Study Type – Diagnostic (exploratory cohort)
Level of Evidence 3a
What's known on the subject? and What does the study add?
Hereditary non‐polyposis colorectal cancer (HNPCC), also known as Lynch syndrome, is an autosomal dominant multi‐organ cancer syndrome. Upper urinary tract urothelial carcinomas belong to HNPCC‐related tumours and rank third within this group after colorectal and endometrial cancer. However, many urologists are not aware of this association and it is presumed that some hereditary cancers are misclassified as sporadic and that their incidence is underestimated. Consequently, family members of patients with upper urinary tract urothelial carcinomas secondary to HNPCC may be denied appropriate surveillance and early detection.
A significant proportion of patients (21.3%) with newly diagnosed upper urinary tract urothelial carcinomas may have underlying HNPCC. Demographic and epidemiological characteristics suggest different mechanisms of carcinogenesis among this population. Recognition of such potential is essential for appropriate clinical and genetic management of patients and family. In order to help to identify these patients, we propose a patient‐specific checklist.
OBJECTIVE
To identify, based on previously described clinical criteria, hereditary upper urinary tract urothelial carcinomas (UUT‐UCs) that are likely to be misclassified as sporadic although they may belong to the spectrum of hereditary non‐polyposis colorectal cancer (HNPCC) associated cancers.
PATIENTS AND METHODS
We identified, using established clinical criteria, suspected hereditary UUT‐UC among 1122 patients included in the French national database for UUT‐UC.
Patients were considered at risk for hereditary status in the following situations: age at diagnosis <60 years with no previous history of bladder cancer; previous history of HNPCC‐related cancer regardless of age; one first‐degree relative with HNPCC‐related cancer diagnosed before 50 years of age or two first‐degree relatives diagnosed regardless of age.
RESULTS
Overall, 239 patients (21.3%) were considered to be at risk of hereditary UUT‐UC.
Compared with sporadic cases, hereditary cases are more likely to be female (P= 0.047) with less exposure to tobacco (P= 0.012) and occupational carcinogens (P= 0.037). A greater proportion of tumours were located in the renal pelvis (54.5% vs 48.4%; P= 0.026) and were lower grade (40% vs 30.1%; P= 0.015) in the hereditary cohort.
The overall, cancer‐specific and recurrence‐free survival rates were similar in both cohorts.
We propose a patient‐specific risk identification tool.
CONCLUSIONS
A significant proportion (21.3%) of patients with newly diagnosed UUT‐UC may have underlying HNPCC as a cause.
Recognition of such potential and application of a patient‐specific checklist upon diagnosis will allow identification and appropriate clinical and genetic management for patient and family.
This is the first report describing long-term follow-up after laparoscopic management of SPT. All three patients developed recurrences. These poor results contrast sharply with the low risk of local or disseminated recurrence after open laparotomy without chemotherapy that has been considered as the treatment of choice up to now. Recurrences after laparoscopic management may have been due to diffusion of tumor cells caused by gas insufflation especially during biopsy. Laparoscopic biopsy should not be performed in patients presenting SPT.
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