TY - JOUR
T1 - MMAC1/PTEN mutations in primary tumor specimens and tumor cell lines
AU - Teng, David H.F.
AU - Hu, Rong
AU - Lin, Huai
AU - Davis, Thaylon
AU - Iliev, Diana
AU - Frye, Cheryl
AU - Swedlund, Brad
AU - Hansen, Kipp L.
AU - Vinson, Vickie L.
AU - Gumpper, Kathryn L.
AU - Ellis, Lee
AU - El-Naggar, Adel
AU - Frazier, Marsha
AU - Jasser, Samar
AU - Langford, Lauren A.
AU - Lee, Jeff
AU - Mills, Gordon B.
AU - Pershouse, Mark A.
AU - Pollack, Raphael E.
AU - Tornos, Carmen
AU - Troncoso, Patricia
AU - Yung, W. K.Alfred
AU - Fujii, Gregory
AU - Berson, Amy
AU - Bookstein, Robert
AU - Bolen, Joseph B.
AU - Tavtigian, Scan V.
AU - Steck, Peter A.
PY - 1997/12/1
Y1 - 1997/12/1
N2 - A candidate tumor suppressor gene, MMAC1/PTEN, located in human chromosome band 10q23, was recently identified based on sequence alterations observed in several glioma, breast, prostate, and kidney tumor specimens or cell lines. To further investigate the mutational profile of this gene in human cancers, we examined a large set of human tumor specimens and cancer cell lines of many types for 10q23 allelic losses and MMAC1 sequence alterations. Loss of heterozygosity (LOH) at the MMAC1 locus was observed in approximately one-half of the samples examined, consistent with the high frequency of 10q allelic loss reported for many cancers. Of 124 tumor specimens exhibiting LOH that have been screened for MMAC1 alterations to date, we have detected variants in 13 (10%) of these primary tumors; the highest frequency of variants was found in glioblastoma specimens (-23%). Novel alterations identified in this gene include a missense variant in a melanoma sample and a splicing variant and a nonsense mutation in pediatric glioblastomas. Of 76 tumor cell lines prescreened for probable LOH, microsequence alterations of MMAC1 were detected in 12 (-16%) of the lines, including these derived from astrocytoma, leukemia, and melanoma tumors, as well as bladder, breast, lung, prostate, submaxillary gland, and testis carcinomas. In addition, in this set of tumor cell lines, we detected 11 (- 145) homozygous deletions that eliminated coding portions of MMAC1, a class of abnormality not detected by our methods in primary tumors. These data support the occurrence of inactivating MMAC1 alterations in multiple human cancer types. In addition, we report the discovery of a putative pseudogene of MMAC1 localized on chromosome 9.
AB - A candidate tumor suppressor gene, MMAC1/PTEN, located in human chromosome band 10q23, was recently identified based on sequence alterations observed in several glioma, breast, prostate, and kidney tumor specimens or cell lines. To further investigate the mutational profile of this gene in human cancers, we examined a large set of human tumor specimens and cancer cell lines of many types for 10q23 allelic losses and MMAC1 sequence alterations. Loss of heterozygosity (LOH) at the MMAC1 locus was observed in approximately one-half of the samples examined, consistent with the high frequency of 10q allelic loss reported for many cancers. Of 124 tumor specimens exhibiting LOH that have been screened for MMAC1 alterations to date, we have detected variants in 13 (10%) of these primary tumors; the highest frequency of variants was found in glioblastoma specimens (-23%). Novel alterations identified in this gene include a missense variant in a melanoma sample and a splicing variant and a nonsense mutation in pediatric glioblastomas. Of 76 tumor cell lines prescreened for probable LOH, microsequence alterations of MMAC1 were detected in 12 (-16%) of the lines, including these derived from astrocytoma, leukemia, and melanoma tumors, as well as bladder, breast, lung, prostate, submaxillary gland, and testis carcinomas. In addition, in this set of tumor cell lines, we detected 11 (- 145) homozygous deletions that eliminated coding portions of MMAC1, a class of abnormality not detected by our methods in primary tumors. These data support the occurrence of inactivating MMAC1 alterations in multiple human cancer types. In addition, we report the discovery of a putative pseudogene of MMAC1 localized on chromosome 9.
UR - http://www.scopus.com/inward/record.url?scp=14444269482&partnerID=8YFLogxK
M3 - Article
C2 - 9393738
AN - SCOPUS:14444269482
SN - 0008-5472
VL - 57
SP - 5221
EP - 5225
JO - Cancer Research
JF - Cancer Research
IS - 23
ER -