more than $9 million for ALS. Shonda serves on the Board of Directors for the Philadelphia, Arizona and Massachusetts chapters. She represents ALS at numerous functions including lobbying in Washington D.C. for government funding and before the Food and Drug Administration to get the first trial drugs approved. Shonda regularly visits ALS patients, their family members and caregivers, and is involved in helping with a variety of events associated with ALS.

She chaired the "The Shonda Schilling Say It with Flowers" Luncheon in Arizona which raised more than $250,000 spanning three years (2002–04). When the Schillings relocated to Boston, Shonda and Dawn Timlin, wife of Red Sox pitcher Mike Timlin, implemented the “Say it with Flowers” campaign in the Boston area which raises over $200,000 annually to benefit the ALS.

The Schilling family participated in ALSA's National ALS Awareness Month public service announcement in 2004 and received the “Telly Award” for excellence in a national television commercial. Schilling and her husband received the 2002 Catfish Hunt Award from the North Carolina Chapter of the ALS Association and she was also presented the All-Star Award by ALSA. In 2001, ALS Association National Office presented Shonda with the Lawrence A. RAND Award recognizing her nationally for continued service and dedication.^[1][2]

Aspergers Syndrome [link]

Shonda and Curt have a son with Aspergers Syndrome (Grant) which has been a struggle for many years, but as Shonda describes in her book, "The Best Kind Of Different" it has been well worth it. Shonda has partnered with The Aspergers Association of New England (AANE) and Autisim speaks Also has done some work with Youth Care.

^[3]

References [link]

Ian Brown
Background information
Birth name	Ian George Brown
Born	(1963-02-20) 20 February 1963 (age 49) Warrington, England[1]
Origin	Manchester England[2][3][4][5]
Genres	Alternative rock, indie rock
Occupations	Musician, songwriter
Instruments	Vocals, keyboards, Tambourine
Years active	1984–1996, 1998–present
Labels	Polydor/Fiction Records (UK) Interscope, E1 Music (US)
Associated acts	The Stone Roses
Website	www.ianbrown.co.uk

Ian George Brown (born 20 February 1963 in Warrington) is an English musician, best known as the lead singer of the alternative rock band The Stone Roses, which broke up in 1996 but are confirmed to reunite in 2012. Since the break-up of the Stone Roses he has led a successful solo career. His latest studio album My Way was released on 28 September 2009.

Biography[link]

Early life[link]

Brown was born in Warrington, England in 1963.^[6] His father, George, was a joiner and his mother Jean worked as a receptionist in a paper factory.^[6] When he was 5, Brown's family, including a brother and sister, moved to Timperley, Altrincham.^[7] He was educated at Park Road County Primary Infant and Junior School and then Altrincham Grammar School for Boys.^[7] His interest in music was inspired by the punk movement, specifically the bands Sex Pistols, The Clash and Manchester band Slaughter & The Dogs.^[8] Brown and original Stone Roses bassist Pete Garner attended the recording of the Clash single "Bankrobber" in Manchester.^[9]

Stone Roses[link]

Brown's music career began in 1980, playing bass guitar in band with John Squire and Simon Wolstencroft.^[10] They eventually became The Patrol, with Andy Couzens on vocals. The band soon split up, with Brown selling his bass to buy a scooter.^[11] Brown moved to Hulme, and attended northern soul "all-nighters" across the north of England in the early 1980s as the scene faded. Around this time, Brown met soul legend Geno Washington, who told him, "You should be a star".^[12] In 1983 Brown joined The Waterfront, the band that would evolve into The Stone Roses, as co-vocalist.^[13]

The Stone Roses rose to prominence in the late 1980s and early 1990s, with their debut album voted the best British album of all time in 2004.^[14] The band's second album, Second Coming, received a mixed reaction, and after several changes of line-up, the band split up in October 1996.

On 17 October 2011, Brown alluded to a Stone Roses reunion via text message, saying: "We are going to rule the world again. It's happening."^[15] On the following day, a reunion was announced for the band with performances planned for June 2012 in Manchester.^[16][17] In a press conference interview, the members of the Stone Roses have said that a new album is planned.^[18]

On 2 December 2011 Ian Brown and John Squire performed together live for the first time since 1995. They joined Mick Jones from The Clash, The Farm and Pete Wylie at the Manchester Ritz in in aid of the Justice for Hillsborough campaign. They performed "Elizabeth My Dear" as a duo before being joined by Mick Jones and The Farm for renditions of the Clash’s "Bankrobber" and "Armagideon Time" with Ian Brown taking on lead vocals for the three songs.

Solo career[link]

After a break from music in Morocco, Brown established his solo career with the debut solo single "My Star", which was released in the UK on 12 January 1998.^[19] The debut album Unfinished Monkey Business followed on 2 February 1998. The album was produced and financed by Brown, and featured ex-Roses members Mani, Nigel Ipinson, Aziz Ibrahim and Robbie Maddix.^[20] The album sold over 300,000 copies.^[21]

Brown toured in Summer 1998 with a band that included Ibrahim, Inder Mathura (percussion), Simon Moore (drums), and Sylvan Richardson (bass), including performances at the Glastonbury Festival and the V Festival.^[22] Brown was arrested after a flight back from his live show in Paris, and later sentenced to four months in prison for using threatening behaviour towards an airline stewardess and captain, a charge which he denied, causing his tour to be rescheduled.^[23][24] His bandmate Aziz Ibrahim condemned the sentence, saying that Brown was "just being cheeky".^[25] While in Strangeways Prison, Brown wrote the lyrics for "Free My Way", "So Many Soldiers", and "Set My Baby Free".^[26] He was released on parole after two months.

His second album, Golden Greats, was released by Polydor Records 1999. It featured more electronic instrumentation and earned high critical acclaim. For his third studio album, Music of the Spheres, Brown sought outside production help for the first time, hiring the services of songwriter and producer Dave McCracken who would go on to become a regular collaborator. He toured the US for the first time as a solo artist in support of the album.^[27]

Brown's fourth solo album, Solarized, was released in the UK on 13 September 2004, and was the first to be released under the revived Polydor imprint Fiction Records. When his new Fiction A&R Jim Chancellor was asked in HitQuarters what contribution he makes to Brown's records he said, "There's not as much to do. Ian is very much the master of his own records."^[28]

Since the break-up of the Stone Roses in 1996, Brown has released six solo albums and fourteen UK Top 40 singles.^[29] He has sold out seven UK tours, and appeared three times at the Glastonbury Festival, including headlining The Other Stage in 2005.^[30] He has appeared five times at V Festival since 1998 along with regular appearances at T in the Park and Oxegen festivals, and played the Move festival in 2002 at Lancashire Cricket Ground.^[31] and two tour of AUSTRALIA IN 2006 AND 2008

Ian Brown at the Witnness festival in Ireland in 2002. Note: he is wearing a bucket-hat with Irish rock band Aslan's logo.

Brown had a cameo role in the 2004 film Harry Potter and the Prisoner of Azkaban'.^[32]

For the 2005/6 season, Brown was the shirt sponsor of London Commercial Division football team Chiswick Homefields, the players wearing an 'IB – The Greatest' logo on their chests.^[33]. Brown is a life-long supporter of Manchester United and is a season ticket holder ^[34].

At the 2006 NME awards, Brown was presented with the "Godlike Genius" award and in 2007 was given the Q "Legend" Award.^[35][36]

In September 2007, Brown released his fifth studio album, The World is Yours. The album represented a more political approach in his music, particularly the anti-war track "Illegal Attacks", which featured Sinéad O'Connor. The album also featured former Smith bassist Andy Rourke and Paul Ryder of Happy Mondays.^[37]and Steve Jones and Paul Cook of the Sex Pistols

My Way, his sixth solo album, was released in September 2009.^[38] It was recorded at London's Battery Studios with producer Dave McCracken; the first single, "Stellify", was released 21 September 2009. Brown played Manchester Arena for the 3rd time in Dec 2009 and in 2010 made his 3rd appearance in Moscow and 2nd in Beijing China Since turning solo in 1998 Brown has played shows in 45 countries

Brown has collaborated several times with UNKLE, appearing on "Be There" in 1999 and on "Reign" on the 2003 album Never, Never, Land, which was also released as a single.^[39]

Awards and achievements[link]

Brown has won numerous awards in his career, in recognition of his work as a solo artist and his work with The Stone Roses. The awards he has won are as follows:

The Stone Roses

• 1997 The Stone Roses reached No. 5 in The Guardian's 100 Best Albums Ever poll
• 1998 The Stone Roses reached No. 4 in Q magazine's 100 Best Albums Ever poll
• 2004 The Stone Roses reached No. 1 in The Observer's 100 Best British Albums Ever poll
• 2006 The Stone Roses reached No. 1 in the NME writers 100 Best British Albums Ever poll
• 2006 The Stone Roses reached No. 7 in NME fans 100 Best Albums Ever poll

Solo

• 2002 Muso Awards Best Single ("Whispers")
• 2002 NME Awards Best Solo Artist^[40]
• 2006 NME Awards Godlike Genius Award^[35]
• 2007 Q Awards Legend Award^[36]
• 1999, 2000,^[41] 2002,^[42] 2006,^[43] 2009^[44] – nominated for Best British Solo Artist at the Brit Awards

Discography[link]

In the UK Ian Brown as a Solo Artist and with The Stone Roses has sold over a Certified 1.7 Million Albums

Albums[link]

Singles[link]

Notes[link]

References[link]

• Larkin, Colin (ed.) (1998) The Virgin Encyclopedia of Indie & New Wave, Virgin Books, ISBN 0-7535-0231-3
• Robb, John (2001) The Stone Roses and the Resurrection of British Pop, Random House, ISBN 0-09-187887-X

External links[link]

• Official website
• Don't Stop / Stone Roses
• The Definitive Ian Brown Discography