Molecular mapping of deletion sites in the short arm of chromosome 3 in human lung cancer
Corresponding Author
Dr. Hiltrud Brauch
Laboratory of Immunobiology, National Cancer Institute, Frederick Cancer Research Facility, Frederick, Maryland
Cellular Immunity Section, Laboratory of Immunobiology, Bldg. 560, Rm. 12–34, National Cancer Institute, Frederick Cancer Research Facility, Frederick, MD 21701Search for more papers by this authorKalman Tory
Laboratory of Immunobiology, National Cancer Institute, Frederick Cancer Research Facility, Frederick, Maryland
Search for more papers by this authorFrederick Kotler
Laboratory of Immunobiology, National Cancer Institute, Frederick Cancer Research Facility, Frederick, Maryland
Search for more papers by this authorAdi F. Gazdar
NCI, Navy Medical Oncology Branch, Naval Hospital, Bethesda, Maryland
Search for more papers by this authorOlive S. Pettengill
Department of Pathology, Dartmouth Medical School, Hanover, New Hampshire
Search for more papers by this authorBruce Johnson
NCI, Navy Medical Oncology Branch, Naval Hospital, Bethesda, Maryland
Search for more papers by this authorStephen Graziano
Department of Medicine, SUNY Health Science Center and Veterans Administration Medical Center, Syracuse, New York
Search for more papers by this authorTim Winton
NCI, Navy Medical Oncology Branch, Naval Hospital, Bethesda, Maryland
Search for more papers by this authorCharles H. C. M. Buys
Department of Human Genetics, State University of Groningen, Groningen, The Netherlands
Search for more papers by this authorGeorge D. Sorenson
Department of Pathology, Dartmouth Medical School, Hanover, New Hampshire
Search for more papers by this authorBernard J. Poiesz
Department of Medicine, SUNY Health Science Center and Veterans Administration Medical Center, Syracuse, New York
Search for more papers by this authorJohn D. Minna
NCI, Navy Medical Oncology Branch, Naval Hospital, Bethesda, Maryland
Search for more papers by this authorBerton Zbar
Laboratory of Immunobiology, National Cancer Institute, Frederick Cancer Research Facility, Frederick, Maryland
Search for more papers by this authorCorresponding Author
Dr. Hiltrud Brauch
Laboratory of Immunobiology, National Cancer Institute, Frederick Cancer Research Facility, Frederick, Maryland
Cellular Immunity Section, Laboratory of Immunobiology, Bldg. 560, Rm. 12–34, National Cancer Institute, Frederick Cancer Research Facility, Frederick, MD 21701Search for more papers by this authorKalman Tory
Laboratory of Immunobiology, National Cancer Institute, Frederick Cancer Research Facility, Frederick, Maryland
Search for more papers by this authorFrederick Kotler
Laboratory of Immunobiology, National Cancer Institute, Frederick Cancer Research Facility, Frederick, Maryland
Search for more papers by this authorAdi F. Gazdar
NCI, Navy Medical Oncology Branch, Naval Hospital, Bethesda, Maryland
Search for more papers by this authorOlive S. Pettengill
Department of Pathology, Dartmouth Medical School, Hanover, New Hampshire
Search for more papers by this authorBruce Johnson
NCI, Navy Medical Oncology Branch, Naval Hospital, Bethesda, Maryland
Search for more papers by this authorStephen Graziano
Department of Medicine, SUNY Health Science Center and Veterans Administration Medical Center, Syracuse, New York
Search for more papers by this authorTim Winton
NCI, Navy Medical Oncology Branch, Naval Hospital, Bethesda, Maryland
Search for more papers by this authorCharles H. C. M. Buys
Department of Human Genetics, State University of Groningen, Groningen, The Netherlands
Search for more papers by this authorGeorge D. Sorenson
Department of Pathology, Dartmouth Medical School, Hanover, New Hampshire
Search for more papers by this authorBernard J. Poiesz
Department of Medicine, SUNY Health Science Center and Veterans Administration Medical Center, Syracuse, New York
Search for more papers by this authorJohn D. Minna
NCI, Navy Medical Oncology Branch, Naval Hospital, Bethesda, Maryland
Search for more papers by this authorBerton Zbar
Laboratory of Immunobiology, National Cancer Institute, Frederick Cancer Research Facility, Frederick, Maryland
Search for more papers by this authorAbstract
We used 10 restriction fragment length polymorphism (RFLP) probes spanning the length of the short arm of chromosome 3 (3p) to map deletion sites in human lung cancer. Two approaches were used. 1) When a patient's tumor and normal tissue were available, loci with allelic heterozygosity in the normal tissue were tested for loss of alleles at 3p. 2) When the corresponding normal tissue was not available, the frequency of heterozygosity at each locus in a panel of tumors was compared to the corresponding published frequencies in nontumor tissue of healthy individuals or patients with lung cancer. In 14 small cell lung carcinomas (SCLC) with normal DNA for comparison, allele loss was found at all heterozygous loci, with one exception at a locus near the 3p centromere (D3S4). In the total of 53 SCLCs, which included tumors without paired normal tissue, frequency of heterozygosity was significantly reduced in all 10 3p loci. Three loci, DNF15S2, RAF1, and D3S18, were homozygous in all tumors in the SCLC panel. These loci, which are in regions 3p21 and 3p25, may thus be involved in the origin or evolution of SCLC. We also investigated 24 non-SCLC tumors. In this panel, frequency of heterozygosity was significantly reduced at seven of the 10 loci tested. Comparison of the results shows that the pattern of allele loss on 3p is different in SCLC and non-SCLC, suggesting a difference in pathogenesis at the genetic level.
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