GUIDELINES ON RENAL CELL CANCER

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20 G. Mickisch (chairman), J. Carballido, S. Hellsten, H. Schulze, H. Mensink Eur Urol 2001;40(3):252-255 Introduction is characterised by a constant rise in incidence over the last 50 years, with a predominance of men over women and an incidence peak in the 6 th and 7 th decade. There are no generally accepted risk factors for RCC although there are some epidemiologic data indicating that a smoking habit, obesity or exposure to certain heavy metals such as cadmium may favour the development of RCCs. Diagnosis Clinical signs and symptoms of RCC: haematuria persistent lower back pain a mass in the abdomen fatigue weight loss fever not obviously associated with infection and swelling of the legs Generally the diagnosis is made through an abdominal ultrasound performed for various reasons. Standard radiological procedure abdominal CT-scan with and without contrast medium (It serves to document the diagnosis of RCC and provides

information on the function and morphology of the contralateral kidney 21 Additional diagnostic procedures: magnetic resonance imaging (MRI) angiography or fine needle biopsy, have a very limited role, but may be considered in selected cases. In case of haematuria, additional tumours of the genitourinary tract should be excluded. The most commonly assessed laboratory parameters are: Haemoglobin and erythrocyte sedimentation rate: prognosis Creatinine: overall kidney function Alkaline phosphatase: liver metastasis, bone metastasis. Serum calcium is frequently included in the preoperative assessment because of its association with paraneoplastic manifestation, which may have clinical implications. Classification: The TNM (UICC, 2002) classification is recommended T T2 T3 Primary tumour TX Primary tumour cannot be assessed T0 No evidence of primary tumour T1 Tumour 7 cm or less in greatest dimension, limited to the kidney T1a Tumour 4 cm or less T1b Tumour more than 4 cm but not more than 7 cm Tumour more than 7 cm in greatest dimension, limited to the kidney Tumour extends into major veins or directly invades

22 adrenal gland or perinephric tissues but not beyond Gerota fascia T3a Tumour directly invades adrenal gland or perinephric tissues 1 but not beyond Gerota fascia T3b Tumour grossly extends into renal vein(s) 2 or vena cava or its wall below diaphragm T3c Tumour grossly extends into vena cava or its wall above diaphragm T4 Tumour directly invades beyond Gerota fascia N Regional lymph nodes NX Regional lymph nodes cannot be assessed N0 No regional lymph node metastasis N1 Metastasis in a single regional lymph node N2 Metastasis in more than one regional lymph node M Distant metastasis MX Distant metastasis cannot be assessed M0 No distant metastasis M1 Distant metastasis 1 Includes renal sinus (peripelvic) fat 2 Includes segmental (muscle-containing) branches Robson s classification (1969) is commonly used and the relationship with TNM 2002 is as follows: Robson s Stage I = T1-2 Robson s Stage II = T3a Robson s Stage IIIa = T3b-c Robson s Stage IVa = T4 Robson s Stage IIIb = N1-2 Robson s stage IVb = M1 Traditionally RCC have been classified according to the

nuclear or cellular morphology. New morphologic, cytogenetic and molecular studies make it possible to distinguish five types of carcinomas: Clear - cell: 60-85% Chromophilic: 7-14% Chromophobic: 4-10% Oncocytic: 2-5% Collecting duct: 1-2% (10). Treatment Surgery is the main treatment for renal cell carcinoma, offering a reasonable chance of curing the disease. The chances of cure by surgery most strongly depend on stage (primarily) and grade (secondarily). Standard operative procedure is a radical nephrectomy including Gerota s fascia. There is no evidence to favour a specific surgical approach. In selected cases of small (< 4 cm) peripheral lesions, an organ sparing approach may be considered. Chemotherapy, apart for Wilm s tumor in children, RCC seems to be very resistant to chemotherapy Radiation therapy (in case of bone-metastases or spreading to the brain) Immunotherapy still under investigation but results are promising Experimental therapies 23

24 Follow up Follow up of patients with RCC after surgical treatment is recommended to detect local recurrence and distant metastases as early as possible to permit additional treatment when indicated and if possible. TABLE 1: Recommended follow-up scheme for renal cell carcinoma Stage Visit Examination All T 4-6 weeks after surgery Physical ex. Creatinine Hb T1, T2 Every 6 months for Physical exam 3 years Every year from 3 to 5 Chest X-ray years T3, T4 Every 6 months for 3 Physical exam years Every year from 3 to Chest X-ray 10 years c Retroperitoneal imaging AP = alkaline phosphatase; LR = local recurrence; LN = lymph node a If elevated preoperatively (recurrent or persisting elevation suggests distant metastases b If the postoperative level is abnormal, it should be repeated at the regular visits. c There is a small, but continuous, risk of recurrence or metastasis from 5-15 yrs.

This short booklet is based on the more comprehensive EAU guidelines (ISBN 90-806179-8-9), available to all members of the European Association of Urology at their website - www.uroweb.org. 25 Optional AP A AP B Kidney imaging Purpose Exclude complications of surgery Establish remaining kidney function 2 To check recovery of perioperative blood loss Exclude complications of surgery and LR and LN metastases Exclude pulmonary metastases and LR afterpartial nephrectomy Exclude complications of surgery and LR and LN metastases Exclude pulmonary metastases and LR after partial nephrectomy To detect LR, contralateral metastases or neo- occurrence or residual tumour) when bone pain is present, suspicion of bone or liver metastasis.