| Literature DB >> 18971934 |
I S D Roberts1, D Besarani, P Mason, G Turner, P J Friend, R Newton.
Abstract
Renal transplant recipients are at increased risk of bladder carcinoma. The aetiology is unknown but a polyoma virus (PV), BK virus (BKV), may play a role; urinary reactivation of this virus is common post-renal transplantation and PV large T-antigen (T-Ag) has transforming activity. In this study, we investigate the potential role of BKV in post-transplant urothelial carcinoma by immunostaining tumour tissue for PV T-Ag. There was no positivity for PV T-Ag in urothelial carcinomas from 20 non-transplant patients. Since 1990, 10 transplant recipients in our unit have developed urothelial carcinoma, and tumour tissue was available in eight recipients. Two patients were transplanted since the first case of PV nephropathy (PVN) was diagnosed in our unit in 2000 and both showed PV reactivation post-transplantation. In one of these patients, there was strong nuclear staining for PV T-Ag in tumour cells, with no staining of non-neoplastic urothelium. We conclude that PV infection is not associated with urothelial carcinoma in non-transplant patients, and is uncommon in transplant-associated tumours. Its presence in all tumour cells in one patient transplanted in the PVN era might suggest a possible role in tumorigenesis in that case.Entities:
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Year: 2008 PMID: 18971934 PMCID: PMC2579688 DOI: 10.1038/sj.bjc.6604711
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Patients with post-renal transplant urothelial carcinoma (UC) of the bladder
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| 1 | F/75 years | 1990 | 129 | Low grade/Ta | Negative |
| 2 | M/53 years | 1990 | 38 | High grade/T1 | Negative |
| 3 | F/69 years | 1992 | 121 | High grade/T2 | Negative |
| 4 | F/41 years | 1993 | 147 | High grade/T2 | Negative |
| 5 | F/56 years | 1995 | 68 | High grade/T2 | Negative |
| 6 | M/61 years | 1996 | 129 | High grade/T3 | Negative |
| 7 | F/40 years | 2001 | 54 | High grade/T3 | Positive |
| 8 | F/65 years | 2004 | 33 | High grade/Tis | Negative |
Figure 1Tumour tissue from patient 7, showing high-grade invasive urothelial carcinoma (A), with focal squamous differentiation (B). High power (C) reveals no evidence of typical viral inclusions on H&E stain. Immunohistochemistry for PV T-Ag is negative in non-neoplastic urothelium adjacent to the tumour (D), but shows intense nuclear staining in almost all tumour cells (E and F).
Figure 2Renal biopsy 2 years post-transplantation from patient 7, showing a minor non-specific inflammatory cell infiltrate on H&E (A). Immunohistochemistry for PV T-Ag (B) shows staining of tubular epithelial cell nuclei, confirming a diagnosis of PVN.
Figure 3Urine cytology in patient 8 initially suggested BKV infection (A) but a sample 3 months later was more in keeping with urothelial carcinoma (B), confirmed as carcinoma in situ on biopsy (C).