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CARCINOMA PENIS
Presenter : DR. RAJGURU SIWACH (P.G. Resident)
Moderator: PROF. DR. SHIVANI B. PARUTHY
ANATOMY
ANATOMY
• Most penile cancers arise from
squamous cell epithelium of the
epidermis and dermis.
• Layers along the shaft are-
1. Skin
2. Dartos fascia
3. Bucks fascia
4. Vessels(dorsal artery and vein)
5. Tunica albuginea
6. Corpus cavernosum
LYMPHATIC DRAINAGE
• The lymphatic drainage of the
penis occurs principally to the
inguinal lymph nodes in each
groin.
• Lymphatic drainage has no
predictable laterality of drainage
patterns with cross-over
occurring in 60-85% of cases.
PREMALIGNANT CUTANEOUS
LESIONS
Carcinoma in situ (Penile Intraepithelial
Neoplasia)
• It is called Erythroplasia of Queyrat (EQ)
if it involves the glans penis and prepuce.
• It is called Bowen disease (BD) if it
involves the penile shaft or the
remainder of the genitalia or perineal
region.
• Progression to invasive carcinoma in men
with BD and EQ may occur in 5% to 33%
of patients, respectively, if it is not
treated.
Bowen disease involving penile
shaft skin.
Non–HPV Related Penile Premalignant
Lesions
1.Cutaneous Horn
• The horn resembles that of an animal and
is characterized by overgrowth and
cornification of the epithelium, which
forms a solid protuberance.
• Tumor may evolve into a carcinoma or may
develop as a result of an underlying
carcinoma.
• Careful histologic evaluation of the base
and close follow-up of the excision site are
essential.
2. Male Lichen Sclerosus (Balanitis Xerotica Obliterans)
• Whitish patch on the prepuce or
glans, often involving the meatus.
• The meatus may appear white,
indurated, and edematous.
• Glanular erosions, fissures, and
meatal stenosis may occur.
BXO
• Symptoms include pain, dyspareunia, pruritus, painful erections, and
urinary obstruction.
• Associated with development of squamous cell carcinoma.
• Almost never occurs in males circumcised at birth, thus implicating that
closed, moist preputial environment is permissive for the disease.
• Treatment involves clobetasol propionate cream for 2 to 3 months.
• Meatal stenosis may require repeated dilations, corticosteroid injection, or
even formal reconstructive surgery.
Virus-Related Penile Lesions
1.Condylomata acuminata
• Soft, papillomatous growths
typically considered benign.
• Also known as genital warts or
venereal warts.
• They have a predilection for the
moist, glabrous areas of the
body and the mucocutaneous
surfaces of the perineal and
genital areas.
• Human immunodeficiency virus (HIV) infection may predispose
affected patients to rapid development of squamous carcinoma from
preexisting condyloma infection.
• Subclinical disease may be detected by the application of 5% acetic
acid solution to the penis, followed by inspection with a magnifying
glass.
• Lesions will turn white, and flat lesions often invisible on regular
inspection may be detected.
• Treatment options-
(1) Podophyllotoxin 0.5% solution or gel (used historically),
(2) Trichloroacetic acid 35% to 85%,
(3) Cryotherapy with liquid nitrogen,
(4) Electrofulguration,
(5) CO2 laser therapy, and
(6) Imiquimod 5% cream
Treatment options-
• Imiquimod cream (5%) has become the topical treatment of choice
for condyloma. Imiquimod is an immune modulator that enhances
natural killer cell activity.
• Intraurethral lesions may be extremely difficult to treat. 5-
Fluorouracil cream applied weekly for 3 weeks has been successful in
eliminating urethral lesions.
• To avoid exposure of the scrotal skin. Use of a scrotal support or zinc
oxide cream may be helpful.
2. Buschke-Löwenstein Tumor (Giant Condyloma
Acuminatum)
• It differs from condyloma acuminatum
in that condylomata, regardless of
size, always remain superficial and
never invade adjacent tissue.
• Buschke-Löwenstein tumor displaces,
invades, and destroys adjacent
structures by compression.
• Aside from unrestrained local growth,
it does not metastasize.
3.Kaposi Sarcoma
• Kaposi sarcoma, first described in 1972, is a tumor of the
reticuloendothelial system
• It appears as a cutaneous neovascular lesion, a raised, painful,
bleeding papule or ulcer with bluish discoloration
• Kaposi sarcoma is now subcategorized as follows:
• (1) Classic Kaposi sarcoma
• (2) Immunosuppressive treatment–related Kaposi sarcoma
• (3) African Kaposi sarcoma
• (4) Epidemic or HIV-related Kaposi sarcoma
• Nonepidemic Kaposi sarcoma- Localized surgical excision/partial
penectomy.
• In the immunosuppressed patient, it often regresses with the
discontinuation of immunosuppressive therapy.
• In the patient with AIDS, partial or total penectomy may be necessary.
• Radiation therapy and the neodymium:yttriumaluminum-garnet
(Nd:YAG) laser is used to alleviate distal urethral obstruction.
SQUAMOUS CELL CARCINOMA
SQUAMOUS CELL CARCINOMA
• Penile carcinoma accounts for 0.4% to 0.6% of all malignant
neoplasms among men in the United States and Europe;
• It may represent up to 10% of malignant neoplasms in men in some
Asian, African, and South American countries.
• Penile cancer is a disease of older men, with an abrupt increase in
incidence in the sixth decade of life.
SQUAMOUS CELL CARCINOMA
• The incidence of carcinoma of the penis varies according to
circumcision practice, hygienic standards, phimosis, number of sexual
partners, HPV infection and exposure to tobacco products.
• Thus far, there is no evidence to link penile cancer with factors such
as occupation, other venereal diseases (gonorrhea, syphilis, and
herpes), marijuana use, or alcohol intake.
Risk factors
• The chronic irritative effects of smegma, a byproduct of bacterial
action on desquamated cells that are within the preputial sac, have
been proposed as a causative agent.
• Incidence of HPV infection directly correlated with the number of
lifetime sexual partners, which was also related to risk of penile
cancer.
• All forms of tobacco products, including cigarettes and chewing
tobacco, were significantly and independently related to the
incidence of penile cancer.
Risk factors (cntd.)
• Penile trauma is another risk factor for penile cancer.
• There is odds ratio of 18:1 for the development of penile cancer for
those men reporting a penile injury within 2 years of the onset of the
disease.
• Lichen sclerosus (balanitis xerotica obliterans) is also a risk factor for
the development of penile cancer.
Prevention
• Routine neonatal circumcision as a preventive strategy for penile
cancer.
• Good hygiene
• Avoidance of HPV infection.
• Avoidance of tobacco products.
Prevention
• Prophylactic HPV vaccines-
• Cervarix, the quadrivalent HPV 16/18/6/11 vaccine.
• Gardasil, 9 HPV 16/18/6/11/31/33/45/52/58 vaccine.
• They have efficacy in preventing HPV infection among HPV-negative young
women and men
• Adult circumcision appears to offer little or no protection from
subsequent development of the disease.
Clinical Presentation
• Penile lesion- ranges from a subtle induration or small papule,
pustule, warty growth, to large exophytic lesion.
• Penile tumors occur most commonly on the glans (48%) and
prepuce (21%).
• Urinary retention or urethral fistula from local corporeal
involvement is a rare presenting sign.
• Rarely, a mass, ulceration or hemorrhage in the inguinal area may
be caused by nodal metastases from a lesion concealed within a
phimotic foreskin.
• Occasionally, blood loss may occur from the penile lesion.
• Weakness, weight loss, fatigue, and systemic malaise may occur
secondary to chronic suppuration.
• Pain does not develop in proportion to the extent of the local
destructive process and usually is not a presenting complaint.
DELAY IN DIAGNOSIS
• Delay seeking medical attention- because of embarrassment, guilt,
fear, ignorance, and personal neglect.
• Delay on the part of the physician- patients have been given
prolonged courses of antibiotics or topical antifungal preparations
before being referred for biopsy.
• Earlier diagnosis and treatment should improve outcome.
Biopsy
• It is gold standard for the confirmation of the diagnosis of carcinoma
of the penis.
• HPE- keratinization, epithelial pearl formation, and various degrees of
mitotic activity.
• Pathologic description of anatomic structures invaded (i.e., stage),
the grade, and the status of vascular and perineural invasion provide
important information to assess the risk of metastasis.
Radiological Imaging
• Soft-tissue detail of penile tumors is best imaged by MRI.
• Penile MRI in combination with artificial erection provide accurate
staging information.
• Physical examination of the inguinal region is used for evaluation of
the lymph node metastasis in the nonobese patient.
• CT or MRI can be useful in evaluating the inguinal region of obese
patients and in those who have had prior inguinal surgery.
• PET/CT is useful among patients with clinically palpable inguinal
lymph nodes to define the presence of pelvic or distant metastasis.
TNM staging
TNM STAGING
Prognosis
• Stage of the disease at the time of diagnosis helps predict the
prognosis of the disease
STAGE OF DISEASE 5 YEAR SURVIVAL RATE
STAGE I or II 85% after surgical management
Stage III 59%
STAGE IV 11%
Management
1. Management of the primary penile tumour
2. Inguinal lymph nodes
a. Non-palpable
b. Palpable
3. Metastatic disease
a. Chemotherapy
b. Radiation therapy
4. Surveillance strategies
SURGICAL MANAGEMENT
• Organ preservation
• Goal of treatment is to preserve glans sensation and penile shaft length.
• Patients with penile primary tumors exhibiting favorable histologic features (stages
Tis, Ta, T1; grade 1 and grade 2 tumors)
• Should be considered to be at a higher risk for local recurrence and require longer-
term follow-up.
• A 2-cm margin may not be necessary for small tumors of lower grade in the presence
of a negative frozen section.
• Penile amputation
• Mohs surgery- It involves sequential excision of tissue layers with
concurrent microscopic examination of the undersurface of each layer
to ensure negative margins.
• Glans resurfacing- Subdermal dissection of the skin and subepithelial
connective tissue off the underlying corpus spongiosus is performed.
Partial penectomy
Total penectomy
TREATMENT OF THE INGUINAL NODES
• The presence and extent of inguinal metastases determine
survival in penile cancer.
• For treatment of inguinal lymph nodes, patients can be divided
into-
• Low risk patients (Tis, Ta, T1a)
• High risk patients (T1b- T4)
• Nonpalpable lymph nodes
• Palpable lymph nodes
High risk patients- non palpable inguinal L.N.
• High risk criteria for inguinal lymph node metastases include-
• Clinical stage T2 or greater
• Greater than 50% poorly differentiated(high grade) tumour
• Presence of lympho-vascular invasion
• Treatment approach-
• Bilateral superficial inguinal lymph node dissection(SILND) +/- deep ILND if
any lymph nodes are identified on the SILND.
• Bilateral DSNB (less common)
High risk patients- palpable inguinal L.N.
POSITIVE IPSILATERAL INGUINAL L.N. (T1b- T4)
• Follow positive algorithm
(i) Ipsilateral inguinal L.N. (superficial + deep) dissection
(ii)Pelvic node dissection
(iii) Contralateral superficial inguinal dissection(frozen section analysis)
• A pelvic lymph node dissection (PLND) should be considered in
patients with-
1. Two or more inguinal lymph nodes with metastases
2. Presence of inguinal lymph node metastasis > 3 cm
3. Presence of inguinal extranodal extension
• A bilateral, rather than unilateral pelvic lymph node dissection should
be contemplated if 4 or more inguinal lymph nodes harbour
metastatic disease.
• PLND serves as an effective staging tool for identifying patients with
pelvic metastases in whom adjunctive therapy should be considered.
SENTINEL LYMPH NODE BIOPSY
• Dynamic Sentinel Node Biopsy (DSNB)-
The goal of DSNB is to define where in the inguinal lymph node field
the sentinel lymph node resides through use of a combination of visual
(vital blue dyes) or gamma emission (hand-held gamma probe)
techniques at the time of surgery.
• The technique involves intradermal injection of a vital blue dye or
technetium-labeled colloid adjacent to the lesion. The dye (or
radioactive tracer) is transported by the afferent lymphatics to a
specific node in the regional nodal basin. This node is designated the
sentinel lymph node.
Superficial Inguinal Lymph Node Dissection
(SILND)
• This technique consists of removal of the ILNs that are located above
the fascia lata.
• The rationale is that if the lymph nodes in the superficial
compartment are negative, there should be no involvement of the
deep package.
Inguinal lymph node dissection
• Incisions for inguinal lymph node dissection
Radical inguinal lymph node dissection
• It is done 4-6 weeks after surgical treatment of the primary tumour
• Extent-
• Superiorly- a line drawn from margin of the external ring to the anterior
superior iliac spine.
• Laterally- by a line drawn from the anterior superior iliac spine extending 20
cm inferiorly.
• Medially- by a line drawn from the pubic tubercle 15 cm down the medial
thigh.
• Superior and inferior limits of dissection
Complications:
• Seroma formation
• Lymphocoele
• Wound infection or necrosis
• Lymphedema
• Flap necrosis
RADIOTHERAPY
• Primary radiation therapy has curative potential and may permit
preservation of penile form and function.
• Before radiation therapy, circumcision is necessary to expose the
lesion, and to prevent preputial edema and subsequent phimosis.
• Types-
• External-Beam Radiotherapy
• Brachytherapy
• Brachytherapy can provide better local control and penile preservation with
faster dose delivery (4 to 5 days rather than 6-7 weeks) compared with
external beam radiotherapy.
• T1 and T2 tumors smaller than 4 cm with no or minimal extension beyond
the coronal sulcus are appropriate for radiotherapy.
• Unresectable lymph nodes may be rendered operable by neoadjuvant
chemoradiation.
• The two most common late side effects associated with radiotherapy are
meatal stenosis and soft-tissue ulceration.
• Neoadjuvant radiation
• Fixed inguinal lymph nodes positive for metastases
• Adjuvant radiation
• After circumcision-
• T1,T2 N0 disease
• EBRT +/- Chemotherapy
• After pelvic lymph node dissection-
• Multiple positive LN
• LN >4cm
• ENE
• B/L pelvic LN
CHEMOTHERAPY
• Neoadjuvant chemotherapy with a cisplatin-containing regimen should be
considered for patients with lymph node metastases, as responses in this
setting may facilitate curative resection.
• Surgical consolidation to achieve disease-free status or palliation should be
considered in fit patients with a proven objective response to systemic
chemotherapy.
• Among patients who progress through chemotherapy, surgery is not
recommended.
SURVEILLANCE
MANAGEMENT OF RECURRENT DISEASE
NONSQUAMOUS MALIGNANT NEOPLASMS
• Basal cell carcinoma represents a highly curable variant with a relatively low
metastatic potential.
• Sarcomas are prone to local recurrence; regional and distant metastases are rare.
Superficial lesions can be treated with less radical procedures.
• Melanoma is an aggressive form of cancer but can be cured if diagnosed and
treated with the appropriate surgical procedure at an early stage.
• Penile metastases most often represent spread from a clinically obvious existing
primary tumor. Prognosis is poor, and therapy should be directed toward the
primary tumor site histology and local palliation.
• (A) Basal cell carcinoma, (B) Melanoma, (C) Leiomyosarcoma, (D) Paget
disease
CONCLUSION
• Penile sparing surgical approaches should be considered for lower
grade/ stage primary penile tumours in favourable anatomic sites.
• Patients exhibiting high risk primary penile tumours should have
their inguinal lymph nodes evaluated to r/o occult disease (even in
absence of palpable adenopathy).
CONCLUSION
• Bulky inguinal adenopathy in the context of penile SCC should be
considered for multimodal therapy consisting of upfront systemic
therapy followed by consolidative surgical resection (in patients with
favourable response).
• Locally recurrent inguinal nodal metastases (post ILND) should be
considered for upfront systemic therapy (+/- XRT).
Thank you

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Carcinoma penis

  • 1. CARCINOMA PENIS Presenter : DR. RAJGURU SIWACH (P.G. Resident) Moderator: PROF. DR. SHIVANI B. PARUTHY
  • 3. ANATOMY • Most penile cancers arise from squamous cell epithelium of the epidermis and dermis. • Layers along the shaft are- 1. Skin 2. Dartos fascia 3. Bucks fascia 4. Vessels(dorsal artery and vein) 5. Tunica albuginea 6. Corpus cavernosum
  • 4.
  • 5. LYMPHATIC DRAINAGE • The lymphatic drainage of the penis occurs principally to the inguinal lymph nodes in each groin. • Lymphatic drainage has no predictable laterality of drainage patterns with cross-over occurring in 60-85% of cases.
  • 6.
  • 8. Carcinoma in situ (Penile Intraepithelial Neoplasia) • It is called Erythroplasia of Queyrat (EQ) if it involves the glans penis and prepuce. • It is called Bowen disease (BD) if it involves the penile shaft or the remainder of the genitalia or perineal region. • Progression to invasive carcinoma in men with BD and EQ may occur in 5% to 33% of patients, respectively, if it is not treated. Bowen disease involving penile shaft skin.
  • 9. Non–HPV Related Penile Premalignant Lesions 1.Cutaneous Horn • The horn resembles that of an animal and is characterized by overgrowth and cornification of the epithelium, which forms a solid protuberance. • Tumor may evolve into a carcinoma or may develop as a result of an underlying carcinoma. • Careful histologic evaluation of the base and close follow-up of the excision site are essential.
  • 10. 2. Male Lichen Sclerosus (Balanitis Xerotica Obliterans) • Whitish patch on the prepuce or glans, often involving the meatus. • The meatus may appear white, indurated, and edematous. • Glanular erosions, fissures, and meatal stenosis may occur.
  • 11. BXO • Symptoms include pain, dyspareunia, pruritus, painful erections, and urinary obstruction. • Associated with development of squamous cell carcinoma. • Almost never occurs in males circumcised at birth, thus implicating that closed, moist preputial environment is permissive for the disease. • Treatment involves clobetasol propionate cream for 2 to 3 months. • Meatal stenosis may require repeated dilations, corticosteroid injection, or even formal reconstructive surgery.
  • 12. Virus-Related Penile Lesions 1.Condylomata acuminata • Soft, papillomatous growths typically considered benign. • Also known as genital warts or venereal warts. • They have a predilection for the moist, glabrous areas of the body and the mucocutaneous surfaces of the perineal and genital areas.
  • 13. • Human immunodeficiency virus (HIV) infection may predispose affected patients to rapid development of squamous carcinoma from preexisting condyloma infection. • Subclinical disease may be detected by the application of 5% acetic acid solution to the penis, followed by inspection with a magnifying glass. • Lesions will turn white, and flat lesions often invisible on regular inspection may be detected.
  • 14. • Treatment options- (1) Podophyllotoxin 0.5% solution or gel (used historically), (2) Trichloroacetic acid 35% to 85%, (3) Cryotherapy with liquid nitrogen, (4) Electrofulguration, (5) CO2 laser therapy, and (6) Imiquimod 5% cream
  • 15. Treatment options- • Imiquimod cream (5%) has become the topical treatment of choice for condyloma. Imiquimod is an immune modulator that enhances natural killer cell activity. • Intraurethral lesions may be extremely difficult to treat. 5- Fluorouracil cream applied weekly for 3 weeks has been successful in eliminating urethral lesions. • To avoid exposure of the scrotal skin. Use of a scrotal support or zinc oxide cream may be helpful.
  • 16. 2. Buschke-Löwenstein Tumor (Giant Condyloma Acuminatum) • It differs from condyloma acuminatum in that condylomata, regardless of size, always remain superficial and never invade adjacent tissue. • Buschke-Löwenstein tumor displaces, invades, and destroys adjacent structures by compression. • Aside from unrestrained local growth, it does not metastasize.
  • 17. 3.Kaposi Sarcoma • Kaposi sarcoma, first described in 1972, is a tumor of the reticuloendothelial system • It appears as a cutaneous neovascular lesion, a raised, painful, bleeding papule or ulcer with bluish discoloration • Kaposi sarcoma is now subcategorized as follows: • (1) Classic Kaposi sarcoma • (2) Immunosuppressive treatment–related Kaposi sarcoma • (3) African Kaposi sarcoma • (4) Epidemic or HIV-related Kaposi sarcoma
  • 18. • Nonepidemic Kaposi sarcoma- Localized surgical excision/partial penectomy. • In the immunosuppressed patient, it often regresses with the discontinuation of immunosuppressive therapy. • In the patient with AIDS, partial or total penectomy may be necessary. • Radiation therapy and the neodymium:yttriumaluminum-garnet (Nd:YAG) laser is used to alleviate distal urethral obstruction.
  • 20. SQUAMOUS CELL CARCINOMA • Penile carcinoma accounts for 0.4% to 0.6% of all malignant neoplasms among men in the United States and Europe; • It may represent up to 10% of malignant neoplasms in men in some Asian, African, and South American countries. • Penile cancer is a disease of older men, with an abrupt increase in incidence in the sixth decade of life.
  • 21. SQUAMOUS CELL CARCINOMA • The incidence of carcinoma of the penis varies according to circumcision practice, hygienic standards, phimosis, number of sexual partners, HPV infection and exposure to tobacco products. • Thus far, there is no evidence to link penile cancer with factors such as occupation, other venereal diseases (gonorrhea, syphilis, and herpes), marijuana use, or alcohol intake.
  • 22. Risk factors • The chronic irritative effects of smegma, a byproduct of bacterial action on desquamated cells that are within the preputial sac, have been proposed as a causative agent. • Incidence of HPV infection directly correlated with the number of lifetime sexual partners, which was also related to risk of penile cancer. • All forms of tobacco products, including cigarettes and chewing tobacco, were significantly and independently related to the incidence of penile cancer.
  • 23. Risk factors (cntd.) • Penile trauma is another risk factor for penile cancer. • There is odds ratio of 18:1 for the development of penile cancer for those men reporting a penile injury within 2 years of the onset of the disease. • Lichen sclerosus (balanitis xerotica obliterans) is also a risk factor for the development of penile cancer.
  • 24. Prevention • Routine neonatal circumcision as a preventive strategy for penile cancer. • Good hygiene • Avoidance of HPV infection. • Avoidance of tobacco products.
  • 25. Prevention • Prophylactic HPV vaccines- • Cervarix, the quadrivalent HPV 16/18/6/11 vaccine. • Gardasil, 9 HPV 16/18/6/11/31/33/45/52/58 vaccine. • They have efficacy in preventing HPV infection among HPV-negative young women and men • Adult circumcision appears to offer little or no protection from subsequent development of the disease.
  • 26. Clinical Presentation • Penile lesion- ranges from a subtle induration or small papule, pustule, warty growth, to large exophytic lesion. • Penile tumors occur most commonly on the glans (48%) and prepuce (21%). • Urinary retention or urethral fistula from local corporeal involvement is a rare presenting sign. • Rarely, a mass, ulceration or hemorrhage in the inguinal area may be caused by nodal metastases from a lesion concealed within a phimotic foreskin.
  • 27. • Occasionally, blood loss may occur from the penile lesion. • Weakness, weight loss, fatigue, and systemic malaise may occur secondary to chronic suppuration. • Pain does not develop in proportion to the extent of the local destructive process and usually is not a presenting complaint.
  • 28. DELAY IN DIAGNOSIS • Delay seeking medical attention- because of embarrassment, guilt, fear, ignorance, and personal neglect. • Delay on the part of the physician- patients have been given prolonged courses of antibiotics or topical antifungal preparations before being referred for biopsy. • Earlier diagnosis and treatment should improve outcome.
  • 29. Biopsy • It is gold standard for the confirmation of the diagnosis of carcinoma of the penis. • HPE- keratinization, epithelial pearl formation, and various degrees of mitotic activity. • Pathologic description of anatomic structures invaded (i.e., stage), the grade, and the status of vascular and perineural invasion provide important information to assess the risk of metastasis.
  • 30. Radiological Imaging • Soft-tissue detail of penile tumors is best imaged by MRI. • Penile MRI in combination with artificial erection provide accurate staging information. • Physical examination of the inguinal region is used for evaluation of the lymph node metastasis in the nonobese patient. • CT or MRI can be useful in evaluating the inguinal region of obese patients and in those who have had prior inguinal surgery. • PET/CT is useful among patients with clinically palpable inguinal lymph nodes to define the presence of pelvic or distant metastasis.
  • 33.
  • 34.
  • 35. Prognosis • Stage of the disease at the time of diagnosis helps predict the prognosis of the disease STAGE OF DISEASE 5 YEAR SURVIVAL RATE STAGE I or II 85% after surgical management Stage III 59% STAGE IV 11%
  • 36. Management 1. Management of the primary penile tumour 2. Inguinal lymph nodes a. Non-palpable b. Palpable 3. Metastatic disease a. Chemotherapy b. Radiation therapy 4. Surveillance strategies
  • 37. SURGICAL MANAGEMENT • Organ preservation • Goal of treatment is to preserve glans sensation and penile shaft length. • Patients with penile primary tumors exhibiting favorable histologic features (stages Tis, Ta, T1; grade 1 and grade 2 tumors) • Should be considered to be at a higher risk for local recurrence and require longer- term follow-up. • A 2-cm margin may not be necessary for small tumors of lower grade in the presence of a negative frozen section. • Penile amputation
  • 38.
  • 39.
  • 40.
  • 41. • Mohs surgery- It involves sequential excision of tissue layers with concurrent microscopic examination of the undersurface of each layer to ensure negative margins. • Glans resurfacing- Subdermal dissection of the skin and subepithelial connective tissue off the underlying corpus spongiosus is performed.
  • 44.
  • 45. TREATMENT OF THE INGUINAL NODES • The presence and extent of inguinal metastases determine survival in penile cancer. • For treatment of inguinal lymph nodes, patients can be divided into- • Low risk patients (Tis, Ta, T1a) • High risk patients (T1b- T4) • Nonpalpable lymph nodes • Palpable lymph nodes
  • 46.
  • 47. High risk patients- non palpable inguinal L.N. • High risk criteria for inguinal lymph node metastases include- • Clinical stage T2 or greater • Greater than 50% poorly differentiated(high grade) tumour • Presence of lympho-vascular invasion • Treatment approach- • Bilateral superficial inguinal lymph node dissection(SILND) +/- deep ILND if any lymph nodes are identified on the SILND. • Bilateral DSNB (less common)
  • 48. High risk patients- palpable inguinal L.N. POSITIVE IPSILATERAL INGUINAL L.N. (T1b- T4) • Follow positive algorithm (i) Ipsilateral inguinal L.N. (superficial + deep) dissection (ii)Pelvic node dissection (iii) Contralateral superficial inguinal dissection(frozen section analysis)
  • 49.
  • 50. • A pelvic lymph node dissection (PLND) should be considered in patients with- 1. Two or more inguinal lymph nodes with metastases 2. Presence of inguinal lymph node metastasis > 3 cm 3. Presence of inguinal extranodal extension • A bilateral, rather than unilateral pelvic lymph node dissection should be contemplated if 4 or more inguinal lymph nodes harbour metastatic disease. • PLND serves as an effective staging tool for identifying patients with pelvic metastases in whom adjunctive therapy should be considered.
  • 51.
  • 52. SENTINEL LYMPH NODE BIOPSY • Dynamic Sentinel Node Biopsy (DSNB)- The goal of DSNB is to define where in the inguinal lymph node field the sentinel lymph node resides through use of a combination of visual (vital blue dyes) or gamma emission (hand-held gamma probe) techniques at the time of surgery. • The technique involves intradermal injection of a vital blue dye or technetium-labeled colloid adjacent to the lesion. The dye (or radioactive tracer) is transported by the afferent lymphatics to a specific node in the regional nodal basin. This node is designated the sentinel lymph node.
  • 53. Superficial Inguinal Lymph Node Dissection (SILND) • This technique consists of removal of the ILNs that are located above the fascia lata. • The rationale is that if the lymph nodes in the superficial compartment are negative, there should be no involvement of the deep package.
  • 54. Inguinal lymph node dissection
  • 55. • Incisions for inguinal lymph node dissection
  • 56. Radical inguinal lymph node dissection • It is done 4-6 weeks after surgical treatment of the primary tumour • Extent- • Superiorly- a line drawn from margin of the external ring to the anterior superior iliac spine. • Laterally- by a line drawn from the anterior superior iliac spine extending 20 cm inferiorly. • Medially- by a line drawn from the pubic tubercle 15 cm down the medial thigh.
  • 57.
  • 58. • Superior and inferior limits of dissection
  • 59. Complications: • Seroma formation • Lymphocoele • Wound infection or necrosis • Lymphedema • Flap necrosis
  • 60. RADIOTHERAPY • Primary radiation therapy has curative potential and may permit preservation of penile form and function. • Before radiation therapy, circumcision is necessary to expose the lesion, and to prevent preputial edema and subsequent phimosis. • Types- • External-Beam Radiotherapy • Brachytherapy
  • 61.
  • 62. • Brachytherapy can provide better local control and penile preservation with faster dose delivery (4 to 5 days rather than 6-7 weeks) compared with external beam radiotherapy. • T1 and T2 tumors smaller than 4 cm with no or minimal extension beyond the coronal sulcus are appropriate for radiotherapy. • Unresectable lymph nodes may be rendered operable by neoadjuvant chemoradiation. • The two most common late side effects associated with radiotherapy are meatal stenosis and soft-tissue ulceration.
  • 63. • Neoadjuvant radiation • Fixed inguinal lymph nodes positive for metastases • Adjuvant radiation • After circumcision- • T1,T2 N0 disease • EBRT +/- Chemotherapy • After pelvic lymph node dissection- • Multiple positive LN • LN >4cm • ENE • B/L pelvic LN
  • 64. CHEMOTHERAPY • Neoadjuvant chemotherapy with a cisplatin-containing regimen should be considered for patients with lymph node metastases, as responses in this setting may facilitate curative resection. • Surgical consolidation to achieve disease-free status or palliation should be considered in fit patients with a proven objective response to systemic chemotherapy. • Among patients who progress through chemotherapy, surgery is not recommended.
  • 66.
  • 68.
  • 69. NONSQUAMOUS MALIGNANT NEOPLASMS • Basal cell carcinoma represents a highly curable variant with a relatively low metastatic potential. • Sarcomas are prone to local recurrence; regional and distant metastases are rare. Superficial lesions can be treated with less radical procedures. • Melanoma is an aggressive form of cancer but can be cured if diagnosed and treated with the appropriate surgical procedure at an early stage. • Penile metastases most often represent spread from a clinically obvious existing primary tumor. Prognosis is poor, and therapy should be directed toward the primary tumor site histology and local palliation.
  • 70. • (A) Basal cell carcinoma, (B) Melanoma, (C) Leiomyosarcoma, (D) Paget disease
  • 71. CONCLUSION • Penile sparing surgical approaches should be considered for lower grade/ stage primary penile tumours in favourable anatomic sites. • Patients exhibiting high risk primary penile tumours should have their inguinal lymph nodes evaluated to r/o occult disease (even in absence of palpable adenopathy).
  • 72. CONCLUSION • Bulky inguinal adenopathy in the context of penile SCC should be considered for multimodal therapy consisting of upfront systemic therapy followed by consolidative surgical resection (in patients with favourable response). • Locally recurrent inguinal nodal metastases (post ILND) should be considered for upfront systemic therapy (+/- XRT).