| Literature DB >> 25918706 |
Ziting Wang1, Anantharaman Vathsala2, Ho Yee Tiong3.
Abstract
Haematuria has a prevalence of 12% in the postrenal transplant patient population. It heralds potentially dangerous causes which could threaten graft loss. It is important to consider causes in light of the unique, urological, and immunological standpoints of these patients. We review the literature on common causes of haematuria in postrenal transplant patients and suggest the salient approach to the evaluation of this condition. A major cause of haematuria is urinary tract infections. There should be a higher index of suspicion for mycobacterial, fungal, and viral infection in this group of immunosuppressed patients. Measures recommended in the prevention of urinary tract infections include early removal of foreign bodies as well as prophylactic antibiotics during the early transplant phase. Another common cause of haematuria is that of malignancies, in particular, renal cell carcinomas. When surgically managing cancer in the setting of a renal transplant, one has to be mindful of the limited retropubic space and the need to protect the anastomoses. Other causes include graft rejections, recurrences of primary disease, and calculus formation. It is important to perform a comprehensive evaluation with the aid of an experienced multidisciplinary transplant team.Entities:
Mesh:
Year: 2015 PMID: 25918706 PMCID: PMC4395992 DOI: 10.1155/2015/292034
Source DB: PubMed Journal: Biomed Res Int Impact factor: 3.411
Figure 1CT findings showing a 1.3 × 1.3 cm enhancing lesion at the upper pole of right kidney.
Figure 2Resection specimen of the papillary renal cell carcinoma.
Patient demographics and treatment regime of renal transplant patients who developed bladder carcinoma.
| Comparison | Rogers et al., BJUI, UK, 2012 [ | Prabharasuth et al., J Urol, USA, 2013 [ | Moses et al., Transplant Proc, USA, 2013 [ | Master et al., J Urol, USA, 2004 [ | Manassero et al., Transplant International, Italy, 2011 [ | Kamal et al., BJU, Egypt, 2008 [ | Tomaszewski, AIU, USA, 2011 [ | Lang et al., J Urol, Germany, 2005 [ |
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| 8 | 17 | 5 | 5 | 4 | 7 | 7 | 4 |
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| Stage | pTa-T2 | pTa-T3 | pT0-T3 | pT1-T3a | pT1-T3a | pTis-T3a | pTis-T3a | pTa-T3b |
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| Mean time to development of TCC after transplant (months) | 60 | 88.1 | 83.9 | 106.8 | 102 | 112.8 | 39 | 126 |
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| Treatment | TURBT (7), RCIUD (1) | RCIUD (4), RCNB (1) TURBT (7), Chemo (3), palliative RT (1) | RCNB (5) | TURBT (1), RCIUD (1), RCNB (2) | RCNB (4) | RCNB (5), TURBT (2) | Palliative RT + IUD (1), palliative RT (1), RCIUD (2), TURBT (3) | RCNB (4) |
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| Mean follow-up (months) | 144 | 9.2 | 24.9 | 33.6 | 31.5 | 10.3 | 36.3 | 52 |
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| Recurrence rate | 2/8 | 8/16 (1 palliative RT) | 2/5 | — | 2/4 | 3/7 | 2/5 (2 palliative RT) | 1/4 |
TURBT: transurethral resection of bladder tumour; RC: radical cystectomy; IUD: incontinent urinary diversion; NB: neobladder.
Oncological outcomes of prostate cancer patients.
| Comparison | Polcari et al., J Urol, USA, 2009 [ | Antonopoulos et al., J Urol, Brazil, 2008 [ |
Kleinclauss et al., J Urol, France, 2008 [ | Mouzin et al., Transplantation, France, 2004 [ | Elkentaoui et al., J Urol, France, 2010 [ | Detti et al., JJ Clinical Onco, Italy, 2011 [ |
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| 7 | 8 | 20 | 8 | 15 | 1 |
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| Clinical stage | pT1c-T2a | pT2a-T2c | pT2a-T3b | pT1c-T3a | pT2a-T3a | pT3b |
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| Treatment | Robot-assisted radical prostatectomy | Radical prostatectomy | Radical prostatectomy | Three-dimensional conformal radiotherapy | Radical prostatectomy | Radical prostatectomy + adjuvant RT |
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| Mean operative duration (min) | 186 | 183 | 163 | — | — | — |
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| Mean blood loss (mL) | — | 656 | 516 | — | — | — |
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| Mean hospital stay (days) | 1.8 | 3 | 11.9 | — | — | — |
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| Postprocedure complications | 42.9% | 0 | 0 | 5/8 grades 1-2 cystitis | 2/15 rectal injuries | Grade 1 cystitis |
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| Mean follow-up (months) | 16 | 10.5 | 23 | 28 | 26 | — |
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| Recurrence rate | 1/7 | 0 | 2/20 | 2/8 | 1/15 | 0/1 |
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| Positive margins | 2/7 | 2/8 | 2/20 | — | 0/15 | 1/1 |