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Retinoblastoma

Retinoblastoma is a cancer of the retina. It is caused by a mutation in the Rb-1 protein. It occurs mostly in younger children and accounts for about 3% of the cancers occurring in children younger than 15 years. The estimated annual incidence is approximately 4 per million children . more...

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The tumor may begin in one or both eyes. Retinoblastoma is usually confined to the eye but can spread to the brain via the optic nerve.

Causes

Retinoblastoma may be hereditary (genetically inherited) or nonhereditary. The hereditary form may be in one or both eyes, and generally affects younger children. Retinoblastoma occurring in only one eye is often not hereditary and is more prevalent in older children. When the disease occurs in both eyes, it is always hereditary. Because of the hereditary factor, patients and their brothers and sisters should have periodic examinations, including genetic counseling, to determine their risk for developing the disease.

A statistical study by Dr Alfred G. Knudson in 1971 led to a hypothesis (later known as the Knudson hypothesis) about why some retinablastomas are hereditary and others occur by chance. This hypothesis led to the first identification of a tumor suppressor gene by a team led by Dr Thaddeus P. Dryja in 1986. Knudson won the 1998 Albert Lasker Medical Research Award for this work.

Hereditary retinoblastoma is caused by an inherited mutation in a single copy of the Rb1 gene. The remaining functional copy prevents most retinal cells from becoming cancerous. However, one or more cells in the retina are likely to undergo a spontaneous loss of this functional copy, causing those cells to transform into cancer. This loss of the second copy of Rb1 is termed loss of heterozygosity, a frequent event in cancer for which retinoblastoma is the canonical example.

Treatment

The patient's choice of treatment depends on the extent of the disease within and beyond the eye. Smaller tumors can be removed with laser surgery, thermo-, or cryotherapy. Larger tumors may require enucleation.

Genetic testing can identify the mutation that lead to the development of retinoblastoma. Testing in unilateral cases can identify the 15% of unilateral cases with a germline mutation, indicating risk in future children. Testing amniotic cells in an at-risk pregnancy can identify a fetus with the mutation, which can then be delivered early before retinal cells have fully developed and before tumors arise. This early treatment can lead to a fully sighted bilaterally affected patient.

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The Development Of Breast Cancer: The Role Of Changes In The Expression Of Cyclins And Retinoblastoma Proteins - Brief Article
From Life Sciences & Biotechnology Update, 5/1/00

These (University of Colorado) studies, together with work carried out in other laboratories, indicates that defects in the Rb-Cyclin D 1-p16 cell cycle regulatory system are present in the vast majority of breast cancer cells. Previous work has focused on characterizing these defects, and on determining the mechanisms responsible for causing them. Current efforts are turned toward demonstrating the contribution of these defects to the tumorigenic properties of breast cancer cells, in order to provide potential targets for therapy. In particular, work is focused on the effects of restoring the expression of the tumor suppressor p16 in breast cancer cells, using constructs in which p16 expression is under the control of the inducible Tet promoter.

After demonstrating the feasibility of this approach in breast cancer cells, in transiently transfected cells, stably transfected ceU lines are produced in order to test the effects of p16 expression on growth in soft agar, and in formation of tumors in nude mice. It is demonstrated that MCF-7 breast cancer cells, stably transformed with constructs expressing p16, are impaired or have lost the ability to grow in soft agar, indicating that defects in p16 expression may make a critical contribution to tumorigenicity. Additional controls are required to establish, unequivocally, that loss of growth of these cells in soft agar is in fact due to restoration of p16 expression.

(Order this LIFE SCIENCES & BIOTECHNOLOGY UPDATE reviewed report from InfoTeam Inc., P.O. Box 15640, Plantation, FL 33318-5640; Phone (954) 473-9560, Fax (954) 473-0544: Report No. L20000517; 1998, 24 pp. Price: $89.00, prepaid. E-mail to: InfoTeamMA@aol.com)

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