Malignant melanoma is a relatively common neoplasm that not long ago was considered almost uniformly deadly. Although the great preponderance of melanomas arise in the skin other sites origin include the oral and anogenital mucosal surfaces, esophagus , meninges, and notably the eye. The following comments apply to cutaneous melanomas. Intaocular melanomas.
Today as a result of increased public awareness of the earliest signs of skin melanomas most are cured surgically. Nonetheless the incidence of these lesions is on the rise, necessitating vigorous surveillance for their development.
As with epithelial malignant neoplasms of the skin sunlight appears to play an important role in the development of skin malignant melanoma. For example men commonly develop this tumor on the upper back whereas women have a relatively high incidence on both the back and the legs. Lightly pigmented individuals are at higher risk for the development of melanoma than are darkly pigmented individuals. Sunlight, however, does not seem to be the only predisposing factor, and the presence of apreexisting nevus, hereditary factors or even exposure to certain carcinogens may play a role in lesion development and evolution.
Molecular Geletics
The molecular basis for nonheritable forms of melanoma is incompletely understood and much of out current knowledge is based upon evaluation of the approximately 10% of melanomas that tend to run in families. As stated before these melanomas are often ( but not invariably) associated with multiple sysplastic nevi. Some of the suspected melanoma associated genes in this setting include: (1) the CMM1 gene on chromosome lp36; (2) the tumor suppressor gene p16 mapped to chromosome 9p21 (Genetic analyses have revealed germline mutations in this gene in certain melanoma patients and their family members. It may be recalled that this tumor suppressor gene is an inhibitor of cyclin dependent kinase4 [CDK 4] and such negatively regulateds the cell cycle and (3) the cyclin dependent kinase gene CDK4on chromosome 12q14. Transgenic mice with melanocyte specific expression of activated ras on a genetic background dificient for alleles of p16 exhibit accelerated development of melanoma thus confirming the role of this tumor suppressor in the pathogenesis of melanomas.
Clinical Features
Malignant melanoma of the skin is usually asymptomatic although itching may be an early manifestation. The most important clinical sign of the disease is change in color in a pigmented lesion. Unlike benign (nondysplastic) navi, melanomas exhibit striking variations in pigmentation, appearing in shades of black , brown , red, dark blue, and gray. On occation , zones of white or flesh colored hypopigmentation are also present. The borders of melanomas are not smooth, round and uniform as in nevocellular nevi, but iregular and often notched. In summary the clinical warming signs of melanoma are (1)enlargement of preexisting mole, (2) itching or pain in apreexisting mole (3) development of a new pigmented lesion during elder life( irregularity of borders of apigmented lesion, and (5) variegation of color within a picmented lesion.
Pictures Of Malignant Melanoma
Whilst this might be alarming, most forms of skin cancer are not life threatening and can be treated. The fact that most of the signs of the disease are on the surface of the skin means that they can be identified and treated early on with complete success.
However of the three types of skin cancer, malignant melanoma is potentially very serious and can be life threatening if not spotted early. This article will cover what is malignant melanoma , how it forms and how to prevent it.
It is generally accepted that any form of cancer is caused based on your genetic predisposition and your exposure to certain environmental conditions. When it comes to malignant melanoma, the environmental condition is thought to be exposure to ultraviolet radiation (UVA and UVB radiation). And the most common source of ultraviolet radiation that we are exposed to is the Sun (however things like sunbeds or tanning salons are just as bad if not worse ).
Too much ultraviolet radiation can mutate the DNA of a cell, making it cancerous. The genes in the DNA that cause this become known as oncogenes. Cells that have undergone this transformation do not die but divide and proliferate. They grow at an unregulated rate. As they continue to multiply their growth can become invasive.
Invasive growth harms the surrounding tissues and organs. In some cases the cancerous growths can prevent the organs from functioning or can start to grow into the organs culminating with the destruction of the organ. Should the cancer get into the lymphatic system then it can spread throughout the body. When this occurs it becomes hard to stop the spread and difficult to treat.
Whilst the primary cause of malignant melanoma is exposure to sunlight there are a number of genetic factors that are thought to increase the chances of developing the disease.
Your skin type can mean you are more at risk to the disease. If you have pale skin that doesn't tan but burns easily in the sun then you are more at risk. If your skin has freckles or you have blond or red hair then you are more at risk. If you have lots of moles on your body you may also be at risk. However, it is thought that people born with moles on their bodies are at less risk. If anyone in your family has had skin cancer then your risk of getting the disease increases.
Melanoma can start as a brown mark or spot on the skin. This may be hard to distinguish from an ordinary mole however if it starts to change color or gets larger then this may be a sign of melanoma. If you notice something like this happening on your body you should see a doctor.
As it is impossible to completely avoid the Sun, all you can do to prevent melanoma is to limit your skins exposure to it. This means wearing a hat, sunglasses, clothing that covers as most of your body and sun cream for areas that are open to the Sun.
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