Aberrant splicing of the TSG101 and FHIT genes occurs frequently in multiple malignancies and in normal tissues and mimics alterations previously described in tumours

Sa, Gayther; Barski, Piotr; Sj, Batley; L, Li; Ka, de Foy; Sn, Cohen; Ba, Ponder; Caldas, Carlos

doi:10.1038/sj.onc.1201591

Cited by 77 publications

(87 citation statements)

References 9 publications

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“…From the perspective of tumor biology, the removal of this control point will permit the expansion of the tumor cell population. This is consistent with the observation of an increase in aberrant TSG101 transcripts in carcinoma cells when compared to normal cells (Gayther et al, 1997;Lin et al, 1998). Other proteins, such as transcription factor NF-kB and retinoblastoma, can also be regulated by ubiquitination.…”

Section: Discussionsupporting

confidence: 90%

“…Most of the TSG101 deletions detected in BL and resulting in non coding transcripts are similar to those reported in breast (Lee and Feinberg, 1997;Li et al, 1997;Steiner et al, 1997), prostate carcinomas (Sun et al, 1997), small cell lung carcinoma (Oh et al, 1998) and acute myeloid leukemia (Lin et al, 1998). These splicing aberrations can also be detected in normal cells although at a much lower frequency, suggesting there is a biological selection for them in tumor cells (Gayther et al, 1997;Oh et al, 1998). Among these, the joining of nucleotides 153 ± 1055 represents the most common and abundant aberrant transcript in all types of tumors breast (Lee and Feinberg, 1997;Li et al, 1997;Lin et al, 1998;Oh et al, 1998;Steiner et al, 1997;Sun et al, 1997).…”

Section: Discussionsupporting

confidence: 73%

“…Normal TSG101 protein can be detected with antibodies in breast carcinoma cell lines (Zhong et al, 1997). These aberrant messages are always coexpressed with a normal transcript in tumor cells (Lee and Feinberg, 1997), and they are also detectable, albeit at a much lower frequency, in normal cells (Gayther et al, 1997;Lin et al, 1998). So far there is no evidence that any of these alternatively spliced TSG101 messages can code for a protein, despite the fact that alternative splicing is a well known mechanism in the generation of variant forms of a protein in cell di erentiation and development.…”

Section: Introductionmentioning

confidence: 99%

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Expression of a new isoform of the tumor susceptibility TSG101 protein lacking a leucine zipper domain in Burkitt lymphoma cell lines

1999

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The tumor susceptibility gene, TSG101, has been identi®ed as a candidate tumor suppressor gene. We have examined the expression of TSG101 in Burkitt lymphoma cell lines. Several aberrant messages were detected in all cell lines. Aberrant splice donor sites are located within exon 1 at positions 132, 154, 172 and 284. Splice acceptors are located at positions 847 and 1054 within exon 5. The aberrant messages are coexpressed with a normal message and could be the result of additional splicing reactions of the mature message that behaves as an intermediate. The normal message codes for 46 kDa protein (TSG101A). One aberrant message joins in frame nucleotides 283 ± 1055 and codes for a protein isoform of 17 kDa (TSG101B), as demonstrated by in vitro translation assays. The TSG101B isoform lacks the leucine zipper near the C-terminus, a transcriptional repressor domain, and retains most of the N-terminal region which has homology to E2 ubiquitin regulatory enzymes and the CROC-1 transcriptional regulator. The TSG101B isoform was detected in sixteen out of twenty-two (72%) BL cell lines, but not in normal lymphoid populations. The presence of two TSG101 isoforms with di erent dimerization potential opens up a new level of regulation of the TSG101 proteins possibly a ecting cell cycle regulation.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionsupporting

confidence: 73%

Section: Introductionmentioning

confidence: 99%

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Expression of a new isoform of the tumor susceptibility TSG101 protein lacking a leucine zipper domain in Burkitt lymphoma cell lines

1999

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“…The sex-lethal autoregulatory circuit in drosophila is one such model where 5' UTR splice variants regulate gene expression (Granadino et al, 1997). Aberrant or alternative splicing of other candidate tumor suppressor genes such as FHIT and TSG101 have been reported, and generally appear to be epigenetic rather than mutations at intron-exon boundaries (Gayther et al, 1997).…”

Section: Discussionmentioning

confidence: 99%

HYAL1LUCA-1, a candidate tumor suppressor gene on chromosome 3p21.3, is inactivated in head and neck squamous cell carcinomas by aberrant splicing of pre-mRNA

et al. 2000

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The hyaluronidase ®rst isolated from human plasma, Hyal-1, is expressed in many somatic tissues. The Hyal-1 gene, HYAL1, also known as LUCA-1, maps to chromosome 3p21.3 within a candidate tumor suppressor gene locus de®ned by homozygous deletions and by functional tumor suppressor activity. Hemizygosity in this region occurs in many malignancies, including squamous cell carcinomas of the head and neck. We have investigated whether cell lines derived from such malignancies expressed Hyal-1 activity, using normal human keratinocytes as controls. Hyal-1 enzyme activity and protein were absent or markedly reduced in six of seven carcinoma cell lines examined. Comparative genomic and¯uorescence in situ hybridization identi®ed chromosomal deletions of one allele of HYAL1 in six of seven cell lines. Initial RT ± PCR analyses demonstrated marked discrepancies between levels of HYAL1 mRNA and protein. Despite repeated sequence analyses, no mutations were found. However, two species of transcripts were identi®ed when primers were used that included the 5' untranslated region. The predominant mRNA species did not correlate with protein translation and contained a retained intron. A second spliced form lacking this intron was found only in cell lines that produced Hyal-1 protein. Inactivation of HYAL1 in these tumor lines is a result of incomplete splicing of its pre-mRNA that appears to be epigenetic in nature.

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“…Whereas LOH is generally associated with decreased protein expression, protein inactivation may be due to complex mechanisms other than deletion within an allele (Tanaka et al, 1998). Alternatively, abnormal protein expression may occur in the absence of genetic alterations through altered splicing fidelity (Gayther et al, 1997). Besides, methylation of FHIT is another important mechanism for loss of Fhit expression (Zöchbauer-Müller et al, 2001).…”

Section: Discussionmentioning

confidence: 99%

Frequent allelic deletion at the FHIT locus associated with p53 overexpression in squamous cell carcinoma subtype of Taiwanese non-small-cell lung cancers

Lee

Shih

et al. 2004

Br J Cancer

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The fragile histidine triad (FHIT) gene, encompassing the FRA3B fragile site at chromosome 3p14.2, is a tumour suppressor gene involved in different tumour types including non-small-cell lung cancers (NSCLCs). In the current study, we examined for allelic deletion at the FHIT locus in 58 primary and microdissected NSCLCs, for which a clinicopathologic profile was available. We found a loss of 87.7% in heterozygosity (LOH) frequency at one or more microsatellite markers (D3S1289, D3S2408, D3S1766, D3S1312, D3S1600). Allelic deletion of D3S1766 was related to tumour histology in 10 of 11 squamous cell carcinomas (90.9%) displaying LOH compared with nine of 17 adenocarcinomas (52.9%; P ¼ 0.049). Besides, in the subset of adenocarcinomas, a higher rate of LOH at D3S1289 was observed in male (six out of eight, 75%) than in female patients (four out of 17, 23.5%; P ¼ 0.028). However, FHIT LOH was not correlated overall with a variety of clinical parameters including sex, smoking status, staging, lymph node metastasis and survival. These results indicated that the high frequency of FHIT gene disruption was important in the development of both squamous cell carcinomas and adenocarcinomas. Furthermore, there was no association between LOH at FHIT and protein expression, suggesting the presence of complex mechanisms of Fhit inactivation. On the other hand, the association between FHIT LOH and p53 protein overexpression assessment reached statistical significance (P ¼ 0.026), implying that common alterations affect the two genes in tumour progression.

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Aberrant splicing of the TSG101 and FHIT genes occurs frequently in multiple malignancies and in normal tissues and mimics alterations previously described in tumours

Cited by 77 publications

References 9 publications

Expression of a new isoform of the tumor susceptibility TSG101 protein lacking a leucine zipper domain in Burkitt lymphoma cell lines

Expression of a new isoform of the tumor susceptibility TSG101 protein lacking a leucine zipper domain in Burkitt lymphoma cell lines

HYAL1LUCA-1, a candidate tumor suppressor gene on chromosome 3p21.3, is inactivated in head and neck squamous cell carcinomas by aberrant splicing of pre-mRNA

Frequent allelic deletion at the FHIT locus associated with p53 overexpression in squamous cell carcinoma subtype of Taiwanese non-small-cell lung cancers

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