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Urologic Malignancies
General Outline of Presentation
Urological Malignancies :
• Renal
• Bladder
• Penis
• Prostate
• Testicular
RENAL MALIGNANCIES
Classification of Neoplasms of The
Kidney
Benign neoplasms
• Adenoma
• Angioma
• Angiomyolipoma
Malignant neoplasms
• Wilms’ tumour (nephroblastoma in children)
• Grawitz’s tumour (adenocarcinoma,
hypernephroma)
• Transitional cell carcinoma of the renal pelvis
and collecting system
• Squamous cell carcinoma of the renal pelvis
Renal Cell Carcinoma
• Grawitz’s/Hypernephroma/Adenocarcinoma
• The most common neoplasm of the kidney (75%
incidence), arises from renal tubular cells.
• Male predominance (1.6:1.0 M:F)
• Highest incidence between age 50-70
• Majority of RCC occurs sporadically
• Highest incidence in Scandinavia and North
America, lowest in Africa
Pathology
• Surface – white to
yellowish
• Semi transparent
• Areas of
haemorrhage and
necrosis
Spread
• Direct/ Lymphatic/Blood
Clinical Features -1
• Asymptomatic in the beginning
• Triad of loin pain, loin mass, haematuria
(10%) and usually indicate advanced disease
• Haematuria is common complaint
• Dragging discomfort in the loin
• Mass
• Rapidly developing varicocele
Clinical Features -2
• Paraneoplastic syndrome : hypercalcemia,
erthrocytosis, non metastasis hepatic
dysfunction (Stauffer syndrome)
• Metastasis symptoms : Bone pain , chronic
cough, hemoptysis
Left Varicocele
Clinical Features -3
Atypical symptoms :
Persistent pyrexia (37.8–38.9ºC) with no
evidence of infection
 Cachexia
Anaemia.
Polycythaemia
Raised ESR
Nephrotic syndrome
Recommended Initial Test
TEST REASON
Renal Function Test Assess remaining renal function
Full Blood Count Polycythemia, Anaemia
ESR Increased in renal cell carcinoma
Serum calcium Hypercalcaemia (paraneoplastic syndrome)
Coagulation Profile Pre-surgery investigation
Liver Function Test Impaired in metastases or paraneoplastic
syndrome, ALP increase in bone metastasis
Chest x-ray Canon ball appearance (metastasis)
Staging of disease
TEST REASON
Transabdominal
Ultrasound
Origin of mass, cystic/solid, sign of
metastasis in liver and lymph nodes
enlargement
Contrast CT Abdomen TNM Staging
MRI Abdomen If renal function is impaired to permit
contrast
Transesophageal
Echocardiogram
If suspected spread of tumour from inferior
vena cava involving right atrium
Excretory Urography Able to access renal function and any filling
defect indicating presence of mass
PET Scan Most sensitive but not widely available
Robson Modification Of the Flocks &
Kadesky Staging of RCC
Staging of RCC
Chest x-ray
• Lung
Metastasis
•Canon ball
appearance
Intravenous urogram
•Hypernephroma of
the left kidney
•Displacement of the
upper pole calyces by
the mass.
Arteriogram
•Vascular ‘blush’
due to metastasis
in the femur from
a Grawitz’s
tumour
CT scan
Large bilateral
renal
adenocarcinomas
Principles of Treatment
• Radiotherapy, Chemotherapy – minimal
respond
• Surgical
• Immunotherapy – Cytokine IL-2, Chemokines
Surgical
• Surgical removal of affected kidney - partial or
complete nephrectomy
• 2 types of approach
 Loin
 Transabdominal
• Vascular control by first ligation of renal artery
and then ligation of renal vein
Indications
1. Bilateral RCC
2. RCC in a solitary functioning kidney
3. Unilateral RCC with contralateral kidney under threat of
its future function
4. Tumour less than 4cms with normal opposite kidney.
5. Five year survival rate 75% to 85%
6. Local tumour recurrence of 10% is reported.
Other Approaches
1. Radio frequency ablations
2. Cryoablation
Nephron Sparing Surgery
• Gold standard treatment for localized RCC with
contralateral normal kidney, adequate surgical
margin.
• Principles of Surgery- Early ligation of renal artery
and vein , removal of kidney including Gerota’s
fascia, removal of ipsilateral adrenal gland,
regional lymphadenectomy from crus of
diaphragm to aortic bifurcation.
Radical nephrectomy
Prognosis
• In operable cases, 70% of patients are well
after three years and 60% after five years.
• Worse prognosis –
- Macroscopic involvement of the renal vein or
its tributaries
- Invasion beyond the capsule
- Lymphatic involvement
Transitional Cell Carcinoma of Kidney
• Less common
• May invade the renal parenchyma, be
multifocal and metastasize.
• Multiple ureteric tumours are thought to arise
from a field change that predisposes the whole
urothelium to metaplasia rather than seeding
down the ureter.
• Carcinogen is chemical or viral is uncertain
Diagnostic Work Up
• Clinical - Haematuria
• Investigations :
Presence of malignant cells in the urine may
indicate well or poorly differentiated.
Obtain cells from the tumour by sampling
using a brush or catheter
Intravenous urography
Retrograde pyelography
Treatment
• Conventional surgical - nephroureterectomy.
• Conservative resection - well-differentiated
upper urinary tract transitional tumours
Squamous Cell Carcinoma of Kidney
• This is rare and often associated with chronic
inflammation and leucoplakia resulting from
stone.
• The tumours are radiosensitive but
metastasise early
• Prognosis is poor
BLADDER CANCER
• Rare before 50 years old.
• Male > Female
• 95% of primary bladder tumor originate in
transitional epithelium (TCC)
• Secondary tumors : Sigmoid & rectum,
prostate, uterus or ovaries
• Histological Types : Urothelial, Squamous and
Adenocarcinoma
INTRODUCTION
• Cigarette Smoking (40%)
• Long term use Analgesic
• Occupational risk factors
- Textile, Dye, Tyre rubber, Petrol etc.
• SCC: Schistosoma Haematobium (in Endemic
areas), usage of catheter, bladder stone.
RISK FACTORS
• Hematuria. Painless, end micturition
• Bladder Outlet Obstruction (Male)
• Cystitis (Female)
• Constant pain in Pelvis
• Referred pain to suprapubic region, groins,
perineum, anus & into thigh
• Loss of Weight, Loss of Appetite
CLINICAL FEATURES
• Usually negative
• Maybe a palpable suprapubic mass
• Rectal Examination:
- May reveal large tumors (Invaded pelvic side
walls)
• Bimanual Examination:
- Necessary for staging evaluation.
PHYSICAL EXAMINATION
• URINE
• BLOOD
• IMAGING
INVESTIGATIONS
URINE TESTS
 Urine FEME
- Hematuria, WBC
 Urine Cytology
- Malignant cell.
 Urine CnS
- To rule out Infection
INVESTIGATIONS
BLOOD TEST
• Full Blood Count
• Renal Profile
• Liver Function Test
• Random Blood Sugar
• Coagulation Profile
• Prostate Specific Antigen (PSA)
• GXM and GSH
IMAGING
Ultrasound/IVU
– Most common defect: Filling defect
– Irregularity of bladder wall (Invasive tumor)
Contrast CT/MRI
– For staging
– Demonstrate lymph node & muscular invasion
Cystourethroscopy
– Mainstay of Diagnosis
Ultrasound of Bladder
• Irregular, echogenic mass
Cystourethroscopy
Cystoscopy of Bladder Cancer
See the cauliflower
appearance of the
tumor?
• Carcinoma In Situ
Superficial Tumor
• Ta. Confined to urothelium
• T1. Lamina propia involvement
Invasive Tumor
• T2a. Sup. Muscle involvement
• T2b. Deep muscle involvement
• T3a. Invades perivesicle tissue
microscopically
• T4. Extravesicle mass (macro)
Fixed Tumor
• T4a. Prostate, uterus, vagina
• T4b. Fixed to pelvic wall.
STAGING (UICC SYSTEM)
STAGING
• Stage 0. pTa & TIS
• Stage 1. T1N0M0
• Stage 2. T2N0M0
• Stage 3. T3 (a/b)
• Stage 4. Any metastasis
 Superficial Tumor (Ta, T1)
 Invasive Tumor ( T2, T3)
 Fixed & Metastatic Tumor (T4)
- Poor prognosis
MANAGEMENT
1. Superficial Tumor (pTa, pT1)
• Trans Urethral Resection Bladder Tumor
(TURBT) and send tissue for HPE
• pT1
- Repeat Cystoscopy & resection
of tumor base after 6 weeks
- Followed by Intravesical BCG
Regular follow up for cystoscopic exam : Every
3monthly for 3 years -> 6 monthly for 2 years
Trans Urethral Resection Bladder
Tumor (TURBT)
TURBT
Cystoscopy
• Endoscopy of the urinary bladder
Intravesical Chemo/Immunotherapy
• Used after TURBT for Stage 0 or Stage 1 Ca.
• It’s used only for early stage Ca – affect
mainly the cell lining inside bladder, no effects
on cells elsewhere.
• BCG : Is put directly into bladder through a
catheter- attract immune system cells to the
bladder –attack the cancer cells.
2. Invasive Tumor (pT2, pT3)
• Partial Cystectomy. Limited to small adenocarcinoma
• Radical Cystectomy.
- Followed by chemotherapy/radiotherapy
- Localised pT2-3 that has no spread and CIS
refractory to BCG, Pt >70 years old
• Neoadjuvant Chemotherapy. To shrink tumor before
surgery
• Chemotherapy & Radiotherapy. Unfit, Older or
decline cystectomy
• Orthotopic Bladder Replacement. If urethra
can be retained, reconstruct new bladder from
intestine
• Ileal Conduit.
3. Metastatic Tumor (pT4)
• Poor prognosis. Incurable
• Palliative. No surgery
• Treat with chemotherapy
PROGNOSIS
• Mucosal Tumor- 50-60% 5 years survival
• Deep muscle invasion: 20-30% 5 years survival
rate
• Overall 1/3 patient survive for 5 years
PROSTATE CANCER
Epidemiology
• Age > 65 years old
• 10-15% of younger men with positive family
history but unclear etiology
• Rates of clinically evident disease are low in
Japan & China
• In Malaysia :6th among top 10 cancers for
men
Risk Factors
• Age >65 years old
• Family history :first degree relatives
• Hormonal : high testosterone
• Exposure to cadmium
Pathology
• Almost all adenocarcinoma
• Origin : peripheral zones of prostatic glands
• Gleason scoring – degree of glandular
differentiation & relationship to stroma
Mode of presentation
i. Found on autopsy or at cystoprostatectomy
ii. Accidental findings during TURP (T1a & T1b)
or by PSA (T1c)
iii. Early, palpable, localised prostate cancer (T2)
iv. Advanced local prostate cancer (T3 & T4)
v. Metastatic disease
Spread
Local
• Seminal vesicle
• Bladder : neck
& trigone
• Lower end of
ureter
• rectum
Hematogenous
• Bone
Lymphatics
• External iliac
• Internal iliac
• Mediastinal
• supraclavicular
Clinical Features - History
• Asymptomatic – screening by per rectal
examination and PSA
- Suspiciously raised serum PSA
- Found on histological examination after TURP
• Only advanced disease gives rise to symptoms,
but even advance disease may be
asymptomatic
• Symptoms of advanced disease
- Bladder outlet obstruction
- Pelvic pain & hematuria
- Bone pain
- Renal failure
Clinical Features – Physical
Examination
• Sign of anaemia
• Nodular, irregular, stony hard, fixed prostate
on per rectal examination
TNM Staging
TUMOUR
• T1 – clinically inapparent tumour neither palpable
nor visible by imaging
• T2a – tumour confined within prostate & 1 lobe
T2b – tumour involved both lobes
• T3 – tumour extends through prostate capsule
T3a – uni or bilateral extension
T3b – seminal vesicle extension
• T4 – tumour is fixed or invades adjacent structure
other than seminal vesicles
NODAL
• N1 – lymph node metastasis
METASTASIS
• M1 – distant metastasis
* If prostate Ca is palpable it is
incurable
Investigations
Diagnostic
• Prostate Specific Antigen (PSA)
- Cancer detection rate 2-4%
- Lack sensitivity & specificity
- 30% men with PSA, cancer confirmed by
biopsy
- 20% men with prostate Ca have normal PSA
- Good at following course of advanced disease
• Also raised in : Acute Urinary Retention, TURP,
prostatitis, large BPH, catheterization
Level Possibility
<4ng/ml Normal
4-10ng/ml Benign prostate hyperplasia, prostatitis
>10ng/ml Suggestive malignancy
>35ng/ml Diagnostic for advanced cancer
>100ng/ml Distant bone metastasis
• Trans-rectal ultrasound (TRUS)
- Image the prostate irrespective findings on
palpation
- Guide transrectal needle biopsy
- Diagnosis of locally extensive disease (T2)
• Prostate biopsy (transrectal)
- Take multiple biopsy
- If patient has bladder outlet obstruction, then
can do transurethral resection of prostate
(TURP)
Transrectal US showing
normal seminal vesicles
Transrectal US showing
local extension of T3
prostate cancer
Obtaining a specimen
of prostatic tissue by
means of a biopsy
needle
Investigation
Routine
• Full blood count
- Anaemia (leucoerytroblastic anaemia, renal
failure or hematuria)
- Thrombocytopenia (DIC)
• Liver function test
- Abnormal if liver metastasis present (ALP in both
bone & liver metastasis)
• Chest X-ray
- Lung metastasis
• Pelvic & lumbar X-ray
- Sclerotic / osteolytic metastasis in lumbar
vertebrae & pelvic bones
• MRI/CT scan
- Local staging, node & metastasis
Osseous metastasis of
the pelvic bones in
carcinoma of the
prostate
• Bone scan
- After establish diagnosis, as part of diagnosis
- If PSA >10nmol/ml or biopsy showed high
grade cancer
- If PSA <10nmol/ml with clinical indication
Bone scan showing
multiple hot spots
suggestive of metastatic
disease in a man with
prostate cancer
Management
Treatment Modalities
• Surgery – radical prostectomy
- Removal of whole prostate until distal
sphincter & seminal vesicle
- Complications : impotence, stress
incontinence
• Radiotherapy
- External Beam : T1, T2, locally advanced T3
- Brachytherapy : T1 disease (Iodine 125,
Palladium 103)
- General radiotherapy : for metastasis
• Androgen ablation
- Orchidectomy : bilateral, subscapular
- Medical : LHRH agonist like goserelin
: anti androgen like flutamide,
bicalutamide or cyproterone
- Anti androgen drugs can cause hormone
resistance & hepatotoxic
Treatment Summary
• At any stage, transurethral resection for bladder
outlet obstruction
Stage T1 & T2
- Active monitoring or radical local treatment i.e.
prostectomy or radiotherapy
Stage T3
- Radiotherapy, often with neoadjuvant or adjuvant
hormonal therapy
Stage T4
- Anti androgen therapies (bilateral
orchidectomy) plus
- Radiotherapy ; painful bone metastases or
spinal cord compression or
- Drug treatment with LHRH agonist anti
androgen drugs
PENILE CARCINOMA
Epidemiology
• Uncommon malignancy
• Elderly man, 50-70 years old
• Mostly squamous cell carcinoma, other rare
carcinomas are melanoma,
haemangiosarcoma or fibrosarcoma
Aetiology & Risk Factors
• Phimosis
- Circumcision at birth confer’s immunity & at
later ages has no immunity
• Pre cancerous lesion :
- Genital warts : HPV, condyloma acuminate
- Leucoplakia, Paget’s Disease of the penis
- Bowen’s Disease (carcinoma in situ)
• Poor hygiene & smoking
• Chronic inflammatory condition of the penis
(balanophostitis)
Pathology
• Typically squamous cell carcinoma arising
from skin of the glans/prepuce
• May be flat & infiltrating - arises from
leukoplakia
• Papillary projections – exists from papilloma,
more common
Penile squamous cell
carcinoma appearing as a
reddish, raised, and firm
nodule in the inner portion
of the foreskin
Spread
• Direct spread
• Lymphatic spread
• Blood spread
Clinical Features
• Many present late (due to embarrassment/
misdiagnosis)
• Growth is often large with foul bloody
discharge (2nd infection)
• Typically little/no pain
• 50% have inguinal lymph node enlargement,
often reflects infection
• The prepuce is non-retractile & must be split
to view the lesion
A squamous cell cancer
of the penis with an
ulcerating groin node
• The whole glans may be replaced by fungating
mass (untreated)
• Later, the inguinal nodes can erode the skin of
the groin
Physical Examination
• Site : glans penis or inner surface of foreskin
• Inspection
- Painless ulcer, irregular margin, rolled edges &
indurated or gray, crusted popular lesion
- Bleeding & yellowish discharge can be seen
• Palpation
- Firm to hard
- Retract foreskin ( some are found under the
foreskin )
- Check for phimosis
- Feel for inguinal lymph nodes
Staging
• Jackson’s staging
Stage 1 Tumour confined to the glans/ prepuce
Stage 2 Tumour invade shaft or corpora but no
nodes involvement
Stage 3 Tumour confined to the penis & operable
nodes involvement
Stage 4 Tumour involves adjacent structures &
inoperable nodes metastasis
TNM staging
Tumour Tis : carcinoma in situ
Ta : noninvasisve verrucous tumour
T1 : Tumour invading subepitelial
connective tissue
T2 : Tumour invading corpora
T3 : tumour invading urethra or prostate
T4 : tumour invading other adjacent
structures
Node N1 : 1 superficial inguinal lymph node
N2 : multiple bilateral inguinal lymph
nodes
N3 : deep inguinal & pelvic lymph
nodes, bilateral or unilateral
Metastasis M1 : distant metastasis
A late presenting
squamous cell cancer of
the penis
Investigations (special)
• Punch or excisional biopsy of the lesion
• Fine needle aspiration for palpable lymph
nodes
• CT/MRI to evaluate metastasis
Management
• Divided into treatment of primary tumour &
inguinal lymph nodes
• Primary treatment : 2 methods
i. Radiotherapy
- Indicated for small & well differentiated growth
limited to penis glans
- Disadvantage : scarring caused painful erection
ii. Surgery
- Indicated : anaplastic growth, big growth,
infiltrate shaft of penis & radiotherapy failed
- Methods of surgery
A. partial amputation of penis : distal growth
limited to glans penis & prepuce
B. total amputation of penis : lesions affecting
the shaft of penis & anaplastic lesions
• Secondary tumour – associated with inguinal
lymph nodes
- No nodes enlarged : follow up carefully
- LN enlarged which are not fixed : wait for 3
weeks after treating primary growth
- LN enlarged are massive & inoperable : deep
radiotherapy is given & may be treated with
chemotherapy
- Sentinel node biopsy
REFERENCES
• William NS, Bulstrode CJK, O’connell PR,
Cholelithiasis. Bailey & Love’s Short Practice
of Surgery. 26th edition, CRC press
THANK YOU!

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Urologic malignancy

  • 2. General Outline of Presentation Urological Malignancies : • Renal • Bladder • Penis • Prostate • Testicular
  • 4. Classification of Neoplasms of The Kidney Benign neoplasms • Adenoma • Angioma • Angiomyolipoma Malignant neoplasms • Wilms’ tumour (nephroblastoma in children) • Grawitz’s tumour (adenocarcinoma, hypernephroma) • Transitional cell carcinoma of the renal pelvis and collecting system • Squamous cell carcinoma of the renal pelvis
  • 5. Renal Cell Carcinoma • Grawitz’s/Hypernephroma/Adenocarcinoma • The most common neoplasm of the kidney (75% incidence), arises from renal tubular cells. • Male predominance (1.6:1.0 M:F) • Highest incidence between age 50-70 • Majority of RCC occurs sporadically • Highest incidence in Scandinavia and North America, lowest in Africa
  • 6. Pathology • Surface – white to yellowish • Semi transparent • Areas of haemorrhage and necrosis
  • 8. Clinical Features -1 • Asymptomatic in the beginning • Triad of loin pain, loin mass, haematuria (10%) and usually indicate advanced disease • Haematuria is common complaint • Dragging discomfort in the loin • Mass • Rapidly developing varicocele
  • 9. Clinical Features -2 • Paraneoplastic syndrome : hypercalcemia, erthrocytosis, non metastasis hepatic dysfunction (Stauffer syndrome) • Metastasis symptoms : Bone pain , chronic cough, hemoptysis
  • 11. Clinical Features -3 Atypical symptoms : Persistent pyrexia (37.8–38.9ºC) with no evidence of infection  Cachexia Anaemia. Polycythaemia Raised ESR Nephrotic syndrome
  • 12. Recommended Initial Test TEST REASON Renal Function Test Assess remaining renal function Full Blood Count Polycythemia, Anaemia ESR Increased in renal cell carcinoma Serum calcium Hypercalcaemia (paraneoplastic syndrome) Coagulation Profile Pre-surgery investigation Liver Function Test Impaired in metastases or paraneoplastic syndrome, ALP increase in bone metastasis Chest x-ray Canon ball appearance (metastasis)
  • 13. Staging of disease TEST REASON Transabdominal Ultrasound Origin of mass, cystic/solid, sign of metastasis in liver and lymph nodes enlargement Contrast CT Abdomen TNM Staging MRI Abdomen If renal function is impaired to permit contrast Transesophageal Echocardiogram If suspected spread of tumour from inferior vena cava involving right atrium Excretory Urography Able to access renal function and any filling defect indicating presence of mass PET Scan Most sensitive but not widely available
  • 14. Robson Modification Of the Flocks & Kadesky Staging of RCC
  • 16.
  • 18. Intravenous urogram •Hypernephroma of the left kidney •Displacement of the upper pole calyces by the mass.
  • 19. Arteriogram •Vascular ‘blush’ due to metastasis in the femur from a Grawitz’s tumour
  • 21. Principles of Treatment • Radiotherapy, Chemotherapy – minimal respond • Surgical • Immunotherapy – Cytokine IL-2, Chemokines
  • 22. Surgical • Surgical removal of affected kidney - partial or complete nephrectomy • 2 types of approach  Loin  Transabdominal • Vascular control by first ligation of renal artery and then ligation of renal vein
  • 23. Indications 1. Bilateral RCC 2. RCC in a solitary functioning kidney 3. Unilateral RCC with contralateral kidney under threat of its future function 4. Tumour less than 4cms with normal opposite kidney. 5. Five year survival rate 75% to 85% 6. Local tumour recurrence of 10% is reported. Other Approaches 1. Radio frequency ablations 2. Cryoablation Nephron Sparing Surgery
  • 24. • Gold standard treatment for localized RCC with contralateral normal kidney, adequate surgical margin. • Principles of Surgery- Early ligation of renal artery and vein , removal of kidney including Gerota’s fascia, removal of ipsilateral adrenal gland, regional lymphadenectomy from crus of diaphragm to aortic bifurcation. Radical nephrectomy
  • 25.
  • 26. Prognosis • In operable cases, 70% of patients are well after three years and 60% after five years. • Worse prognosis – - Macroscopic involvement of the renal vein or its tributaries - Invasion beyond the capsule - Lymphatic involvement
  • 27. Transitional Cell Carcinoma of Kidney • Less common • May invade the renal parenchyma, be multifocal and metastasize. • Multiple ureteric tumours are thought to arise from a field change that predisposes the whole urothelium to metaplasia rather than seeding down the ureter. • Carcinogen is chemical or viral is uncertain
  • 28.
  • 29. Diagnostic Work Up • Clinical - Haematuria • Investigations : Presence of malignant cells in the urine may indicate well or poorly differentiated. Obtain cells from the tumour by sampling using a brush or catheter Intravenous urography Retrograde pyelography
  • 30.
  • 31. Treatment • Conventional surgical - nephroureterectomy. • Conservative resection - well-differentiated upper urinary tract transitional tumours
  • 32. Squamous Cell Carcinoma of Kidney • This is rare and often associated with chronic inflammation and leucoplakia resulting from stone. • The tumours are radiosensitive but metastasise early • Prognosis is poor
  • 34. • Rare before 50 years old. • Male > Female • 95% of primary bladder tumor originate in transitional epithelium (TCC) • Secondary tumors : Sigmoid & rectum, prostate, uterus or ovaries • Histological Types : Urothelial, Squamous and Adenocarcinoma INTRODUCTION
  • 35. • Cigarette Smoking (40%) • Long term use Analgesic • Occupational risk factors - Textile, Dye, Tyre rubber, Petrol etc. • SCC: Schistosoma Haematobium (in Endemic areas), usage of catheter, bladder stone. RISK FACTORS
  • 36. • Hematuria. Painless, end micturition • Bladder Outlet Obstruction (Male) • Cystitis (Female) • Constant pain in Pelvis • Referred pain to suprapubic region, groins, perineum, anus & into thigh • Loss of Weight, Loss of Appetite CLINICAL FEATURES
  • 37. • Usually negative • Maybe a palpable suprapubic mass • Rectal Examination: - May reveal large tumors (Invaded pelvic side walls) • Bimanual Examination: - Necessary for staging evaluation. PHYSICAL EXAMINATION
  • 38. • URINE • BLOOD • IMAGING INVESTIGATIONS
  • 39. URINE TESTS  Urine FEME - Hematuria, WBC  Urine Cytology - Malignant cell.  Urine CnS - To rule out Infection INVESTIGATIONS
  • 40. BLOOD TEST • Full Blood Count • Renal Profile • Liver Function Test • Random Blood Sugar • Coagulation Profile • Prostate Specific Antigen (PSA) • GXM and GSH
  • 41. IMAGING Ultrasound/IVU – Most common defect: Filling defect – Irregularity of bladder wall (Invasive tumor) Contrast CT/MRI – For staging – Demonstrate lymph node & muscular invasion Cystourethroscopy – Mainstay of Diagnosis
  • 42. Ultrasound of Bladder • Irregular, echogenic mass
  • 43.
  • 45. Cystoscopy of Bladder Cancer See the cauliflower appearance of the tumor?
  • 46. • Carcinoma In Situ Superficial Tumor • Ta. Confined to urothelium • T1. Lamina propia involvement Invasive Tumor • T2a. Sup. Muscle involvement • T2b. Deep muscle involvement • T3a. Invades perivesicle tissue microscopically • T4. Extravesicle mass (macro) Fixed Tumor • T4a. Prostate, uterus, vagina • T4b. Fixed to pelvic wall. STAGING (UICC SYSTEM)
  • 47. STAGING • Stage 0. pTa & TIS • Stage 1. T1N0M0 • Stage 2. T2N0M0 • Stage 3. T3 (a/b) • Stage 4. Any metastasis
  • 48.  Superficial Tumor (Ta, T1)  Invasive Tumor ( T2, T3)  Fixed & Metastatic Tumor (T4) - Poor prognosis MANAGEMENT
  • 49. 1. Superficial Tumor (pTa, pT1) • Trans Urethral Resection Bladder Tumor (TURBT) and send tissue for HPE • pT1 - Repeat Cystoscopy & resection of tumor base after 6 weeks - Followed by Intravesical BCG Regular follow up for cystoscopic exam : Every 3monthly for 3 years -> 6 monthly for 2 years
  • 50. Trans Urethral Resection Bladder Tumor (TURBT)
  • 51. TURBT
  • 52. Cystoscopy • Endoscopy of the urinary bladder
  • 53. Intravesical Chemo/Immunotherapy • Used after TURBT for Stage 0 or Stage 1 Ca. • It’s used only for early stage Ca – affect mainly the cell lining inside bladder, no effects on cells elsewhere. • BCG : Is put directly into bladder through a catheter- attract immune system cells to the bladder –attack the cancer cells.
  • 54. 2. Invasive Tumor (pT2, pT3) • Partial Cystectomy. Limited to small adenocarcinoma • Radical Cystectomy. - Followed by chemotherapy/radiotherapy - Localised pT2-3 that has no spread and CIS refractory to BCG, Pt >70 years old • Neoadjuvant Chemotherapy. To shrink tumor before surgery • Chemotherapy & Radiotherapy. Unfit, Older or decline cystectomy
  • 55. • Orthotopic Bladder Replacement. If urethra can be retained, reconstruct new bladder from intestine • Ileal Conduit.
  • 56. 3. Metastatic Tumor (pT4) • Poor prognosis. Incurable • Palliative. No surgery • Treat with chemotherapy
  • 57. PROGNOSIS • Mucosal Tumor- 50-60% 5 years survival • Deep muscle invasion: 20-30% 5 years survival rate • Overall 1/3 patient survive for 5 years
  • 59. Epidemiology • Age > 65 years old • 10-15% of younger men with positive family history but unclear etiology • Rates of clinically evident disease are low in Japan & China • In Malaysia :6th among top 10 cancers for men
  • 60. Risk Factors • Age >65 years old • Family history :first degree relatives • Hormonal : high testosterone • Exposure to cadmium
  • 61. Pathology • Almost all adenocarcinoma • Origin : peripheral zones of prostatic glands • Gleason scoring – degree of glandular differentiation & relationship to stroma
  • 62.
  • 63. Mode of presentation i. Found on autopsy or at cystoprostatectomy ii. Accidental findings during TURP (T1a & T1b) or by PSA (T1c) iii. Early, palpable, localised prostate cancer (T2) iv. Advanced local prostate cancer (T3 & T4) v. Metastatic disease
  • 64. Spread Local • Seminal vesicle • Bladder : neck & trigone • Lower end of ureter • rectum Hematogenous • Bone Lymphatics • External iliac • Internal iliac • Mediastinal • supraclavicular
  • 65. Clinical Features - History • Asymptomatic – screening by per rectal examination and PSA - Suspiciously raised serum PSA - Found on histological examination after TURP • Only advanced disease gives rise to symptoms, but even advance disease may be asymptomatic
  • 66. • Symptoms of advanced disease - Bladder outlet obstruction - Pelvic pain & hematuria - Bone pain - Renal failure
  • 67. Clinical Features – Physical Examination • Sign of anaemia • Nodular, irregular, stony hard, fixed prostate on per rectal examination
  • 68. TNM Staging TUMOUR • T1 – clinically inapparent tumour neither palpable nor visible by imaging • T2a – tumour confined within prostate & 1 lobe T2b – tumour involved both lobes • T3 – tumour extends through prostate capsule T3a – uni or bilateral extension T3b – seminal vesicle extension • T4 – tumour is fixed or invades adjacent structure other than seminal vesicles
  • 69.
  • 70. NODAL • N1 – lymph node metastasis METASTASIS • M1 – distant metastasis * If prostate Ca is palpable it is incurable
  • 71. Investigations Diagnostic • Prostate Specific Antigen (PSA) - Cancer detection rate 2-4% - Lack sensitivity & specificity - 30% men with PSA, cancer confirmed by biopsy - 20% men with prostate Ca have normal PSA - Good at following course of advanced disease
  • 72. • Also raised in : Acute Urinary Retention, TURP, prostatitis, large BPH, catheterization Level Possibility <4ng/ml Normal 4-10ng/ml Benign prostate hyperplasia, prostatitis >10ng/ml Suggestive malignancy >35ng/ml Diagnostic for advanced cancer >100ng/ml Distant bone metastasis
  • 73. • Trans-rectal ultrasound (TRUS) - Image the prostate irrespective findings on palpation - Guide transrectal needle biopsy - Diagnosis of locally extensive disease (T2) • Prostate biopsy (transrectal) - Take multiple biopsy - If patient has bladder outlet obstruction, then can do transurethral resection of prostate (TURP)
  • 74. Transrectal US showing normal seminal vesicles Transrectal US showing local extension of T3 prostate cancer
  • 75. Obtaining a specimen of prostatic tissue by means of a biopsy needle
  • 76. Investigation Routine • Full blood count - Anaemia (leucoerytroblastic anaemia, renal failure or hematuria) - Thrombocytopenia (DIC) • Liver function test - Abnormal if liver metastasis present (ALP in both bone & liver metastasis)
  • 77. • Chest X-ray - Lung metastasis • Pelvic & lumbar X-ray - Sclerotic / osteolytic metastasis in lumbar vertebrae & pelvic bones • MRI/CT scan - Local staging, node & metastasis
  • 78. Osseous metastasis of the pelvic bones in carcinoma of the prostate
  • 79. • Bone scan - After establish diagnosis, as part of diagnosis - If PSA >10nmol/ml or biopsy showed high grade cancer - If PSA <10nmol/ml with clinical indication
  • 80. Bone scan showing multiple hot spots suggestive of metastatic disease in a man with prostate cancer
  • 81. Management Treatment Modalities • Surgery – radical prostectomy - Removal of whole prostate until distal sphincter & seminal vesicle - Complications : impotence, stress incontinence
  • 82. • Radiotherapy - External Beam : T1, T2, locally advanced T3 - Brachytherapy : T1 disease (Iodine 125, Palladium 103) - General radiotherapy : for metastasis
  • 83. • Androgen ablation - Orchidectomy : bilateral, subscapular - Medical : LHRH agonist like goserelin : anti androgen like flutamide, bicalutamide or cyproterone - Anti androgen drugs can cause hormone resistance & hepatotoxic
  • 84. Treatment Summary • At any stage, transurethral resection for bladder outlet obstruction Stage T1 & T2 - Active monitoring or radical local treatment i.e. prostectomy or radiotherapy Stage T3 - Radiotherapy, often with neoadjuvant or adjuvant hormonal therapy
  • 85. Stage T4 - Anti androgen therapies (bilateral orchidectomy) plus - Radiotherapy ; painful bone metastases or spinal cord compression or - Drug treatment with LHRH agonist anti androgen drugs
  • 87. Epidemiology • Uncommon malignancy • Elderly man, 50-70 years old • Mostly squamous cell carcinoma, other rare carcinomas are melanoma, haemangiosarcoma or fibrosarcoma
  • 88. Aetiology & Risk Factors • Phimosis - Circumcision at birth confer’s immunity & at later ages has no immunity • Pre cancerous lesion : - Genital warts : HPV, condyloma acuminate - Leucoplakia, Paget’s Disease of the penis - Bowen’s Disease (carcinoma in situ)
  • 89. • Poor hygiene & smoking • Chronic inflammatory condition of the penis (balanophostitis)
  • 90. Pathology • Typically squamous cell carcinoma arising from skin of the glans/prepuce • May be flat & infiltrating - arises from leukoplakia • Papillary projections – exists from papilloma, more common
  • 91. Penile squamous cell carcinoma appearing as a reddish, raised, and firm nodule in the inner portion of the foreskin
  • 92. Spread • Direct spread • Lymphatic spread • Blood spread
  • 93. Clinical Features • Many present late (due to embarrassment/ misdiagnosis) • Growth is often large with foul bloody discharge (2nd infection) • Typically little/no pain • 50% have inguinal lymph node enlargement, often reflects infection • The prepuce is non-retractile & must be split to view the lesion
  • 94. A squamous cell cancer of the penis with an ulcerating groin node
  • 95. • The whole glans may be replaced by fungating mass (untreated) • Later, the inguinal nodes can erode the skin of the groin
  • 96. Physical Examination • Site : glans penis or inner surface of foreskin • Inspection - Painless ulcer, irregular margin, rolled edges & indurated or gray, crusted popular lesion - Bleeding & yellowish discharge can be seen
  • 97. • Palpation - Firm to hard - Retract foreskin ( some are found under the foreskin ) - Check for phimosis - Feel for inguinal lymph nodes
  • 98. Staging • Jackson’s staging Stage 1 Tumour confined to the glans/ prepuce Stage 2 Tumour invade shaft or corpora but no nodes involvement Stage 3 Tumour confined to the penis & operable nodes involvement Stage 4 Tumour involves adjacent structures & inoperable nodes metastasis
  • 99. TNM staging Tumour Tis : carcinoma in situ Ta : noninvasisve verrucous tumour T1 : Tumour invading subepitelial connective tissue T2 : Tumour invading corpora T3 : tumour invading urethra or prostate T4 : tumour invading other adjacent structures
  • 100. Node N1 : 1 superficial inguinal lymph node N2 : multiple bilateral inguinal lymph nodes N3 : deep inguinal & pelvic lymph nodes, bilateral or unilateral Metastasis M1 : distant metastasis
  • 101. A late presenting squamous cell cancer of the penis
  • 102. Investigations (special) • Punch or excisional biopsy of the lesion • Fine needle aspiration for palpable lymph nodes • CT/MRI to evaluate metastasis
  • 103. Management • Divided into treatment of primary tumour & inguinal lymph nodes • Primary treatment : 2 methods i. Radiotherapy - Indicated for small & well differentiated growth limited to penis glans - Disadvantage : scarring caused painful erection
  • 104. ii. Surgery - Indicated : anaplastic growth, big growth, infiltrate shaft of penis & radiotherapy failed - Methods of surgery A. partial amputation of penis : distal growth limited to glans penis & prepuce B. total amputation of penis : lesions affecting the shaft of penis & anaplastic lesions
  • 105. • Secondary tumour – associated with inguinal lymph nodes - No nodes enlarged : follow up carefully - LN enlarged which are not fixed : wait for 3 weeks after treating primary growth - LN enlarged are massive & inoperable : deep radiotherapy is given & may be treated with chemotherapy - Sentinel node biopsy
  • 106. REFERENCES • William NS, Bulstrode CJK, O’connell PR, Cholelithiasis. Bailey & Love’s Short Practice of Surgery. 26th edition, CRC press

Editor's Notes

  1. FBC – Anemia , Urosepsis LFT – Hypoalbunimenia RBS – Hypoglycemia Coagulation Profile – TRO Coagulation ds PSA – TRO Prostat Ca
  2. How is the procedure performed? The procedure requires general or spinal anaesthesia, with patient placed in the gynaecological examination position. Initially, the genital area is cleansed and the urethra lubricated. A special camera is inserted through the urethra searching for abnormal areas of the bladder to be removed with the use of an instrument attached to the camera. This instrument uses heat to remove abnormal tissue. Then the site is cauterized to prevent bleeding. If there is suspicion for malignancy, the surgeon obtains tissue sample for biopsy. At the end of the procedure, a catheter is placed for continuous bladder irrigation with normal saline. The average length of hospital stay is about 3 days, depending on the size of bladder tumor. The catheter is usually removed on the first postoperative day.
  3. It is used only for these early-stage cancers because medicines given this way mainly affect the cells lining the inside of the bladder, with little to no effect on cells elsewhere. This means that any cancer cells outside of the bladder lining, including those that have grown deeply into the bladder wall, are not treated. Drugs put into the bladder also can’t reach cancer cells in the kidneys, ureters, and urethra, or those that have spread to other organs.