Second-line Regimen Combined With Radiotherapy Versus Without Radiotherapy in Patients With Locally Advanced/Oligometastatic Intrahepatic Cholangiocarcinoma After Failure of First-line Treatment：an Open-label, Randomized, Controlled Phase II Clinical Study

Second-line regimen with or without consolidative radiotherapy in patients with oligometastatic/locally advanced unresectable intrahepatic cholangiocarcinoma: an open-label, randomised, controlled study.

Start Date01 Jun 2025

Sponsor / Collaborator-

NCT06925516

/ RecruitingPhase 2IIT

Efficacy and Safety of Apatinib Combined With Adebrelimab and GEMOX Regimen Chemotherapy as the First-line Treatment for Unresectable Intrahepatic Cholangiocarcinoma (ICC): A Single-arm, Multicenter, Phase II Study

The study aims to evaluate the efficacy and safety of Apatinib and Adebrelimab in Combination With chemotherapy in patients with advanced intrahepatic cholangiocarcinoma (ICC)

Start Date22 Jan 2025

Sponsor / Collaborator

Sun Yat-Sen Memorial Hospital

[+1]

NCT05702515

/ CompletedNot Applicable

Vascular Positioning System G4 Algorithm ECG Data Collection for Model Training Study, A Single Center Prospective Clinical Study

The objective of this study is to collect intravascular and extravascular echocardiogram (ECG) data from subjects receiving peripherally inserted central catheters (PICC) while using the Vascular Positioning System G4 and a 12 lead ECG machine. The data obtained will be used to update the G4 algorithm.

Start Date21 Jul 2023

Sponsor / Collaborator

Teleflex, Inc. /Respiratory Business/

[+1]

100 Clinical Results associated with Cirrhosis, Familial, With Pulmonary Hypertension

100 Translational Medicine associated with Cirrhosis, Familial, With Pulmonary Hypertension

0 Patents (Medical) associated with Cirrhosis, Familial, With Pulmonary Hypertension

1,394

Literatures (Medical) associated with Cirrhosis, Familial, With Pulmonary Hypertension

01 Dec 2025·Journal of Gastrointestinal Cancer

Identification of Novel Protein Biomarkers for Intrahepatic Cholangiocarcinoma by Integrating Human Plasma Proteome with Genome

Article

Author: Xu, Jin-Yang ; Li, Jian-Hui ; Jiang, Xiao-Feng ; Huang, Si-Min ; Wei, Yu-Xuan ; Li, Yi-Hu ; Yang, Wei-Bang ; Chen, Yu-Sen

BACKGROUNDThe proteome serves as a key source for the discovery of therapeutic targets. This study utilized proteome-wide Mendelian randomization (MR) to identify protein biomarkers potentially associated with intrahepatic cholangiocarcinoma (ICC).METHODSWe derived protein quantitative trait loci (pQTLs) from the deCODE plasma proteome GWAS and genetic ICC associations from a European meta-analysis. Proteome-wide MR identified candidate proteins linked to ICC risk. Expression of MR-identified biomarkers in the plasma of ICC patients was detected by ELISA. ScRNA-seq analysis detected the specific cell type with enrichment expression. Prognostic and diagnostic evaluations in ICC of these proteins were performed using samples derived from TCGA and GTEx databases.RESULTSMR analysis genetically predicted 5 proteins were associated with ICC risk (STX12, A2M, CD163, CXADR and FOXJ2). The results of the MR analysis for the five identified targets were consistent with the measured plasma concentrations of these targets in ICC patients and healthy volunteers. The differential RNA-seq analysis between tumor and adjacent normal tissues showed that STX12 was expressed at higher levels in tumor tissues, while A2M, CXADR, CD163, and FOXJ2 were expressed at higher levels in adjacent normal tissues. ScRNA-seq analysis revealed that these protein-coding genes are mainly expressed in TAMs, TEC, HPC-like cells and malignant cells in ICC tumor tissue. Prognosis analysis showed higher CXADR expression correlated with longer OS in CHOL (P = 0.041). The AUC for A2M, CD163, CXADR, FOXJ2, and STX12 were 0.975, 0.705, 0.917, 0.997, and 0.956, respectively.CONCLUSIONThis study represents the first Proteome-MR analysis of ICC, revealing its complex genetic architecture and identifying five novel blood proteins with potential causal links to the disease. Through proteome-MR analysis, scRNA-seq analysis, and diagnostic-prognostic evaluation using TCGA and GTEx databases, these proteins were assessed as promising therapeutic and diagnostic targets. The findings provide a theoretical foundation for future ICC treatment strategies.

01 Jun 2025·International Journal of Pediatric Otorhinolaryngology

Pediatric acute mastoiditis: A comparison of patients with and without intracranial complications

Article

Author: Nguyen, Justin Dat ; Lambert, Elton M ; Zhang, Wynne ; Sitton, Matthew S ; Laryea, Richmond ; Glaun, Mica ; Lee, Jae Eun

OBJECTIVETo assess pediatric patients presenting with acute mastoiditis with and without intracranial complications (ICC) METHODS: A case series with retrospective review was performed on pediatric patients who presented to a pediatric tertiary care center with the diagnosis of mastoiditis from 2012 to 2020. All patients had a documented microbiology culture. The main factors compared among patients were bacteria isolated from cultures, antibiotic resistance, and occurrence of intracranial complications of mastoiditis.RESULTS298 patients with mastoiditis were included in this study with an average age of 8.6 years (SD = 4.45). 41 of those patients presented with at least one intracranial complication (ICC) with the most common being epidural abscess (51 %). 143 (48 %) of patients had a history of acute otitis media prior to presentation, and thirty-eight patients (13 %) had a history of chronic otitis media prior to presentation. Patients with a history of acute otitis media were less likely to develop ICC compared to patients without a history of otologic infections OR: 0.49 (95 % CI = 0.24-0.99), p = 0.047. Patients with history of chronic otitis media were less likely to develop ICC compared to patients with no history of otologic infections OR: 0.20 (95 % CI = 0.04-0.90), p = 0.036. Patients with antibiotic use were more likely to develop ICC compared to antibiotic naïve patients OR: 2.64 (95 % CI = 1.31-5.32) p = 0.006. There was also no significant effect of patient sex, and ethnicity in the development of ICC.CONCLUSIONThe occurrence of intracranial complications from mastoiditis are noted to be higher in patients with no history of otologic infections. Additionally, the occurrence of ICC is noted to be higher among patients with prior antibiotic use.LEVEL OF EVIDENCElevel 4 LEVEL OF EVIDENCE: level 4.

01 Jun 2025·Phytomedicine

Fufang-Biejia-Ruangan tablet targeting both cancer-associated fibroblasts and tumor cells by HIPPO-PI3K/AKT cascades in intrahepatic cholangiocarcinoma treatment

Article

Author: Yin, Donghao ; Cui, Miao ; Pan, Tao ; Song, Xinhua ; Li, Xiang ; Xu, Yanyu ; Wang, Jiabo ; Zheng, Shuwen ; Shang, Zimeng ; Xu, Yang ; Yang, Zhiyun

BACKGROUNDIntrahepatic cholangiocarcinoma (ICC) ranks second among primary liver cancers in terms of prevalence, characterized by poor prognosis and scarce therapeutic interventions. Fufang-Biejia-Ruangan tablet (BJRG), a traditional Chinese herbal remedy, has been widely used for liver diseases. However, its therapeutic efficacy and underlying mechanisms in ICC remain poorly understood.AIM OF THE STUDYThis study aims to systematically investigate the anti-ICC effects of BJRG, focusing on tumor progression and microenvironment modulation, through experimental and transcriptomic analyses.METHODSThe chemical composition of BJRG was analyzed employing ultra-performance liquid chromatography-mass spectrometry (UPLC-MS). In vitro assays were performed with QBC939 and LX-2 cell lines. Two primary ICC models (AKT/YAP and sgP53/KRAS) were established via hydrodynamic tail-vein injection of corresponding plasmids. A co-culture system for subcutaneous tumor formation was developed using cancer-associated fibroblasts (CAFs) derived from the AKT/YAP model and primary tumor cells derived from the sgP53/KRAS model.RESULTSUPLC-MS analysis identified 1091 chemical components, primarily terpenoids, sugars, glycosides, and phenylpropanoids. The therapeutic efficacy of BJRG was evaluated for the treatment of ICC. BJRG treatment slowed down the growth of both human ICC cell lines and AKT/YAP ICC mouse model. Mechanistically, BJRG inhibited HIPPO-PI3K/AKT signaling pathway in ICC tumor cells. Importantly, BJRG significantly inhibited the growth of CAFs via HIPPO-PI3K/AKT cascades. Of note, co-culture CAFs with ICC cell lines substantially sensitized the efficacy of BJRG in sgP53/KRAS syngeneic tumor model. Furthermore, BJRG therapy not only affected CAFs but also induced alterations in vascular structures and hypoxic conditions within lesions in the AKT/YAP model. This intervention promoted the infiltration of T lymphocytes and macrophages into the tumor microenvironment, which may further augment the anti-proliferative effects of BJRG by enhancing the immune response within ICC tumor tissues.CONCLUSIONOur research demonstrates BJRG's anti-ICC efficacy via diverse pathways, including the suppression of tumor cell proliferation, regulation of CAFs activity, and promotion of immune cell infiltration. These findings underscore BJRG as a promising therapeutic candidate for ICC, offering novel mechanistic insights and highlighting its potential for clinical translation.

News (Medical) associated with Cirrhosis, Familial, With Pulmonary Hypertension

18 Feb 2024

·synapse.patsnap.com

Decoding Floxuridine: a comprehensive study of its R&D trends and its clinical results in 2024 ASCO_GI

On 18 Jan 2024, the phase II trial of induction systemic mFOLFIRINOX followed by hepatic arterial infusion of floxuridine and dexamethasone given concurrently with systemic mFOLFIRI as a first-line therapy in patients with unresectable liver-dominant intrahepatic cholangiocarcinoma (HELIX-1) was presented in 2024 ASCO_GI. Floxuridine's R&D ProgressFloxuridine is a small molecule drug that falls under the therapeutic areas of neoplasms, digestive system disorders, respiratory diseases, and skin and musculoskeletal diseases. It is primarily indicated for the treatment of breast cancer, esophageal carcinoma, liver cancer, lung cancer, rectal cancer, and stomach cancer. According to the Patsnap Synapse, Floxuridine has received approval for use in various countries. And the clinical trial distributions for Floxuridine are primarily in the United States, China and Italy. The key indication is Colorectal Liver Metastases. Detailed Clinical Result of FloxuridineThis investigator-initiated, first-line, single-center, single-arm phase II clinical trial (NCT04251715) was designed with a patient safety run-in evaluating toxicity from the combined therapy. In this study, eligible patients were treated with systemic mFOLFIRINOX for 4 cycles in order to select those likely to benefit from HAI. Patients with disease control on restaging proceeded to HAI pump placement and treatment with HAI floxuridine for 14 days followed by systemic mFOLFIRI on a 28-day cycle. The co-primary objectives were to assess safety of the combined therapeutic strategy and the disease control rate (DCR) at 6 months (RECIST v1.1) at end of trial (EOT). The result showed that a total of n=5 patients with liver-only ICC enrolled in the trial and completed the entire study protocol. The median age was 60 years (range 42-69) with a dominant lesion size of 9.8cm (range 8.4-14.5). All patients had both right and left hemiliver involvement with a median of 9 intrahepatic tumors (range 1-15). No patients experienced grade 3 or 4 adverse events, or hepatic dysfunction leading to cessation of HAI therapy. The DCR at 6 months was 100%, with a mPFS of 18.2 months. All five patients achieved partial radiographic response (PR) while receiving HAI therapy, and remain alive with liver-only disease at a median of 18.4 months (range 12.7-20) after study enrollment. After continuing treatment with HAI and systemic mFOLFIRI beyond the EOT, two patients transitioned to HAI treatment only and then to biochemical and radiographic surveillance without therapy after demonstrating PR and CA19-9 normalization. It can be concluded that Integration of HAI floxuridine with mFOLFIRI following mFOLFIRINOX induction for patients with liver-only advanced ICC is well-tolerated and demonstrates longer DCR in comparison to historical controls. The combined regimen minimized systemic toxicity and allowed a large proportion of patients to transition to liver-only HAI treatment with maintained disease control. Future directions include combining HAI with new first-line systemic regimens for patients with advanced ICC. How to Easily View the Clinical Results Using Synapse Database?If you want to know the other clinical results of popular conferences, please lick on the “Clinical Results” on the homepage of Patsnap Synapse, which provides multi-dimensional screening and filtering of drugs, indications, targets, companies, result evaluation, release date, popular conferences, etc. to help you quickly locate the data you need. Select the clinical meeting you are interested in, such as ESMO. In the results, you can quickly locate the data you want to view by indication, phase and drug name. A single result clearly shows important information such as registration number, phase, indication, Sponsor/Collaborator, biomarker, Trial number, dosing regimen and more. If you would like to view more information about this result, you can go to the result detail page by clicking on the title. Above the headings, we provide the original source of the outcome data. The basic information is supplemented with more information beyond the list, such as company, study. design, etc. In the important Outcome Measures section, we provide both list and flowchart forms, which are convenient for you to overview the comparison group information and core indicator data. Finally, if you need to download these results, you can conveniently check the check boxes on the left side of the list, or directly click the "Export" button to download the data for personalized analysis and file sharing. Click on the image below to embark on a brand new journey of drug discovery!

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