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THE URINARY BLADDER
                   TUMORS




Dr. Ali Kamal M. Sami
M.B.Ch.B.  M.A.U.A.
F.I.B.M.S.  M.I.U.A.
Ninety-five per cent of primary bladder tumours
originate in the epithelium;
 the remainder arise from connective tissue
angioma, myoma, fibroma and sarcoma) .
secondary tumours of the bladder from the
sigmoid and rectum, the prostate, the uterus or
ovary,
Pathology
Benign papillary tumours.
 The papilloma consists of a single
frond with a central vascular core
with villi; it looks like a red sea-
anemone .
Carcinoma arising
within the bladder may
be of three cell types:
Transitional 90%
 Squamous 5%
 Adenocarcinoma 1-
2%, which arises either
from the urachal
remnant.
Transitional cell carcinoma (TCC):

Occupations which have been reported to have a
significantly excess risk of bladder cancer are shown below
Occupations with an excess risk of bladder cancer

1.    Textile workers
2.    Dye workers
3.    Tire rubber and cable workers
4.    Petrol workers
5.    Leather workers
6.    Shoe manufacturers and cleaners
7.    Painters
8.    Hairdressers
9.    Lorry drivers
10.   Drill press operators
11.   Chemical workers
12.   Rodent exterminators and sewage workers
Cigarette smoking is associated with a two to three-fold excess risk.In areas where S.
haematobium is endemic bladder cancer is more common, and this tends to be squamous
Tumour staging and grading
Study of the biological behaviour of transitional cell cancer of the
bladder shows that they fall into the three following groups.
• Non muscle invasive tumours (pTa) and (pT1) account for 70%.
 These tumours may be single or multiple. Histological examination may
reveal invasion of the lamina propria (pT1) but not of the muscle or no
invasion of lamina propria (pTa) .
• Muscle invasive disease(T2)(T3)(T4) (accounts for 25 per cent of new
cases). Such tumours carry a much worse prognosis as they are subject
to local invasion and distant metastasis.
• Flat, noninvasive carcinoma in situ (CIS) accounts for 5%.
Superficial bladder cancer (pTa
            and pT1)

These are usually papillary tumours
which grow in an exophytic fashion
     into the bladder lumen.

They may be single or multiple and
may appear pedunculated arising on
    a stalk with a narrow base,

  but if the’ tumours are less well
 differentiated they are more solid
         with a wider base.

    The most common sites for
superficial tumours are the trigone
  and lateral walls of the bladder.
Muscle invasive transitional cell carcinoma

The tumour with muscle invasion is nearly
always solid. These tumours are often large and
broad based, having an irregular, ugly,
sometimes ulcerated, appearance within the
bladder. The incidence of metastases, whether
from lymphatic invasion in the pelvis or blood-
born to the lung, liver or bones, is much more
common and will cause the death of 3 0—50
per cent of patients.
In situ
carcinoma



     The histological
appearance of irregularly
arranged cells with large
nuclei and a high mitotic
   index replacing the
  normally well ordered
 urothelium is known as
    carcinoma in situ.
Pure squamous cell carcinoma of the bladder


Squamous cell tumours tend to be solid and are
nearly always associated with muscle invasion. This is
the most prevalent form of bladder cancer in areas
where bilharzia is endemic. Squamous cell tumours
may be associated with chronic irritation caused by
stone disease in the bladder as a result of metaplasia.
Pure adenocarcinoma
This accounts for approximately 1—2
per cent of bladder cancer. It usually
arises in the fundus of the bladder at
the site of the urachal remnant.
Clinical features
1. Painless Intermittent haematuria is by far the most
   common symptom and should be regarded as indicative of
   a bladder carcinoma until proven otherwise.
2. Constant pain in the pelvis usually heralds extravesical
   spread.
3. There is often frequency and discomfort associated with
   urination.
4. Pain in the loin or pyelonephritis may indicate ureteric
   obstruction and hydronephrosis.
5. A late manifestation is nerve involvement causing pain
   referred to the suprapubic region, groins, perineum, anus
   and into the thighs.
Investigation
•Urine.
Urine should be cultured and examined cytologically for malignant cells. This is not a
good screening test for patients with haematuria as, particularly with low-grade
tumours, malignant cells may not be identified .
•Blood tests like (Hb , S.electrolytes , B.Urea).
•IVU.
-The most common radiological sign is a filling defect.
-Hydronephrosis may occur if a superficial tumour grows up the intramural ureter or if
direct invasion of the ureteric wall occurs.
•- Ultrasound scanning should be carried out if the kidney is nonfunctioning.
•Cystourethroscopy.
Cystourethroscopy is the mainstay of diagnosis and should always be performed on
patients with haematunia. It can be done with a rigid instrument under general
anaesthesia or with a flexible instrument under local anaesthesia. The urethra is
inspected at the initial insertion of the instrument (urethroscopy) and the bladder is
then examined in a systematic fashion (cystoscopy).
•Bimanual examination.
A bimanual examination with the patient fully relaxed under general anaesthesia
should be performed both before and after endoscopic surgical treatment of these
tumours.
Noninvasive tumours•
Endoscopic surgery (TURBT)(Trans Urethral Resection of Bladder Tumor)
The tumour should be carefully resected in layers using a resectoscope. The base
of the tumour is sent separately for histological examination. Small biopsies are
taken near to and distant from the primary lesion to diagnose unsuspected CIS.
The bimanual examination is repeated at the end of each endoscopic procedure.
Follow-up. Most urologists agree that patients with a single, low- or medium-
grade pTa tumour can safely be treated by resection alone and followed up by
means of regular cystoscopies.
The resection may be followed by a 6-week course of intravesical chemotherapy
with mitomycin C, adriamycin or epirubicin.
Others will treat such patients by means of endoscopic treatment followed by
intravesical immunotherapy with intravesical bacillus of Calmette and Guérin
(BCG).
Follow-up cystoscopies are essential; they may be carried out by means of local
anaesthesia with a flexible cystoscope on by means of general anaesthesia if the
urologist feels that the patient has a high risk of recurrence.
They are usually done in 3 months intervals in first year.
6 months intervals in the second year.
Yearly intervals for the next 3 years.
Intravesical chemotherapy and
immunotherapy
Various agents have been used as
chemotherapy. These include
•Thiotepa.
•mitomycin C.
•epirubicin.
•adriamycin.
Immunotherapy agent includes:
BCG is now frequently used as intravesical
immunotherapy
Open surgical excision
This should be totally avoided. If by some
error a bladder containing a tumour is
entered, then the tumour may be removed
with a diathermy needle and the base
coagulated and the bladder closed.
Postoperative radiotherapy to the wound
will diminish the chance of tumour
implantation.
2.Invasive tumours
•Radical cystectomy.
•Radical radiotherapy.
•Combination of the two.
•Primary surgery(radical
cystectomy) followed by
a combination of agents
using cis-
platinum, methotrexate, a
driamycin and vinblastine
(MVAC)
Radiotherapy
                                           Local radiotherapy. For
                                                 small invasive
                                                  lesions, local
 Deep external beam X-ray therapy.           radiotherapy can be
External beam radiotherapy is usually          delivered by open
  given by means of high-powered                placement of a
     linear accelerators. Radical           radioactive tantalum
radiotherapy giving 60 Gy over a 4—             wire. It is used
6-week period will produce a 40—50            infrequently today.
    per cent complete response.
Surgery
Partial cystectomy. This should be limited to the
treatment of small adenocarcinomas at the dome of
the bladder.
Radical cystectomy and pelvic lymphadenectomy. This
is now standard treatment for localised pT2—pT3
disease without evidence of secondary spread.
Operation
The radical cystectomy
Needs diversion of urine by:
•Ileal conduit.
•Ureterosigmodostomy:
Orthotopic ileal neobladder
Leukoplakia
This condition is simply squamous metaplasia of the bladder. Profuse
production of keratin may result in the passing of white particles in the
urine. It cannot be treated easily. Localised areas may be resected
endoscopically.

Diffuse leucoplakia of the bladder is premalignant and results in
squamous bladder cancer. Careful cystoscopic assessment is required.
The condition may require cystectomy.
Endometriosis
Endometriosis within the bladder wall is rare, but can have the
appearance of a vascular bladder tumour or a tumour which contains
chocolate-coloured or bluish cysts. The swelling enlarges and bleeds
during menstruation. If medical management fails, by means of danazol
or luteinising hormone-releasing agonists (LHRH), further treatment is
usually by means of partial cystectomy or full-thickness endoscopic
resection, depending on its site. The condition may be part of more
widespread disease. Endometriosis is also a cause of ureteric stricture.
THANK YOU

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Bladder tumor

  • 1. THE URINARY BLADDER TUMORS Dr. Ali Kamal M. Sami M.B.Ch.B. M.A.U.A. F.I.B.M.S. M.I.U.A.
  • 2. Ninety-five per cent of primary bladder tumours originate in the epithelium; the remainder arise from connective tissue angioma, myoma, fibroma and sarcoma) . secondary tumours of the bladder from the sigmoid and rectum, the prostate, the uterus or ovary,
  • 3. Pathology Benign papillary tumours. The papilloma consists of a single frond with a central vascular core with villi; it looks like a red sea- anemone .
  • 4. Carcinoma arising within the bladder may be of three cell types: Transitional 90% Squamous 5% Adenocarcinoma 1- 2%, which arises either from the urachal remnant.
  • 5. Transitional cell carcinoma (TCC): Occupations which have been reported to have a significantly excess risk of bladder cancer are shown below Occupations with an excess risk of bladder cancer 1. Textile workers 2. Dye workers 3. Tire rubber and cable workers 4. Petrol workers 5. Leather workers 6. Shoe manufacturers and cleaners 7. Painters 8. Hairdressers 9. Lorry drivers 10. Drill press operators 11. Chemical workers 12. Rodent exterminators and sewage workers Cigarette smoking is associated with a two to three-fold excess risk.In areas where S. haematobium is endemic bladder cancer is more common, and this tends to be squamous
  • 6. Tumour staging and grading Study of the biological behaviour of transitional cell cancer of the bladder shows that they fall into the three following groups. • Non muscle invasive tumours (pTa) and (pT1) account for 70%. These tumours may be single or multiple. Histological examination may reveal invasion of the lamina propria (pT1) but not of the muscle or no invasion of lamina propria (pTa) . • Muscle invasive disease(T2)(T3)(T4) (accounts for 25 per cent of new cases). Such tumours carry a much worse prognosis as they are subject to local invasion and distant metastasis. • Flat, noninvasive carcinoma in situ (CIS) accounts for 5%.
  • 7. Superficial bladder cancer (pTa and pT1) These are usually papillary tumours which grow in an exophytic fashion into the bladder lumen. They may be single or multiple and may appear pedunculated arising on a stalk with a narrow base, but if the’ tumours are less well differentiated they are more solid with a wider base. The most common sites for superficial tumours are the trigone and lateral walls of the bladder.
  • 8. Muscle invasive transitional cell carcinoma The tumour with muscle invasion is nearly always solid. These tumours are often large and broad based, having an irregular, ugly, sometimes ulcerated, appearance within the bladder. The incidence of metastases, whether from lymphatic invasion in the pelvis or blood- born to the lung, liver or bones, is much more common and will cause the death of 3 0—50 per cent of patients.
  • 9. In situ carcinoma The histological appearance of irregularly arranged cells with large nuclei and a high mitotic index replacing the normally well ordered urothelium is known as carcinoma in situ.
  • 10. Pure squamous cell carcinoma of the bladder Squamous cell tumours tend to be solid and are nearly always associated with muscle invasion. This is the most prevalent form of bladder cancer in areas where bilharzia is endemic. Squamous cell tumours may be associated with chronic irritation caused by stone disease in the bladder as a result of metaplasia.
  • 11. Pure adenocarcinoma This accounts for approximately 1—2 per cent of bladder cancer. It usually arises in the fundus of the bladder at the site of the urachal remnant.
  • 12. Clinical features 1. Painless Intermittent haematuria is by far the most common symptom and should be regarded as indicative of a bladder carcinoma until proven otherwise. 2. Constant pain in the pelvis usually heralds extravesical spread. 3. There is often frequency and discomfort associated with urination. 4. Pain in the loin or pyelonephritis may indicate ureteric obstruction and hydronephrosis. 5. A late manifestation is nerve involvement causing pain referred to the suprapubic region, groins, perineum, anus and into the thighs.
  • 13. Investigation •Urine. Urine should be cultured and examined cytologically for malignant cells. This is not a good screening test for patients with haematuria as, particularly with low-grade tumours, malignant cells may not be identified . •Blood tests like (Hb , S.electrolytes , B.Urea). •IVU. -The most common radiological sign is a filling defect. -Hydronephrosis may occur if a superficial tumour grows up the intramural ureter or if direct invasion of the ureteric wall occurs. •- Ultrasound scanning should be carried out if the kidney is nonfunctioning. •Cystourethroscopy. Cystourethroscopy is the mainstay of diagnosis and should always be performed on patients with haematunia. It can be done with a rigid instrument under general anaesthesia or with a flexible instrument under local anaesthesia. The urethra is inspected at the initial insertion of the instrument (urethroscopy) and the bladder is then examined in a systematic fashion (cystoscopy). •Bimanual examination. A bimanual examination with the patient fully relaxed under general anaesthesia should be performed both before and after endoscopic surgical treatment of these tumours.
  • 14.
  • 15. Noninvasive tumours• Endoscopic surgery (TURBT)(Trans Urethral Resection of Bladder Tumor) The tumour should be carefully resected in layers using a resectoscope. The base of the tumour is sent separately for histological examination. Small biopsies are taken near to and distant from the primary lesion to diagnose unsuspected CIS. The bimanual examination is repeated at the end of each endoscopic procedure. Follow-up. Most urologists agree that patients with a single, low- or medium- grade pTa tumour can safely be treated by resection alone and followed up by means of regular cystoscopies. The resection may be followed by a 6-week course of intravesical chemotherapy with mitomycin C, adriamycin or epirubicin. Others will treat such patients by means of endoscopic treatment followed by intravesical immunotherapy with intravesical bacillus of Calmette and Guérin (BCG). Follow-up cystoscopies are essential; they may be carried out by means of local anaesthesia with a flexible cystoscope on by means of general anaesthesia if the urologist feels that the patient has a high risk of recurrence. They are usually done in 3 months intervals in first year. 6 months intervals in the second year. Yearly intervals for the next 3 years.
  • 16. Intravesical chemotherapy and immunotherapy Various agents have been used as chemotherapy. These include •Thiotepa. •mitomycin C. •epirubicin. •adriamycin. Immunotherapy agent includes: BCG is now frequently used as intravesical immunotherapy
  • 17. Open surgical excision This should be totally avoided. If by some error a bladder containing a tumour is entered, then the tumour may be removed with a diathermy needle and the base coagulated and the bladder closed. Postoperative radiotherapy to the wound will diminish the chance of tumour implantation.
  • 18. 2.Invasive tumours •Radical cystectomy. •Radical radiotherapy. •Combination of the two. •Primary surgery(radical cystectomy) followed by a combination of agents using cis- platinum, methotrexate, a driamycin and vinblastine (MVAC)
  • 19. Radiotherapy Local radiotherapy. For small invasive lesions, local Deep external beam X-ray therapy. radiotherapy can be External beam radiotherapy is usually delivered by open given by means of high-powered placement of a linear accelerators. Radical radioactive tantalum radiotherapy giving 60 Gy over a 4— wire. It is used 6-week period will produce a 40—50 infrequently today. per cent complete response.
  • 20. Surgery Partial cystectomy. This should be limited to the treatment of small adenocarcinomas at the dome of the bladder. Radical cystectomy and pelvic lymphadenectomy. This is now standard treatment for localised pT2—pT3 disease without evidence of secondary spread. Operation The radical cystectomy Needs diversion of urine by: •Ileal conduit. •Ureterosigmodostomy: Orthotopic ileal neobladder
  • 21. Leukoplakia This condition is simply squamous metaplasia of the bladder. Profuse production of keratin may result in the passing of white particles in the urine. It cannot be treated easily. Localised areas may be resected endoscopically. Diffuse leucoplakia of the bladder is premalignant and results in squamous bladder cancer. Careful cystoscopic assessment is required. The condition may require cystectomy.
  • 22. Endometriosis Endometriosis within the bladder wall is rare, but can have the appearance of a vascular bladder tumour or a tumour which contains chocolate-coloured or bluish cysts. The swelling enlarges and bleeds during menstruation. If medical management fails, by means of danazol or luteinising hormone-releasing agonists (LHRH), further treatment is usually by means of partial cystectomy or full-thickness endoscopic resection, depending on its site. The condition may be part of more widespread disease. Endometriosis is also a cause of ureteric stricture.