Unusual Cancers of Childhood Treatment (PDQ®)—Patient Version - National Cancer Institute

Unusual Cancers of Childhood Treatment (PDQ®)–Patient Version

Neuroendocrine Tumors (Carcinoid Tumors)

Neuroendocrine tumors (including carcinoid tumors) usually form in the lining of the stomach or intestines, but they can form in other organs, such as the pancreas, lungs, or liver. These tumors are usually small, slow-growing, and benign (not cancer). Some neuroendocrine tumors are malignant (cancer) and spread to other places in the body. Sometimes neuroendocrine tumors in children form in the appendix (a pouch that sticks out from the first part of the large intestine near the end of the small intestine). The tumor is often found during surgery to remove the appendix.

See the Tracheobronchial tumors section of this summary for information on tracheobronchial carcinoid tumors.

Signs and Symptoms

Some neuroendocrine tumors release hormones and other substances. If the tumor is in the liver, high amounts of these hormones may remain in the body and cause a group of signs and symptoms called carcinoid syndrome. Carcinoid syndrome caused by the hormone somatostatin may cause any of the following signs and symptoms. Check with your child’s doctor if your child has any of the following:

Redness and a warm feeling in the face and neck.
A fast heartbeat.
Trouble breathing.
Sudden drop in blood pressure (restlessness, confusion, weakness, dizziness, and pale, cool, and clammy skin).
Diarrhea.

Other conditions that are not neuroendocrine tumors may cause these same signs and symptoms.

Diagnostic and Staging Tests

Tests that check for signs of cancer are used to diagnose and stage neuroendocrine tumors. They may include:

Physical exam and history.
Blood chemistry studies.

See the General Information section for a description of these tests and procedures.

Other tests used to diagnose neuroendocrine tumors include the following:

Complete blood count (CBC): A procedure in which a sample of blood is drawn and checked for the following:
- The number of red blood cells, white blood cells, and platelets.
- The amount of hemoglobin (the protein that carries oxygen) in the red blood cells.
- The portion of the blood sample made up of red blood cells.
Twenty-four-hour urine test: A test in which urine is collected for 24 hours to measure the amounts of certain substances, such as hormones. An unusual (higher or lower than normal) amount of a substance can be a sign of disease in the organ or tissue that makes it. The urine sample is checked to see if it contains a hormone made by carcinoid tumors. This test is used to help diagnose carcinoid syndrome.
Somatostatin receptor scintigraphy : A type of radionuclide scan that may be used to find tumors. A very small amount of radioactive octreotide (a hormone that attaches to tumors) is injected into a vein and travels through the blood. The radioactive octreotide attaches to the tumor and a special camera that detects radioactivity is used to show where the tumors are in the body. This procedure is also called octreotide scan and SRS.

Prognosis

The prognosis for neuroendocrine tumors in the appendix in children is usually excellent after surgery to remove the tumor. Neuroendocrine tumors that are not in the appendix are usually larger or have spread to other parts of the body at the time of diagnosis and do not respond well to chemotherapy. Larger tumors are more likely to recur (come back).

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of neuroendocrine tumors in the appendix in children may include the following:

Surgery to remove the appendix.

Treatment of neuroendocrine tumors that have spread to the large intestine, pancreas, or stomach is usually surgery. Treatment of tumors that cannot be removed by surgery, multiple tumors, or tumors that have spread may include the following:

Radioembolization.
Somatostatin analogue therapy (octreotide or lanreotide).
Peptide receptor radionuclide therapy.
Targeted therapy (sunitinib or everolimus).

Treatment of recurrent neuroendocrine tumors in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

See the PDQ summary on adult Gastrointestinal Carcinoid Tumors Treatment for more information.

Gastrointestinal Stromal Tumors

Gastrointestinal stromal cell tumors (GIST) usually begin in cells in the wall of the stomachor intestines. GISTs may be benign (not cancer) or malignant (cancer). Childhood GISTs are more common in girls, and usually appear in the teen years.

Risk Factors and Signs and Symptoms

GISTs in children are not the same as GISTs in adults. Patients should be seen at centers that specialize in the treatment of GISTs and the tumors should be tested for geneticchanges. A small number of children have tumors with genetic changes like those found in adult patients. The risk of GIST is increased by the following genetic disorders:

Most children with GIST have tumors in the stomach and develop anemia caused by bleeding. Signs and symptoms of anemia include the following:

Feeling tired.
Dizziness.
A fast or irregular heartbeat.
Shortness of breath.
Pale skin.

A lump in the abdomen or a blockage of the intestine (crampy pain in the abdomen, nausea, vomiting, diarrhea, constipation, and swelling of the abdomen) are also signs of GIST.

Other conditions that are not anemia caused by GIST may cause these same signs and symptoms.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment for children who have tumors with genetic changes like those found in adult patients is targeted therapy with a tyrosine kinase inhibitor.

Treatment for children whose tumors do not show genetic changes may include the following:

Surgery to remove the tumor.

Treatment of recurrent GIST in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

Unusual Cancers of the Reproductive and Urinary Systems

Bladder Cancer

Bladder cancer is a disease in which malignant (cancer) cells form in the tissues of the bladder. The bladder is a hollow organ in the lower part of the abdomen. It is shaped like a small balloon and has a muscle wall that allows it to get bigger or smaller. Tiny tubules in the kidneys filter and clean the blood. They take out waste products and make urine. The urine passes from each kidney through a long tube called a ureter into the bladder. The bladder holds the urine until it passes through the urethra and leaves the body.

Anatomy of the female urinary system; drawing shows a front view of the right and left kidneys, the ureters, urethra, and bladder filled with urine. The inside of the left kidney shows the renal pelvis. An inset shows the renal tubules and urine. The spine, adrenal glands, and uterus are also shown. — Anatomy of the female urinary system showing the kidneys, adrenal glands, ureters, bladder, and urethra. Urine is made in the renal tubules and collects in the renal pelvis of each kidney. The urine flows from the kidneys through the ureters to the bladder. The urine is stored in the bladder until it leaves the body through the urethra.

The most common type of bladder cancer is transitional cell cancer. Squamous cell and other more aggressive types of bladder cancer are less common.

Risk Factors, Signs and Symptoms, and Diagnostic and Staging Tests

The risk of bladder cancer is increased in females who have been treated for cancer with certain anticancer drugs called alkylating agents.

Bladder cancer may cause any of the following signs and symptoms. Check with your child’s doctor if your child has any of the following:

Blood in the urine (slightly rusty to bright red in color).
Frequent urination or feeling the need to urinate without being able to do so.
Pain during urination.
Lower back pain.

Other conditions that are not bladder cancer may cause the same signs and symptoms.

Tests to diagnose and stage bladder cancer may include the following:

Physical exam and history.
CT scan.
Ultrasound of the bladder.
Biopsy.

See the General Information section for a description of these tests and procedures.

Other tests used to diagnose bladder cancer include the following:

Urinalysis : A test to check the color of urine and its contents, such as sugar, protein, red blood cells, and white blood cells.
Urine cytology : A laboratory test in which a sample of urine is checked under a microscope for abnormal cells.
Cystoscopy : A procedure to look inside the bladder and urethra to check for abnormal areas. A cystoscope is inserted through the urethra into the bladder. A cystoscope is a thin, tube-like instrument with a light and a lens for viewing. It may also have a tool to remove tissue samples, which are checked under a microscope for signs of cancer.

Prognosis

In children, bladder cancer is usually low grade (not likely to spread) and the prognosis is usually excellent after surgery to remove the tumor.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of bladder cancer in children is usually the following:

Transurethral resection (TUR). This is a surgical procedure to remove tissue from the bladder using a resectoscope inserted into the bladder through the urethra. A resectoscope is a thin, tube-like instrument with a light, a lens for viewing, and a tool to remove tissue and burn away any remaining tumor cells. Tissue samples are checked under a microscope for signs of cancer.

Treatment of recurrent bladder cancer in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

See the PDQ summary on adult Bladder Cancer Treatment for more information.

Testicular Cancer

Testicular cancer is a disease in which malignant (cancer) cells form in the tissues of one or both testicles. The testicles are 2 egg-shaped glands located inside the scrotum (a sac of loose skin that lies directly below the penis). The testicles are held within the scrotum by the spermatic cord, which also contains the vas deferens and vessels and nerves of the testicles.

Anatomy of the male reproductive and urinary systems; drawing shows front and side views of ureters, lymph nodes, rectum, bladder, prostate gland, vas deferens, penis, testicles, urethra, seminal vesicle, and ejaculatory duct. — Anatomy of the male reproductive and urinary systems, showing the prostate, testicles, bladder, and other organs.

There are two types of testicular tumors:

Germ cell tumors: Tumors that start in sperm cells in males. Testicular germ cell tumors may be benign (not cancer) or malignant (cancer). The most common testicular germ cell tumors in young boys are benign teratomas and malignant nonseminomas. Seminomas usually occur in young men and are rare in boys.
Non-germ cell tumors: Tumors that begin in the tissues that surround and support the testicles. These tumors may be benign or malignant.

Signs and Symptoms and Diagnostic and Staging Tests

Testicular cancer and its spread to other parts of the body may cause any of the following signs and symptoms. Check with your child’s doctor if your child has any of the following:

Painless lump in the testicles.
Pain in the abdomen or back.
Trouble breathing.
Streaks of blood in sputum (mucus coughed up from the lungs).

A painless lump in the testicles may be a sign of a testicular tumor. Other conditions may also cause a lump in the testicles.

Tests to diagnose and stage non-germ cell testicular cancer may include the following:

See the General Information section for a description of these tests and procedures.

Other tests used to diagnose testicular tumors include the following:

Serum tumor marker test : A procedure in which a sample of blood is examined to measure the amounts of certain substances released into the blood by organs, tissues, or tumor cells in the body. Certain substances are linked to specific types of cancer when found in increased levels in the blood. These are called tumor markers. The tumor marker alpha-fetoprotein is used to diagnose germ cell tumors.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of non-germ cell testicular cancer in children may include the following:

Surgery to remove the tumor.

Treatment of recurrent non-germ cell testicular cancer in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

See the PDQ summary on Childhood Extracranial Germ Cell Tumors Treatment for more information on testicular germ cell tumors.

Ovarian Cancer

Ovarian cancer is a disease in which malignant (cancer) cells form in the ovary. The ovaries are a pair of organs in the female reproductive system. They are located in the pelvis, one on each side of the uterus (the hollow, pear-shaped organ where a fetus grows). Each ovary is about the size and shape of an almond. The ovaries produce eggs and female hormones (chemicals that control the way certain cells or organs function).

Anatomy of the female reproductive system; drawing shows the uterus, myometrium (muscular outer layer of the uterus), endometrium (inner lining of the uterus), ovaries, fallopian tubes, cervix, and vagina. — Anatomy of the female reproductive system. The organs in the female reproductive system include the uterus, ovaries, fallopian tubes, cervix, and vagina. The uterus has a muscular outer layer called the myometrium and an inner lining called the endometrium.

Most ovarian tumors in children are benign (not cancer). They occur most often in females aged 15 to 19 years.

There are several types of malignant ovarian tumors:

Germ cell tumors: Tumors that start in egg cells in females. These are the most common ovarian tumors in girls. (See the PDQ summary on Childhood Extracranial Germ Cell Tumors Treatment for more information on ovarian germ cell tumors.)
Epithelial tumors: Tumors that start in the tissue covering the ovary. These are the second most common ovarian tumors in girls.
Stromal tumors: Tumors that begin in stromal cells, which make up tissues that surround and support the ovaries. Juvenile granulosa cell tumors and Sertoli-Leydig cell tumors are two types of stromal tumors.
Other tumors, such as small cell carcinoma of the ovary (a very rare tumor).

Risk Factors, Signs and Symptoms, and Diagnostic and Staging Tests

The risk of ovarian cancer is increased by having one of the following conditions:

Ollier disease (a disorder that causes abnormal growth of cartilage at the end of long bones).
Maffucci syndrome (a disorder that causes abnormal growth of cartilage at the end of long bones and of blood vessels in the skin).
Peutz-Jeghers syndrome.
Pleuropulmonary blastoma syndrome (a disorder that may cause cystic nephroma, cysts in the lung, thyroid problems, and other cancers of the kidney, ovary, and soft tissue).
DICER1 syndrome (a disorder that may cause goiter, polyps in the colon, and tumors of the ovary, cervix, testicle, kidney, brain, eye, and lining of the lung).

Ovarian cancer may cause any of the following signs and symptoms. Check with your child’s doctor if your child has any of the following:

Pain or swelling in the abdomen.
A lump in the abdomen.
Constipation.
Painful or missing menstrual periods.
Unusual vaginal bleeding.
Having male sex traits, such as body hair or a deep voice.
Early signs of puberty.

Other conditions that are not ovarian cancer may cause these same signs and symptoms.

Tests to diagnose and stage ovarian cancer may include the following:

See the General Information section for a description of these tests and procedures.

During surgery to remove the tumor, fluid in the abdomen will be checked for signs of cancer.

Prognosis

Ovarian epithelial cancer is usually found at an early stage in children and is easier to treat than in adult patients.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of ovarian epithelial cancer in children may include the following:

Treatment of ovarian stromal tumors in children may include the following:

Surgery to remove one ovary and one fallopian tube for early cancer.
Surgery followed by chemotherapy for cancer that is advanced.
Chemotherapy for cancer that has recurred (come back).

Treatment of recurrent ovarian cancer in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

See the following PDQ summaries for more information:

Cervical and Vaginal Cancer

Cervical cancer is a disease in which malignant (cancer) cells form in the cervix. The cervix is the lower, narrow end of the uterus (the hollow, pear-shaped organ where a fetusgrows). The cervix leads from the uterus to the vagina (birth canal). Vaginal cancer forms in the vagina. The vagina is the canal leading from the cervix to the outside of the body. At birth, a baby passes out of the body through the vagina (also called the birth canal).

The most common sign of cervical and vaginal cancer is bleeding from the vagina. Other conditions may also cause vaginal bleeding. Children are often diagnosed with advanced disease.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of childhood cervical and vaginal cancer may include the following:

Surgery to remove as much of the cancer as possible, followed by radiation therapy.
Chemotherapy may also be used but it is not yet known how well this treatment works.

Treatment of recurrent cervical and vaginal cancer in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

Other Rare Unusual Cancers of Childhood

Multiple Endocrine Neoplasia Syndromes

Multiple endocrine neoplasia (MEN) syndromes are inherited disorders that affect the endocrine system. The endocrine system is made up of glands and cells that make hormones and release them into the blood. MEN syndromes may cause hyperplasia (the growth of too many normal cells) or tumors that may be benign (not cancer) or malignant(cancer).

There are several types of MEN syndromes and each type may cause different conditionsor cancers. Patients and family members with an increased risk of these syndromes should have genetic counseling and tests to check for the syndromes.

The two main types of MEN syndromes are MEN1 and MEN2:

MEN1 syndrome is also called Werner syndrome. This syndrome usually causes tumors in the parathyroid gland, pituitary gland, and pancreas. Rarely, it causes tumors in the adrenal glands, gastrointestinal tract, fibrous tissue, and fat cells. The tumors make extra hormones and cause certain signs or symptoms of disease. The signs and symptoms depend on the type of hormone made by the tumor.
The most common sign of MEN1 syndrome is hypercalcemia. Hypercalcemia occurs when the parathyroid gland makes too much parathyroid hormone. Signs and symptoms of hypercalcemia include the following:
- Weakness.
- Feeling very tired.
- Nausea and vomiting.
- Loss of appetite.
- Being very thirsty.
- Urinating more than usual.
- Constipation.
A diagnosis of MEN1 syndrome is usually made when tumors are found in two different places. The prognosis (chance of recovery) is usually good.
Children who are diagnosed with MEN1 syndrome are checked for signs of cancer starting at age 5 and continuing for the rest of their life. Talk to your doctor about the tests and procedures that should be done to check for signs of cancer and how often they should be done.
Children with MEN1 syndrome may also have primary hyperparathyroidism. In primary hyperparathyroidism, one or more of the parathyroid glands makes too much parathyroid hormone. The most common sign of primary hyperparathyroidism is kidney stones. Children with primary hyperparathyroidism may have genetic testing to check for gene changes linked to MEN1 syndrome.
MEN2 syndrome includes three subgroups:
- MEN2A syndrome
  MEN2A syndrome is also called Sipple syndrome. A diagnosis of MEN2A syndrome may be made when the patient or the patient's parents, brothers, sisters, or children have two or more of the following:
  - Medullary thyroid cancer.
  - Pheochromocytoma (a tumor of the adrenal gland).
  - Parathyroid gland disease (a benign tumor of the parathyroid gland or increase in the size of the parathyroid gland).
  Signs and symptoms of medullary thyroid cancer may include:
  - A lump in the throat or neck.
  - Trouble breathing.
  - Trouble swallowing.
  - Hoarseness.
  Signs and symptoms of pheochromocytoma may include:
  - Pain in the abdomen or chest.
  - A strong, fast, or irregular heartbeat.
  - Headache.
  - Heavy sweating for no known reason.
  - Dizziness.
  - Feeling shaky.
  - Being irritable or nervous.
  Signs and symptoms of parathyroid disease may include:
  - Hypercalcemia.
  - Pain in the abdomen, side, or back that doesn't go away.
  - Pain in the bones.
  - A broken bone.
  - A lump in the neck.
  - Change in voice, such as hoarseness.
  - Trouble swallowing.
  Family members of patients with the MEN2A syndrome should have genetic counseling and be tested in early childhood, before age 5, for the gene changes that lead to this type of cancer.
  A small number of medullary thyroid cancers may occur at the same time as Hirschsprung disease (chronic constipation that begins when a child is an infant), which has been found in some families with MEN2A syndrome. Hirschsprung disease may appear before other signs of MEN2A syndrome do. Patients who are diagnosed with Hirschsprung disease should be checked for certain gene changes that cause MEN2A syndrome.
  Familial medullary carcinoma of the thyroid (FMTC) is a type of MEN2A syndrome that causes medullary thyroid cancer. A diagnosis of FMTC may be made when two or more family members have medullary thyroid cancer and no family members have parathyroid or adrenal gland problems.
- MEN2B syndrome
  Patients with MEN2B syndrome may have a slender body build with long, thin arms and legs. The lips may appear thick and bumpy because of benign tumors in the mucous membranes. MEN2B syndrome may cause the following conditions:
  - Medullary thyroid cancer.
  - Parathyroid hyperplasia.
  - Adenomas.
  - Pheochromocytoma.
  - Nerve cell tumors in the mucous membranes or other places.

Tests used to diagnose and stage MEN syndromes depend on the signs and symptoms and the patient's family history. They may include:

Physical exam and history.
Blood chemistry studies.
Ultrasound.
MRI.
CT scan.
PET scan.
Fine-needle aspiration (FNA) or surgical biopsy.

See the General Information section for a description of these tests and procedures.

Other tests and procedures used to diagnose MEN syndromes include the following:

Genetic testing : A laboratory test that analyzes cells or tissues to look for changes in a gene, chromosome, or protein. These changes may be a sign of a genetic disease or condition. They may also be linked to an increased risk of developing a specific disease or condition.
Blood hormone studies: A procedure in which a blood sample is checked to measure the amounts of certain hormones released into the blood by organs and tissues in the body. An unusual (higher or lower than normal) amount of a substance can be a sign of disease in the organ or tissue that makes it. The blood may be checked for abnormallevels of thyroid-stimulating hormone (TSH). TSH is made by the pituitary gland in the brain. It stimulates the release of thyroid hormone and controls how fast follicular thyroid cells grow. The blood may also be checked for high levels of the hormone calcitonin or parathyroid hormone (PTH).
Radioactive iodine scan (RAI scan): A procedure to find areas in the body where thyroid cancer cells may be dividing quickly. Radioactive iodine (RAI) is used because only thyroid cells take up iodine. A very small amount of RAI is swallowed, travels through the blood, and collects in thyroid tissue and thyroid cancer cells anywhere in the body. Abnormal thyroid cells take up less iodine than normal thyroid cells do. Areas that do not take up the iodine normally are called cold spots. Cold spots show up lighter in the picture made by the scan. They can be either benign (not cancer) or malignant, so a biopsy is done to find out if they are cancer.
Sestamibi scan : A type of radionuclide scan used to find an overactive parathyroid gland. A very small amount of a radioactive substance called technetium 99 is injectedinto a vein and travels through the bloodstream to the parathyroid gland. The radioactive substance will collect in the overactive gland and show up brightly on a special camera that detects radioactivity.
Angiogram : A procedure to look at blood vessels and the flow of blood. A contrast dyeis injected into a blood vessel. As the contrast dye moves through the blood vessel, x-rays are taken to see if there are any blockages.
Venous sampling for an overactive parathyroid gland: A procedure in which a sample of blood is taken from veins near the parathyroid glands. The sample is checked to measure the amount of parathyroid hormone released into the blood by each gland. Venous sampling may be done if blood tests show there is an overactive parathyroid gland but imaging tests don’t show which one it is.
Somatostatin receptor scintigraphy : A type of radionuclide scan that may be used to find tumors. A very small amount of radioactive octreotide (a hormone that attaches to tumors) is injected into a vein and travels through the blood. The radioactive octreotide attaches to the tumor and a special camera that detects radioactivity is used to show where the tumors are in the body. This procedure is also called octreotide scan and SRS.
MIBG scan : A procedure used to find neuroendocrine tumors, such as pheochromocytoma. A very small amount of a substance called radioactive MIBG is injected into a vein and travels through the bloodstream. Neuroendocrine tumor cells take up the radioactive MIBG and are detected by a scanner. Scans may be taken over 1-3 days. An iodine solution may be given before or during the test to keep the thyroid gland from absorbing too much of the MIBG.
Twenty-four-hour urine test: A test in which urine is collected for 24 hours to measure the amounts of catecholamines in the urine. Substances caused by the breakdown of these catecholamines are also measured. An unusual (higher- or lower-than-normal) amount of a substance can be a sign of disease in the organ or tissue that makes it. Higher-than-normal amounts may be a sign of pheochromocytoma.
Pentagastrin stimulation test: A test in which blood samples are checked to measure the amount of calcitonin in the blood. Calcium gluconate and pentagastrin are injected into the blood and then several blood samples are taken over the next 5 minutes. If the level of calcitonin in the blood increases, it may be a sign of medullary thyroid cancer.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

There are several types of MEN syndrome, and each type may need different treatment:

Patients with the MEN1 syndrome are treated for parathyroid, pancreatic and pituitary tumors.
Patients with the MEN1 syndrome and primary hyperparathyroidism may have surgeryto remove at least three parathyroid glands and the thymus.
Patients with the MEN2A syndrome usually have surgery to remove the thyroid by age 5 or earlier if genetic tests show certain changes in the RET gene. The surgery is done to diagnose cancer or to prevent cancer from forming or spreading.
Infants with the MEN2B syndrome may have surgery to remove the thyroid to prevent cancer.
Children with the MEN2B syndrome who have medullary thyroid cancer may be treated with targeted therapy (kinase inhibitor).
Patients with Hirschsprung disease and certain gene changes may have the thyroid removed to prevent cancer.

Treatment of recurrent MEN syndrome in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

Pheochromocytoma and Paraganglioma

Pheochromocytoma and paraganglioma are rare tumors that come from the same type of nerve tissue.

Pheochromocytoma forms in the adrenal glands. There are two adrenal glands, one on top of each kidney in the back of the upper abdomen. Each adrenal gland has two parts. The outer layer of the adrenal gland is the adrenal cortex. The center of the adrenal gland is the adrenal medulla. Pheochromocytoma is a tumor of the adrenal medulla. The adrenal glands make important hormones called catecholamines. Adrenaline (epinephrine) and noradrenaline (norepinephrine) are two types of catecholamines that help control heart rate, blood pressure, blood sugar, and the way the body reacts to stress. Some pheochromocytomas release extra adrenaline and noradrenaline into the blood and cause symptoms.
Paraganglioma forms outside the adrenal glands near the carotid artery, along nerve pathways in the head and neck, and in other parts of the body. Some paragangliomas make extra catecholamines called adrenaline and noradrenaline. The release of extra adrenaline and noradrenaline into the blood may cause symptoms.

Risk Factors, Signs and Symptoms, and Diagnostic and Staging Tests

Anything that increases your chance of getting a disease is called a risk factor. Having a risk factor doesn't mean that you will get cancer; not having risk factors doesn’t mean that you will not get cancer. Talk with your child’s doctor if you think your child may be at risk.

The risk of pheochromocytoma or paraganglioma is increased by having any of the following inherited syndromes or gene changes:

Multiple endocrine neoplasia type 1 (MEN1) syndrome.
Multiple endocrine neoplasia type 2 syndrome (MEN2A and MEN2B).
von Hippel-Lindau disease (VHL).
Neurofibromatosis type 1 (NF1).
Carney-Stratakis dyad (paraganglioma and gastrointestinal stromal tumor [GIST]).
Carney triad (paraganglioma, GIST, and pulmonary chondroma).
Changes in certain genes including the VHL, NF1, RET, SDHD, SDHB, SDHA, MAX, and TMEM127 genes.

More than half of the children and adolescents diagnosed with pheochromocytoma or paraganglioma have an inherited syndrome or gene change that increased the risk of cancer. Genetic counseling (a discussion with a trained professional about inherited diseases) and testing is an important part of the treatment plan.

Some tumors do not make extra adrenaline or noradrenaline and do not cause symptoms. These tumors may be found when a lump forms in the neck or when a test or procedure is done for another reason. Signs and symptoms of pheochromocytoma and paraganglioma occur when too much adrenaline or noradrenaline is released into the blood. These and other symptoms may be caused by pheochromocytoma, paraganglioma, or other conditions. Check with your child’s doctor if your child has any of the following:

High blood pressure.
Headache.
Heavy sweating for no known reason.
A strong, fast, or irregular heartbeat.
Feeling shaky.
Being extremely pale.
Dizziness.
Being irritable or nervous.

These signs and symptoms may come and go but high blood pressure is more likely to occur for long periods of time in young patients. These signs and symptoms may also occur with physical activity, injury, anesthesia, surgery to remove the tumor, eating foods such as chocolate and cheese, or while passing urine (if the tumor is in the bladder).

Tests used to diagnose and stage pheochromocytoma and paraganglioma depend on the signs and symptoms and the patient's family history. They may include:

Physical exam and history.
PET scan.
CT scan (CAT scan).
MRI (magnetic resonance imaging).

See the General Information section for a description of these tests and procedures.

Other tests and procedures used to diagnose pheochromocytoma and paraganglioma include the following:

Plasma-free metanephrines test: A blood test that measures the amount of metanephrines in the blood. Metanephrines are substances that are made when the body breaks down adrenaline or noradrenaline. Pheochromocytomas and paragangliomas can make large amounts of adrenaline and noradrenaline and cause high levels of metanephrines in both the blood and urine.
Blood catecholamine studies: A procedure in which a blood sample is checked to measure the amount of certain catecholamines (adrenaline or noradrenaline) released into the blood. Substances caused by the breakdown of these catecholamines are also measured. An unusual (higher- or lower-than-normal) amount of a substance can be a sign of disease in the organ or tissue that makes it. Higher-than-normal amounts may be a sign of pheochromocytoma or paraganglioma.
Twenty-four-hour urine test: A test in which urine is collected for 24 hours to measure the amounts of catecholamines (adrenaline or noradrenaline) or metanephrines in the urine. Substances caused by the breakdown of these catecholamines are also measured. An unusual (higher- or lower-than-normal) amount of a substance can be a sign of disease in the organ or tissue that makes it. Higher-than-normal amounts may be a sign of pheochromocytoma or paraganglioma.
MIBG scan : A procedure used to find neuroendocrine tumors, such as pheochromocytoma and paraganglioma. A very small amount of a substance called radioactive MIBG is injected into a vein and travels through the bloodstream. Neuroendocrine tumor cells take up the radioactive MIBG and are detected by a scanner. Scans may be taken over 1-3 days. An iodine solution may be given before or during the test to keep the thyroid gland from absorbing too much of the MIBG.
Somatostatin receptor scintigraphy : A type of radionuclide scan that may be used to find tumors. A very small amount of radioactive octreotide (a hormone that attaches to tumors) is injected into a vein and travels through the blood. The radioactive octreotide attaches to the tumor and a special camera that detects radioactivity is used to show where the tumors are in the body. This procedure is also called octreotide scan and SRS.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of pheochromocytoma and paraganglioma in children may include the following:

Surgery to completely remove the tumor.
Combination chemotherapy, high-dose 131I-MIBG, and targeted therapy for tumors that have spread.

Before surgery, drug therapy with alpha-blockers to control blood pressure and beta-blockers to control heart rate are given. If both adrenal glands are removed, life-long hormone therapy to replace hormones made by the adrenal glands is needed after surgery.

Treatment of recurrent pheochromocytoma and paraganglioma in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

Skin Cancer (Melanoma, Squamous Cell Cancer, Basal Cell Cancer)

Skin cancer is a disease in which malignant (cancer) cells form in the tissues of the skin. The skin is the body’s largest organ. It protects against heat, sunlight, injury, and infection. Skin also helps control body temperature and stores water, fat, and vitamin D. The skin has several layers, but the two main layers are the epidermis (upper or outer layer) and the dermis (lower or inner layer). Skin cancer begins in the epidermis, which is made up of three kinds of cells:

Melanocytes: Found in the lower part of the epidermis, these cells make melanin, the pigment that gives skin its natural color. When skin is exposed to the sun, melanocytes make more pigment and cause the skin to darken.
Squamous cells: Thin, flat cells that form the top layer of the epidermis.
Basal cells: Round cells under the squamous cells.

Anatomy of the skin with melanocytes; drawing shows normal skin anatomy, including the epidermis, dermis, hair follicles, sweat glands, hair shafts, veins, arteries, fatty tissue, nerves, lymph vessels, oil glands, and subcutaneous tissue. The pullout shows a close-up of the squamous cell and basal cell layers of the epidermis above the dermis with blood vessels. Melanin is shown in the cells. A melanocyte is shown in the layer of basal cells at the deepest part of the epidermis. — Anatomy of the skin, showing the epidermis, dermis, and subcutaneous tissue. Melanocytes are in the layer of basal cells at the deepest part of the epidermis.

There are three types of skin cancer:

Melanoma

Even though melanoma is rare, it is the most common skin cancer in children. It occurs more often in adolescents aged 15 to 19 years.

The risk of having melanoma is increased by having the following conditions:

Giant melanocytic nevi (large black spots, which may cover the trunk and thigh).
Xeroderma pigmentosum.
Multiple endocrine neoplasia type I (MEN1) syndrome (Werner syndrome).
Hereditary retinoblastoma.
Having a weakened immune system.

Other risk factors for melanoma in all age groups include:

Having a fair complexion, which includes the following:
- Fair skin that freckles and burns easily, does not tan, or tans poorly.
- Blue or green or other light-colored eyes.
- Red or blond hair.
Being exposed to natural sunlight or artificial sunlight (such as from tanning beds) over long periods of time.
Having several large or many small moles.
Having a family history or personal history of unusual moles (atypical nevus syndrome).
Having a family history of melanoma.

Signs and symptoms of melanoma include the following:

A mole that:
- changes in size, shape, or color.
- has irregular edges or borders.
- is more than one color.
- is asymmetrical (if the mole is divided in half, the 2 halves are different in size or shape).
- itches.
- oozes, bleeds, or is ulcerated (a hole forms in the skin when the top layer of cells breaks down and the tissue below shows through).
Change in pigmented (colored) skin.
Satellite moles (new moles that grow near an existing mole).

Tests to diagnose and stage melanoma may include the following:

Physical exam and history.
X-ray of the chest.
CT scan.
MRI.
PET scan.

See the General Information section for a description of these tests and procedures.

Other tests and procedures used to diagnose melanoma include the following:

Skin exam: A doctor or nurse checks the skin for bumps or spots that look abnormal in color, size, shape, or texture.
Biopsy : All or part of the abnormal-looking growth is cut from the skin and viewed under a microscope by a pathologist to check for cancer cells. There are four main types of skin biopsies:
- Shave biopsy : A sterile razor blade is used to “shave off” the abnormal-looking growth.
- Punch biopsy : A special instrument called a punch or a trephine is used to remove a circle of tissue from the abnormal-looking growth.
- Excisional biopsy : A scalpel is used to remove the entire growth.
- Wide local excision : A scalpel is used to remove the growth and some of the normal tissue around the area, to check for cancer cells. Skin grafting may be needed to cover the area where tissue was removed.
Sentinel lymph node biopsy : The removal of the sentinel lymph node during surgery. The sentinel lymph node is the first lymph node to receive lymphatic drainage from a tumor. It is the first lymph node the cancer is likely to spread to from the tumor. A radioactive substance and/or blue dye is injected near the tumor. The substance or dye flows through the lymph ducts to the lymph nodes. The first lymph node to receive the substance or dye is removed. A pathologist views the tissue under a microscope to look for cancer cells. If cancer cells are not found, it may not be necessary to remove more lymph nodes.
Lymph node dissection : A surgical procedure in which lymph nodes are removed and a sample of tissue is checked under a microscope for signs of cancer. For a regional lymph node dissection, some of the lymph nodes in the tumor area are removed. For a radical lymph node dissection, most or all of the lymph nodes in the tumor area are removed. This procedure is also called a lymphadenectomy.

Treatment of Melanoma

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of melanoma is surgery to remove the tumor and some tissue around the tumor.

If cancer has spread to nearby lymph nodes, treatment is surgery to remove the lymph nodes with cancer. Immunotherapy with high-dose interferon or ipilimumab may also be given.

Treatment of melanoma that has spread beyond the lymph nodes may include the following:

Immunotherapy (ipilimumab).
A clinical trial of a new targeted therapy drug.

Treatment of recurrent melanoma in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.
A clinical trial of a new targeted therapy or immunotherapy drug.

See the PDQ summary on adult Melanoma Treatment for more information.

Squamous Cell and Basal Cell Skin Cancer

Nonmelanoma skin cancers (squamous cell and basal cell cancers) are very rare in children and adolescents. The risk of squamous cell or basal cell cancer is increased by the following:

Being exposed to natural sunlight or artificial sunlight (such as from tanning beds) over long periods of time.
Having a fair complexion, which includes the following:
- Fair skin that freckles and burns easily, does not tan, or tans poorly.
- Blue or green or other light-colored eyes.
- Red or blond hair.
Having actinic keratosis.
Past treatment with radiation.
Having a weakened immune system.

Signs of squamous cell and basal cell skin cancer include the following:

A sore that does not heal.
Areas of the skin that are:
- Small, raised, smooth, shiny, and waxy.
- Small, raised, and red or reddish-brown.
- Flat, rough, red or brown, and scaly.
- Scaly, bleeding, or crusty.
- Similar to a scar and firm.

Tests to diagnose squamous cell and basal cell skin cancer include the following:

Skin exam: A doctor or nurse checks the skin for bumps or spots that look abnormal in color, size, shape, or texture.
Biopsy: All or part of a growth that doesn't look normal is cut from the skin and viewed under a microscope by a pathologist to check for signs of cancer. There are three main types of skin biopsies:
- Shave biopsy: A sterile razor blade is used to “shave off” the growth that does not look normal.
- Punch biopsy: A special instrument called a punch or a trephine is used to remove a circle of tissue from the growth that does not look normal.
- Excisional biopsy: A scalpel is used to remove the entire growth.

Treatment of Squamous Cell and Basal Cell Skin Cancer

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of squamous cell and basal cell cancer in children may include the following:

Surgery to remove the tumor. This may include Mohs micrographic surgery.
Mohs micrographic surgery is a type of surgery used for skin cancers. The tumor is cut from the skin in thin layers. During surgery, the edges of the tumor and each layer of tumor removed are viewed through a microscope to check for cancer cells. Layers continue to be removed until no more cancer cells are seen. This type of surgery removes as little normal tissue as possible and is often used to remove skin cancer on the face.

Treatment of recurrent squamous cell and basal cell cancer in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

See the PDQ summary on adult Skin Cancer Treatment for more information.

Intraocular (Uveal) Melanoma

Intraocular melanoma begins in the middle of three layers of the wall of the eye. The outer layer includes the white sclera (the "white of the eye") and the clear cornea at the front of the eye. The inner layer has a lining of nerve tissue, called the retina, which senses light and sends images along the optic nerve to the brain. The middle layer, where intraocular melanoma forms, is called the uvea or uveal tract, and has three main parts: the iris, the ciliary body, and the choroid.

Eye anatomy; two-panel drawing shows the outside and inside of the eye. The top panel shows outside of the eye including the eyelid, pupil, sclera, and iris; the bottom panel shows inside of the eye including the cornea, lens, ciliary body, retina, choroid, optic nerve, and vitreous humor. — Anatomy of the eye, showing the outside and inside of the eye including the sclera, cornea, iris, ciliary body, choroid, retina, vitreous humor, and optic nerve. The vitreous humor is a liquid that fills the center of the eye.

Risk Factors

The risk of intraocular melanoma is increased by any of the following:

Light eye color.
Fair skin color.
Not being able to tan.
Oculodermal melanocytosis.
Presence of cutaneous nevi.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of intraocular melanoma in children is similar to treatment for adults and may include the following:

Surgery to remove the tumor.
Laser surgery.
Radiation therapy.

Treatment of recurrent intraocular melanoma in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

See the PDQ summary on adult Intraocular (Uveal) Melanoma Treatment for more information.

Chordoma

Chordoma is a very rare type of bone tumor that forms anywhere along the spine from the base of the skull to the tailbone. In children and adolescents, chordomas develop more often in the base of the skull, making them hard to remove completely with surgery.

Childhood chordoma is linked to the condition tuberous sclerosis, a genetic disorder in which tumors that are benign (not cancer) form in the kidneys, brain, eyes, heart, lungs, and skin.

Signs and Symptoms

Chordoma may cause any of the following signs and symptoms. Check with your child’s doctor if your child has any of the following:

Headache.
Neck or back pain.
Double vision.
Paralysis of the muscles in the face.
Numbness, tingling, or weakness of the arms and legs.
A change in bowel or bladder habits.

Other conditions that are not chordoma may cause these same signs and symptoms.

Chordomas may recur (come back), usually in the same place, but sometimes they recur in other areas of bone or in the lungs.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment of chordoma in children may include the following:

Surgery to remove as much of the tumor as possible, followed by radiation therapy. Proton beam radiation therapy may be used.

Treatment of recurrent chordoma in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change. Patients with changes in the SMARCB1 gene may be treated with tazemetostat in this clinical trial.

Cancer of Unknown Primary Site

Carcinoma of unknown primary is a rare disease in which malignant (cancer) cells are found in the body but the place the cancer began is not known. Cancer can form in any tissue of the body. The primary cancer (the cancer that first formed) can spread to other parts of the body. This process is called metastasis. Cancer cells usually look like the cells in the type of tissue in which the cancer began. For example, breast cancer cells may spread to the lung. Because the cancer began in the breast, the cancer cells in the lung look like breast cancer cells.

Sometimes doctors find where the cancer has spread but cannot find where in the body the cancer first began to grow. This type of cancer is called a cancer of unknown primary or occult primary tumor.

Carcinoma of unknown primary; drawing shows a primary tumor that has spread from an unknown site to other parts of the body (the lung and the brain). An inset shows cancer cells spreading from the primary cancer, through the blood and lymph systems, to another part of the body where a metastatic tumor has formed. — In carcinoma of unknown primary, cancer cells have spread in the body but the place where the primary cancer began is unknown.

Tests are done to find where the primary cancer began and to get information about where the cancer has spread. When tests are able to find the primary cancer, the cancer is no longer a cancer of unknown primary and treatment is based on the type of primary cancer.

Because the place where the cancer started is not known, many different tests and procedures may be needed to find out what type of cancer it is. If tests show there may be cancer, a biopsy is done. A biopsy is the removal of cells or tissues so they can be viewed under a microscope by a pathologist. The pathologist views the tissue to look for cancer cells and to find out the type of cancer. The type of biopsy that is done depends on the part of the body being tested for cancer. One of the following types of biopsies may be used:

Fine-needle aspiration (FNA) biopsy : The removal tissue or fluid using a thin needle.
Core biopsy : The removal of tissue using a wide needle.
Incisional biopsy : The removal of part of a lump or a sample of tissue.
Excisional biopsy : The removal of an entire lump of tissue.

When the type of cancer cells or tissue removed is different from the type of cancer cells expected to be found, a diagnosis of cancer of unknown primary may be made. The cells in the body have a certain look that depends on the type of tissue they come from. For example, a sample of cancer tissue taken from the breast is expected to be made up of breast cells. However, if the sample of tissue is a different type of cell (not made up of breast cells), it is likely that the cells have spread to the breast from another part of the body.

Adenocarcinomas, melanomas, and embryonal tumors are common tumor types that appear and it is not known where the cancer first formed. Embryonal tumors such as rhabdomyosarcomas and neuroblastomas are most common in children.

Treatment

For information about the treatments listed below, see the Treatment Option Overviewsection.

Treatment depends on what the cancer cells look like under a microscope, the patient's age, signs and symptoms, and where the cancer has spread in the body. Treatment is usually the following:

Treatment of recurrent cancer of unknown primary in children may include the following:

A clinical trial that checks a sample of the patient's tumor for certain gene changes. The type of targeted therapy that will be given to the patient depends on the type of gene change.

See the PDQ summary on adult Carcinoma of Unknown Primary for more information.

To Learn More About Childhood Cancer

For more information from the National Cancer Institute about unusual cancers of childhood, see the following:

For more childhood cancer information and other general cancer resources, see the following:

About This PDQ Summary

About PDQ

Physician Data Query (PDQ) is the National Cancer Institute's (NCI's) comprehensive cancer information database. The PDQ database contains summaries of the latest published information on cancer prevention, detection, genetics, treatment, supportive care, and complementary and alternative medicine. Most summaries come in two versions. The health professional versions have detailed information written in technical language. The patient versions are written in easy-to-understand, nontechnical language. Both versions have cancer information that is accurate and up to date and most versions are also available in Spanish.

PDQ is a service of the NCI. The NCI is part of the National Institutes of Health (NIH). NIH is the federal government’s center of biomedical research. The PDQ summaries are based on an independent review of the medical literature. They are not policy statements of the NCI or the NIH.

Purpose of This Summary

This PDQ cancer information summary has current information about the treatment of unusual cancers of childhood. It is meant to inform and help patients, families, and caregivers. It does not give formal guidelines or recommendations for making decisions about health care.

Reviewers and Updates

Editorial Boards write the PDQ cancer information summaries and keep them up to date. These Boards are made up of experts in cancer treatment and other specialties related to cancer. The summaries are reviewed regularly and changes are made when there is new information. The date on each summary ("Updated") is the date of the most recent change.

The information in this patient summary was taken from the health professional version, which is reviewed regularly and updated as needed, by the PDQ Pediatric Treatment Editorial Board.

Clinical Trial Information

A clinical trial is a study to answer a scientific question, such as whether one treatment is better than another. Trials are based on past studies and what has been learned in the laboratory. Each trial answers certain scientific questions in order to find new and better ways to help cancer patients. During treatment clinical trials, information is collected about the effects of a new treatment and how well it works. If a clinical trial shows that a new treatment is better than one currently being used, the new treatment may become "standard." Patients may want to think about taking part in a clinical trial. Some clinical trials are open only to patients who have not started treatment.

Clinical trials can be found online at NCI's website. For more information, call the Cancer Information Service (CIS), NCI's contact center, at 1-800-4-CANCER (1-800-422-6237).

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The best way to cite this PDQ summary is:

PDQ® Pediatric Treatment Editorial Board. PDQ Unusual Cancers of Childhood Treatment. Bethesda, MD: National Cancer Institute. Updated <MM/DD/YYYY>. Available at: https://www.cancer.gov/types/childhood-cancers/patient/unusual-cancers-childhood-pdq. Accessed <MM/DD/YYYY>. [PMID: 26389276]

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