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Gene stifled in some lung, breast cancers.


Many genes encode proteins whose job is to inhibit cell growth. Some of these genes suppress the growth of tumors, and a few have become household names History
Formation (1998-2000)
Household Names have been together since 1998, with various members rotating throughout the line-up with singer, Jason Garcia, until it was solidified in the summer of 2000 with bassist/keyboardist, Chris Peters, and drummer, C. J.
, such as the BRCA BRCA  

One of two genes (designated BRCA1 and BRCA2) that help repair damage to DNA, but when inherited in a defective state increase the risk of breast and ovarian cancer.
1 gene, which inhibits breast cancer.

A gene called RASSF1A could become the next member of this rarefied rar·e·fied also rar·i·fied  
adj.
1. Belonging to or reserved for a small select group; esoteric.

2. Elevated in character or style; lofty.


rarefied
Adjective

1.
 club. A study in the May 2 JOURNAL OF THE NATIONAL CANCER INSTITUTE establishes that many lung and breast tumors lack a functional RASSF1A. The findings suggest that the protein encoded by RASSF1A helps choke off malignancies and could lead to new cancer therapies. Indeed, the scientists found that restoring RASSF1A function to implanted human cancer cells cells once believed to be peculiar to cancers, but now know to be epithelial cells differing in no respect from those found elsewhere in the body, and distinguished only by peculiarity of location and grouping.

See also: Cancer
 prevented them from developing into tumors in mice.

The precise role of the RASSF1A protein is unclear. Nevertheless, the protein may hold one of the molecular keys to disrupting runaway cell growth in cancer, says study coauthor John D. Minna of the University of Texas, Southwestern, in Dallas

For cancer to grow, several tumor-suppressor genes may need to be turned off in unison, says coauthor Adi F. Gazdar, also of Southwestern. "You might reverse the malignancy by correcting just one of these defects," he says.

The researchers used tumor cells surgically removed from lung and breast cancer patients to create cell lines that they could grow in the laboratory. RASSF1A was silenced in 32 of 32 cell lines grown from small-cell lung cancer lung cancer, cancer that originates in the tissues of the lungs. Lung cancer is the leading cause of cancer death in the United States in both men and women. Like other cancers, lung cancer occurs after repeated insults to the genetic material of the cell.  patients, in 17 of 26 nonsmall-cell lung cancer lines, and in 15 of 25 breast cancer cell lines.

Since their earlier work suggested that RASSF1A hadn't been mutated in cancerous cells, the researchers looked for a chemical modification of the gene. They found clusters of atoms, known as methyl groups, clinging to DNA DNA: see nucleic acid.
DNA
 or deoxyribonucleic acid

One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes.
 in RASSF1A. This methylation methylation,
n a phase-II detoxification pathway in the liver; methyl groups combine with toxins to rid the body of various substances.

methylation
(meth´
 occurs normally on some parts of chromosomes, but it doesn't show up in RASSF1A of normal tissues.

Nearly all small-cell lung cancer cells and about half of the breast cancer cells that Minna's group tested had aberrant methylation. Attaching to the RASSF1A promoter, the gene's on switch, these methyl groups turned off the gene.

An analysis of a separate sample of 107 nonsmall-cell lung cancer patients showed that 32 had methylated meth·yl·ate  
n.
An organic compound in which the hydrogen of the hydroxyl group of methyl alcohol is replaced by a metal.

tr.v. meth·yl·at·ed, meth·yl·at·ing, meth·yl·ates
1.
 promoter regions on RASSF1A in their tumor cells. The researchers checked hospital records of these patients and found that those without the aberrant methylation survived, on average, 49 months from the date of diagnosis, whereas those with a methylated RASSF1A promoter region survived only an average of 28 months.

In their mouse experiments, the researchers tested immune-deficient animals. The researchers injected one group of mice with lung cancer cells that lacked RASSF1A and another group with the same kind of cells containing added, functional RASSF1A. Whereas the first group of mice grew tumors, the others remained free of cancer.

Minna says, "The findings represent an early diagnostic tool for lung and breast cancer and will also lead to new therapy trials using drugs that block methylation in patients."

"This work was very nicely done," says James G. Herman, a medical oncologist medical oncologist  Oncology An oncologist who diagnoses and treats cancer with chemotherapy, hormones, biologicals, or immunologic agents; the MO becomes a cancer Pt's de facto primary care giver, and coordinates treatment provided by other specialists.  at Johns Hopkins University Johns Hopkins University, mainly at Baltimore, Md. Johns Hopkins in 1867 had a group of his associates incorporated as the trustees of a university and a hospital, endowing each with $3.5 million. Daniel C.  Medical Institutions in Baltimore. As scientists improve their understanding of the human genome, they'll encounter more genes that are switched on or off in cancer, he says.

Researchers investigating potential tumor suppressors will need to determine whether the proteins encoded by those genes play critical roles in the genesis of cancer or are simply signposts of the disease, says Herman. Putting such genes into human cancer cells and gauging whether they can stop cancer--as Gazdar and his colleagues did in mice--"is an important step," Herman says.
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Article Details
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Author:Seppa, N.
Publication:Science News
Article Type:Brief Article
Geographic Code:1USA
Date:May 12, 2001
Words:588
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