SlideShare una empresa de Scribd logo

Germ cell tumor ovary.pptx

Dr. Abani Kanta Nanda
Dr. Abani Kanta Nanda

This document discusses germ cell tumors of the ovary. It begins by explaining that germ cell tumors originate from primordial germ cells and make up about 90-95% of ovarian malignancies in young women. It then covers the various subtypes of germ cell tumors, including their incidence rates, typical patient demographics, clinical presentations, diagnostic markers, pathological classifications, treatment approaches, and prognosis. Dysgerminoma is discussed as the most common subtype, while immature teratoma, endodermal sinus tumor, embryonal carcinoma, and choriocarcinoma are also described in terms of their defining characteristics and management. Throughout, the focus remains on applying knowledge from testicular germ cell tumor research

Atención sanitaria
1 de 57
Germ Cell Tumor Ovary Dr Abani Kanta Nanda MD Radiation Oncology AHPGIC, Cuttack
(90-95%) (2-3%) (2-8%)
• Germ cell tumors are derived from the primordial germ cells of the ovary. • Occur with only about one-tenth the incidence of malignant germ cell tumors of the testis. • Although they can arise in extragonadal sites such as the mediastinum and the retroperitoneum, the majority of germ cell tumors arise in the gonad from undifferentiated germ cells. • The variation in the site of these cancers is explained by the embryonic migration of the germ cells from the caudal part of the yolk sac to the dorsal mesentery before their incorporation into the sex cords of the developing gonads
• Germ cell tumors are a model of a curable cancer. • The management of patients with ovarian germ cell tumors has largely been extrapolated from the much greater experience of treating males with the more common testicular germ cell tumors. • There have been many randomized trials for testicular germ cell tumors, which have provided a strong evidence base for treatment decision making. • The outcome of patients with testicular germ cell tumors is better in experienced centers, and it is reasonable to suggest the same will be true for the less common ovarian counterparts. • The cure rate is high, and attention is now being directed at reducing toxicity without compromising survival. • There are still a small number of patients who die from the disease, and studies are in progress to try to improve the outcome for this high-risk, poor-prognostic subset
• Murugaesu et al. reported that stage and elevated tumor markers were independent poor prognostic indicators. • These findings are important because they identify similar prognostic factors for ovarian and testicular germ cell tumors, and are in accordance with the clinical observation that testicular and ovarian germ cell tumors behave similarly.
Classification
Embryology
• Ovarian germ cell tumors have a variable pattern of differentiation. • Dysgerminomas are primitive neoplasms that do not have the potential for further differentiation. • Embryonal carcinomas are composed of multipotential cells that are capable of further differentiation. • This lesion is the precursor of several other types of extraembryonic (yolk sac tumor, choriocarcinoma) or embryonic (teratoma) germ cell tumors. • The process of differentiation is dynamic, and the resulting neoplasms may be composed of different elements that show various stages of development (Teilum, 1965).
Serum markers • Both α fetoprotein (AFP) and human chorionic gonadotropin (hCG) are secreted by some germ cell malignancies. • An elevated AFP and β-hCG can be clinically useful in the differential diagnosis of patients with a pelvic mass, and in monitoring patients after surgery. • Placental alkaline phosphatase (PLAP) and lactate dehydrogenase (LDH) are elevated in up to 95% of patients with dysgerminomas, and serial monitoring of serum LDH levels may be useful for monitoring the disease. • PLAP is more useful as an immunohistochemical marker than as a serum marker. • The classification of germ cell tumors is based both on histologic features and immunohistochemical expression of tumor markers.
• In this scheme, embryonal carcinoma, which is composed of undifferentiated cells that synthesize both hCG and AFP, is the progenitor of several other germ cell tumors. • More differentiated germ cell tumors—such as the endodermal sinus tumor (EST) (Yolk sac tumor), which secretes AFP, and choriocarcinoma, which secretes hCG—are derived from the extraembryonic tissues; immature teratomas are derived from the embryonic cells and do not secrete hCG, but may be associated with an elevated AFP. • Elevated hCG levels are seen in 3% of dysgerminomas and the level is typically less than 100 International Unit. • AFP is never elevated in pure dysgerminomas.
Symptoms • In contrast to the relatively slow-growing epithelial ovarian tumors, germ cell malignancies grow rapidly, and often are characterized by subacute pelvic pain related to capsular distention, hemorrhage, or necrosis. • The rapidly enlarging pelvic mass may produce pressure symptoms on the bladder or rectum, and menstrual irregularities also may occur in menarchal patients. • Acute symptoms associated with torsion or rupture can develop. • In more advanced cases, ascites may develop, and the patient may present with abdominal distention.
Diagnosis and treatment • Adnexal masses measuring 2 cm or more in premenarchal girls or complex masses 8 cm or more in premenopausal patients will usually require surgical exploration. • In young patients, preoperative blood tests should include serum hCG, AFP, LDH and CA125 levels, a complete blood count, and liver function tests. • A radiograph of the chest is important because germ cell tumors can metastasize to the lungs or mediastinum. • A karyotype should ideally be obtained preoperatively on all premenarchal girls because of the propensity of these tumors to arise in dysgenetic gonads, but this may not be practical. • A preoperative computed tomographic (CT) scan or magnetic resonance imaging (MRI) may document the presence and extent of retroperitoneal lymphadenopathy or liver metastases, but unless there is very extensive metastatic disease, is unlikely to influence the decision to operate on the patient initially. • If postmenarchal patients have predominantly cystic lesions up to 8 cm in diameter, they may undergo observation or a trial of hormonal suppression for two cycles.
Dysgerminoma
• Dysgerminomas are the most common malignant germ cell tumor, accounting for approximately 30–40% of all ovarian cancers of germ cell origin. • They represent only 1–3% of all ovarian cancers, but represent as many as 5–10% of ovarian cancers in patients younger than 20 years of age. • Seventy-five percent of dysgerminomas occur between the ages of 10 and 30 years, 5% occur before the age of 10 years and they rarely occur after age 50. • They typically occur in young women and 20–30% of ovarian malignancies associated with pregnancy are dysgerminomas.
• Approximately 5% of dysgerminomas occur in phenotypic females with abnormal gonads. • Dysgerminomas can be associated with patients who have pure gonadal dysgenesis (46XY, bilateral streak gonads), mixed gonadal dysgenesis (45X/46XY, unilateral streak gonad, contralateral testis), and the androgen insensitivity syndrome (46XY, testicular feminization). • Therefore, in premenarchal patients with a pelvic mass, the karyotype should be determined, particularly if a dysgerminoma is considered as the likely diagnosis.
• Approximately 65% of dysgerminomas are stage I at diagnosis. • 85-90% of stage I tumors are confined to one ovary, while 10–15% are bilateral. • All other germ cell tumors are rarely bilateral. • In patients whose contralateral ovary has been preserved, a dysgerminoma can develop in 5–10% of them over the next 2 years. • This figure includes patients who have not received systemic chemotherapy, as well as patients with gonadal dysgenesis
• In the 25% of patients who present with metastatic disease, the tumor most commonly spreads via the lymphatics, particularly to the higher para-aortic nodes. • Metastases to the contralateral ovary may be present • An uncommon site of metastatic disease is bone, and when metastasis to this site occurs, the metastases are seen typically in the lower vertebrae. • Metastases to the lungs, liver, brain, mediastinum and supraclavicular lymph nodes are rare.
Treatment • The treatment of patients with early dysgerminoma is primarily surgical, including • resection of the primary lesion and • limited surgical staging–washings, omental biopsy, careful palpation of all peritoneal surfaces and retroperitoneal nodes, and biopsy of anything suspicious. • Chemotherapy is administered to patients with metastatic disease. • Because the disease principally affects young women, special consideration must be given to the preservation of fertility.
• The role of surgery to resect residual masses following chemotherapy for dysgerminomas is not clear, as the vast majority of these patients will only have necrotic tissue and nonviable tumor. • In general, these patients should be closely monitored with scans and tumor markers. • A positron emission tomography (PET–CT) scan should be considered in patients who have bulky residual masses larger than 3 cm more than 4 weeks after chemotherapy. • If the PET–CT is positive or if there is a suggestion of progressive disease on scans, ideally there should be histologic confirmation of residual disease before embarking on salvage therapy.
• In patients with stage IA dysgerminoma, unilateral oophorectomy alone results in a 5-year disease-free survival rate of greater than 95%. • The 5-year survival for patients with negative nodes was 95.7% compared to 82.8% for patients with positive nodes.
Immature Teratomas
• Immature teratomas typically contain immature neuroepithelium and may be pure immature teratomas or occur in combination with other germ cell tumors as mixed germ cell tumors. • The pure immature teratoma accounts for fewer than 1% of all ovarian cancers, but it is the second most common germ cell malignancy and represents 10–20% of all ovarian malignancies seen in women younger than 20 years of age. • Approximately 50% of pure immature teratomas of the ovary occur between the ages of 10 and 20 years, and they rarely occur in postmenopausal women.
Grading • Those with less than one lower-power field of immature neuroepithelium on the slide with the greatest amount of immature neuroepithelium (grade 1) have a survival of at least 95%, whereas greater amounts of immature neuroepithelium (grades 2 and 3) appear to have a lower overall survival (approximately 85%). • This may not apply to immature teratomas of the ovary in children, because they appear to have a very good outcome with surgery alone, regardless of the degree of immaturity.
Treatment • Surgery- • In a premenopausal patient where the tumor appears confined to a single ovary, unilateral oophorectomy and limited surgical staging should be performed. • Contralateral involvement is rare, and routine resection or wedge biopsy of the contralateral ovary is unnecessary. • Any suspicious lesions on the peritoneal surfaces should be sampled and submitted for histologic evaluation.
• The most frequent site of dissemination is the peritoneum and, much less commonly, the retroperitoneal lymph nodes. • Blood-borne metastases to organ parenchyma such as the lungs, liver, or brain are uncommon. • Cure ultimately depends on the ability to deliver chemotherapy promptly. • Any surgical resection that may be potentially morbid and therefore delay chemotherapy should be resisted. • Surgical resection of any residual disease should be considered at the completion of chemotherapy.
• Patients with stage IA, grade 1 tumors have an excellent prognosis, and no adjuvant therapy is required. In patients with high-grade, stage IA immature teratomas, adjuvant chemotherapy has commonly been given. • The inferiority of carboplatin was confirmed in a larger randomized trial reported by Horwich et al.. • In view of these results, BEP is the preferred treatment regimen. • The 3-day schedule has been found to be equivalent to a 5-day schedule for BEP chemotherapy. • A cycle of BEP consisted of etoposide 500 mg/m2 , administered at either 100 mg/m2 days 1 through 5 or 165 mg/m2 days 1 through 3, cisplatin 100 mg/m2 , administered at either 20 mg/m2 days 1 through 5 or 50 mg/m2 days 1 and 2. Bleomycin 30,000 International Unit is administered on days 1, 8, and 15 during cycles 1 through 3.
Mature cystic teratoma • Malignant transformation of a mature teratoma is a rare event. • Squamous cell carcinoma is the most frequent subtype of malignancy, but adenocarcinomas, primary melanomas, and carcinoids may also rarely occur. • The risk is reported to be between 0.5% and 2% of teratomas, and usually occurs in postmenopausal patients. • Platinum-based chemotherapy with or without pelvic radiation is most often used for adjuvant treatment of early-stage disease (DosSantos, 2007). • However, regardless of treatment received. patients with advanced disease do poorly
Endodermal Sinus Tumor/ Yolk Sac Carcinoma
• yolk sac carcinomas because they are derived from the primitive yolk sac. • They are the third most frequent malignant germ cell tumor of the ovary. • median age of 18 years at diagnosis. • Approximately one-third of the patients are premenarchal at presentation. • Abdominal or pelvic pain occurs in approximately 75% of patients, whereas an asymptomatic pelvic mass is documented in 10% of patients. • Most ESTs secrete AFP and rarely may also elaborate detectable alpha-1- antitrypsin (AAT). • There is a good correlation between the extent of disease and the level of AFP, although discordance also has been observed. • The serum level of AFP is useful in monitoring the patient’s response to treatment, as well as in follow-up.
Treatment • The treatment of an EST consists of surgical exploration, unilateral salpingo- oophorectomy, a frozen section for diagnosis, and limited surgical staging. • A hysterectomy and contralateral salpingo-oophorectomy should not be done. • Conservative surgery and adjuvant chemotherapy allow fertility preservation as with other germ cell tumors. • In patients with metastatic disease, all gross disease should be resected if possible. • Bilaterality is not seen in EST, and the other ovary is involved with metastatic disease only. • Most patients have early-stage disease: 71% stage I, 6% stage II, and 23% stage III
• All patients should be treated with a cisplatin-based regimen such as BEP, which is considered the standard of care. • The chance of cure now approaches 100% for patients with early-stage disease, and is at least 75% for patients with more advanced-stage disease. • 3 cycles of BEP is considered optimal for good prognosis for low risk patients and four cycles for patients with intermediate to high-risk tumors. (extrapolated from GCT testis) • An alternative approach is to use VIP (etoposide, ifosfamide, and cisplatin) in patients with more advanced disease in whom bleomycin is contraindicated. • Four cycles of VIP are equivalent to four cycles of BEP.
• Neoadjuvant chemotherapy followed by fertility-sparing surgery may also be a reasonable option for patients with advanced ovarian germ cell tumors not suitable for optimal cytoreduction. • POMB-ACE (cisplatin, vincristine, methotrexate, bleomycin, actinomycin D, cyclophosphamide, etoposide) regimen for high-risk germ cell tumors of any histologic type. • This protocol introduces seven drugs into the initial management, which is intended to reduce the chances of developing drug resistance, which may be particularly relevant for patients with large volume metastatic disease
Embryonal Carcinoma • Embryonal carcinoma of the ovary is an extremely rare tumor that is distinguished from a choriocarcinoma of the ovary by the absence of syncytiotrophoblastic and cytotrophoblastic cells. • The patients are very young, their ages ranging between 4 and 28 years (median = 14 years). • Older patients have been reported. • Embryonal carcinomas may secrete estrogens, with the patient exhibiting symptoms and signs of precocious pseudopuberty or irregular bleeding. • The presentation is otherwise similar to that of the EST. • The primary lesions tend to be large, and approximately two-thirds are confined to one ovary at the time of presentation. • These lesions frequently secrete AFP and hCG, which are useful for following the response to subsequent therapy. • The treatment of embryonal carcinomas is the same as that for ESTs
Choriocarcinoma of the Ovary • Pure nongestational choriocarcinoma of the ovary is an extremely rare tumor. • Histologically, it has the same appearance as gestational choriocarcinoma metastatic to the ovaries. • The majority of patients with this cancer are younger than 20 years. • The presence of hCG can be useful in monitoring the patient’s response to treatment. • In the presence of high hCG levels, isosexual precocity has been seen, occurring in approximately 50% of patients whose tumors appear before menarche.
• There are only a few limited reports on the use of chemotherapy for these nongestational choriocarcinomas, but complete responses have been reported to the MAC regimen (methotrexate, actinomycin D, and cyclophosphamide) as described for gestational trophoblastic disease. • These tumors are so rare that no good data are available, but the options also include the BEP or POMB-ACE regimens. • The prognosis for ovarian choriocarcinomas has been poor. • The majority of patients have metastases to organ parenchyma at the time of initial diagnosis, and they should be managed as high-risk germ cell tumors.
Polyembryoma • Polyembryoma of the ovary is another extremely rare tumor, which is composed of “embryoid bodies.” • This tumor replicates the structures of early embryonic differentiation (i.e., the three somatic layers: Endoderm, mesoderm, and ectoderm). • They occur in very young, premenarchal girls with signs of pseudopuberty, and AFP and hCG levels are elevated. • Women with polyembryomas confined to one ovary may be followed with serial tumor markers and diagnostic-imaging techniques to avoid cytotoxic chemotherapy. • In patients who require chemotherapy, the BEP regimen is appropriate.
Mixed germ cell malignancies • Mixed germ cell malignancies of the ovary contain two or more elements of the tumors described above. • In one series (107), the most common component of a mixed germ cell tumor was dysgerminoma, which occurred in 80%, followed by EST in 70%, immature teratoma in 53%, choriocarcinoma in 20%, and embryonal carcinoma in 16%. • The most frequent combination was a dysgerminoma and an EST. • The mixed germ cell tumors may secrete either AFP or hCG— or both or neither—depending on the components. • These tumors should be managed with combination chemotherapy, preferably BEP. • The serum marker, if positive initially, may become negative during chemotherapy, but this may reflect regression of only a particular component of the mixed lesion.
• Therefore, a second-look laparotomy may be indicated if there is residual disease following chemotherapy, particularly if there was an immature teratomatous component in the original tumor. • The most important prognostic features are the size of the primary tumor and the relative percentage of its most malignant component. • In stage IA lesions smaller than 10 cm, survival is 100%. • Tumors composed of less than one-third EST, choriocarcinoma, or grade 3 immature teratoma also have an excellent prognosis, but it is possibly less favorable when these components comprise the majority of the tumor.
Take home message • Germ cell tumors are derived from the primordial germ cells of the ovary. • The primary treatment is surgery followed by chemotherapy. • Surgical treatment of GCT ovary is resection of tumor with limited surgical staging. Fertility is preserved if required. • BEP is the most effective chemotherapy. • Tumor markers are very very important for response to treatment and follow up.
Thank you

Recomendados

Molecular testing of breast ca
Molecular testing of breast caMolecular testing of breast ca
Molecular testing of breast caAyshax12
 
Molecular biology of breast cancer [autosaved]
Molecular biology of breast cancer [autosaved]Molecular biology of breast cancer [autosaved]
Molecular biology of breast cancer [autosaved]kamali purushothaman
 
MANAGEMENT OF TRIPLE NEGATIVE BREAST CANCER.pptx
MANAGEMENT OF TRIPLE NEGATIVE BREAST CANCER.pptxMANAGEMENT OF TRIPLE NEGATIVE BREAST CANCER.pptx
MANAGEMENT OF TRIPLE NEGATIVE BREAST CANCER.pptxCancer surgery By Royapettah Oncology Group
 
Chapter 5 cancer susceptibility syndromes
Chapter 5 cancer susceptibility syndromesChapter 5 cancer susceptibility syndromes
Chapter 5 cancer susceptibility syndromesNilesh Kucha
 
Esophageal carcinoma trials
Esophageal carcinoma trialsEsophageal carcinoma trials
Esophageal carcinoma trialskoduruvijay7
 
Oligometastases
OligometastasesOligometastases
OligometastasesCancer surgery By Royapettah Oncology Group
 
Molecular subtypes of breast cancer
Molecular subtypes of breast cancerMolecular subtypes of breast cancer
Molecular subtypes of breast cancerJoydeep Ghosh
 
Triple Negative Breast Cancer
Triple Negative Breast CancerTriple Negative Breast Cancer
Triple Negative Breast CancerMohamed Abdulla
 

Recomendados

Molecular testing of breast ca
Molecular testing of breast caMolecular testing of breast ca
Molecular testing of breast caAyshax12
 
Molecular biology of breast cancer [autosaved]
Molecular biology of breast cancer [autosaved]Molecular biology of breast cancer [autosaved]
Molecular biology of breast cancer [autosaved]kamali purushothaman
 
MANAGEMENT OF TRIPLE NEGATIVE BREAST CANCER.pptx
MANAGEMENT OF TRIPLE NEGATIVE BREAST CANCER.pptxMANAGEMENT OF TRIPLE NEGATIVE BREAST CANCER.pptx
MANAGEMENT OF TRIPLE NEGATIVE BREAST CANCER.pptxCancer surgery By Royapettah Oncology Group
 
Chapter 5 cancer susceptibility syndromes
Chapter 5 cancer susceptibility syndromesChapter 5 cancer susceptibility syndromes
Chapter 5 cancer susceptibility syndromesNilesh Kucha
 
Esophageal carcinoma trials
Esophageal carcinoma trialsEsophageal carcinoma trials
Esophageal carcinoma trialskoduruvijay7
 
Oligometastases
OligometastasesOligometastases
OligometastasesCancer surgery By Royapettah Oncology Group
 
Molecular subtypes of breast cancer
Molecular subtypes of breast cancerMolecular subtypes of breast cancer
Molecular subtypes of breast cancerJoydeep Ghosh
 
Triple Negative Breast Cancer
Triple Negative Breast CancerTriple Negative Breast Cancer
Triple Negative Breast CancerMohamed Abdulla
 
Strategies for Managing Recurrent Ovarian Cancer
Strategies for Managing Recurrent Ovarian CancerStrategies for Managing Recurrent Ovarian Cancer
Strategies for Managing Recurrent Ovarian Cancerbkling
 
Molecular profiling of breast cancer
Molecular profiling of breast cancerMolecular profiling of breast cancer
Molecular profiling of breast cancerHriman Sharma Sarkar
 
Breast Cancer: A focus on BRCA Mutations.
Breast Cancer: A focus on BRCA Mutations.Breast Cancer: A focus on BRCA Mutations.
Breast Cancer: A focus on BRCA Mutations.Mohamed Abdulla
 
Pancreatic cancer presentaion
Pancreatic cancer presentaionPancreatic cancer presentaion
Pancreatic cancer presentaionChi-Hua(Richard) Lu, PharmD, RPh
 
Neuroblastoma presentation
Neuroblastoma presentationNeuroblastoma presentation
Neuroblastoma presentationNational Cancer Institute, Cairo University - Children's Cancer Hospital - Egypt 57357
 
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCER
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCEREVOLUTION OF CHEMOTHERAPY IN BREAST CANCER
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCERIsha Jaiswal
 
Endometrial cancer recommendations
Endometrial cancer recommendationsEndometrial cancer recommendations
Endometrial cancer recommendationsLAKSHMI DEEPTHI GEDELA
 
Basics of immunotherapy in colorectal cancer
Basics of immunotherapy in colorectal cancerBasics of immunotherapy in colorectal cancer
Basics of immunotherapy in colorectal cancerMohamed Abdulla
 
Pathology of Endometrial cancer 2022.pptx
Pathology of Endometrial cancer 2022.pptxPathology of Endometrial cancer 2022.pptx
Pathology of Endometrial cancer 2022.pptxDr ABU SURAIH SAKHRI
 
Cervix landmark trials- kiran
Cervix landmark trials- kiran Cervix landmark trials- kiran
Cervix landmark trials- kiran Kiran Ramakrishna
 
Primary CNS Lymphoma
Primary CNS Lymphoma Primary CNS Lymphoma
Primary CNS Lymphoma Dr.Rashmi Yadav
 
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)bkling
 
High Grade Glioma
High Grade GliomaHigh Grade Glioma
High Grade GliomaDrAyush Garg
 
Neuroendocrine tumours.pptx
Neuroendocrine tumours.pptxNeuroendocrine tumours.pptx
Neuroendocrine tumours.pptxMona Rashed
 
Uterine sarcoma
Uterine sarcoma Uterine sarcoma
Uterine sarcoma Beena K
 
EBRT IN CARCINOMA CERVIX
EBRT IN CARCINOMA CERVIXEBRT IN CARCINOMA CERVIX
EBRT IN CARCINOMA CERVIXIsha Jaiswal
 
How Radiation Therapy Is Used in the Treatment of Lymphoma
How Radiation Therapy Is Used in the Treatment of Lymphoma How Radiation Therapy Is Used in the Treatment of Lymphoma
How Radiation Therapy Is Used in the Treatment of Lymphoma Dana-Farber Cancer Institute
 
Molecular profiling in breast cancer
Molecular profiling in breast cancerMolecular profiling in breast cancer
Molecular profiling in breast cancerShashidhara TS
 
Approach to the patients with brain metastases
Approach to the patients with brain metastasesApproach to the patients with brain metastases
Approach to the patients with brain metastasesVenkata pradeep babu koyyala
 
Uterine sarcoma mine
Uterine sarcoma mineUterine sarcoma mine
Uterine sarcoma mineLAKSHMI DEEPTHI GEDELA
 
Germ cell tumors of ovary
Germ cell tumors of ovaryGerm cell tumors of ovary
Germ cell tumors of ovaryPriyanka Malekar
 
Management of Testicular Tumors
Management of Testicular TumorsManagement of Testicular Tumors
Management of Testicular TumorsPhilip Mensah
 

Más contenido relacionado

La actualidad más candente

Strategies for Managing Recurrent Ovarian Cancer
Strategies for Managing Recurrent Ovarian CancerStrategies for Managing Recurrent Ovarian Cancer
Strategies for Managing Recurrent Ovarian Cancerbkling
 
Molecular profiling of breast cancer
Molecular profiling of breast cancerMolecular profiling of breast cancer
Molecular profiling of breast cancerHriman Sharma Sarkar
 
Breast Cancer: A focus on BRCA Mutations.
Breast Cancer: A focus on BRCA Mutations.Breast Cancer: A focus on BRCA Mutations.
Breast Cancer: A focus on BRCA Mutations.Mohamed Abdulla
 
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCER
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCEREVOLUTION OF CHEMOTHERAPY IN BREAST CANCER
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCERIsha Jaiswal
 
Basics of immunotherapy in colorectal cancer
Basics of immunotherapy in colorectal cancerBasics of immunotherapy in colorectal cancer
Basics of immunotherapy in colorectal cancerMohamed Abdulla
 
Pathology of Endometrial cancer 2022.pptx
Pathology of Endometrial cancer 2022.pptxPathology of Endometrial cancer 2022.pptx
Pathology of Endometrial cancer 2022.pptxDr ABU SURAIH SAKHRI
 
Cervix landmark trials- kiran
Cervix landmark trials- kiran Cervix landmark trials- kiran
Cervix landmark trials- kiran Kiran Ramakrishna
 
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)bkling
 
Neuroendocrine tumours.pptx
Neuroendocrine tumours.pptxNeuroendocrine tumours.pptx
Neuroendocrine tumours.pptxMona Rashed
 
Uterine sarcoma
Uterine sarcoma Uterine sarcoma
Uterine sarcoma Beena K
 
EBRT IN CARCINOMA CERVIX
EBRT IN CARCINOMA CERVIXEBRT IN CARCINOMA CERVIX
EBRT IN CARCINOMA CERVIXIsha Jaiswal
 
How Radiation Therapy Is Used in the Treatment of Lymphoma
How Radiation Therapy Is Used in the Treatment of Lymphoma How Radiation Therapy Is Used in the Treatment of Lymphoma
How Radiation Therapy Is Used in the Treatment of Lymphoma Dana-Farber Cancer Institute
 
Molecular profiling in breast cancer
Molecular profiling in breast cancerMolecular profiling in breast cancer
Molecular profiling in breast cancerShashidhara TS
 

La actualidad más candente (20)

Strategies for Managing Recurrent Ovarian Cancer
Strategies for Managing Recurrent Ovarian CancerStrategies for Managing Recurrent Ovarian Cancer
Strategies for Managing Recurrent Ovarian Cancer
 
Molecular profiling of breast cancer
Molecular profiling of breast cancerMolecular profiling of breast cancer
Molecular profiling of breast cancer
 
Breast Cancer: A focus on BRCA Mutations.
Breast Cancer: A focus on BRCA Mutations.Breast Cancer: A focus on BRCA Mutations.
Breast Cancer: A focus on BRCA Mutations.
 
Pancreatic cancer presentaion
Pancreatic cancer presentaionPancreatic cancer presentaion
Pancreatic cancer presentaion
 
Neuroblastoma presentation
Neuroblastoma presentationNeuroblastoma presentation
Neuroblastoma presentation
 
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCER
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCEREVOLUTION OF CHEMOTHERAPY IN BREAST CANCER
EVOLUTION OF CHEMOTHERAPY IN BREAST CANCER
 
Endometrial cancer recommendations
Endometrial cancer recommendationsEndometrial cancer recommendations
Endometrial cancer recommendations
 
Basics of immunotherapy in colorectal cancer
Basics of immunotherapy in colorectal cancerBasics of immunotherapy in colorectal cancer
Basics of immunotherapy in colorectal cancer
 
Pathology of Endometrial cancer 2022.pptx
Pathology of Endometrial cancer 2022.pptxPathology of Endometrial cancer 2022.pptx
Pathology of Endometrial cancer 2022.pptx
 
Cervix landmark trials- kiran
Cervix landmark trials- kiran Cervix landmark trials- kiran
Cervix landmark trials- kiran
 
Primary CNS Lymphoma
Primary CNS Lymphoma Primary CNS Lymphoma
Primary CNS Lymphoma
 
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)
Report Back from San Antonio Breast Cancer Symposium (SABCS 2022)
 
High Grade Glioma
High Grade GliomaHigh Grade Glioma
High Grade Glioma
 
Neuroendocrine tumours.pptx
Neuroendocrine tumours.pptxNeuroendocrine tumours.pptx
Neuroendocrine tumours.pptx
 
Uterine sarcoma
Uterine sarcoma Uterine sarcoma
Uterine sarcoma
 
EBRT IN CARCINOMA CERVIX
EBRT IN CARCINOMA CERVIXEBRT IN CARCINOMA CERVIX
EBRT IN CARCINOMA CERVIX
 
How Radiation Therapy Is Used in the Treatment of Lymphoma
How Radiation Therapy Is Used in the Treatment of Lymphoma How Radiation Therapy Is Used in the Treatment of Lymphoma
How Radiation Therapy Is Used in the Treatment of Lymphoma
 
Molecular profiling in breast cancer
Molecular profiling in breast cancerMolecular profiling in breast cancer
Molecular profiling in breast cancer
 
Approach to the patients with brain metastases
Approach to the patients with brain metastasesApproach to the patients with brain metastases
Approach to the patients with brain metastases
 
Uterine sarcoma mine
Uterine sarcoma mineUterine sarcoma mine
Uterine sarcoma mine
 

Similar a Germ cell tumor ovary.pptx

Management of Testicular Tumors
Management of Testicular TumorsManagement of Testicular Tumors
Management of Testicular TumorsPhilip Mensah
 
Ovarian cancer
Ovarian cancerOvarian cancer
Ovarian cancerMamso
 
OVARY CANCER: BORDERLINE
OVARY CANCER: BORDERLINEOVARY CANCER: BORDERLINE
OVARY CANCER: BORDERLINEDr. Sumit KUMAR
 
Ovarian Malignant PPT.pptx
Ovarian Malignant PPT.pptxOvarian Malignant PPT.pptx
Ovarian Malignant PPT.pptxssuser17701d
 
Ovaries and Ovarian Tumours
Ovaries and Ovarian TumoursOvaries and Ovarian Tumours
Ovaries and Ovarian TumoursMujeeb M
 
malignant ovarian tumour
malignant ovarian tumourmalignant ovarian tumour
malignant ovarian tumourAisha Nazeer
 
Ovarian carcinoma by Dr najeeb ur rehman
Ovarian carcinoma by Dr najeeb ur rehmanOvarian carcinoma by Dr najeeb ur rehman
Ovarian carcinoma by Dr najeeb ur rehmanAyub Medical College
 
Epithelial ovarian cancer n.pptx
Epithelial ovarian cancer n.pptxEpithelial ovarian cancer n.pptx
Epithelial ovarian cancer n.pptxShilpa248480
 
Neuroblastoma & Wilms tumor.pptx
Neuroblastoma & Wilms tumor.pptxNeuroblastoma & Wilms tumor.pptx
Neuroblastoma & Wilms tumor.pptxIrfanNashad1
 
Carcinoma Cervix.pptx
Carcinoma Cervix.pptxCarcinoma Cervix.pptx
Carcinoma Cervix.pptxAeyshaBegum
 
ca uterus cancer in uterus, common female problem
ca uterus cancer in uterus, common female problemca uterus cancer in uterus, common female problem
ca uterus cancer in uterus, common female problemSasiSoman3
 
SACROCOXYGEAL TERATOMA.pdf
SACROCOXYGEAL TERATOMA.pdfSACROCOXYGEAL TERATOMA.pdf
SACROCOXYGEAL TERATOMA.pdfDR SETH JOTHAM
 
NEOPLASMS OF TESTIS (1).pptx
NEOPLASMS OF TESTIS (1).pptxNEOPLASMS OF TESTIS (1).pptx
NEOPLASMS OF TESTIS (1).pptxManoj Vaidya
 
The hormonal disorder of the thyroid tu.pptx
The hormonal disorder of the thyroid tu.pptxThe hormonal disorder of the thyroid tu.pptx
The hormonal disorder of the thyroid tu.pptxBilisumaTAyana
 
Malignant ovarian tumors
Malignant ovarian tumorsMalignant ovarian tumors
Malignant ovarian tumorsrajeev sood
 
04. thyroid tumors
04. thyroid tumors04. thyroid tumors
04. thyroid tumorsFahad Zakwan
 

Similar a Germ cell tumor ovary.pptx (20)

Germ cell tumors of ovary
Germ cell tumors of ovaryGerm cell tumors of ovary
Germ cell tumors of ovary
 
Management of Testicular Tumors
Management of Testicular TumorsManagement of Testicular Tumors
Management of Testicular Tumors
 
Ovarian cancer
Ovarian cancerOvarian cancer
Ovarian cancer
 
OVARY CANCER: BORDERLINE
OVARY CANCER: BORDERLINEOVARY CANCER: BORDERLINE
OVARY CANCER: BORDERLINE
 
Testicular carcinoma
Testicular carcinomaTesticular carcinoma
Testicular carcinoma
 
Ovarian Malignant PPT.pptx
Ovarian Malignant PPT.pptxOvarian Malignant PPT.pptx
Ovarian Malignant PPT.pptx
 
Ovaries and Ovarian Tumours
Ovaries and Ovarian TumoursOvaries and Ovarian Tumours
Ovaries and Ovarian Tumours
 
malignant ovarian tumour
malignant ovarian tumourmalignant ovarian tumour
malignant ovarian tumour
 
Ovarian carcinoma by Dr najeeb ur rehman
Ovarian carcinoma by Dr najeeb ur rehmanOvarian carcinoma by Dr najeeb ur rehman
Ovarian carcinoma by Dr najeeb ur rehman
 
Ovarian cancer
Ovarian cancerOvarian cancer
Ovarian cancer
 
Epithelial ovarian cancer n.pptx
Epithelial ovarian cancer n.pptxEpithelial ovarian cancer n.pptx
Epithelial ovarian cancer n.pptx
 
Neuroblastoma & Wilms tumor.pptx
Neuroblastoma & Wilms tumor.pptxNeuroblastoma & Wilms tumor.pptx
Neuroblastoma & Wilms tumor.pptx
 
Carcinoma Cervix.pptx
Carcinoma Cervix.pptxCarcinoma Cervix.pptx
Carcinoma Cervix.pptx
 
ca uterus cancer in uterus, common female problem
ca uterus cancer in uterus, common female problemca uterus cancer in uterus, common female problem
ca uterus cancer in uterus, common female problem
 
Endometrium part 1 2018
Endometrium part 1 2018Endometrium part 1 2018
Endometrium part 1 2018
 
SACROCOXYGEAL TERATOMA.pdf
SACROCOXYGEAL TERATOMA.pdfSACROCOXYGEAL TERATOMA.pdf
SACROCOXYGEAL TERATOMA.pdf
 
NEOPLASMS OF TESTIS (1).pptx
NEOPLASMS OF TESTIS (1).pptxNEOPLASMS OF TESTIS (1).pptx
NEOPLASMS OF TESTIS (1).pptx
 
The hormonal disorder of the thyroid tu.pptx
The hormonal disorder of the thyroid tu.pptxThe hormonal disorder of the thyroid tu.pptx
The hormonal disorder of the thyroid tu.pptx
 
Malignant ovarian tumors
Malignant ovarian tumorsMalignant ovarian tumors
Malignant ovarian tumors
 
04. thyroid tumors
04. thyroid tumors04. thyroid tumors
04. thyroid tumors
 

Más de Dr. Abani Kanta Nanda

Management of locally advanced rectal cancer
Management of locally advanced rectal cancerManagement of locally advanced rectal cancer
Management of locally advanced rectal cancerDr. Abani Kanta Nanda
 

Más de Dr. Abani Kanta Nanda (8)

Lungs contouring Dr. Abani.pdf
Lungs contouring Dr. Abani.pdfLungs contouring Dr. Abani.pdf
Lungs contouring Dr. Abani.pdf
 
CERVIX CONTURING.pdf
CERVIX CONTURING.pdfCERVIX CONTURING.pdf
CERVIX CONTURING.pdf
 
Esophagus Contouring.pptx
Esophagus Contouring.pptxEsophagus Contouring.pptx
Esophagus Contouring.pptx
 
Ca endometrium
Ca endometriumCa endometrium
Ca endometrium
 
Management of locally advanced rectal cancer
Management of locally advanced rectal cancerManagement of locally advanced rectal cancer
Management of locally advanced rectal cancer
 
craniospinal irradiation
craniospinal irradiationcraniospinal irradiation
craniospinal irradiation
 
Principles of chemoradiations
Principles of chemoradiationsPrinciples of chemoradiations
Principles of chemoradiations
 
Electron beam therapy
Electron beam therapyElectron beam therapy
Electron beam therapy
 

Último

❤️♀️@ Jaipur Call Girl Agency ❤️♀️@ Manjeet Russian Call Girls Service in Jai...
❤️♀️@ Jaipur Call Girl Agency ❤️♀️@ Manjeet Russian Call Girls Service in Jai...❤️♀️@ Jaipur Call Girl Agency ❤️♀️@ Manjeet Russian Call Girls Service in Jai...
❤️♀️@ Jaipur Call Girl Agency ❤️♀️@ Manjeet Russian Call Girls Service in Jai...Gfnyt.com
 
Call Girls Amritsar 💯Call Us 🔝 8725944379 🔝 💃 Independent Escort Service Amri...
Call Girls Amritsar 💯Call Us 🔝 8725944379 🔝 💃 Independent Escort Service Amri...Call Girls Amritsar 💯Call Us 🔝 8725944379 🔝 💃 Independent Escort Service Amri...
Call Girls Amritsar 💯Call Us 🔝 8725944379 🔝 💃 Independent Escort Service Amri...Niamh verma
 
Local Housewife and effective ☎️ 8250192130 🍉🍓 Sexy Girls VIP Call Girls Chan...
Local Housewife and effective ☎️ 8250192130 🍉🍓 Sexy Girls VIP Call Girls Chan...Local Housewife and effective ☎️ 8250192130 🍉🍓 Sexy Girls VIP Call Girls Chan...
Local Housewife and effective ☎️ 8250192130 🍉🍓 Sexy Girls VIP Call Girls Chan...Russian Call Girls Amritsar
 
❤️♀️@ Jaipur Call Girls ❤️♀️@ Jaispreet Call Girl Services in Jaipur QRYPCF ...
❤️♀️@ Jaipur Call Girls ❤️♀️@ Jaispreet Call Girl Services in Jaipur QRYPCF ...❤️♀️@ Jaipur Call Girls ❤️♀️@ Jaispreet Call Girl Services in Jaipur QRYPCF ...
❤️♀️@ Jaipur Call Girls ❤️♀️@ Jaispreet Call Girl Services in Jaipur QRYPCF ...Gfnyt.com
 
Call Girl Raipur 📲 9999965857 ヅ10k NiGhT Call Girls In Raipur
Call Girl Raipur 📲 9999965857 ヅ10k NiGhT Call Girls In RaipurCall Girl Raipur 📲 9999965857 ヅ10k NiGhT Call Girls In Raipur
Call Girl Raipur 📲 9999965857 ヅ10k NiGhT Call Girls In Raipurgragmanisha42
 
Call Now ☎ 9999965857 !! Call Girls in Hauz Khas Escort Service Delhi N.C.R.
Call Now ☎ 9999965857 !! Call Girls in Hauz Khas Escort Service Delhi N.C.R.Call Now ☎ 9999965857 !! Call Girls in Hauz Khas Escort Service Delhi N.C.R.
Call Now ☎ 9999965857 !! Call Girls in Hauz Khas Escort Service Delhi N.C.R.ktanvi103
 
VIP Call Girls Noida Sia 9711199171 High Class Call Girl Near Me
VIP Call Girls Noida Sia 9711199171 High Class Call Girl Near MeVIP Call Girls Noida Sia 9711199171 High Class Call Girl Near Me
VIP Call Girls Noida Sia 9711199171 High Class Call Girl Near Memriyagarg453
 
Chandigarh Call Girls 👙 7001035870 👙 Genuine WhatsApp Number for Real Meet
Chandigarh Call Girls 👙 7001035870 👙 Genuine WhatsApp Number for Real MeetChandigarh Call Girls 👙 7001035870 👙 Genuine WhatsApp Number for Real Meet
Chandigarh Call Girls 👙 7001035870 👙 Genuine WhatsApp Number for Real Meetpriyashah722354
 
Dehradun Call Girls Service ❤️🍑 8854095900 👄🫦Independent Escort Service Dehradun
Dehradun Call Girls Service ❤️🍑 8854095900 👄🫦Independent Escort Service DehradunDehradun Call Girls Service ❤️🍑 8854095900 👄🫦Independent Escort Service Dehradun
Dehradun Call Girls Service ❤️🍑 8854095900 👄🫦Independent Escort Service DehradunNiamh verma
 
❤️♀️@ Jaipur Call Girls ❤️♀️@ Meghna Jaipur Call Girls Number CRTHNR Call G...
❤️♀️@ Jaipur Call Girls ❤️♀️@ Meghna Jaipur Call Girls Number CRTHNR Call G...❤️♀️@ Jaipur Call Girls ❤️♀️@ Meghna Jaipur Call Girls Number CRTHNR Call G...
❤️♀️@ Jaipur Call Girls ❤️♀️@ Meghna Jaipur Call Girls Number CRTHNR Call G...Gfnyt.com
 
Bangalore call girl 👯‍♀️@ Simran Independent Call Girls in Bangalore GIUXUZ...
Bangalore call girl 👯‍♀️@ Simran Independent Call Girls in Bangalore GIUXUZ...Bangalore call girl 👯‍♀️@ Simran Independent Call Girls in Bangalore GIUXUZ...
Bangalore call girl 👯‍♀️@ Simran Independent Call Girls in Bangalore GIUXUZ...Gfnyt
 
Basics of Anatomy- Language of Anatomy.pptx
Basics of Anatomy- Language of Anatomy.pptxBasics of Anatomy- Language of Anatomy.pptx
Basics of Anatomy- Language of Anatomy.pptxAyush Gupta
 
💚😋Chandigarh Escort Service Call Girls, ₹5000 To 25K With AC💚😋
💚😋Chandigarh Escort Service Call Girls, ₹5000 To 25K With AC💚😋💚😋Chandigarh Escort Service Call Girls, ₹5000 To 25K With AC💚😋
💚😋Chandigarh Escort Service Call Girls, ₹5000 To 25K With AC💚😋Sheetaleventcompany
 
Call Girls Hyderabad Just Call 9907093804 Top Class Call Girl Service Available
Call Girls Hyderabad Just Call 9907093804 Top Class Call Girl Service AvailableCall Girls Hyderabad Just Call 9907093804 Top Class Call Girl Service Available
Call Girls Hyderabad Just Call 9907093804 Top Class Call Girl Service AvailableDipal Arora
 
No Advance 9053900678 Chandigarh Call Girls , Indian Call Girls For Full Ni...
No Advance 9053900678 Chandigarh Call Girls , Indian Call Girls For Full Ni...No Advance 9053900678 Chandigarh Call Girls , Indian Call Girls For Full Ni...
No Advance 9053900678 Chandigarh Call Girls , Indian Call Girls For Full Ni...Vip call girls In Chandigarh
 
Call Girl Price Amritsar ❤️🍑 9053900678 Call Girls in Amritsar Suman
Call Girl Price Amritsar ❤️🍑 9053900678 Call Girls in Amritsar SumanCall Girl Price Amritsar ❤️🍑 9053900678 Call Girls in Amritsar Suman
Call Girl Price Amritsar ❤️🍑 9053900678 Call Girls in Amritsar SumanCall Girls Service Chandigarh Ayushi
 
💚😋Kolkata Escort Service Call Girls, ₹5000 To 25K With AC💚😋
💚😋Kolkata Escort Service Call Girls, ₹5000 To 25K With AC💚😋💚😋Kolkata Escort Service Call Girls, ₹5000 To 25K With AC💚😋
💚😋Kolkata Escort Service Call Girls, ₹5000 To 25K With AC💚😋Sheetaleventcompany
 
VIP Call Girl Sector 32 Noida Just Book Me 9711199171
VIP Call Girl Sector 32 Noida Just Book Me 9711199171VIP Call Girl Sector 32 Noida Just Book Me 9711199171
VIP Call Girl Sector 32 Noida Just Book Me 9711199171Call Girls Service Gurgaon
 

Último (20)

❤️♀️@ Jaipur Call Girl Agency ❤️♀️@ Manjeet Russian Call Girls Service in Jai...
❤️♀️@ Jaipur Call Girl Agency ❤️♀️@ Manjeet Russian Call Girls Service in Jai...❤️♀️@ Jaipur Call Girl Agency ❤️♀️@ Manjeet Russian Call Girls Service in Jai...
❤️♀️@ Jaipur Call Girl Agency ❤️♀️@ Manjeet Russian Call Girls Service in Jai...
 
Call Girls Amritsar 💯Call Us 🔝 8725944379 🔝 💃 Independent Escort Service Amri...
Call Girls Amritsar 💯Call Us 🔝 8725944379 🔝 💃 Independent Escort Service Amri...Call Girls Amritsar 💯Call Us 🔝 8725944379 🔝 💃 Independent Escort Service Amri...
Call Girls Amritsar 💯Call Us 🔝 8725944379 🔝 💃 Independent Escort Service Amri...
 
Local Housewife and effective ☎️ 8250192130 🍉🍓 Sexy Girls VIP Call Girls Chan...
Local Housewife and effective ☎️ 8250192130 🍉🍓 Sexy Girls VIP Call Girls Chan...Local Housewife and effective ☎️ 8250192130 🍉🍓 Sexy Girls VIP Call Girls Chan...
Local Housewife and effective ☎️ 8250192130 🍉🍓 Sexy Girls VIP Call Girls Chan...
 
❤️♀️@ Jaipur Call Girls ❤️♀️@ Jaispreet Call Girl Services in Jaipur QRYPCF ...
❤️♀️@ Jaipur Call Girls ❤️♀️@ Jaispreet Call Girl Services in Jaipur QRYPCF ...❤️♀️@ Jaipur Call Girls ❤️♀️@ Jaispreet Call Girl Services in Jaipur QRYPCF ...
❤️♀️@ Jaipur Call Girls ❤️♀️@ Jaispreet Call Girl Services in Jaipur QRYPCF ...
 
Call Girl Raipur 📲 9999965857 ヅ10k NiGhT Call Girls In Raipur
Call Girl Raipur 📲 9999965857 ヅ10k NiGhT Call Girls In RaipurCall Girl Raipur 📲 9999965857 ヅ10k NiGhT Call Girls In Raipur
Call Girl Raipur 📲 9999965857 ヅ10k NiGhT Call Girls In Raipur
 
Call Now ☎ 9999965857 !! Call Girls in Hauz Khas Escort Service Delhi N.C.R.
Call Now ☎ 9999965857 !! Call Girls in Hauz Khas Escort Service Delhi N.C.R.Call Now ☎ 9999965857 !! Call Girls in Hauz Khas Escort Service Delhi N.C.R.
Call Now ☎ 9999965857 !! Call Girls in Hauz Khas Escort Service Delhi N.C.R.
 
VIP Call Girls Noida Sia 9711199171 High Class Call Girl Near Me
VIP Call Girls Noida Sia 9711199171 High Class Call Girl Near MeVIP Call Girls Noida Sia 9711199171 High Class Call Girl Near Me
VIP Call Girls Noida Sia 9711199171 High Class Call Girl Near Me
 
Chandigarh Call Girls 👙 7001035870 👙 Genuine WhatsApp Number for Real Meet
Chandigarh Call Girls 👙 7001035870 👙 Genuine WhatsApp Number for Real MeetChandigarh Call Girls 👙 7001035870 👙 Genuine WhatsApp Number for Real Meet
Chandigarh Call Girls 👙 7001035870 👙 Genuine WhatsApp Number for Real Meet
 
Dehradun Call Girls Service ❤️🍑 8854095900 👄🫦Independent Escort Service Dehradun
Dehradun Call Girls Service ❤️🍑 8854095900 👄🫦Independent Escort Service DehradunDehradun Call Girls Service ❤️🍑 8854095900 👄🫦Independent Escort Service Dehradun
Dehradun Call Girls Service ❤️🍑 8854095900 👄🫦Independent Escort Service Dehradun
 
❤️♀️@ Jaipur Call Girls ❤️♀️@ Meghna Jaipur Call Girls Number CRTHNR Call G...
❤️♀️@ Jaipur Call Girls ❤️♀️@ Meghna Jaipur Call Girls Number CRTHNR Call G...❤️♀️@ Jaipur Call Girls ❤️♀️@ Meghna Jaipur Call Girls Number CRTHNR Call G...
❤️♀️@ Jaipur Call Girls ❤️♀️@ Meghna Jaipur Call Girls Number CRTHNR Call G...
 
Model Call Girl in Subhash Nagar Delhi reach out to us at 🔝9953056974🔝
Model Call Girl in Subhash Nagar Delhi reach out to us at 🔝9953056974🔝Model Call Girl in Subhash Nagar Delhi reach out to us at 🔝9953056974🔝
Model Call Girl in Subhash Nagar Delhi reach out to us at 🔝9953056974🔝
 
Bangalore call girl 👯‍♀️@ Simran Independent Call Girls in Bangalore GIUXUZ...
Bangalore call girl 👯‍♀️@ Simran Independent Call Girls in Bangalore GIUXUZ...Bangalore call girl 👯‍♀️@ Simran Independent Call Girls in Bangalore GIUXUZ...
Bangalore call girl 👯‍♀️@ Simran Independent Call Girls in Bangalore GIUXUZ...
 
#9711199012# African Student Escorts in Delhi 😘 Call Girls Delhi
#9711199012# African Student Escorts in Delhi 😘 Call Girls Delhi#9711199012# African Student Escorts in Delhi 😘 Call Girls Delhi
#9711199012# African Student Escorts in Delhi 😘 Call Girls Delhi
 
Basics of Anatomy- Language of Anatomy.pptx
Basics of Anatomy- Language of Anatomy.pptxBasics of Anatomy- Language of Anatomy.pptx
Basics of Anatomy- Language of Anatomy.pptx
 
💚😋Chandigarh Escort Service Call Girls, ₹5000 To 25K With AC💚😋
💚😋Chandigarh Escort Service Call Girls, ₹5000 To 25K With AC💚😋💚😋Chandigarh Escort Service Call Girls, ₹5000 To 25K With AC💚😋
💚😋Chandigarh Escort Service Call Girls, ₹5000 To 25K With AC💚😋
 
Call Girls Hyderabad Just Call 9907093804 Top Class Call Girl Service Available
Call Girls Hyderabad Just Call 9907093804 Top Class Call Girl Service AvailableCall Girls Hyderabad Just Call 9907093804 Top Class Call Girl Service Available
Call Girls Hyderabad Just Call 9907093804 Top Class Call Girl Service Available
 
No Advance 9053900678 Chandigarh Call Girls , Indian Call Girls For Full Ni...
No Advance 9053900678 Chandigarh Call Girls , Indian Call Girls For Full Ni...No Advance 9053900678 Chandigarh Call Girls , Indian Call Girls For Full Ni...
No Advance 9053900678 Chandigarh Call Girls , Indian Call Girls For Full Ni...
 
Call Girl Price Amritsar ❤️🍑 9053900678 Call Girls in Amritsar Suman
Call Girl Price Amritsar ❤️🍑 9053900678 Call Girls in Amritsar SumanCall Girl Price Amritsar ❤️🍑 9053900678 Call Girls in Amritsar Suman
Call Girl Price Amritsar ❤️🍑 9053900678 Call Girls in Amritsar Suman
 
💚😋Kolkata Escort Service Call Girls, ₹5000 To 25K With AC💚😋
💚😋Kolkata Escort Service Call Girls, ₹5000 To 25K With AC💚😋💚😋Kolkata Escort Service Call Girls, ₹5000 To 25K With AC💚😋
💚😋Kolkata Escort Service Call Girls, ₹5000 To 25K With AC💚😋
 
VIP Call Girl Sector 32 Noida Just Book Me 9711199171
VIP Call Girl Sector 32 Noida Just Book Me 9711199171VIP Call Girl Sector 32 Noida Just Book Me 9711199171
VIP Call Girl Sector 32 Noida Just Book Me 9711199171
 

Germ cell tumor ovary.pptx

  • 1. Germ Cell Tumor Ovary Dr Abani Kanta Nanda MD Radiation Oncology AHPGIC, Cuttack
  • 3. • Germ cell tumors are derived from the primordial germ cells of the ovary. • Occur with only about one-tenth the incidence of malignant germ cell tumors of the testis. • Although they can arise in extragonadal sites such as the mediastinum and the retroperitoneum, the majority of germ cell tumors arise in the gonad from undifferentiated germ cells. • The variation in the site of these cancers is explained by the embryonic migration of the germ cells from the caudal part of the yolk sac to the dorsal mesentery before their incorporation into the sex cords of the developing gonads
  • 4. • Germ cell tumors are a model of a curable cancer. • The management of patients with ovarian germ cell tumors has largely been extrapolated from the much greater experience of treating males with the more common testicular germ cell tumors. • There have been many randomized trials for testicular germ cell tumors, which have provided a strong evidence base for treatment decision making. • The outcome of patients with testicular germ cell tumors is better in experienced centers, and it is reasonable to suggest the same will be true for the less common ovarian counterparts. • The cure rate is high, and attention is now being directed at reducing toxicity without compromising survival. • There are still a small number of patients who die from the disease, and studies are in progress to try to improve the outcome for this high-risk, poor-prognostic subset
  • 5. • Murugaesu et al. reported that stage and elevated tumor markers were independent poor prognostic indicators. • These findings are important because they identify similar prognostic factors for ovarian and testicular germ cell tumors, and are in accordance with the clinical observation that testicular and ovarian germ cell tumors behave similarly.
  • 8.
  • 9.
  • 10.
  • 11.
  • 12. • Ovarian germ cell tumors have a variable pattern of differentiation. • Dysgerminomas are primitive neoplasms that do not have the potential for further differentiation. • Embryonal carcinomas are composed of multipotential cells that are capable of further differentiation. • This lesion is the precursor of several other types of extraembryonic (yolk sac tumor, choriocarcinoma) or embryonic (teratoma) germ cell tumors. • The process of differentiation is dynamic, and the resulting neoplasms may be composed of different elements that show various stages of development (Teilum, 1965).
  • 13.
  • 14.
  • 15. Serum markers • Both α fetoprotein (AFP) and human chorionic gonadotropin (hCG) are secreted by some germ cell malignancies. • An elevated AFP and β-hCG can be clinically useful in the differential diagnosis of patients with a pelvic mass, and in monitoring patients after surgery. • Placental alkaline phosphatase (PLAP) and lactate dehydrogenase (LDH) are elevated in up to 95% of patients with dysgerminomas, and serial monitoring of serum LDH levels may be useful for monitoring the disease. • PLAP is more useful as an immunohistochemical marker than as a serum marker. • The classification of germ cell tumors is based both on histologic features and immunohistochemical expression of tumor markers.
  • 16. • In this scheme, embryonal carcinoma, which is composed of undifferentiated cells that synthesize both hCG and AFP, is the progenitor of several other germ cell tumors. • More differentiated germ cell tumors—such as the endodermal sinus tumor (EST) (Yolk sac tumor), which secretes AFP, and choriocarcinoma, which secretes hCG—are derived from the extraembryonic tissues; immature teratomas are derived from the embryonic cells and do not secrete hCG, but may be associated with an elevated AFP. • Elevated hCG levels are seen in 3% of dysgerminomas and the level is typically less than 100 International Unit. • AFP is never elevated in pure dysgerminomas.
  • 17.
  • 18.
  • 19. Symptoms • In contrast to the relatively slow-growing epithelial ovarian tumors, germ cell malignancies grow rapidly, and often are characterized by subacute pelvic pain related to capsular distention, hemorrhage, or necrosis. • The rapidly enlarging pelvic mass may produce pressure symptoms on the bladder or rectum, and menstrual irregularities also may occur in menarchal patients. • Acute symptoms associated with torsion or rupture can develop. • In more advanced cases, ascites may develop, and the patient may present with abdominal distention.
  • 20. Diagnosis and treatment • Adnexal masses measuring 2 cm or more in premenarchal girls or complex masses 8 cm or more in premenopausal patients will usually require surgical exploration. • In young patients, preoperative blood tests should include serum hCG, AFP, LDH and CA125 levels, a complete blood count, and liver function tests. • A radiograph of the chest is important because germ cell tumors can metastasize to the lungs or mediastinum. • A karyotype should ideally be obtained preoperatively on all premenarchal girls because of the propensity of these tumors to arise in dysgenetic gonads, but this may not be practical. • A preoperative computed tomographic (CT) scan or magnetic resonance imaging (MRI) may document the presence and extent of retroperitoneal lymphadenopathy or liver metastases, but unless there is very extensive metastatic disease, is unlikely to influence the decision to operate on the patient initially. • If postmenarchal patients have predominantly cystic lesions up to 8 cm in diameter, they may undergo observation or a trial of hormonal suppression for two cycles.
  • 21.
  • 22.
  • 23.
  • 24.
  • 25.
  • 26.
  • 27.
  • 28.
  • 30. • Dysgerminomas are the most common malignant germ cell tumor, accounting for approximately 30–40% of all ovarian cancers of germ cell origin. • They represent only 1–3% of all ovarian cancers, but represent as many as 5–10% of ovarian cancers in patients younger than 20 years of age. • Seventy-five percent of dysgerminomas occur between the ages of 10 and 30 years, 5% occur before the age of 10 years and they rarely occur after age 50. • They typically occur in young women and 20–30% of ovarian malignancies associated with pregnancy are dysgerminomas.
  • 31. • Approximately 5% of dysgerminomas occur in phenotypic females with abnormal gonads. • Dysgerminomas can be associated with patients who have pure gonadal dysgenesis (46XY, bilateral streak gonads), mixed gonadal dysgenesis (45X/46XY, unilateral streak gonad, contralateral testis), and the androgen insensitivity syndrome (46XY, testicular feminization). • Therefore, in premenarchal patients with a pelvic mass, the karyotype should be determined, particularly if a dysgerminoma is considered as the likely diagnosis.
  • 32. • Approximately 65% of dysgerminomas are stage I at diagnosis. • 85-90% of stage I tumors are confined to one ovary, while 10–15% are bilateral. • All other germ cell tumors are rarely bilateral. • In patients whose contralateral ovary has been preserved, a dysgerminoma can develop in 5–10% of them over the next 2 years. • This figure includes patients who have not received systemic chemotherapy, as well as patients with gonadal dysgenesis
  • 33. • In the 25% of patients who present with metastatic disease, the tumor most commonly spreads via the lymphatics, particularly to the higher para-aortic nodes. • Metastases to the contralateral ovary may be present • An uncommon site of metastatic disease is bone, and when metastasis to this site occurs, the metastases are seen typically in the lower vertebrae. • Metastases to the lungs, liver, brain, mediastinum and supraclavicular lymph nodes are rare.
  • 34. Treatment • The treatment of patients with early dysgerminoma is primarily surgical, including • resection of the primary lesion and • limited surgical staging–washings, omental biopsy, careful palpation of all peritoneal surfaces and retroperitoneal nodes, and biopsy of anything suspicious. • Chemotherapy is administered to patients with metastatic disease. • Because the disease principally affects young women, special consideration must be given to the preservation of fertility.
  • 35.
  • 36. • The role of surgery to resect residual masses following chemotherapy for dysgerminomas is not clear, as the vast majority of these patients will only have necrotic tissue and nonviable tumor. • In general, these patients should be closely monitored with scans and tumor markers. • A positron emission tomography (PET–CT) scan should be considered in patients who have bulky residual masses larger than 3 cm more than 4 weeks after chemotherapy. • If the PET–CT is positive or if there is a suggestion of progressive disease on scans, ideally there should be histologic confirmation of residual disease before embarking on salvage therapy.
  • 37. • In patients with stage IA dysgerminoma, unilateral oophorectomy alone results in a 5-year disease-free survival rate of greater than 95%. • The 5-year survival for patients with negative nodes was 95.7% compared to 82.8% for patients with positive nodes.
  • 39. • Immature teratomas typically contain immature neuroepithelium and may be pure immature teratomas or occur in combination with other germ cell tumors as mixed germ cell tumors. • The pure immature teratoma accounts for fewer than 1% of all ovarian cancers, but it is the second most common germ cell malignancy and represents 10–20% of all ovarian malignancies seen in women younger than 20 years of age. • Approximately 50% of pure immature teratomas of the ovary occur between the ages of 10 and 20 years, and they rarely occur in postmenopausal women.
  • 40. Grading • Those with less than one lower-power field of immature neuroepithelium on the slide with the greatest amount of immature neuroepithelium (grade 1) have a survival of at least 95%, whereas greater amounts of immature neuroepithelium (grades 2 and 3) appear to have a lower overall survival (approximately 85%). • This may not apply to immature teratomas of the ovary in children, because they appear to have a very good outcome with surgery alone, regardless of the degree of immaturity.
  • 41. Treatment • Surgery- • In a premenopausal patient where the tumor appears confined to a single ovary, unilateral oophorectomy and limited surgical staging should be performed. • Contralateral involvement is rare, and routine resection or wedge biopsy of the contralateral ovary is unnecessary. • Any suspicious lesions on the peritoneal surfaces should be sampled and submitted for histologic evaluation.
  • 42. • The most frequent site of dissemination is the peritoneum and, much less commonly, the retroperitoneal lymph nodes. • Blood-borne metastases to organ parenchyma such as the lungs, liver, or brain are uncommon. • Cure ultimately depends on the ability to deliver chemotherapy promptly. • Any surgical resection that may be potentially morbid and therefore delay chemotherapy should be resisted. • Surgical resection of any residual disease should be considered at the completion of chemotherapy.
  • 43. • Patients with stage IA, grade 1 tumors have an excellent prognosis, and no adjuvant therapy is required. In patients with high-grade, stage IA immature teratomas, adjuvant chemotherapy has commonly been given. • The inferiority of carboplatin was confirmed in a larger randomized trial reported by Horwich et al.. • In view of these results, BEP is the preferred treatment regimen. • The 3-day schedule has been found to be equivalent to a 5-day schedule for BEP chemotherapy. • A cycle of BEP consisted of etoposide 500 mg/m2 , administered at either 100 mg/m2 days 1 through 5 or 165 mg/m2 days 1 through 3, cisplatin 100 mg/m2 , administered at either 20 mg/m2 days 1 through 5 or 50 mg/m2 days 1 and 2. Bleomycin 30,000 International Unit is administered on days 1, 8, and 15 during cycles 1 through 3.
  • 44. Mature cystic teratoma • Malignant transformation of a mature teratoma is a rare event. • Squamous cell carcinoma is the most frequent subtype of malignancy, but adenocarcinomas, primary melanomas, and carcinoids may also rarely occur. • The risk is reported to be between 0.5% and 2% of teratomas, and usually occurs in postmenopausal patients. • Platinum-based chemotherapy with or without pelvic radiation is most often used for adjuvant treatment of early-stage disease (DosSantos, 2007). • However, regardless of treatment received. patients with advanced disease do poorly
  • 46. • yolk sac carcinomas because they are derived from the primitive yolk sac. • They are the third most frequent malignant germ cell tumor of the ovary. • median age of 18 years at diagnosis. • Approximately one-third of the patients are premenarchal at presentation. • Abdominal or pelvic pain occurs in approximately 75% of patients, whereas an asymptomatic pelvic mass is documented in 10% of patients. • Most ESTs secrete AFP and rarely may also elaborate detectable alpha-1- antitrypsin (AAT). • There is a good correlation between the extent of disease and the level of AFP, although discordance also has been observed. • The serum level of AFP is useful in monitoring the patient’s response to treatment, as well as in follow-up.
  • 47. Treatment • The treatment of an EST consists of surgical exploration, unilateral salpingo- oophorectomy, a frozen section for diagnosis, and limited surgical staging. • A hysterectomy and contralateral salpingo-oophorectomy should not be done. • Conservative surgery and adjuvant chemotherapy allow fertility preservation as with other germ cell tumors. • In patients with metastatic disease, all gross disease should be resected if possible. • Bilaterality is not seen in EST, and the other ovary is involved with metastatic disease only. • Most patients have early-stage disease: 71% stage I, 6% stage II, and 23% stage III
  • 48. • All patients should be treated with a cisplatin-based regimen such as BEP, which is considered the standard of care. • The chance of cure now approaches 100% for patients with early-stage disease, and is at least 75% for patients with more advanced-stage disease. • 3 cycles of BEP is considered optimal for good prognosis for low risk patients and four cycles for patients with intermediate to high-risk tumors. (extrapolated from GCT testis) • An alternative approach is to use VIP (etoposide, ifosfamide, and cisplatin) in patients with more advanced disease in whom bleomycin is contraindicated. • Four cycles of VIP are equivalent to four cycles of BEP.
  • 49. • Neoadjuvant chemotherapy followed by fertility-sparing surgery may also be a reasonable option for patients with advanced ovarian germ cell tumors not suitable for optimal cytoreduction. • POMB-ACE (cisplatin, vincristine, methotrexate, bleomycin, actinomycin D, cyclophosphamide, etoposide) regimen for high-risk germ cell tumors of any histologic type. • This protocol introduces seven drugs into the initial management, which is intended to reduce the chances of developing drug resistance, which may be particularly relevant for patients with large volume metastatic disease
  • 50. Embryonal Carcinoma • Embryonal carcinoma of the ovary is an extremely rare tumor that is distinguished from a choriocarcinoma of the ovary by the absence of syncytiotrophoblastic and cytotrophoblastic cells. • The patients are very young, their ages ranging between 4 and 28 years (median = 14 years). • Older patients have been reported. • Embryonal carcinomas may secrete estrogens, with the patient exhibiting symptoms and signs of precocious pseudopuberty or irregular bleeding. • The presentation is otherwise similar to that of the EST. • The primary lesions tend to be large, and approximately two-thirds are confined to one ovary at the time of presentation. • These lesions frequently secrete AFP and hCG, which are useful for following the response to subsequent therapy. • The treatment of embryonal carcinomas is the same as that for ESTs
  • 51. Choriocarcinoma of the Ovary • Pure nongestational choriocarcinoma of the ovary is an extremely rare tumor. • Histologically, it has the same appearance as gestational choriocarcinoma metastatic to the ovaries. • The majority of patients with this cancer are younger than 20 years. • The presence of hCG can be useful in monitoring the patient’s response to treatment. • In the presence of high hCG levels, isosexual precocity has been seen, occurring in approximately 50% of patients whose tumors appear before menarche.
  • 52. • There are only a few limited reports on the use of chemotherapy for these nongestational choriocarcinomas, but complete responses have been reported to the MAC regimen (methotrexate, actinomycin D, and cyclophosphamide) as described for gestational trophoblastic disease. • These tumors are so rare that no good data are available, but the options also include the BEP or POMB-ACE regimens. • The prognosis for ovarian choriocarcinomas has been poor. • The majority of patients have metastases to organ parenchyma at the time of initial diagnosis, and they should be managed as high-risk germ cell tumors.
  • 53. Polyembryoma • Polyembryoma of the ovary is another extremely rare tumor, which is composed of “embryoid bodies.” • This tumor replicates the structures of early embryonic differentiation (i.e., the three somatic layers: Endoderm, mesoderm, and ectoderm). • They occur in very young, premenarchal girls with signs of pseudopuberty, and AFP and hCG levels are elevated. • Women with polyembryomas confined to one ovary may be followed with serial tumor markers and diagnostic-imaging techniques to avoid cytotoxic chemotherapy. • In patients who require chemotherapy, the BEP regimen is appropriate.
  • 54. Mixed germ cell malignancies • Mixed germ cell malignancies of the ovary contain two or more elements of the tumors described above. • In one series (107), the most common component of a mixed germ cell tumor was dysgerminoma, which occurred in 80%, followed by EST in 70%, immature teratoma in 53%, choriocarcinoma in 20%, and embryonal carcinoma in 16%. • The most frequent combination was a dysgerminoma and an EST. • The mixed germ cell tumors may secrete either AFP or hCG— or both or neither—depending on the components. • These tumors should be managed with combination chemotherapy, preferably BEP. • The serum marker, if positive initially, may become negative during chemotherapy, but this may reflect regression of only a particular component of the mixed lesion.
  • 55. • Therefore, a second-look laparotomy may be indicated if there is residual disease following chemotherapy, particularly if there was an immature teratomatous component in the original tumor. • The most important prognostic features are the size of the primary tumor and the relative percentage of its most malignant component. • In stage IA lesions smaller than 10 cm, survival is 100%. • Tumors composed of less than one-third EST, choriocarcinoma, or grade 3 immature teratoma also have an excellent prognosis, but it is possibly less favorable when these components comprise the majority of the tumor.
  • 56. Take home message • Germ cell tumors are derived from the primordial germ cells of the ovary. • The primary treatment is surgery followed by chemotherapy. • Surgical treatment of GCT ovary is resection of tumor with limited surgical staging. Fertility is preserved if required. • BEP is the most effective chemotherapy. • Tumor markers are very very important for response to treatment and follow up.