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Ovarian tumours

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Kapila Gunawardana

This document discusses ovarian tumours, including their epidemiology, embryology, risk factors, classification, staging, pathology, screening, management, and various treatment options. It addresses how ovarian cancer accounts for nearly 4% of cancers in women and is a leading cause of death from female genital tract malignancies. Various types of ovarian tumours are described, such as epithelial tumours including serous, mucinous and endometrioid tumours, as well as sex cord-stromal tumours and germ cell tumours. Risk factors, prevention strategies, and challenges with screening for early detection are also summarized.

TechnologieSanté & Médecine
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Ovarian TumoursOvarian Tumours Kapila GunawardanaKapila Gunawardana M.B.B.S.,M.S.(Obs & Gyn), F.R.C.O.G.,F.C.O.C.(S.L )M.B.B.S.,M.S.(Obs & Gyn), F.R.C.O.G.,F.C.O.C.(S.L ) Consultant Obstetrician and GynaecologistConsultant Obstetrician and Gynaecologist Teaching Hospital,Teaching Hospital, Peradeniya.Peradeniya.
OvarianOvarian TumoursTumours  EpidemiologyEpidemiology  EmbryologyEmbryology  AetiologyAetiology  Risk factorsRisk factors  WHO classificationWHO classification  StagingStaging  Pathology of ovarianPathology of ovarian tumourstumours  ScreeningScreening  Natural historyNatural history  Prognostic factorsPrognostic factors  Management (diagnosis &Management (diagnosis & management)management)  SurgerySurgery  RadiotherapyRadiotherapy  ChemotherapyChemotherapy  HRT for post treatmentHRT for post treatment  Immune therapyImmune therapy  Gene therapyGene therapy
WhyWhy is it important?is it important?  Accounts for nearly 4% of all cancers occurring in womenAccounts for nearly 4% of all cancers occurring in women  Leading cause of death from malignancies arising in theLeading cause of death from malignancies arising in the female genital tractfemale genital tract  Life time riskLife time risk in the general population is 1.5%in the general population is 1.5% with one affected family member is 4%with one affected family member is 4% with two affected family members is 7%with two affected family members is 7% with BRCA-1 & BRCA-2 gene mutation 16-65%with BRCA-1 & BRCA-2 gene mutation 16-65%  Most fatal and most feared cancerMost fatal and most feared cancer  The risk could be reducedThe risk could be reduced
EmbryologyEmbryology of the ovaryof the ovary  Primitive gonads appear around the 5Primitive gonads appear around the 5thth week of IUL as theweek of IUL as the gonadal ridge from the coelomic epithelium on the medialgonadal ridge from the coelomic epithelium on the medial aspect of the urogenital ridge.aspect of the urogenital ridge.  In the xx embryo , the cortex develop as the ovary and theIn the xx embryo , the cortex develop as the ovary and the medulla regress to a small area.medulla regress to a small area.  The ovarian serosa is the direct descent of the coelomicThe ovarian serosa is the direct descent of the coelomic epithelium and it give rises toepithelium and it give rises to endocervical,endometrial,endosalphinx and theendocervical,endometrial,endosalphinx and the epithelium of the urogenital system.epithelium of the urogenital system.  The undifferentiated serosal cells can undergo neoplasticThe undifferentiated serosal cells can undergo neoplastic changes and lead to tumours of the above tissues.changes and lead to tumours of the above tissues.
Development of the ovaryDevelopment of the ovary 1. Cortical cords 2. Degenerating mesonephric tubule 3. Mesonephric duct 4. Paramesonephric duct 5. Degenerating medullary cords 6. Surface epithelium
WHO Classification of ovarian tumoursWHO Classification of ovarian tumours 1.Epithelial tumours1.Epithelial tumours Benign,Boarderline tumours andBenign,Boarderline tumours and CarcinomasCarcinomas 2.Sex cord and Mesenchymal tumours2.Sex cord and Mesenchymal tumours Benign,Boarderline tumours andBenign,Boarderline tumours and carcinomascarcinomas 3.Germ cell tumours3.Germ cell tumours Benign,Boarderline tumours andBenign,Boarderline tumours and carcinomascarcinomas
WHO Classification,contWHO Classification,cont 1.EPITHELIAL TUMOURS1.EPITHELIAL TUMOURS  Serous tumoursSerous tumours  Mucinous tumoursMucinous tumours  Endometroid tumoursEndometroid tumours  Clear cell tumoursClear cell tumours  Brenner tumoursBrenner tumours  Mixed tumoursMixed tumours  Undifferentiated tumoursUndifferentiated tumours  Unclassified epithelial tumoursUnclassified epithelial tumours  Metastatic tumoursMetastatic tumours
1.Epithelial tumours1.Epithelial tumours ClassificationClassification  Pathway of differentiationPathway of differentiation  Potential biologic behaviourPotential biologic behaviour  Epithelium of fallopian tube(serous tumours)  Endocervix (mucinous tumours)  Endometrium (endometroid tumours)  Urinary bladder (Brenner tumours)
Serous tumours – Serous cystadenomaSerous tumours – Serous cystadenoma  Reproductive yearsReproductive years  10% bilateral10% bilateral  Cystic and unilocularCystic and unilocular  No solid areasNo solid areas  Smooth inner and outerSmooth inner and outer cystic linings and clearcystic linings and clear serous contentsserous contents
Serous cystadenofibromaSerous cystadenofibroma  Size 1 - 20 cmSize 1 - 20 cm  Similar appearance toSimilar appearance to serous cystadenoma withserous cystadenoma with clusters of small firmclusters of small firm whitish noduleswhitish nodules
Serous tumour of low malignant potentialSerous tumour of low malignant potential (LMP, borderline tumours)(LMP, borderline tumours)  Mostly cysticMostly cystic  Exuberant papillaryExuberant papillary projections on inner/outerprojections on inner/outer surfacessurfaces  Usually no necrosis orUsually no necrosis or haemorrhagehaemorrhage  20-40% of cases have20-40% of cases have omental implantsomental implants  Also pelvic, peritoneum,Also pelvic, peritoneum, mesosalpinxmesosalpinx
Serous carcinomaSerous carcinoma  Commonest primaryCommonest primary malignant ovarianmalignant ovarian neoplasmneoplasm  40-60 years40-60 years  50% bilateral50% bilateral  Serosanguinous fluid,Serosanguinous fluid, friable haemorrhagicfriable haemorrhagic cyst contentscyst contents
Mucinous tumours – MucinousMucinous tumours – Mucinous cystadenomacystadenoma  Reproductive age  5% bilateral  Cystic and multilocular, smooth lining, thick mucinous contents  Large in size : 1 - 50 cm
WHO Classification - contWHO Classification - cont 2 .2 .SEX CORD STROMAL(GONADAL) TUMOURSSEX CORD STROMAL(GONADAL) TUMOURS  Granulose theca cell tumoursGranulose theca cell tumours  Sertoli-Leydig cell tumourSertoli-Leydig cell tumour  Malignant thecomas(Gynandroblastomas)Malignant thecomas(Gynandroblastomas)
SCST with ovarian differentiationSCST with ovarian differentiation Adult granulosa cell tumoursAdult granulosa cell tumours  95% post pubertal95% post pubertal  50% post menopausal50% post menopausal  5% bilateral5% bilateral  Frequently associated withFrequently associated with hyperoestrogenismhyperoestrogenism (DUB, endometrial(DUB, endometrial hyperplasia and evenhyperplasia and even carcinoma)carcinoma)  Prognostic factors-Prognostic factors- size(<5cm-100%, 6-size(<5cm-100%, 6- 15cm- 60%,>15cm-15cm- 60%,>15cm- 50%)50%) mitotic activitymitotic activity stage- best prognosticstage- best prognostic indicatorindicator tumour rupturetumour rupture
SCST with testicular differentiationSCST with testicular differentiation Sertoli leydig cell tumourSertoli leydig cell tumour  Mixed cell typesMixed cell types  0.2% of ovarian tumours0.2% of ovarian tumours  Reproductive ageReproductive age  50% androgenized, rare50% androgenized, rare estrogenic effectsestrogenic effects  1.5% bilateral1.5% bilateral  Well differentiated tumoursWell differentiated tumours – good prognosis– good prognosis
FibromaFibroma
WHO Classification - ctdWHO Classification - ctd 3.3.GERM CELL TUMOURSGERM CELL TUMOURS  DysgerminomasDysgerminomas  Embroyonal (tumours of totipotential cells) carcinomasEmbroyonal (tumours of totipotential cells) carcinomas -Embroyonic-Teratomas(mature/immature)-Embroyonic-Teratomas(mature/immature) -Extra embryonic –Endodermal sinus tumours-Extra embryonic –Endodermal sinus tumours .Yolk sac and non-gestational choriocarcinomas.Yolk sac and non-gestational choriocarcinomas .Mixed germ cell tumours.Mixed germ cell tumours
 2nd most common germ cell tumour2nd most common germ cell tumour  Elevated AFP (alpha feto protein)Elevated AFP (alpha feto protein)  MalignantMalignant  RadioresistantRadioresistant  UnilateralUnilateral Endodermal sinus tumour (yolk sac tumours)
 Large, solid and lobulatedLarge, solid and lobulated  Grey white with necrosisGrey white with necrosis  Schiller-Duvall bodiesSchiller-Duvall bodies (glomeruloid tufts)(glomeruloid tufts)  Microscopic patterns-Microscopic patterns- papillary, alveolar,papillary, alveolar, microcystic, cystic, solidmicrocystic, cystic, solid  Myxomatous, polyvesicularMyxomatous, polyvesicular  PAS positive hyalinePAS positive hyaline globulesglobules Endodermal sinus tumour (yolk sac tumours) cont.
TeratomaTeratoma  Derived from all threeDerived from all three germ layers; ectoderm,germ layers; ectoderm, mesoderm andmesoderm and endodermendoderm  Variable according toVariable according to the degree ofthe degree of “maturity”“maturity”  Immature elementsImmature elements show features ofshow features of primitive embryonicprimitive embryonic tissuestissues
Metastatic carcinoma of the ovary
AetiologyAetiology  Hereditary cancersHereditary cancers 10% occurs in women who carry mutations in cancer10% occurs in women who carry mutations in cancer susceptibility genes BRCA-1,BRCA-2(these aresusceptibility genes BRCA-1,BRCA-2(these are tumour suppressor genes)tumour suppressor genes)
AetiologyAetiology - ctd- ctd  Sporadic cancersSporadic cancers -90% of the cases-90% of the cases -alteration of the p53 tumour suppressor is the most-alteration of the p53 tumour suppressor is the most frequent genetic eventfrequent genetic event (amplification,overexpression,mutation and deletion)(amplification,overexpression,mutation and deletion)
AetiologyAetiology  Incessant ovulationIncessant ovulation  Gonadotrophin and sex hormone therapyGonadotrophin and sex hormone therapy -Inclusion cyst formation-Inclusion cyst formation -Repair of the germinal epithelium following-Repair of the germinal epithelium following ovulationovulation -Persistent stimulation and exposure to-Persistent stimulation and exposure to gonadotrophinsgonadotrophins and sex hormones(proliferation and mitotic activity)and sex hormones(proliferation and mitotic activity) -Theoretical risk of artificial ovulation induction-Theoretical risk of artificial ovulation induction
Risk factorsRisk factors  Advanced age(average age is 60 yrs)Advanced age(average age is 60 yrs) -90%of the tumours occur among post menapausal-90%of the tumours occur among post menapausal femalesfemales -<40 yrs infrequent-<40 yrs infrequent -<30 yrs fewer than 3/100,00-<30 yrs fewer than 3/100,00  Caucasian 1Caucasian 1stst degree relative with Ca-3.5 fold riskdegree relative with Ca-3.5 fold risk  BRCA-1, BRCA-2 mutant genes (17q,13q)BRCA-1, BRCA-2 mutant genes (17q,13q)  NulliparityNulliparity  Early age of menarcheEarly age of menarche  Late age of menopauseLate age of menopause  Non usage of contraceptivesNon usage of contraceptives  Personal or family history of breast, ovarian or colonic CaPersonal or family history of breast, ovarian or colonic Ca (hnpcc)(hnpcc)
PREVENTION (FACTORS REDUCING THEPREVENTION (FACTORS REDUCING THE RISK FOR OVARIAN CANCER)RISK FOR OVARIAN CANCER)  ““Reduction of ovarian cancer predominantly are associatedReduction of ovarian cancer predominantly are associated with reduction in the number of ovulatory cycleswith reduction in the number of ovulatory cycles  Prolong use of OCPProlong use of OCP  MultiparityMultiparity  Breast feedingBreast feeding  Tubal legationsTubal legations  Place of prophylactic oophorectomy (performed when she isPlace of prophylactic oophorectomy (performed when she is still in the reproductive age-specially with a family history ofstill in the reproductive age-specially with a family history of ovarian cancer. There is reduction in the incidence of ovarianovarian cancer. There is reduction in the incidence of ovarian and breast cancer)and breast cancer)  Use of vitamin A derivativesUse of vitamin A derivatives  ScreeningScreening
SCREENING FOR OVARIAN TUMOURSSCREENING FOR OVARIAN TUMOURS WHO CRETERIA FOR A SCREENING PROGRAMMEWHO CRETERIA FOR A SCREENING PROGRAMME  The condition should an important health problemThe condition should an important health problem  There should be an accepted treatment for the patients withThere should be an accepted treatment for the patients with recognized diseaserecognized disease  Facilities for diagnosis and treatment should be availableFacilities for diagnosis and treatment should be available  There should be a recognized early stage of the diseaseThere should be a recognized early stage of the disease  There should be a suitable testThere should be a suitable test  The test should be acceptable to the populationThe test should be acceptable to the population  The natural history of the condition should be wellThe natural history of the condition should be well understoodunderstood  There should be an agreed policy on whom to screenThere should be an agreed policy on whom to screen  It should be cost effectiveIt should be cost effective  Case finding should be a continuning processCase finding should be a continuning process
OVARIAN TUMOUR SCREENING MULTIOVARIAN TUMOUR SCREENING MULTI MODELMODEL ca 125 and vaginal scanningca 125 and vaginal scanning Ca 125 >30 uml is abnormalCa 125 >30 uml is abnormal Ca 125 is an antigen found in the foetal amniotic and coelomic epithelium.inCa 125 is an antigen found in the foetal amniotic and coelomic epithelium.in adults it is found in mesothelial cells of pleuraadults it is found in mesothelial cells of pleura Pericardium and tubal, endometrial, endocervical and the ovary.Pericardium and tubal, endometrial, endocervical and the ovary. The surface epithelium of normal foetal and adult ovaries does not expressThe surface epithelium of normal foetal and adult ovaries does not express the antigen , except in inclusion cysts, papillae or metaplasiathe antigen , except in inclusion cysts, papillae or metaplasia An elevated level is found in 50% of stage 1 and >90% in women withAn elevated level is found in 50% of stage 1 and >90% in women with advanced disease.advanced disease. Sensitivity is 97%Sensitivity is 97% Specificity is 96%Specificity is 96% False positive in ca endometrium ca colon, endometriosis, fibroid, PID,False positive in ca endometrium ca colon, endometriosis, fibroid, PID, pregnancy and menstruationpregnancy and menstruation
OVARIAN TUMOUR SCREENINGOVARIAN TUMOUR SCREENING-ctd-ctd  Ovarian volume >20ml in reproductive age, andOvarian volume >20ml in reproductive age, and >8-10ml in post menopausal are abnormal.>8-10ml in post menopausal are abnormal.  Ultrasound findings (scoring system)Ultrasound findings (scoring system)  VolumeVolume  Thick wallThick wall  SeptaeSeptae  Solid areaSolid area  Cystic areas with solid areasCystic areas with solid areas  PapillaePapillae  AscitisAscitis  SecondarySecondary
Microscopic features suggestive ofMicroscopic features suggestive of MalignancyMalignancy  HyperchromaciaHyperchromacia  PolychromasiaPolychromasia  Nuclear atypiaNuclear atypia  Increased nuclearIncreased nuclear cytoplasmic ratiocytoplasmic ratio  Invasion of basementInvasion of basement membranemembrane
Macroscopic features suggestiveMacroscopic features suggestive of malignancyof malignancy  Cystic and solid areasCystic and solid areas  Hemorrhagic areasHemorrhagic areas  Necrotic areasNecrotic areas  Increased vascularityIncreased vascularity  Bilateral tumoursBilateral tumours  Associated ascitisAssociated ascitis
SURGICAL STAGINGSURGICAL STAGING Stage 1-growth limited to ovariesStage 1-growth limited to ovaries 1a growth limited to one ovary1a growth limited to one ovary 1b growth limited to both ovaries1b growth limited to both ovaries 1c tumour either 1a or 1b with any of the1c tumour either 1a or 1b with any of the followingfollowing - tumuor on the surface- tumuor on the surface - capsular rupture- capsular rupture - Ascitis containing malignant cells- Ascitis containing malignant cells - Positive peritoneal washings- Positive peritoneal washings
SURGICAL STAGING-ctdSURGICAL STAGING-ctd Stage ii growth involving one or both ovaries withStage ii growth involving one or both ovaries with pelvic extensionspelvic extensions ii a extension or metastasis to the uterus or tubesii a extension or metastasis to the uterus or tubes ii b extension to other pelvic tissuesii b extension to other pelvic tissues ii c tumour either 1a or 1b with any of the followingii c tumour either 1a or 1b with any of the following -tumour on the surface-tumour on the surface -capsular rupture-capsular rupture -ascitis containing malignant cells-ascitis containing malignant cells -positive peritoneal washings-positive peritoneal washings
SURGICAL STAGING- ContSURGICAL STAGING- Cont Stage iii growth involving one or both ovaries withStage iii growth involving one or both ovaries with peritoneal implants out side the pelvis or positiveperitoneal implants out side the pelvis or positive inguinal or retro-peritoneal nodes (superficial liveringuinal or retro-peritoneal nodes (superficial liver metastasis or histologically proven omental or bowelmetastasis or histologically proven omental or bowel metastasis)metastasis) iii a limited to true pelvis with negative nodes butiii a limited to true pelvis with negative nodes but with microscopically positive seedingswith microscopically positive seedings iii b tumour implants in the abdominal cavity<2cmiii b tumour implants in the abdominal cavity<2cm iii c tumour implants in the abdominal cavity >2cmiii c tumour implants in the abdominal cavity >2cm with positive nodeswith positive nodes
SURGICAL STAGING- ContSURGICAL STAGING- Cont  Stage iv growth involving one or both ovariesStage iv growth involving one or both ovaries with distant metastasiswith distant metastasis  If pleural effusion is present there must beIf pleural effusion is present there must be positive cytologypositive cytology
PROGNOSTIC FACTORSPROGNOSTIC FACTORS  Pathological factorsPathological factors -architecture and grade of lesion-architecture and grade of lesion -differentiation and anaplasia-differentiation and anaplasia  Biological factorsBiological factors - flow cytometry- flow cytometry - diploidy/anaploidy- diploidy/anaploidy  Clinical factorsClinical factors
NATURAL HISORYNATURAL HISORY  2/3 of the patients present with advanced disease2/3 of the patients present with advanced disease  Pattern of spread-trans-coelomicPattern of spread-trans-coelomic -lymphatic-lymphatic -haematogenic-haematogenic  stage i-5 years survival 90%stage i-5 years survival 90%  stage ii-5 year survival 70%stage ii-5 year survival 70%  stage iii& iv – 5 year survival 30%stage iii& iv – 5 year survival 30%  Most of them succumb following anorexia, vomitingMost of them succumb following anorexia, vomiting and catchexiaand catchexia
MANAGEMENTMANAGEMENT DIADNOSIS, PRE-OPERATIVEDIADNOSIS, PRE-OPERATIVE ASSESMENT &TREATMENTASSESMENT &TREATMENT  DiagnosisDiagnosis -History-History -Examination-Examination -Investigation-Investigation  Treatment optionTreatment option -Surgery-Surgery -Chemotherapy-Chemotherapy -Radiotherapy-Radiotherapy -Immunotherapy-Immunotherapy -Gene- therapy-Gene- therapy
DIAGNOSISDIAGNOSIS  HISTORYHISTORY -most women with epithelial tumours are-most women with epithelial tumours are asymptomatic for a long durationasymptomatic for a long duration -often the symptoms are vague-often the symptoms are vague -irregular menstruation-irregular menstruation -bowel and urinary symptoms-bowel and urinary symptoms -distention, bloating,constipation,nausea,vomiting-distention, bloating,constipation,nausea,vomiting and anorexia in advanced stagesand anorexia in advanced stages
DIAGNOSISDIAGNOSIS  EXAMINATIONEXAMINATION - information about the tumour and the- information about the tumour and the fitness for surgeryfitness for surgery - post-menopausal palpable ovary- post-menopausal palpable ovary syndromesyndrome - the presence of a pelvic mass (fixed,- the presence of a pelvic mass (fixed, irregular, solid ,cystic and solid, bilateralirregular, solid ,cystic and solid, bilateral - if in additional, an upper abdominal mass- if in additional, an upper abdominal mass or ascitis is present, the diagnosis ofor ascitis is present, the diagnosis of ovarian malignancy is certain.ovarian malignancy is certain.
INVESTIGATIONSINVESTIGATIONS  Routine investigationRoutine investigation - Hb- Hb - UFR- UFR - FBS- FBS - BUSE- BUSE - LFT- LFT - ECG- ECG - CXR- CXR
INVESTIGATIONSINVESTIGATIONS  Special investigationSpecial investigation - Ca 125- Ca 125 - Alpha feto protein- Alpha feto protein - Ultrasound scan- Ultrasound scan - CT scan- CT scan - MRI scan- MRI scan
PRE-OPERATIVE ASSESMENTPRE-OPERATIVE ASSESMENT  Optimize the healthOptimize the health - Correction- Correction - Medical fitness- Medical fitness - Anti-coagulation- Anti-coagulation
SURGICALSURGICAL MANAGEMENTMANAGEMENT  THE CORNER STONE OF THEREPY FOR OVARIANTHE CORNER STONE OF THEREPY FOR OVARIAN MALINANCY IS SURGERYMALINANCY IS SURGERY
SURGICALSURGICAL MANAGEMENTMANAGEMENT  Conservative surgeryConservative surgery -stage 1a-stage 1a -if the patient has not completed her family-if the patient has not completed her family  Radical surgeryRadical surgery -stage 1b-c-stage 1b-c  Cytoreductive surgeryCytoreductive surgery -advanced stage-advanced stage  Second look laparotomy/laparoscopySecond look laparotomy/laparoscopy  Second cytoreductivesurgerySecond cytoreductivesurgery  Salvage therapySalvage therapy
SURGICALSURGICAL MANAGEMENTMANAGEMENT  ProcedureProcedure - vertical abdominal incision- vertical abdominal incision - collect peritoneal fluid- collect peritoneal fluid - systematic exploration- systematic exploration - biopsies- biopsies - TAH+BSO- TAH+BSO - omentectomy- omentectomy - appendicetomy- appendicetomy - pelvic and para-aortic lymph node sampling- pelvic and para-aortic lymph node sampling
CHEMOTHERAPYCHEMOTHERAPY  Alkylating agentsAlkylating agents -interfere with base pairing leading to inhibition of-interfere with base pairing leading to inhibition of DNA,RNA and protein synthesis (Cyclophoshamide,DNA,RNA and protein synthesis (Cyclophoshamide, melphalan, chlorambucil)melphalan, chlorambucil)  Anti-tumour antibioticsAnti-tumour antibiotics -Inserted between DNA base pairs-Inserted between DNA base pairs (Bleomycin,Mitomycin)(Bleomycin,Mitomycin)  Ante-metabolites(Methotrexate,5FU)Ante-metabolites(Methotrexate,5FU)  Plant alkaloidPlant alkaloid -bind to vital intra-cellular micro-tubular proteins-bind to vital intra-cellular micro-tubular proteins (Vincristine , vinblastine , paclitaxel)(Vincristine , vinblastine , paclitaxel)
CHEMOTHERAPYCHEMOTHERAPY Early stageEarly stage -stage 1a,1b,grade 1&2-stage 1a,1b,grade 1&2 -no further adjuvant therapy is needed-no further adjuvant therapy is needed Early stageEarly stage -1c or poorly differentiated-1c or poorly differentiated -low risk-low risk -alkylating agents and plant alkaloids-alkylating agents and plant alkaloids Advanced ovarian caAdvanced ovarian ca -carboplatin and paclitaxel – 3H every 3 weeks for 6 cycles-carboplatin and paclitaxel – 3H every 3 weeks for 6 cycles -single agent carboplatin-single agent carboplatin
RADIORADIO THERAPYTHERAPY  Intra peritoneal radio-colloids (p53)Intra peritoneal radio-colloids (p53)  Whole abdominal radiationWhole abdominal radiation
IMMUNOTHERAPYIMMUNOTHERAPY  Biological response modifier therapyBiological response modifier therapy (corynebacterium parvum,BCD)(corynebacterium parvum,BCD) -enhancement of host immune response & tumour rejection-enhancement of host immune response & tumour rejection  Cytokines therapyCytokines therapy -interferons,tumour necrosis factor-alpha, interleukin-2.-interferons,tumour necrosis factor-alpha, interleukin-2.  Adaptive immunotherapyAdaptive immunotherapy -infusion of LAK cells-infusion of LAK cells  Intra-peritoneal gene therapyIntra-peritoneal gene therapy -expression of cytokine genes or genetic-expression of cytokine genes or genetic immunopotentiation (enhancement of anti-tumour immuneimmunopotentiation (enhancement of anti-tumour immune response)response)
GENEGENE THERAPYTHERAPY  Potential intervention at the molecular levelPotential intervention at the molecular level  Genetic immuno–potentiationGenetic immuno–potentiation

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Ovarian tumours

  • 1. Ovarian TumoursOvarian Tumours Kapila GunawardanaKapila Gunawardana M.B.B.S.,M.S.(Obs & Gyn), F.R.C.O.G.,F.C.O.C.(S.L )M.B.B.S.,M.S.(Obs & Gyn), F.R.C.O.G.,F.C.O.C.(S.L ) Consultant Obstetrician and GynaecologistConsultant Obstetrician and Gynaecologist Teaching Hospital,Teaching Hospital, Peradeniya.Peradeniya.
  • 2. OvarianOvarian TumoursTumours  EpidemiologyEpidemiology  EmbryologyEmbryology  AetiologyAetiology  Risk factorsRisk factors  WHO classificationWHO classification  StagingStaging  Pathology of ovarianPathology of ovarian tumourstumours  ScreeningScreening  Natural historyNatural history  Prognostic factorsPrognostic factors  Management (diagnosis &Management (diagnosis & management)management)  SurgerySurgery  RadiotherapyRadiotherapy  ChemotherapyChemotherapy  HRT for post treatmentHRT for post treatment  Immune therapyImmune therapy  Gene therapyGene therapy
  • 3. WhyWhy is it important?is it important?  Accounts for nearly 4% of all cancers occurring in womenAccounts for nearly 4% of all cancers occurring in women  Leading cause of death from malignancies arising in theLeading cause of death from malignancies arising in the female genital tractfemale genital tract  Life time riskLife time risk in the general population is 1.5%in the general population is 1.5% with one affected family member is 4%with one affected family member is 4% with two affected family members is 7%with two affected family members is 7% with BRCA-1 & BRCA-2 gene mutation 16-65%with BRCA-1 & BRCA-2 gene mutation 16-65%  Most fatal and most feared cancerMost fatal and most feared cancer  The risk could be reducedThe risk could be reduced
  • 4. EmbryologyEmbryology of the ovaryof the ovary  Primitive gonads appear around the 5Primitive gonads appear around the 5thth week of IUL as theweek of IUL as the gonadal ridge from the coelomic epithelium on the medialgonadal ridge from the coelomic epithelium on the medial aspect of the urogenital ridge.aspect of the urogenital ridge.  In the xx embryo , the cortex develop as the ovary and theIn the xx embryo , the cortex develop as the ovary and the medulla regress to a small area.medulla regress to a small area.  The ovarian serosa is the direct descent of the coelomicThe ovarian serosa is the direct descent of the coelomic epithelium and it give rises toepithelium and it give rises to endocervical,endometrial,endosalphinx and theendocervical,endometrial,endosalphinx and the epithelium of the urogenital system.epithelium of the urogenital system.  The undifferentiated serosal cells can undergo neoplasticThe undifferentiated serosal cells can undergo neoplastic changes and lead to tumours of the above tissues.changes and lead to tumours of the above tissues.
  • 5. Development of the ovaryDevelopment of the ovary 1. Cortical cords 2. Degenerating mesonephric tubule 3. Mesonephric duct 4. Paramesonephric duct 5. Degenerating medullary cords 6. Surface epithelium
  • 6. WHO Classification of ovarian tumoursWHO Classification of ovarian tumours 1.Epithelial tumours1.Epithelial tumours Benign,Boarderline tumours andBenign,Boarderline tumours and CarcinomasCarcinomas 2.Sex cord and Mesenchymal tumours2.Sex cord and Mesenchymal tumours Benign,Boarderline tumours andBenign,Boarderline tumours and carcinomascarcinomas 3.Germ cell tumours3.Germ cell tumours Benign,Boarderline tumours andBenign,Boarderline tumours and carcinomascarcinomas
  • 7. WHO Classification,contWHO Classification,cont 1.EPITHELIAL TUMOURS1.EPITHELIAL TUMOURS  Serous tumoursSerous tumours  Mucinous tumoursMucinous tumours  Endometroid tumoursEndometroid tumours  Clear cell tumoursClear cell tumours  Brenner tumoursBrenner tumours  Mixed tumoursMixed tumours  Undifferentiated tumoursUndifferentiated tumours  Unclassified epithelial tumoursUnclassified epithelial tumours  Metastatic tumoursMetastatic tumours
  • 8. 1.Epithelial tumours1.Epithelial tumours ClassificationClassification  Pathway of differentiationPathway of differentiation  Potential biologic behaviourPotential biologic behaviour  Epithelium of fallopian tube(serous tumours)  Endocervix (mucinous tumours)  Endometrium (endometroid tumours)  Urinary bladder (Brenner tumours)
  • 9. Serous tumours – Serous cystadenomaSerous tumours – Serous cystadenoma  Reproductive yearsReproductive years  10% bilateral10% bilateral  Cystic and unilocularCystic and unilocular  No solid areasNo solid areas  Smooth inner and outerSmooth inner and outer cystic linings and clearcystic linings and clear serous contentsserous contents
  • 10. Serous cystadenofibromaSerous cystadenofibroma  Size 1 - 20 cmSize 1 - 20 cm  Similar appearance toSimilar appearance to serous cystadenoma withserous cystadenoma with clusters of small firmclusters of small firm whitish noduleswhitish nodules
  • 11. Serous tumour of low malignant potentialSerous tumour of low malignant potential (LMP, borderline tumours)(LMP, borderline tumours)  Mostly cysticMostly cystic  Exuberant papillaryExuberant papillary projections on inner/outerprojections on inner/outer surfacessurfaces  Usually no necrosis orUsually no necrosis or haemorrhagehaemorrhage  20-40% of cases have20-40% of cases have omental implantsomental implants  Also pelvic, peritoneum,Also pelvic, peritoneum, mesosalpinxmesosalpinx
  • 12. Serous carcinomaSerous carcinoma  Commonest primaryCommonest primary malignant ovarianmalignant ovarian neoplasmneoplasm  40-60 years40-60 years  50% bilateral50% bilateral  Serosanguinous fluid,Serosanguinous fluid, friable haemorrhagicfriable haemorrhagic cyst contentscyst contents
  • 13. Mucinous tumours – MucinousMucinous tumours – Mucinous cystadenomacystadenoma  Reproductive age  5% bilateral  Cystic and multilocular, smooth lining, thick mucinous contents  Large in size : 1 - 50 cm
  • 14. WHO Classification - contWHO Classification - cont 2 .2 .SEX CORD STROMAL(GONADAL) TUMOURSSEX CORD STROMAL(GONADAL) TUMOURS  Granulose theca cell tumoursGranulose theca cell tumours  Sertoli-Leydig cell tumourSertoli-Leydig cell tumour  Malignant thecomas(Gynandroblastomas)Malignant thecomas(Gynandroblastomas)
  • 15. SCST with ovarian differentiationSCST with ovarian differentiation Adult granulosa cell tumoursAdult granulosa cell tumours  95% post pubertal95% post pubertal  50% post menopausal50% post menopausal  5% bilateral5% bilateral  Frequently associated withFrequently associated with hyperoestrogenismhyperoestrogenism (DUB, endometrial(DUB, endometrial hyperplasia and evenhyperplasia and even carcinoma)carcinoma)  Prognostic factors-Prognostic factors- size(<5cm-100%, 6-size(<5cm-100%, 6- 15cm- 60%,>15cm-15cm- 60%,>15cm- 50%)50%) mitotic activitymitotic activity stage- best prognosticstage- best prognostic indicatorindicator tumour rupturetumour rupture
  • 16. SCST with testicular differentiationSCST with testicular differentiation Sertoli leydig cell tumourSertoli leydig cell tumour  Mixed cell typesMixed cell types  0.2% of ovarian tumours0.2% of ovarian tumours  Reproductive ageReproductive age  50% androgenized, rare50% androgenized, rare estrogenic effectsestrogenic effects  1.5% bilateral1.5% bilateral  Well differentiated tumoursWell differentiated tumours – good prognosis– good prognosis
  • 18. WHO Classification - ctdWHO Classification - ctd 3.3.GERM CELL TUMOURSGERM CELL TUMOURS  DysgerminomasDysgerminomas  Embroyonal (tumours of totipotential cells) carcinomasEmbroyonal (tumours of totipotential cells) carcinomas -Embroyonic-Teratomas(mature/immature)-Embroyonic-Teratomas(mature/immature) -Extra embryonic –Endodermal sinus tumours-Extra embryonic –Endodermal sinus tumours .Yolk sac and non-gestational choriocarcinomas.Yolk sac and non-gestational choriocarcinomas .Mixed germ cell tumours.Mixed germ cell tumours
  • 19.  2nd most common germ cell tumour2nd most common germ cell tumour  Elevated AFP (alpha feto protein)Elevated AFP (alpha feto protein)  MalignantMalignant  RadioresistantRadioresistant  UnilateralUnilateral Endodermal sinus tumour (yolk sac tumours)
  • 20.  Large, solid and lobulatedLarge, solid and lobulated  Grey white with necrosisGrey white with necrosis  Schiller-Duvall bodiesSchiller-Duvall bodies (glomeruloid tufts)(glomeruloid tufts)  Microscopic patterns-Microscopic patterns- papillary, alveolar,papillary, alveolar, microcystic, cystic, solidmicrocystic, cystic, solid  Myxomatous, polyvesicularMyxomatous, polyvesicular  PAS positive hyalinePAS positive hyaline globulesglobules Endodermal sinus tumour (yolk sac tumours) cont.
  • 21. TeratomaTeratoma  Derived from all threeDerived from all three germ layers; ectoderm,germ layers; ectoderm, mesoderm andmesoderm and endodermendoderm  Variable according toVariable according to the degree ofthe degree of “maturity”“maturity”  Immature elementsImmature elements show features ofshow features of primitive embryonicprimitive embryonic tissuestissues
  • 23. AetiologyAetiology  Hereditary cancersHereditary cancers 10% occurs in women who carry mutations in cancer10% occurs in women who carry mutations in cancer susceptibility genes BRCA-1,BRCA-2(these aresusceptibility genes BRCA-1,BRCA-2(these are tumour suppressor genes)tumour suppressor genes)
  • 24. AetiologyAetiology - ctd- ctd  Sporadic cancersSporadic cancers -90% of the cases-90% of the cases -alteration of the p53 tumour suppressor is the most-alteration of the p53 tumour suppressor is the most frequent genetic eventfrequent genetic event (amplification,overexpression,mutation and deletion)(amplification,overexpression,mutation and deletion)
  • 25. AetiologyAetiology  Incessant ovulationIncessant ovulation  Gonadotrophin and sex hormone therapyGonadotrophin and sex hormone therapy -Inclusion cyst formation-Inclusion cyst formation -Repair of the germinal epithelium following-Repair of the germinal epithelium following ovulationovulation -Persistent stimulation and exposure to-Persistent stimulation and exposure to gonadotrophinsgonadotrophins and sex hormones(proliferation and mitotic activity)and sex hormones(proliferation and mitotic activity) -Theoretical risk of artificial ovulation induction-Theoretical risk of artificial ovulation induction
  • 26. Risk factorsRisk factors  Advanced age(average age is 60 yrs)Advanced age(average age is 60 yrs) -90%of the tumours occur among post menapausal-90%of the tumours occur among post menapausal femalesfemales -<40 yrs infrequent-<40 yrs infrequent -<30 yrs fewer than 3/100,00-<30 yrs fewer than 3/100,00  Caucasian 1Caucasian 1stst degree relative with Ca-3.5 fold riskdegree relative with Ca-3.5 fold risk  BRCA-1, BRCA-2 mutant genes (17q,13q)BRCA-1, BRCA-2 mutant genes (17q,13q)  NulliparityNulliparity  Early age of menarcheEarly age of menarche  Late age of menopauseLate age of menopause  Non usage of contraceptivesNon usage of contraceptives  Personal or family history of breast, ovarian or colonic CaPersonal or family history of breast, ovarian or colonic Ca (hnpcc)(hnpcc)
  • 27. PREVENTION (FACTORS REDUCING THEPREVENTION (FACTORS REDUCING THE RISK FOR OVARIAN CANCER)RISK FOR OVARIAN CANCER)  ““Reduction of ovarian cancer predominantly are associatedReduction of ovarian cancer predominantly are associated with reduction in the number of ovulatory cycleswith reduction in the number of ovulatory cycles  Prolong use of OCPProlong use of OCP  MultiparityMultiparity  Breast feedingBreast feeding  Tubal legationsTubal legations  Place of prophylactic oophorectomy (performed when she isPlace of prophylactic oophorectomy (performed when she is still in the reproductive age-specially with a family history ofstill in the reproductive age-specially with a family history of ovarian cancer. There is reduction in the incidence of ovarianovarian cancer. There is reduction in the incidence of ovarian and breast cancer)and breast cancer)  Use of vitamin A derivativesUse of vitamin A derivatives  ScreeningScreening
  • 28. SCREENING FOR OVARIAN TUMOURSSCREENING FOR OVARIAN TUMOURS WHO CRETERIA FOR A SCREENING PROGRAMMEWHO CRETERIA FOR A SCREENING PROGRAMME  The condition should an important health problemThe condition should an important health problem  There should be an accepted treatment for the patients withThere should be an accepted treatment for the patients with recognized diseaserecognized disease  Facilities for diagnosis and treatment should be availableFacilities for diagnosis and treatment should be available  There should be a recognized early stage of the diseaseThere should be a recognized early stage of the disease  There should be a suitable testThere should be a suitable test  The test should be acceptable to the populationThe test should be acceptable to the population  The natural history of the condition should be wellThe natural history of the condition should be well understoodunderstood  There should be an agreed policy on whom to screenThere should be an agreed policy on whom to screen  It should be cost effectiveIt should be cost effective  Case finding should be a continuning processCase finding should be a continuning process
  • 29. OVARIAN TUMOUR SCREENING MULTIOVARIAN TUMOUR SCREENING MULTI MODELMODEL ca 125 and vaginal scanningca 125 and vaginal scanning Ca 125 >30 uml is abnormalCa 125 >30 uml is abnormal Ca 125 is an antigen found in the foetal amniotic and coelomic epithelium.inCa 125 is an antigen found in the foetal amniotic and coelomic epithelium.in adults it is found in mesothelial cells of pleuraadults it is found in mesothelial cells of pleura Pericardium and tubal, endometrial, endocervical and the ovary.Pericardium and tubal, endometrial, endocervical and the ovary. The surface epithelium of normal foetal and adult ovaries does not expressThe surface epithelium of normal foetal and adult ovaries does not express the antigen , except in inclusion cysts, papillae or metaplasiathe antigen , except in inclusion cysts, papillae or metaplasia An elevated level is found in 50% of stage 1 and >90% in women withAn elevated level is found in 50% of stage 1 and >90% in women with advanced disease.advanced disease. Sensitivity is 97%Sensitivity is 97% Specificity is 96%Specificity is 96% False positive in ca endometrium ca colon, endometriosis, fibroid, PID,False positive in ca endometrium ca colon, endometriosis, fibroid, PID, pregnancy and menstruationpregnancy and menstruation
  • 30. OVARIAN TUMOUR SCREENINGOVARIAN TUMOUR SCREENING-ctd-ctd  Ovarian volume >20ml in reproductive age, andOvarian volume >20ml in reproductive age, and >8-10ml in post menopausal are abnormal.>8-10ml in post menopausal are abnormal.  Ultrasound findings (scoring system)Ultrasound findings (scoring system)  VolumeVolume  Thick wallThick wall  SeptaeSeptae  Solid areaSolid area  Cystic areas with solid areasCystic areas with solid areas  PapillaePapillae  AscitisAscitis  SecondarySecondary
  • 31. Microscopic features suggestive ofMicroscopic features suggestive of MalignancyMalignancy  HyperchromaciaHyperchromacia  PolychromasiaPolychromasia  Nuclear atypiaNuclear atypia  Increased nuclearIncreased nuclear cytoplasmic ratiocytoplasmic ratio  Invasion of basementInvasion of basement membranemembrane
  • 32. Macroscopic features suggestiveMacroscopic features suggestive of malignancyof malignancy  Cystic and solid areasCystic and solid areas  Hemorrhagic areasHemorrhagic areas  Necrotic areasNecrotic areas  Increased vascularityIncreased vascularity  Bilateral tumoursBilateral tumours  Associated ascitisAssociated ascitis
  • 33. SURGICAL STAGINGSURGICAL STAGING Stage 1-growth limited to ovariesStage 1-growth limited to ovaries 1a growth limited to one ovary1a growth limited to one ovary 1b growth limited to both ovaries1b growth limited to both ovaries 1c tumour either 1a or 1b with any of the1c tumour either 1a or 1b with any of the followingfollowing - tumuor on the surface- tumuor on the surface - capsular rupture- capsular rupture - Ascitis containing malignant cells- Ascitis containing malignant cells - Positive peritoneal washings- Positive peritoneal washings
  • 34. SURGICAL STAGING-ctdSURGICAL STAGING-ctd Stage ii growth involving one or both ovaries withStage ii growth involving one or both ovaries with pelvic extensionspelvic extensions ii a extension or metastasis to the uterus or tubesii a extension or metastasis to the uterus or tubes ii b extension to other pelvic tissuesii b extension to other pelvic tissues ii c tumour either 1a or 1b with any of the followingii c tumour either 1a or 1b with any of the following -tumour on the surface-tumour on the surface -capsular rupture-capsular rupture -ascitis containing malignant cells-ascitis containing malignant cells -positive peritoneal washings-positive peritoneal washings
  • 35. SURGICAL STAGING- ContSURGICAL STAGING- Cont Stage iii growth involving one or both ovaries withStage iii growth involving one or both ovaries with peritoneal implants out side the pelvis or positiveperitoneal implants out side the pelvis or positive inguinal or retro-peritoneal nodes (superficial liveringuinal or retro-peritoneal nodes (superficial liver metastasis or histologically proven omental or bowelmetastasis or histologically proven omental or bowel metastasis)metastasis) iii a limited to true pelvis with negative nodes butiii a limited to true pelvis with negative nodes but with microscopically positive seedingswith microscopically positive seedings iii b tumour implants in the abdominal cavity<2cmiii b tumour implants in the abdominal cavity<2cm iii c tumour implants in the abdominal cavity >2cmiii c tumour implants in the abdominal cavity >2cm with positive nodeswith positive nodes
  • 36. SURGICAL STAGING- ContSURGICAL STAGING- Cont  Stage iv growth involving one or both ovariesStage iv growth involving one or both ovaries with distant metastasiswith distant metastasis  If pleural effusion is present there must beIf pleural effusion is present there must be positive cytologypositive cytology
  • 37. PROGNOSTIC FACTORSPROGNOSTIC FACTORS  Pathological factorsPathological factors -architecture and grade of lesion-architecture and grade of lesion -differentiation and anaplasia-differentiation and anaplasia  Biological factorsBiological factors - flow cytometry- flow cytometry - diploidy/anaploidy- diploidy/anaploidy  Clinical factorsClinical factors
  • 38. NATURAL HISORYNATURAL HISORY  2/3 of the patients present with advanced disease2/3 of the patients present with advanced disease  Pattern of spread-trans-coelomicPattern of spread-trans-coelomic -lymphatic-lymphatic -haematogenic-haematogenic  stage i-5 years survival 90%stage i-5 years survival 90%  stage ii-5 year survival 70%stage ii-5 year survival 70%  stage iii& iv – 5 year survival 30%stage iii& iv – 5 year survival 30%  Most of them succumb following anorexia, vomitingMost of them succumb following anorexia, vomiting and catchexiaand catchexia
  • 39. MANAGEMENTMANAGEMENT DIADNOSIS, PRE-OPERATIVEDIADNOSIS, PRE-OPERATIVE ASSESMENT &TREATMENTASSESMENT &TREATMENT  DiagnosisDiagnosis -History-History -Examination-Examination -Investigation-Investigation  Treatment optionTreatment option -Surgery-Surgery -Chemotherapy-Chemotherapy -Radiotherapy-Radiotherapy -Immunotherapy-Immunotherapy -Gene- therapy-Gene- therapy
  • 40. DIAGNOSISDIAGNOSIS  HISTORYHISTORY -most women with epithelial tumours are-most women with epithelial tumours are asymptomatic for a long durationasymptomatic for a long duration -often the symptoms are vague-often the symptoms are vague -irregular menstruation-irregular menstruation -bowel and urinary symptoms-bowel and urinary symptoms -distention, bloating,constipation,nausea,vomiting-distention, bloating,constipation,nausea,vomiting and anorexia in advanced stagesand anorexia in advanced stages
  • 41. DIAGNOSISDIAGNOSIS  EXAMINATIONEXAMINATION - information about the tumour and the- information about the tumour and the fitness for surgeryfitness for surgery - post-menopausal palpable ovary- post-menopausal palpable ovary syndromesyndrome - the presence of a pelvic mass (fixed,- the presence of a pelvic mass (fixed, irregular, solid ,cystic and solid, bilateralirregular, solid ,cystic and solid, bilateral - if in additional, an upper abdominal mass- if in additional, an upper abdominal mass or ascitis is present, the diagnosis ofor ascitis is present, the diagnosis of ovarian malignancy is certain.ovarian malignancy is certain.
  • 42. INVESTIGATIONSINVESTIGATIONS  Routine investigationRoutine investigation - Hb- Hb - UFR- UFR - FBS- FBS - BUSE- BUSE - LFT- LFT - ECG- ECG - CXR- CXR
  • 43. INVESTIGATIONSINVESTIGATIONS  Special investigationSpecial investigation - Ca 125- Ca 125 - Alpha feto protein- Alpha feto protein - Ultrasound scan- Ultrasound scan - CT scan- CT scan - MRI scan- MRI scan
  • 44. PRE-OPERATIVE ASSESMENTPRE-OPERATIVE ASSESMENT  Optimize the healthOptimize the health - Correction- Correction - Medical fitness- Medical fitness - Anti-coagulation- Anti-coagulation
  • 45. SURGICALSURGICAL MANAGEMENTMANAGEMENT  THE CORNER STONE OF THEREPY FOR OVARIANTHE CORNER STONE OF THEREPY FOR OVARIAN MALINANCY IS SURGERYMALINANCY IS SURGERY
  • 46. SURGICALSURGICAL MANAGEMENTMANAGEMENT  Conservative surgeryConservative surgery -stage 1a-stage 1a -if the patient has not completed her family-if the patient has not completed her family  Radical surgeryRadical surgery -stage 1b-c-stage 1b-c  Cytoreductive surgeryCytoreductive surgery -advanced stage-advanced stage  Second look laparotomy/laparoscopySecond look laparotomy/laparoscopy  Second cytoreductivesurgerySecond cytoreductivesurgery  Salvage therapySalvage therapy
  • 47. SURGICALSURGICAL MANAGEMENTMANAGEMENT  ProcedureProcedure - vertical abdominal incision- vertical abdominal incision - collect peritoneal fluid- collect peritoneal fluid - systematic exploration- systematic exploration - biopsies- biopsies - TAH+BSO- TAH+BSO - omentectomy- omentectomy - appendicetomy- appendicetomy - pelvic and para-aortic lymph node sampling- pelvic and para-aortic lymph node sampling
  • 48. CHEMOTHERAPYCHEMOTHERAPY  Alkylating agentsAlkylating agents -interfere with base pairing leading to inhibition of-interfere with base pairing leading to inhibition of DNA,RNA and protein synthesis (Cyclophoshamide,DNA,RNA and protein synthesis (Cyclophoshamide, melphalan, chlorambucil)melphalan, chlorambucil)  Anti-tumour antibioticsAnti-tumour antibiotics -Inserted between DNA base pairs-Inserted between DNA base pairs (Bleomycin,Mitomycin)(Bleomycin,Mitomycin)  Ante-metabolites(Methotrexate,5FU)Ante-metabolites(Methotrexate,5FU)  Plant alkaloidPlant alkaloid -bind to vital intra-cellular micro-tubular proteins-bind to vital intra-cellular micro-tubular proteins (Vincristine , vinblastine , paclitaxel)(Vincristine , vinblastine , paclitaxel)
  • 49. CHEMOTHERAPYCHEMOTHERAPY Early stageEarly stage -stage 1a,1b,grade 1&2-stage 1a,1b,grade 1&2 -no further adjuvant therapy is needed-no further adjuvant therapy is needed Early stageEarly stage -1c or poorly differentiated-1c or poorly differentiated -low risk-low risk -alkylating agents and plant alkaloids-alkylating agents and plant alkaloids Advanced ovarian caAdvanced ovarian ca -carboplatin and paclitaxel – 3H every 3 weeks for 6 cycles-carboplatin and paclitaxel – 3H every 3 weeks for 6 cycles -single agent carboplatin-single agent carboplatin
  • 50. RADIORADIO THERAPYTHERAPY  Intra peritoneal radio-colloids (p53)Intra peritoneal radio-colloids (p53)  Whole abdominal radiationWhole abdominal radiation
  • 51. IMMUNOTHERAPYIMMUNOTHERAPY  Biological response modifier therapyBiological response modifier therapy (corynebacterium parvum,BCD)(corynebacterium parvum,BCD) -enhancement of host immune response & tumour rejection-enhancement of host immune response & tumour rejection  Cytokines therapyCytokines therapy -interferons,tumour necrosis factor-alpha, interleukin-2.-interferons,tumour necrosis factor-alpha, interleukin-2.  Adaptive immunotherapyAdaptive immunotherapy -infusion of LAK cells-infusion of LAK cells  Intra-peritoneal gene therapyIntra-peritoneal gene therapy -expression of cytokine genes or genetic-expression of cytokine genes or genetic immunopotentiation (enhancement of anti-tumour immuneimmunopotentiation (enhancement of anti-tumour immune response)response)
  • 52. GENEGENE THERAPYTHERAPY  Potential intervention at the molecular levelPotential intervention at the molecular level  Genetic immuno–potentiationGenetic immuno–potentiation