These are reviewed studies whose abstracts concern Ovarian Carcinosarcoma. Each describes only what that study reported. This is not a claim by OncoForge that any compound helps or harms Ovarian Carcinosarcoma. Most are early lab, animal, or small human studies, and findings often conflict.
ReviewInconclusiveLimited evidenceTier 4 · clinical
Therapeutic advances in medical oncology · Dec 2025 · review
epithelial ovarian cancerhigh-grade serous ovarian cancerovarian clear cell carcinomaendometrioid ovarian carcinomamucinous ovarian carcinomalow-grade serous ovarian carcinomaovarian carcinosarcoma
This review describes the main genomic subtypes of epithelial ovarian cancer and how those differences may help match patients to targeted therapies. It highlights PARP inhibitors, MAPK pathway inhibitors, cell cycle checkpoint inhibitors, immune checkpoint inhibitors, and antibody-drug conjugate approaches that are being investigated for specific ovarian cancer types. The article also notes that resistance to PARP inhibitors remains a problem and that more evidence is needed for effective combination therapies.
Key findings
- High-grade serous ovarian cancer is linked mainly to homologous recombination repair gene alterations such as BRCA1 and BRCA2.
- Ovarian clear cell carcinoma is associated with ARID1A and PIK3CA alterations; endometrioid ovarian carcinoma with PIK3CA and KRAS; mucinous ovarian carcinoma with CDKN2A and KRAS; and low-grade serous ovarian carcinoma with MAPK pathway genes such as BRAF and KRAS.
- PARP inhibitor therapy has improved survival for women with homologous recombination repair defects in high-grade serous ovarian cancer, but acquired resistance remains an issue.
- The review emphasizes that genomically targeted combination therapies are urgently needed and that some reported responses are preliminary.
Limitations: Review article only; no new experimental or clinical data presented in the abstract.; No quantitative outcomes or effect sizes are reported in the abstract.; The abstract is broad and does not provide trial-level details, sample sizes, or follow-up durations.; Some therapies discussed are preliminary and require further evidence..
The article is about ovarian cancer genomics and targeted therapies, not a single compound experiment.
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text
Human · observationalMechanismReported positiveLimited evidenceTier 3 · early humann = 8
The American journal of surgical pathology · May 2025 · case series with clinicopathologic evaluation and next-generation sequencing
gynecologic carcinosarcomaendometrial carcinosarcomalower uterine segment carcinosarcomaovarian carcinosarcoma
The authors report a clinicopathologic and genomic analysis of eight gynecologic carcinosarcomas with a mesonephric-like carcinomatous component. Sequencing (done separately for carcinomatous and sarcomatous parts in some tumors) showed identical single-nucleotide variants between components, low tumor mutational burden (<10 mutations/Mb), microsatellite stability, and KRAS codon 12 mutations in all sequenced cases. Additional alterations (eg, PTEN, PIK3CA, ARID1A) were identified in several tumors. This is a small descriptive case series and does not include functional experiments or outcome correlations beyond staging.
Reported effects: n_cases 8, n=8 · mean_age 65.6 · +11 more
Key findings
- Eight cases of gynecologic MLCS (endometrial, lower uterine segment, and ovarian) were identified and evaluated.
- Genomic DNA extraction and NGS were performed separately on carcinomatous and sarcomatous components of 4 tumors and on combined components of 2 tumors.
- The carcinomatous and sarcomatous components were observed to harbor the same single nucleotide variations when sequenced separately.
- All cases had less than 10 mutations/Mb and were microsatellite stable.
- All sequenced cases (6/6, 100%) harbored KRAS point mutations in codon 12 (p.G12D n=2; p.G12A n=2; p.G12V n=2).
- Five cases showed additional alterations including ARID1A, PTEN, PIK3CA, SPOP, TET1, BUB1, LYN and PTPRD.
- Authors suggest the combination of KRAS and PTEN/PIK3CA alterations is consistent with combined endometrioid and mesonephric differentiation in MLCS.
Limitations: Small sample size (8 cases) limits generalizability.; Only 6 tumors underwent NGS (4 separately by component, 2 combined), so not all cases had component-specific sequencing.; Descriptive molecular profiling without functional validation of mutations.; No survival or treatment-outcome correlations reported beyond FIGO stage..
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed
Human · observationalReported positiveLimited evidenceTier 3 · early humann = 10
BMC cancer · Dec 2024 · retrospective cohort
Trastuzumab-deruxtecan-t-dxdTrastuzumab-deruxtecanendometrial neoplasmsovarian neoplasmscervical neoplasmsuterine carcinosarcomauterine leiomyosarcomauterine serous carcinomaovarian carcinosarcomahigh-grade serous ovarian carcinomamucinous ovarian carcinomasquamous cervical carcinoma This retrospective single-center study identified 10 patients with HER2-expressing (IHC 2+/3+) recurrent or metastatic gynecological cancers who received trastuzumab deruxtecan (5.4 mg/kg IV every 3 weeks). The cohort had a median progression-free survival of 5.4 months (95% CI 0.8-9.8). Five patients had a partial response, one had stable disease at 12 weeks, and four had disease progression at initial assessment. Clinical benefit was observed mainly in tumors with HER2 IHC 3+.
Reported effects: median PFS 5.4 mo [0.8–9.8], n=10 · partial responses 5, n=10 · +2 more
Key findings
- 10 patients with recurrent/metastatic HER2-expressing gynecological malignancies were treated with T-DXd.
- Histologies included uterine neoplasms (n=5), cervical squamous carcinoma (n=1) and ovarian cancers (n=4).
- Median age was 65.4 years (25th-75th percentile, 58.1-75.2 years).
- HER2 by IHC: 5 patients were 3+ and 5 patients were 2+.
- Median number of prior therapy lines was 4 (range 2-6); 2 uterine serous carcinoma patients were pretreated with trastuzumab and 4 patients had prior immunotherapy.
- Dose: T-DXd 5.4 mg/kg IV every 3 weeks until progression/toxicity.
- Median progression-free survival (PFS) in the cohort was 5.4 months (95% CI 0.8-9.8 months).
- Responses: 5 patients had partial response (including 2 previously treated with trastuzumab), 1 patient had stable disease at 12 weeks, 4 patients had disease progression at initial assessment.
- Most patients who derived clinical benefit had HER2 IHC 3+ expression.
Limitations: Retrospective, single-center design; Very small sample size (n=10); No control or comparator arm; Heterogeneous mix of gynecologic histologies; Heavily pre-treated population limits generalizability; Limited/absent reporting of safety or adverse event data in the abstract; Potential selection and reporting bias inherent to retrospective series.
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text
Human · observationalMechanismReported positiveLimited evidenceTier 3 · early humann = 32
Virchows Archiv : an international journal of pathology · Dec 2024 · targeted next-generation sequencing of tumor specimens (molecular profiling)
tubo-ovarian carcinosarcoma
The authors performed targeted next-generation sequencing of 32 tubo-ovarian carcinosarcoma specimens (including 7 serous effusions) covering 50 genes. They found 31 mutations in 25 of 32 tumors, with TP53 alterations predominant (25 mutations in 24 tumors); other mutations (RB1, MET, KRAS, PTEN, KIT) were rare. Patient-matched specimens shared the same TP53 mutation, and specimens with no detected mutations were more frequent among serous effusions than surgical specimens. The authors conclude TP53 mutations dominate the molecular landscape and note it is uncertain whether effusion-derived cells differ from solid lesions.
Reported effects: specimens_n 32, n=32 · patients_n 25, n=25 · +11 more
Key findings
- Specimens (n=32) consisted of 25 biopsies/surgical resection specimens and 7 serous effusions (6 peritoneal, 1 pleural) from 25 patients.
- Targeted next-generation sequencing covered 50 unique genes.
- A total of 31 mutations were found in 25 of the 32 tumors studied, of which 1 had 3 mutations, 4 had 2 different mutations, and 20 had a single mutation.
- The most common mutations were in TP53 (n=25 in 24 tumors; 1 tumor with 2 different mutations).
- Less common mutations were found in RB1 (n=2), MET (n=1), KRAS (n=1), PTEN (n=1), and KIT (n=1).
- Patient-matched specimens harbored the same TP53 mutation.
- Tumors with no detected mutations were more common in serous effusion specimens (3/7; 43%) compared with surgical specimens (4/25; 16%).
Limitations: Small sample size (32 specimens from 25 patients).; Use of a targeted 50-gene panel limits detection to predefined genes and may miss other relevant alterations.; Observational molecular profiling without functional validation of variants.; Unclear generalizability given limited anatomic sampling and small number of effusion specimens..
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text
Human · observationalMechanismReported positiveModerate evidenceTier 3 · early humann = 122
Histopathology · Nov 2024 · immunohistochemical analysis of a cohort of human tumours (122 cases) including STK11 adnexal tumours and morphological mimics
STK11 adnexal tumourovarian neoplasmsovarian endometrioid carcinomatubo-ovarian high-grade serous carcinomaovarian mesonephric-like adenocarcinomaovarian carcinosarcomaperitoneal malignant mesotheliomapelvic plexiform leiomyomaovarian solid pseudopapillary tumourgranulosa cell tumourSertoli-Leydig cell tumourLeydig cell tumourSertoli cell tumoursteroid cell tumourfemale adnexal tumour of Wolffian originextra-ovarian sex cord-stromal tumour
Researchers performed STK11 (LKB1) immunohistochemistry on 122 human tumour samples, including 17 STK11 adnexal tumours and 105 morphological mimics. All 17 STK11 adnexal tumours showed complete loss of cytoplasmic STK11 staining. Nearly all other tumour types retained cytoplasmic STK11 staining, with the exception of one endometrioid carcinoma with mucinous differentiation showing complete loss and one high-grade serous carcinoma showing subclonal loss. The authors conclude STK11 IHC is a highly sensitive and specific marker for distinguishing STK11 adnexal tumour in the appropriate morphological context and could obviate confirmatory molecular testing.
Reported effects: total tumours tested 122, n=122 · STK11 adnexal tumours included 17, n=17 · +3 more
Key findings
- IHC for STK11 was performed on 122 tumours, including 17 STK11 adnexal tumours and 105 morphological mimics (full list of mimics given in abstract).
- All STK11 adnexal tumours showed complete loss of cytoplasmic staining for STK11.
- All other tumour types showed retained cytoplasmic staining, except for one endometrioid carcinoma with mucinous differentiation which showed complete loss of STK11 expression and a high-grade serous carcinoma with subclonal loss.
- Authors conclude STK11 IHC is a highly sensitive and specific immunohistochemical marker for distinguishing STK11 adnexal tumour from histological mimics and may obviate the need for confirmatory molecular studies in the appropriate morphological context.
Limitations: Small number of STK11 adnexal tumours (n=17), reflecting rarity of the entity.; Study reports a single cohort with no external validation cohort mentioned in the abstract.; Potential selection bias because tumour types were a selected set of morphological mimics.; Abstract does not report blinding, interobserver reproducibility, or diagnostic performance statistics (sensitivity/specificity values) beyond descriptive counts.; Two non-STK11 tumours showed loss/subclonal loss of STK11, indicating imperfect specificity in this cohort..
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text
Human · observationalMechanismReported positiveLimited evidenceTier 3 · early humann = 1
Journal of Zhejiang University. Science. B · Aug 2024 · single-cell RNA sequencing (scRNA-seq) analysis of resected primary tumor with comparison to published scRNA-seq datasets
ovarian carcinosarcomahigh-grade serous ovarian carcinoma
The authors performed single-cell RNA sequencing on a resected primary ovarian carcinosarcoma and compared the data with published high-grade serous ovarian carcinoma and other OCS datasets. They identified malignant epithelial and malignant mesenchymal cells, four epithelial subclusters (one with high BRCA1 and TOP2A expression linked to cell cycle and drug-resistance features), and a mesenchymal subcluster C14 with an OCS-specific expression pattern. They also report FGF and PTN signaling as major pathways mediating epithelial–mesenchymal communication. The study provides a single-cell transcriptomic resource for exploring OCS heterogeneity.
Key findings
- Both malignant epithelial and malignant mesenchymal cells were observed in the OCS patient sample.
- Four epithelial cell subclusters were identified; epithelial subcluster 4 had high BRCA1 and TOP2A expression and was related to drug resistance and cell cycle.
- Intercellular interaction analysis indicated FGF and PTN signaling as main pathways contributing to communication between epithelial and mesenchymal cells.
- A mesenchymal subcluster (C14) showed OCS-specific expression (elevated CYP24A1, COL23A1, CCK, BMP7, PTN, WIF1, and IGF2) and distinct characteristics compared with another published OCS tumor and normal ovarian tissue.
Limitations: Analysis appears to be from a single resected tumor/patient, limiting generalizability.; Observational transcriptomic profiling without functional validation of identified pathways or subclusters.; No clinical outcome, treatment response, or longitudinal data reported.; Comparisons rely on previously published datasets rather than additional contemporaneous samples..
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text
Human · observationalReported negativeModerate evidenceTier 3 · early humann = 47028
Frontiers in oncology · May 2024 · multi-cohort cross-sectional study
ovarian carcinosarcoma (OCS)high-grade serous ovarian carcinoma (HGSOC)endometrioid ovarian carcinoma (EnOC)clear cell ovarian carcinoma (CCOC)mucinous ovarian carcinoma (MOC)low-grade serous ovarian carcinoma (LGSOC)
The authors performed a multi-cohort cross-sectional analysis using Scottish and SEER registries to compare characteristics and overall survival between ovarian carcinosarcoma (OCS) and other major ovarian cancer histotypes. They found OCS patients were older at diagnosis, presented frequently with advanced stage, and had significantly shorter survival than most other histotypes, including when adjusted for prognostic factors; this poor outcome was evident even for early-stage disease.
Reported effects: Scottish cohort sample size 2082, n=2082 · SEER cohort sample size 44946, n=44946 · +14 more
Key findings
- Study cohorts: Scotland (n=2082) and SEER (n=44946).
- OCS patients had median ages at diagnosis of 69 (Scottish) and 67 (SEER) and demonstrated the shortest survival on univariable analysis.
- Within the Scottish cohort, 59.3% and 16.9% of OCS patients presented with FIGO stage III and IV disease, respectively.
- Multivariable analysis showed other histotypes had lower hazards (better survival) than OCS in both cohorts: Scottish multivariable HRs vs OCS — HGSOC 0.45, EnOC 0.39, LGSOC 0.26, MOC 0.43.
- SEER multivariable HRs vs OCS — HGSOC 0.59, EnOC 0.34, LGSOC 0.30, MOC 0.81.
- Within SEER, CCOC had a multivariable HR 0.63 (95% CI 0.58-0.68) versus OCS, while in the Scottish cohort the multivariable HR for CCOC was 1.05 (95% CI 0.74-1.51).
- OCS was associated with the poorest survival among histotypes even for early-stage disease across both cohorts; in late-stage disease OCS, MOC and CCOC had the poorest survival.
Limitations: Observational cross-sectional design (not randomized), so causal inference is limited.; Potential for residual confounding despite multivariable adjustment.; Some results differed between cohorts (e.g., CCOC comparison), indicating cohort heterogeneity or population differences.; No intervention or treatment effects were tested..
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text
Human · observationalMixed resultsLimited evidenceTier 3 · early humann = 458
Journal of gynecologic oncology · Jan 2024 · registry-based retrospective cohort analysis
ovarian carcinosarcomaepithelial ovarian cancer
This study used the Korea Central Cancer Registry to identify 458 cases of ovarian carcinosarcoma diagnosed from 1999–2018. The authors report that incidence increased over time (ASR 0.029 per 100,000 in 1999 to 0.073 in 2018; APC 5.86%, p<0.001) and that median overall survival was 39 months with a 5-year overall survival of 42.5%. Localized disease and age under 50 were associated with better 5-year survival than more advanced stage and older age.
Reported effects: proportion_of_epithelial_ovarian_cancers 1.5%, n=458 · ASR 1999-2018 0.064 · +8 more
Key findings
- 458 cases of ovarian carcinosarcoma detected, accounting for 1.5% (458/30,679) of all epithelial ovarian cancers in Korea between 1999 and 2018.
- Overall age-standardized incidence rate (ASR) of ovarian carcinosarcoma between 1999 and 2018 was 0.064 per 100,000 women.
- ASR increased from 0.029 per 100,000 in 1999 to 0.073 per 100,000 in 2018.
- Annual percent change (APC) during 1999-2018 was 5.86 (p<0.001).
- Median overall survival (OS) of patients with ovarian carcinosarcoma was 39 months.
- 5-year OS rate was 42.5%.
- Stage-specific 5-year OS: localized 60.8%, regional 57.9%, distant 32.8% (p<0.001).
- Age-specific 5-year OS: patients <50 years 52.6% vs ≥50 years 40.2% (p<0.001).
Limitations: Observational registry study—cannot establish causal relationships.; Relatively small number of carcinosarcoma cases (458) limits precision for subgroup analyses.; The abstract does not report detailed clinical variables (treatments, comorbidities) or adjustment for confounders.; Potential for misclassification or incomplete data inherent to cancer registry reporting..
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text
ReviewReported negativeLimited evidenceTier 4 · clinical
Acta medica (Hradec Kralove) · Jan 2024 · Scoping review
ovarian carcinosarcoma
This scoping review summarizes the literature on ovarian carcinosarcoma, a rare, highly aggressive biphasic ovarian tumour. The authors report it accounts for about 1–4% of ovarian tumours, spreads outside the ovary in ~90% of cases, and has a poor prognosis with median survival under 2 years. Standard management is cytoreductive surgery followed by chemotherapy, but the optimal chemotherapy regimen, the role of radiotherapy, and novel therapies require further study.
Studied with: cytoreductive surgery, chemotherapy.
Key findings
- Ovarian carcinosarcoma (malignant mixed Müllerian tumour) is uncommon and highly aggressive, comprising 1 to 4% of ovarian tumours.
- It is biphasic, involving malignant sarcomatous (mesenchymal) and carcinomatous (epithelial) cells, with subtypes such as serous and endometrioid.
- About 90% of cases of ovarian carcinosarcoma spread outside the ovary.
- Theories of origin include collision, conversion, and combination theories.
- Prognosis remains poor even when localized; the median survival is reported as lower than 2 years with no recent change in survival rates.
- Clinical presentation mainly includes lower abdominal pain and a palpable abdominal mass.
- Main treatment involves cytoreductive surgery followed by chemotherapy; the type of chemotherapy, role of radiotherapy, and novel therapies need further study.
- Ovarian carcinosarcoma is poorly understood and understudied, and no elaborate therapeutic consensus is available.
Limitations: Scoping review design: no new primary patient-level data are generated by this article.; Rare tumour with limited and understudied literature, implying small patient numbers and sparse high-quality evidence.; Lack of therapeutic consensus and few high-quality trials are available to define optimal treatment.; Review reports general survival trends but does not present new pooled quantitative analyses or trial data..
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed
ReviewMechanismInconclusiveLimited evidenceTier 4 · clinical
American journal of clinical oncology · Dec 2023 · review
ovarian carcinosarcoma
This review summarizes the genomic and molecular features of ovarian carcinosarcoma, a rare and aggressive ovarian cancer. It notes mutations and biomarkers that have been reported in this tumor, including evidence of homologous recombination deficiency and some VEGF positivity. The paper also mentions case reports and preclinical studies involving PARP inhibitors, VEGF inhibitors, and immunotherapy, but it does not present new treatment results.
Key findings
- OCS has been reported to harbor mutations such as TP53, PIK3CA, c-myc, ZNF217, ARID1A, and CTNNB1.
- Some tumors show VEGF positivity and limited HER2 expression.
- There is evidence of homologous recombination deficiency in OCS.
- The review states that data for non-chemotherapy treatments are largely based on in vitro and in vivo studies, with case reports of PARP inhibitors, VEGF inhibitors, and immunotherapy showing varying degrees of success.
Limitations: Review article with no original experimental or clinical data.; No quantitative effect estimates reported in the abstract.; Treatment evidence cited is largely from in vitro and in vivo studies and case reports.; Mixed biomarker findings and no direct comparative outcomes in this abstract..
Provides background on molecular features and reported targeted-therapy case reports in ovarian carcinosarcoma.
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed
ReviewInconclusiveLimited evidenceTier 4 · clinical
Current treatment options in oncology · Dec 2023 · narrative review
ovarian carcinosarcomaovarian cancer
This review summarizes what is known about ovarian carcinosarcoma, a rare and aggressive ovarian cancer. It discusses risk factors, prognostic markers, and current treatment approaches such as surgery followed by platinum-based chemotherapy, while noting that immunotherapy and HRD testing may be useful in some patients. The article does not report new experimental results from a trial or laboratory study.
Key findings
- Ovarian carcinosarcoma is described as rare and aggressive, with median overall survival under 2 years.
- Poor prognostic factors include advanced stage, older age, lymph node metastasis, suboptimal cytoreduction, heterologous histology, and increased VEGF, p53, and WT1 expression.
- Main treatment approach is cytoreductive surgery followed by platinum-based chemotherapy.
- Immunotherapy is described as promising, and HRD testing may help personalize therapy.
Limitations: Narrative review rather than original research.; No new patient cohort, control group, or quantitative treatment effect data reported in the abstract.; Most evidence discussed is from case reports and small studies.; The abstract does not specify which therapies or biomarkers were evaluated in detail..
Provides an overview of ovarian carcinosarcoma epidemiology, prognosis, and treatment options rather than testing a specific compound.
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text
Human trialTrialMixed resultsModerate evidenceTier 4 · clinicaln = 178
Journal of clinical oncology : official journal of the American Society of Clinical Oncology · Oct 2023 · three-arm, randomized, controlled, open-label phase II study
Relacorilantovarian cancerovarian epithelial carcinomaprimary peritoneal cancerfallopian tube cancerovarian carcinosarcoma This phase II study tested relacorilant added to nab-paclitaxel in women with recurrent platinum-resistant or refractory ovarian and related cancers. The intermittent relacorilant schedule improved progression-free survival and duration of response compared with nab-paclitaxel alone, while overall response rate was similar across groups. Side effects were broadly comparable between arms, and the study did not meet its prespecified statistical threshold after multiplicity adjustment.
Reported effects: PFS HR 0.66, p P = .038, n=178 · DOR HR 0.36, p P = .006, n=178 · +1 more
Studied with: nab-paclitaxel.
Key findings
- Intermittent relacorilant plus nab-paclitaxel improved PFS versus nab-paclitaxel monotherapy (HR 0.66; P = .038).
- Intermittent relacorilant plus nab-paclitaxel improved DOR versus nab-paclitaxel monotherapy (HR 0.36; P = .006).
- ORR was similar across arms.
- At the preplanned OS analysis, the OS HR was 0.67 with P = .066 for the intermittent arm versus nab-paclitaxel monotherapy.
- Continuous relacorilant plus nab-paclitaxel showed numerically improved median PFS but no significant improvement over monotherapy.
- Adverse events were comparable across study arms; common grade ≥3 events included neutropenia, anemia, peripheral neuropathy, and fatigue/asthenia.
Limitations: Phase II study with relatively small sample size.; Open-label design.; Primary end point did not reach statistical significance after protocol-prespecified Hochberg step-up multiplicity adjustment.; Median follow-up was limited for PFS and OS analyses.; Safety and efficacy were compared against nab-paclitaxel monotherapy, but the abstract does not provide detailed absolute event rates..
Relacorilant was studied as an add-on to chemotherapy in recurrent platinum-resistant ovarian cancer.
AI summary of the abstract, human-reviewed · Jun 2026. Describes what this study reported, not medical advice. View on PubMed · Full text