HUIDTUMOREN Huidcarcinoom in beeld

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Title: HUIDTUMOREN Huidcarcinoom in beeld

1
HUIDTUMOREN Huidcarcinoom
in beeld

Nascholing oncologische neurologie,
endocrinologie, dermatologie en sarcomen

Leslie Sabajo, dermatoloog Thorarica, zaterdag
17 maart 2007
2
De huid
3
Ze bestaat uit drie delen.

Het bovenste (buitenste) gedeelte wordt gevormd
door de opperhuid de epidermis
Daaronder ligt de lederhuid het corium of de
dermis. Deze lagen vormen de huid in engere zin
Het onderste gedeelte is het onderhuidse
bindweefsel de zogenaamde subcutis (bindweefsel
is weefsel dat dient tot verbinding en steun van
andere weefsels en organen).

4
Epidermis
5
Functies

Scheidt (omhulsel)
Beschermt (verdedigingslinie)
Reguleert (oververhitting, onderkoeling of
uitdroging)
Verbindt (gevoel-tast)
Identificeert (herkenbaar)
Steunt (structuren)
Produceert (vitamine D3 uit previtamine D3 ofwel
precholecalciferol )
Zonder huid is leven en bestaan niet mogelijk

6
Opmerkingen

De huid is het grootste orgaan van het menselijk
lichaam
Bij de volwassene is het oppervlak 1.5 - 2.0 m2
Het gewicht van de huid, inclusief het onderhuids
bindweefsel is 15-20 kg
In de huid bevinden zich ook huidaanhangsels
talgklieren, zweetklieren, haarwortels en het
nagelbed plaatsen waar nagels worden aangemaakt
worden.

7
een gezwel of tumor of neoplasma

is een min of meer omschreven, abnormale
weefselmassa die in vergelijking met normaal
weefsel een overmatige, zelfstandige en
ongecoördineerde groeiwijze toont , die blijft
voortduren ook wanneer de prikkel die aanleiding
gaf tot die versterkte groei is verdwenen.
onderscheid wordt gemaakt in
Goedaardige niet infiltrerend en geen
metastasen
en
Kwaadaardige infiltrerend en wel metastasen

8
indeling van huidtumoren

Huidtumoren kunnen op verschillende manieren
ingedeeld worden.
Histologisch
Leeftijdscategorie
Klinisch beeld
De meest gangbare indeling gaat uit van de
histologische (weefsels) waaruit de tumor
ontstaat.Terwille van de eenvoud kan men een
aantal groepen huidtumoren onderscheiden-
epitheliale tumoren- melanocytentumoren-
mesenchymale tumoren- neurogene
tumoren.Epitheliale tumorenDe epitheliale
tumoren kunnen nog worden onderverdeeld in-
gezwellen van de oppervlakkige opperhuid waarbij
vaak verhoorning optreedt- gezwellen van de
diepere gedeelten van de opperhuid, van de
kiemlaag en van de cellen die klierstructuren
vormen.MelanocytentumorenSamenhangend met de
melanocyten kunnen zich afwijkingen voordoen
als- sproeten- lentigo senilis toename van
melanocyten bij oudere mensen- premaligne
dermatosen- maligne melanomen.Mesenchymale en
neurogene huidtumorenMesenchymale en neurogene
huidtumoren kunnen in principe ontstaan uit alle
weefselcomponenten van de huid- bindweefsel-
glad spierweefsel- bloedvaten- zenuwcellen.

9
Precancers
A number of abnormal but relatively harmless skin
growths constitute the early warning signs of
skin cancer. These may be precancerous lesions,
benign tumors that mask or mimic more serious
ones, or malignant tumors that are at the moment
just on the topmost layer of the skin. They are
important to recognize, because they are a
warning sign of potential skin cancer.
10
Actinic keratosis of keratosis solaris

the result of prolonged exposure to sunlight.
It is a small crusty, scaly or crumbly bump or
horn that arises on the skin surface.
The base may be light or dark, tan, pink, red, or
a combination of these... or the same color as
your skin.
The scale or crust is horny, dry, and rough, and
is often recognized by touch rather than sight.
Occasionally it itches or produces a pricking or
tender sensation.
It can also become inflamed and surrounded by
redness.
In rare instances, actinic keratoses can bleed.
lesion develops slowly
usually reaches a size from 2mm to 4mm but can
sometimes be as large as one inch.
most likely appear on the face, lips, ears,
scalp, neck, backs of the hands and forearms,
shoulders and back the parts of the body most
often exposed to sunshine.
The growths may be flat and pink or raised and
rough.

11
Actinic cheilitis

Actinic cheilitis is a type of actinic keratosis
occurring on the lips.
It causes them to become dry, cracked, scaly and
pale or white.
It mainly affects the lower lip, which typically
receives more sun exposure than the upper lip.

12
Leukoplakia

Leukoplakia is a disease of the mucous membrane.
White patches or plaques develop on the tongue or
inside of the mouth, and have the ability to
develop into SCC.
It is caused by sources of continuous irritation,
including smoking or other tobacco use, rough
teeth or rough edges on dentures and fillings.
Leukoplakia on the lips are mainly caused by sun
damage.

13
Bowen's Disease

This is generally considered to be a superficial
SCC that has not yet spread.
It appears as a persistent redbrown, scaly patch
which may resemble psoriasis or eczema.
If untreated, it may invade deeper structures.

14
Actinic Keratosis
15
Tip

Regardless of appearance, any change in a
preexisting skin growth, or the development of a
new growth or open sore that fails to heal,
should prompt an immediate visit to a physician.
If it is a precursor condition, early treatment
will prevent it from developing into SCC.
Often, all that is needed is a simple surgical
procedure or application of a topical
chemotherapeutic agent.

16
Treatment

There is no one best method to treat all skin
cancers and precancers.
The choice is determined by many factors,
including the location, type, size, whether it is
a primary tumor or a recurrent one, and also
health and preference of the patient.
Almost all treatments can be performed in the
physicians office or in a special surgical
facilities.
Most skin cancer removal can be done using a
local anesthetic.
Rarely, extensive tumors may require general
anesthesia and hospital admission.
There are many effective methods

17
Treatment

Cryosurgery
(Liquid nitrogen Critical Temperature -232.5F
(-146.9C) ) condenses (liquifies) at 77 K
(-195.8C) and freezes at 63 K (-210.0C) cooled
down to minus 196 degrees Celsius
Curettage and Desiccation
Bleeding is stopped with an electrocautery
needle, and local anesthesia is required.
Topical Medications
5-fluorouracil (5-FU) cream or solution, in
concentrations from 0.5 to 5 percent(cytostaticum-
Efudix)
Kan met tretinoine worden gecombineerd
Another preparation, imiquimod cream, is used for
multiple keratoses. It causes cells to produce
interferon, a chemical that destroys cancerous
and precancerous cells.
An alternative treatment, a gel combining,
hyaluronic acid and the anti-inflammatory drug
diclofenac, also may prove effective.
Chemical Peeling
This method makes use of trichloroacetic acid
(TCA) or a similar agent applied directly to the
skin.
Laser Surgery
A carbon dioxide or erbium YAG laser is focused
onto the lesion, removing epidermis and different
amounts of deeper skin

18
Behandeling na Tri Chloorazijn Zuur
19
Basal Cell Carcinoma/Basal Cell
Epithelioma/Basalioma

Basal cell carcinoma (BCC) is the most common
form of cancer,
With more than 800,000 new cases estimated in the
US each year.
Basal cells are cells that line the deepest layer
of the epidermis.
An abnormal growth a tumor of this layer is
known as basal cell carcinoma.
Basal cell carcinoma can usually be diagnosed
with a simple biopsy
is fairly easy to treat when detected early.
However, 5 to 10 percent of BCCs can be resistant
to treatment or locally aggressive, eating away
at the skin around then, sometimes even into bone
and cartilage.
When not treated quickly, they can be difficult
to eliminate.
Fortunately, however, this is a cancer that has
an extremely low rate of metastasis,
Although it can result in scars and
disfigurement, it is not usually
life-threatening.
Cause
The sun is responsible for over 90 percent of all
skin cancers, including BCC, and chronic
overexposure to the sun is the cause for most
cases of basal cell carcinoma.
BCCs the tumors themselves occur most
frequently on the face, ears, neck, scalp,
shoulders, and back.

20
Types of Basal Cell Carcinomas

Nodular basal cell carcinoma is the most common
type. These tumors are often depressed in the
middle and show ulceration.
Superficial. This is a less common type of BCC.
Sclerosing or Fibrosing. Fibrosing basal cell
carcinoma is also called morphea-like carcinoma.
Pigmented. Pigmented basal cell carcinoma is
similar to nodular basal cell carcinoma, but is
more likely to appear in people with dark hair or
dark eyes. As its name implies, this growth is
almost black and can easily be mistaken for the
more aggressive malignant melanoma.
Fibroepithelioma. This is a rare type of basal
cell carcinoma
Basosquamous carcinoma. Squamous and basal cell
carcinoma can coexist as one tumor growth at the
same time. Clinically, it can appear as a basal
cell or a squamous cell carcinoma. Basosquamous
cell carcinomas are believed by some researchers
to have a greater tendency to metastasize. These
tumors have to be treated immediately and
aggressively.
Basal cell nevus syndrome. Rarely, basal cell
carcinoma may develop as part of an inherited
condition, commonly referred to as nevoid basal
cell carcinoma syndrome or Gorlin syndrome.
Unlike other skin cancer conditions, this
syndrome may develop during childhood or
adolescence, and as many as 50-100 cancers may be
involved. Sometimes, the skin cancers increase
in number as the person reaches adulthood.
Clinically, they have the same appearance as
basal cell carcinomas.

21
Warning SignsThe typical characteristics of
basal cell carcinoma are shown in the pictures
below. Frequently, two or more features are
present in one tumor. In addition, BCC sometimes
resembles non-cancerous skin conditions such as
psoriasis or eczema.
A Reddish Patch or irritated area, frequently
occurring on the chest, shoulders, arms, or legs.
Sometimes the patch crusts. It may also itch or
hurt. At other times, it persists with no
noticeable discomfort.
An Open Sore that bleeds, oozes, or crusts and
remains open for three or more weeks. A
persistent, non-healing sore is a very common
sign of an early basal cell carcinoma.
A Pink Growth with a slightly elevated rolled
border and a crusted indentation in the center.
As the growth slowly enlarges, tiny blood vessels
may develop on the surface.
A Shiny Bump or nodule that is pearly or
translucent and is often pink, red, or white. The
bump can also be tan, black, or brown, especially
in dark-haired people, and can be confused with a
mole
22
Basalioom
23
Who is At Risk?

Anyone with a history of frequent sun exposure
can develop BCC.
But risk can increase with certain genetic or
environmental factors.
Time Spent Outdoors
People who work outdoors construction workers,
groundskeepers, farmers, lifeguards, etc. are
at greater risk than people who work indoors.
Skin Type
Fair-skinned individuals who sunburn easily have
a higher incidence of skin cancer than
dark-skinned individuals. Check our skin type
chart to see how at risk you are.
Hours of sunlight
The more hours of sunlight in the day, the
greater the incidence of skin cancer.

24
Skin Types and At-Risk Groups
Type I Is very fair, burns easily and severely
and does not tan. Eyes are blue or green and
hair is blond or red.
Type III Is somewhat darker and sometimes burns
then tans.
Type II Is also fair and burns easily, but does
get a minimal tan. Eyes are blue, hazel or
brown, and hair is blond, red or brown.
Type IV Is darker still, never burns, and
always tans rapidly
Types V Is brown
Type VI Is black.
25
After Treatment

Treatment does not end when your skin cancer has
been removed.
Cancerous and precancerous conditions can recur
even when they appear to have been adequately
treated. No fail-safe method of treatment yet
exists. A patient should continue to see the
physician for regular follow-up visits for
several years to make sure that the growth has
not recurred, patients who have had one skin
tumor have a 40 percent greater risk of
developing new tumors in the next five years.
The program recommended for most patients is a
visit to the doctor one month after the treatment
has been completed, with follow-up visits at
three-month intervals for one year. After that,
if all is well, the patient will be asked to
visit the doctor on a semiannual and then annual
basis. The minimum recommended follow-up period
is five years.

26
Squamous Cell Carcinoma/Carcinoma
Spinocellulare/Plaveiselcelca

Squamous cell carcinoma (SCC) is the second most
common form of skin cancer.
Squamous cells are cells that compose most of the
epidermis(keratinocyten).
An abnormal growth of these cells is known as a
squamous cell carcinoma.
Most SCCs are not serious.
When identified early and treated promptly, the
future is bright.
However, if overlooked, they are harder to treat
and can cause disfigurement.
While 96 to 97 percent of SCCs are localized, the
small percentage of remaining cases can spread to
other parts of the body, and the results are
often fatal.

27
Who is at Risk?

Anyone with a substantial history of sun exposure
can develop squamous cell carcinoma but certain
environmental and genetic factors can increase
the potential for this disease.
Sun Exposure
Sunlight is responsible for over 90 percent of
all skin cancers. Working primarily outdoors,
living in an area that gets a lot of high
intensity sunlight (like Australia), spending
time in tanning booths all increase your exposure
to UV rays and thus increase your risk for
developing skin cancer, including squamous cell
carcinoma.
Skin Type
People who have fair skin, light hair, and blue,
green, or gray eyes are at highest risk.
Dark-skinned individuals of African descent are
far less likely than fair-skinned individuals to
develop skin cancer. Check out your skin type
and how it affects your skin cancer risk. More
than two thirds of the skin cancers that
individuals of African descent develop are SCCs,
usually arising on the sites of preexisting
inflammatory skin conditions or burn injuries.
Although dark-skinned individuals of any
background are less likely than fair-skinned
individuals to develop skin cancer, it is still
essential for them to practice sun protection.
Previous Skin Cancer
If you have had a skin cancer of any type, it
increases your risk of developing another one.
Reduced Immunity
People with weakened immune systems due
to excessive unprotected sun exposure,
chemotherapy, or those with certain illnesses
such as HIV are more likely to develop squamous
cell carcinoma.
Precancers and Early Cancers
There are some precursor conditions, called preca
ncers and early cancers (also called cancer in
situ) that are sometimes associated with the
later development of SCC. They include actinic
keratosis, actinic chelitis, leukoplakia, and Bowe
n's disease, although most dermatologists believe
that Bowen's disease is just another name for a
type of superficial SCC that hasn't spread yet.
It appears as a persistent, scaly red-brown,
scaly patch. It may resemble eczema or
psoriasis.

28
Plaveiselcelca
29
Warning Signs
An elevated growth with a central depression that
occasionally bleeds. A growth of this type may
rapidly increase in size.
A wart-like growth that crusts and occasionally
bleeds
A persistent, scaly red patch with irregular
borders that sometimes crusts or bleeds.
An open sore that bleeds and crusts and persists
for weeks.
30
Tips

Seek the shade, especially between 10 A.M. and 4
P.M.
Do not burn.
Avoid tanning and UV tanning booths.
Use a sunscreen with an SPF of 15 or higher every
day.
Apply 1 ounce (2 tablespoons) of sunscreen to
your entire body 30 minutes before going
outside. Reapply every two hours.
Cover up with clothing, including a broad-brimmed
hat and UV-blocking sunglasses, umbrella
Keep newborns out of the sun. Sunscreens should
be used on babies over the age of six months.
Examine your skin head-to-toe every month.

31
What Is SPF?

Most sunscreens with an SPF of 15 or higher do an
excellent job of protecting against UVB. SPF or
Sun Protection Factor is a measure of a
sunscreen's ability to prevent UVB from damaging
the skin. Here's how it works If it takes 20
minutes for your unprotected skin to start
turning red, using an SPF 15 sunscreen
theoretically prevents reddening 15 times longer
about five hours.
Another way to look at it is in terms of
percentages SPF 15 blocks approximately 93
percent of all incoming UVB rays. SPF 30 blocks
97 percent and SPF 50 blocks 99 percent. They
may seem like negligible differences, but if you
are light-sensitive, or have a history of skin
cancer, those extra percentages will make a
difference. And as you can see, no sunscreen can
block all UV rays.
But there are problems with the SPF model
First, no sunscreen, regardless of strength,
should be expected to stay effective longer than
two hours without reapplication. Second,
"reddening" of the skin is a reaction to UVB rays
alone and tells you little about what UVA damage
you may be getting. Plenty of damage can be done
without the red flag of sunburn being raised.
Many of the sunscreens available in the US today
combine several different active chemical
sunscreen ingredients in order to provide
broad-spectrum protection. Usually, at least
three active ingredients are called for. These
generally include PABA derivatives, salicylates,
and/or cinnamates (octylmethoxycinnamate and
cinoxate) for UVB absorption(kortgolvig
290-315nm) benzophenones (such as oxybenzone and
sulisobenzone) for shorter-wavelength
UVA(langgolvig 315-400nm) protection and
avobenzone (Parsol 1789), ecamsule (Mexoryl),
titanium dioxide, or zinc oxide for the remaining
UVA spectrum.

32
Melanoma

Melanoma is the most serious form of skin
cancer.
However, if it is recognized and treated early,
it is nearly 100 percent curable.
But if it is not, the cancer can advance and
spread to other parts of the body, where it
becomes hard to treat and can be fatal.
While it is not the most common of the skin
cancers, it causes the most deaths.
Melanoma is a malignant tumor that originates in
melanocytes, the cells which produce the pigment
melanin that colors our skin, hair, and eyes and
is heavily concentrated in most
moles(naevusbeauty spot).
The majority of melanomas, therefore, are black
or brown.
However, melanomas occasionally stop producing
pigment. When that happens, the melanomas may no
longer be dark, but are skin-colored, pink, red
or purple.

33
Who is at Risk?

Everyone is at some risk for melanoma, but
increased risk depends on several factors sun
exposure, number of moles on the skin, skin type
and family history (genetics).
Sun exposure
Both UVA and UVB rays are dangerous to the skin,
and can induce skin cancer, including melanoma.
Blistering sunburns in early childhood increase
risk, but cumulative exposure also is a factor.
Moles
There are two kinds of moles that a person can
have normal moles the small brown blemishes,
growths, or "beauty marks" that appear in the
first few decades of life in almost everyone
and atypical moles, known as dysplastic nevi.
Regardless of type, the more moles you have, the
greater your risk for melanoma.
Skin Type
As with all skin cancers, people with fairer skin
are at increased risk.
Family History
About one in every ten patients diagnosed with
the disease has a family member with a history of
melanoma.
Personal History
Once you have had melanoma, you run an increased
chance of recurrence. Also, people who have or
had basal cell carcinoma and squamous cell
carcinoma are at increased risk for developing
melanoma.
Weakened Immune System
Compromised immune systems as the result of
chemotherapy, excessive sun exposure, and
diseases such as HIV or lymphoma can increase
your risk of melanoma.

34
Statistics

BCC with more than 800,000 new cases estimated in
the US each year
SCC with over 200,000 new cases per year
estimated in the United States
The American Cancer Society estimates that in
2007, there will be 59,940 new cases of melanoma
in the United States.
In Nederland wordt per jaar bij ongeveer 2.850
mensen een melanoom ontdekt.Het melanoom komt op
alle leeftijden voor, maar meestal bij mensen van
30-60 jaar. Melanomen komen iets vaker voor bij
vrouwen dan bij mannen.

35
Warning Signs The ABCDs of Melanoma
Border The borders of an early melanoma tend to
be uneven. The edges may be scalloped or notched.
Asymmetry If you draw a line through this mole,
the two halves will not match, meaning it is
asymmetrical, a warning sign for melanoma.
Color Having a variety of colors is another
warning signal. A number of different shades of
brown, tan or black could appear. A melanoma may
also become red, white or blue.
Diameter Melanomas usually are larger in diameter
than the size of the eraser on your pencil (1/4
inch or 6 mm), but they may sometimes be smaller
when first detected.
36
BENIGNE
MALIGNE
Asymmetrical
Symmetrical
Borders are uneven
Borders are even
37
BENIGNE
MALIGNE
One shade
Two or more shades
Smaller than 1/4 inch(6mm)
Larger than 1/4(6mm)
38
Types of Melanoma

The Four Basic TypesMelanomas fall into four
basic categories. Three of them begin in situ
meaning they occupy only the top layers of the
skin and sometimes become invasive the fourth
is invasive from the start.
Superficial spreading melanoma is by far the most
common type, accounting for about 70 percent of
all cases. As the name suggests, this melanoma
travels along the top layer of the skin for a
fairly long time before penetrating more deeply.
The first sign is the appearance of a flat or
slightly raised discolored patch that has
irregular borders and is somewhat geometrical in
form. The color varies, and you may see areas of
tan, brown, black, red, blue or white. This type
of melanoma can occur in a previously benign
mole. The melanoma can be found almost anywhere
on the body, but is most likely to occur on the
trunk in men, the legs in women, and the upper
back in both. Young people who have melanoma
usually have this type.
Lentigo maligna is similar to the superficial
spreading type, as it also remains close to the
skin surface for quite a while, and usually
appears as a flat or mildly elevated mottled tan,
brown or dark brown discoloration.
This type of in situ melanoma is found most often
in the elderly, arising on chronically
sun-exposed, damaged skin on the face, ears,
arms, and upper trunk. Lentigo maligna is the
most common form of melanoma in Hawaii. When
this cancer becomes invasive, it is referred to
as lentigo maligna melanoma.
Acral lentiginous melanoma also spreads
superficially before penetrating more deeply.
It is quite different from the others, though, as
it usually appears as a black or brown
discoloration under the nails or on the soles of
the feet or palms of the hands. It is the most
common melanoma in African-Americans and Asians,
and the least common among Caucasians.
Nodular melanoma is usually invasive at the time
it is first diagnosed.
The malignancy is recognized when it becomes a
bump. It is usually black, but occasionally is
blue, gray, white, brown, tan, red or skin tone.
The most frequent locations are the trunk, legs,
and arms, mainly of elderly people, as well as
the scalp in men. This is the most aggressive of
the melanomas, and is found in 10 to 15 percent
of cases.

39
Breslow's thickness

Guide to StagingThe most important factors in
the staging system are the thickness of the
tumor, known as Breslow's thickness, and the
appearance of microscopic ulceration, meaning
that the skin covering the tumor is not intact.
Breslow's thickness measures in millimeters the
distance between the upper layer of the epidermis
and the deepest point of the tumor's
penetration. The thinner the melanoma, the
better the chance of a cure.
In situ melanoma remains confined to the
epidermis
Very thin tumors are less than 1.0 millimeter
Thin tumors are 1.012.0 mm
Intermediate tumors are 2.0-4.0 mm
Thick melanomas are 4.00 mm or more.

40
Clark's level of invasion

The presence of microscopic ulceration moves the
tumor into a later stage. Your doctor may elect
to treat a tumor with ulceration more
aggressively because of this.
Very thin tumors are classified according to
Clark's level of invasion, which describes the
number of layers of skin penetrated by the tumor.
Clark's level I. The melanoma occupies only the
epidermis.
Clark's level II. The melanoma penetrates to the
layer immediately under the epidermis, the
papillary dermis.
Clark's level III. The melanoma fills the
papillary dermis and impinges on the reticular
dermis, the next layer down.
Clark's level IV. The melanoma penetrates into
the reticular or deep dermis.
Clark's level V. The melanoma invades the
subcutaneous fat.

41
Breslow's thickness/ Clark's level of invasion
Melanoom
42

Stage I. This category is subdivided according to
the thickness of the primary (original) tumor.
Stage 1a The tumor is less than 1.0 mm in
Breslow's thickness without ulceration and is in
Clark's level II or III.
Stage Ib The tumor is less than 1.0 mm in
Breslow's thickness with ulceration and/or
Clark's level III or IV, or it is 1.01 - 2.0 mm
in thickness without ulceration
Stage II. This is also subdivided according to
gradations in thickness and/or depth, and the
presence or absence of ulceration.
Stage IIa The tumor is 1.01 - 2.0 mm in
Breslow's thickness with ulceration, or is
2.01-4.0 mm in thickness without ulceration.
Stage IIb The tumor is 2.01-4.0 mm in Breslow's
thickness with ulceration, or is greater than 4.0
mm in thickness without ulceration.
Stage IIc The tumor is greater than 4.0 mm in
Breslow's thickness with ulceration.
Later Stages Stages III and IVBy the time a
melanoma advances to Stage III or beyond,an
important change has occurred. The Breslow's
thickness is by then irrelevant and is no longer
included, but the presence of microscopic
ulceration continues to be used in staging, as it
has an important effect on the progression of the
disease. At this point, the tumor has either
spread to the lymph nodes small organs located
in various locations within the body that fight
cancer, disease and other infections or to the
skin between the primary tumor and the nearby
lymph nodes.
Stage III. A tumor is assigned to Stage III if it
has metastasized or spread. This can be
determined by examining a biopsy of the node
nearest the tumor, known as the sentinel node.
Such a biopsy is now frequently done when a tumor
ismore than 1 mm in thickness, or when a thinner
melanoma shows evidence of ulceration. As the
sentinel node biopsy is not considered necessary
in all cases, you may wish to discuss the matter
with your physician. In-transit or satellite
metastases are also included in Stage III. In
this case, the spread isto skin or underlying
tissue (subcutaneous) for a distance of more than
2 centimeters (1 cm equals 0.4 inch) from the
primary tumor, but not beyond the regional lymph
nodes. In addition, the new staging system
includes metastases so tiny they can be seen only
through the microscope.
Stage IV. The melanoma has metastasized to lymph
nodes far away from the primary tumor or to
internal organs, most often the lung, followed in
descending order of frequency by the liver,
brain, bone, and gastrointestinal tract.

43
Treatment

When it comes to the early stages of the disease,
the future is bright. Most people with thin,
localized melanomas are cured by appropriate
surgery. Early detection still remains the best
weapon in fighting skin cancer.
For people with more advanced disease, there is
still good news. The cure rate continues to
rise. Treatments are varied and many new
discoveries are being made to improve the chances
of those with metastatic disease.
Surgical Excision The first step in treatment is
the removal of the melanoma, usually by surgical
excision (cutting it out). Most surgical
excisions also called resections are done in
a doctor's office or as an outpatient procedure
using local anesthesia. Scars are usually small
and improve over time.
There is now a trend towards performing a
sentinel lymph node biopsy and tumor removal at
the same time, provided the tumor is 1mm or more
thick.
Setting the Margins
In today's technique, much less of the normal
skin around the tumor is removed. The borders of
the entire area to be excised both tumor and
healthy skin are known as the margins. Margins
are much narrower than they ever were before.
Most surgeons today are following the guidelines
recommended by the National Institutes of Health
(NIH) and the American Academy of Dermatology
Task Force on Cutaneous Melanoma
When there is an in situ melanoma, the surgeon
excises 0.5 centimeter of the normal skin
surrounding the tumor and takes off the skin
layers down to the fat.
In removing a melanoma that is 1 mm or less in
thickness, the margins of surrounding skin are
extended to 1 cm, and the excision goes through
all skin layers and down to the fascia.
If the melanoma is equal to or greater than 2 mm
in Breslows thickness, a margin of 23 cm is
taken.

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Adjuvant (Additional) Treatment

Chemotherapy
A number of drugs that are active in fighting
cancercells are being used to treat melanoma,
either one at a time or incombinations.
Currently, Dacarbazine (DTIC), given by
injection, is the only chemotherapy approved by
the FDA. Another agent you may be hearing about
is temozolomide, anoral drug which closely
resembles DTIC.
Isolation-Perfusion Method
This palliative treatment is sometimes used when
the melanoma is on an arm or leg.Isolation
means that the chemotherapy is perfused (added
to) theblood flowing through the affected limb,
and no other part of the body.
Immunotherapy/Biochemotherapy
Gene therapy

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TipDysplastic Nevi Syndrome

Dysplastic nevi are atypical moles, which,
although benign, resemble melanoma and indicate
an increased risk. Those who have dysplastic
nevi and a family history of melanoma have a
200-fold increase in risk of developing
melanoma. Those who have dysplastic nevi but no
family history of melanoma also have up to
fifteen times greater risk of developing melanoma
than the general population.
Research has shown that the risk of melanoma in
members of families affected by atypical mole
(dysplastic nevus) syndrome is 49 in persons
1-50 years old and 82 by age 72. People with
classic atypical mole syndrome have the
following three characteristics
100 or more moles
One or more moles greater than 8mm (1/3 inch) in
diameter
One or more moles that look atypical
Shape Border Color Diameter Location
Uniformity
Onset most often during early childhood through
ages 35 - 40