Detailed mapping and loss of heterozygosity analysis suggests a suppressor locus involved in sporadic breast cancer within a distal region of chromosome band 17p13.3

Stack, Maria; Jones, David J.; White, Gavin R M; Liscia, Daniel S.; Venesio, Tiziana; Casey, Graham; Crichton, David; Varley, Jenny; Mitchell, Erika L D; Heighway, Jim; Santibanez‐Koref, Mauro

doi:10.1093/hmg/4.11.2047

Cited by 48 publications

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“…British Journal of Cancer (1998) 77(5) YNZ22 allelic imbalance reported in this study (52%) lies within the range (37-65%) previously published by other groups (Chen et al, 1991;Singh et al, 1993;Thorlacius et al, 1993;Comelis et al, 1994;Harada et al, 1994;Ito et al, 1995;Stack et al, 1995). The proportion of cancers with p53 mutation (20%), p53 allele loss (41%), p53 mRNA expression (54%) and overexpression (28%) or p53 protein expression (32%) are similar to the reported series (Cattoretti et al, 1988;Davidoff, 1991;Iwaya, 1991;Kovach et al, 1991;Osborne et al, 1991;Runnebaum et al, 1991;Varley et al, 1991;Vojtesek et al, 1992;Andersen et al, 1993;Barnes, 1993;Friedrichs, 1993;Martinazzi, 1993;Thorlacius et al, 1993;Tsuda et al, 1993;Marks et al, 1994;Bergh et al, 1995;Borressen et al, 1995;Stenmark-Askmalm et al, 1995).…”

Section: Discussionsupporting

confidence: 86%

“…Given that YNZ allele imbalance is more common than p53 mutation in breast cancer, the independence of YNZ22 allele imbalance from any p53 changes suggests that the greater discriminatory power of the YNZ22 locus as a marker for disease behaviour is not simply due to chance. Emerging mapping data for 17pl3.3 (Stack et al, 1995;White et al, 1996) have suggested two regions: YNZ22 and a more telomeric region (defined by markers D17S926, D17S695, D17S849) may be of interest in human breast cancer. Alongside the HIC-1 (hypermethylated in cancer), ABR and CRK genes (Heisterkamp et al, 1989;Morris et al, 1995;Wales et al, 1995) in this region, 17pl3.3 may carry a gene or genes of both scientific interest and clinical importance in breast cancer.…”

Section: Discussionmentioning

confidence: 99%

“…Up to two-thirds of tumours may show allelic imbalance at the YNZ22 locus at 17pl3.3 (Mackay et al, 1988;Devilee et al, 1989;Thompson et al, 1990;Chen et al, 1991;Singh et al, 1993;Thorlacius et al, 1993;Cornelis et al, 1994;Harada et al, 1994;Stack et al, 1995) and this finding has been associated with markers of tumour aggression Chen et al, 1991;Merlo et al, 1992;Harada et al, 1994;Ito et al, 1995).…”

mentioning

confidence: 99%

“…Although molecular lesions at p53 and at YNZ22 loci occur independently (Coles et al, 1990), it is not clear to what extent allelic imbalance on chromosome 17p telomeric to the p53 locus may reflect direct or indirect involvement of p53 itself. However, there is increasingly strong evidence for potential tumoursuppressor genes telomeric to p53 (Chen et al, 1991;Thorlacius et al, 1993;Comelis et al, 1994;Harada et al, 1994;Nagai et al, 1995;Stack et al, 1995;Wales et al, 1995;White et al, 1996). To test the hypothesis that allelic imbalance at YNZ22 is an independent predictor of poor prognosis in breast cancer and to examine the associations between YNZ22 allelic imbalance and abnormalities of p53, this study examined YNZ22 allelic imbalance, p53 mutation status, p53 allelic imbalance, p53 mRNA expression, p53 immunostaining and clinical outcome with medium-term follow-up.…”

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confidence: 99%

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Allelic imbalance at chromosome 17p13.3 (YNZ22) in breast cancer is independent of p53 mutation or p53 overexpression and is associated with poor prognosis at medium-term follow-up

Thompson

Crichton²,

Elton³

et al. 1998

Br J Cancer

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Summary Molecular and immunohistochemical studies of genetic events on chromosome 17p were prospectively compared with conventional clinical and pathological parameters and disease behaviour at a minimum of 72 months follow-up. In a series of 91 patients with primary operable breast cancer, 37 out of 91 (41 %) patients had disease relapse and 23 out of 91 (25%) had died during the follow-up period. Allelic imbalance at the YNZ22 locus (1 7p1 3.3), demonstrated in 33 out of 63 (52%) informative patients, was significantly associated with disease recurrence (P < 0.01, 2 d.f. Cox analysis) and showed a trend towards impaired survival (P = 0.08, 2 d.f. Cox analysis) after a mean follow-up of 84 months for survivors. By contrast, p53 mutation (in 10 out of 60, 17% of cancers), p53 allelic imbalance (in 23 out of 56, 41% informative patients), p53 mRNA expression (in 47 out of 87, 54% patients), p53 mRNA overexpression (in 24 out of 87, 28%) or p53 protein expression (detected in 25/76, 32%) were not associated with disease behaviour. There was no significant association between allelic imbalance at YNZ22 and any abnormality of p53 DNA, RNA or protein. Allelic imbalance at 17p13.3 (YNZ22) serves as a marker of poor prognosis in breast cancer. As yet unidentified genes on 17p13.3, distinct from and telomeric to p53, are therefore likely to be of clinical importance in breast cancer.

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Section: Discussionsupporting

confidence: 86%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Allelic imbalance at chromosome 17p13.3 (YNZ22) in breast cancer is independent of p53 mutation or p53 overexpression and is associated with poor prognosis at medium-term follow-up

Thompson

Crichton²,

Elton³

et al. 1998

Br J Cancer

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“…However, LOH studies in breast cancer have suggested the presence of another tumoursuppressor gene mapped to chromosomal region 17pl3.3 (Coles et al, 1990;Cornelis et al, 1994;Merlo et al, 1994). Our recent work revealed a complex pattern of LOH in this region in breast tumours (Stack et al, 1995). The highest loss (60-70%), and therefore perhaps the most likely site of the putative suppressor gene, was defined by the three most distal 17p markers, D17S926, D17S695 and D17S849, which were mapped and ordered by fluorescence in situ hybridisation (FISH) to a position near the telomere (for physical map of markers, see Stack et al, 1995).…”

mentioning

confidence: 57%

High levels of loss at the 17p telomere suggest the close proximity of a tumour suppressor

White

Stack²,

Santibanez‐Koref³

et al. 1996

Br J Cancer

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Fine mapping of an apparently targeted latent human herpesvirus type 6 integration site in chromosome band 17p13.3

et al. 1999

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An unusually high level of latent HHV-6 infection has been documented in the peripheral blood and/or bone marrow cells of a small group of patients with predominantly malignant lymphoid disorders, and in at least one healthy individual. We have shown previously in peripheral blood mononuclear cells (PBMCs) of three patients, two with a history of lymphoma and one with multiple sclerosis, a specific target site for latent integration of the full-length HHV-6 viral genome on the distal short arm of chromosome 17, in band p13.3. Fluorescence in situ hybridization (FISH) procedures were used to map more precisely the location of the viral integration site in one of those patients, relative to two known oncogenes mapped previously, namely CRK, and the more telomeric ABR oncogene. It is shown that the HHV-6 integration site is located at least 1,000 kb telomeric of ABR, and is very likely to map close to or within the telomeric sequences of 17p. This finding is significant given that human telomeric-like repeats flank the terminal ends of the HHV-6 genome. Cytogenetic studies showed evidence of karyotype instability in the peripheral blood cells infected latently.

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Detailed mapping and loss of heterozygosity analysis suggests a suppressor locus involved in sporadic breast cancer within a distal region of chromosome band 17p13.3

Cited by 48 publications

References 0 publications

Allelic imbalance at chromosome 17p13.3 (YNZ22) in breast cancer is independent of p53 mutation or p53 overexpression and is associated with poor prognosis at medium-term follow-up

Allelic imbalance at chromosome 17p13.3 (YNZ22) in breast cancer is independent of p53 mutation or p53 overexpression and is associated with poor prognosis at medium-term follow-up

High levels of loss at the 17p telomere suggest the close proximity of a tumour suppressor

Fine mapping of an apparently targeted latent human herpesvirus type 6 integration site in chromosome band 17p13.3

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