ANZCTR search results

These search results are from the Australian New Zealand Clinical Trials Registry (ANZCTR).

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33283 results sorted by trial registration date.
  • An open-label, first-in-human, dose escalation study to determine the pharmacokinetics, pharmacodynamics, tolerability and safety of BYT-1007 in patients with hematologic malignancies

    This study aims to explore the safety of BYT-1007 and BYT-1007/venetoclax combination and their potential to treat certain blood cancers. Who is it for? You may be eligible for this study if you are male or female, aged 18 to 74. To be eligible for Part A you must be diagnosed with specific hematologic malignancies such as acute lymphoblastic leukaemia (ALL), acute myeloid leukaemia (AML), and high-risk myelodysplastic syndromes (HR-MDS), either in relapsed/refractory status or, in some cases, treatment-naive but unfit for intensive chemotherapy. To be eligible for Part B you must only be diagnosed with acute myeloid leukaemia (AML). Participants must also be unsuitable for standard intensive treatment and have adequate organ function, including kidney function (creatinine clearance of at least 30 mL/min), liver function within the study-specified limits, and a white blood cell count below 25 billion cells/L (supportive treatment may be used to achieve this threshold). Study details Part A will evaluate increasing dose levels of BYT-1007 given alone. Participants will be enrolled sequentially into dose-escalation cohorts and receive five doses of BYT-1007 during a 28-day treatment period. Information collected from Part A will help determine the most appropriate dose for further evaluation. Part B will evaluate BYT-1007 given together with venetoclax. Participants will receive BYT-1007 at dose levels determined based on the results from Part A, in combination with venetoclax during a 28-day treatment period. Participants will attend regular study visits and undergo blood tests, bone marrow assessments, physical examinations, and other safety evaluations to monitor their health and response to treatment. It is hoped that the results of this study will help determine whether BYT-1007, alone or in combination with venetoclax, may be further developed as a potential treatment option for patients with blood cancers, particularly AML.

  • A Prospective Cohort Study of Percutaneous Needle Biopsy, Morphologic and Molecular Evaluation of Uterine Tumours with Imaging Features of Concern for Sarcoma

    Brief description of the study purpose This study aims to assess the feasibility and accuracy of using core biopsies to diagnose uterine masses at two hospital centres. Who is it for? You are eligible for this study if you are aged 18 years or over, are not pregnant and have a uterine mass at least 5cm or greater with either rapid growth on sequential assessment, suspicious features on MRI or have known or suspected cancer predisposition syndromes including pathogenic mutations in BRCA1 or BRCA2 and mismatch repair genes (Lynch syndrome). Study details All those who are eligible will undergo a one-off percutaneous uterine needle biopsy (PUB) which will be performed by the treating gynecology oncologist at the hospital site where you are being treated. A comparison will be made with the findings from your resected specimen as part of the planned surgery. If surgery is not performed then the comparator will be the clinical course of the uterine mass at 6 and 12 month clinical follow up visits. If you are not eligible for PUB prior to surgery then you may still have the option to participate by consenting to a biopsy of your removed uterine mass. The cases contributed via this alternate pathway will help to improve the determination of the accuracy and reliability of core biopsies. It is hoped that the results from this study will help explore the possibility of using core biopsies for diagnosis of uterine masses, particularly for women who wish to preserve their fertility.

  • Can use of the LipReader communication app improve communication in voiceless intensive care patients?

    This study will evaluate LipReader, a smartphone-based artificial intelligence communication tool designed to support voiceless intensive care unit and step-down patients. LipReader uses the device camera to analyse silently mouthed phrases and convert them into text and speech output. Participants will complete a single supervised study session using both LipReader and standard bedside communication tools such as alphabet charts and pen-and-paper. The study will assess time to successful message understanding, message success rate, usability and perceived impact on nursing workflow. Findings will inform future refinement of the technology and the design of larger clinical trials.

  • A Study in Healthy Adults Comparing a Recombinant Polio Vaccine (rPV) With the IPOL Vaccine to Assess Safety, Immune Response, and Vaccine Reactions.

    The primary purpose of this study is to test a new experimental recombinant Poliomyelitis vaccine (rPV) in comparison to the commercially available inactivated poliovirus vaccine. The design of the study is double-blinded, randomised and active controlled. The active controlled product is considered the commercially available vaccine (IPOL).

  • A First-in-Human Study to Assess the Safety of a New Investigational Medicine (MQ005) in Adults with Sepsis

    This study is testing a new experimental antibody treatment called MQ005 for adults with sepsis, a serious infection that can cause organ failure. The main goal is to evaluate whether MQ005 is safe and well-tolerated when given in single ascending doses. Researchers will also explore how the drug affects the immune system and sepsis outcomes. The study aims to determine the best dose for future research while monitoring participants closely for side effects.

  • Feasibility Study to Evaluate a Continuous Blood Glucose Monitor in Adults with Diabetes Mellitus -Australia

    The single group assignment, open label, clinical trial will enroll up to 30 participants with the goal of at least 20 participants completing the yearlong study implant duration. Enrolled Participants will have the CBGM system implanted via a 20–30-minute procedure. Post procedure, after the initial 14-day post implant assessment, Participants will undergo In-Clinic visits every few months during their yearlong implant duration that include both safety and performance assessments of the CBGM System. Outside of the clinic, Participants will complete a minimum of 3 fingerpicks per day (with a study provided commercially approved BG meter and supplies, carry a study phone to collect investigational sensor data (data is blinded to the participant) and complete a study diary. Removal of the CBGM System will be similar to the implant procedure. A final 14-Day post removal visit will occur to follow-up with the participant to assess the wound. If there are not outstanding safety events or items for follow-up, this will be considered the participants final visit and they can safely exit the study.

  • Effectiveness of a Virtual Reality Walking Program for Spinal Cord Injury Neuropathic Pain Over the Medium to Long Term.

    This study will use a combined multiple-baseline with reversal single-case experimental design (SCED) to evaluate the efficacy and feasibility of a virutal reality walking intervention. The study will use an ABABC design. A refers to the non-intervention phases, B will be the intervention phases. C phase will be used as an assessment of feasibility. The duration of each phase will be Baseline(~2-3wks), Intervention1 (4wks), Wash out (~3-4wks), Intervention2 (4wks), Follow-up (2wks). . We will measure changes in pain, and wellbeing as well as feasibility through questionnaires before and after the intervention. The results will help us understand whether this type of intervention is effective and feasiblity in the medium to long term for people with SCI-related NP. We hypothesise that VRWalk will have positive long-term effects on NP intensity. Additionally, we hypothesise that VRWalk will be feasible.

  • Effectiveness of Innovative Low-dose Radiotherapy for Osteoarthritis Relief (iROAR) and Management: A multicentre clinical registry

    The iROAR registry is a prospective, multicentre observational study designed to evaluate the real-world effectiveness of low-dose radiotherapy (LDRT) in adults with symptomatic osteoarthritis across Australia. Participants receiving standard-of-care LDRT will be followed for up to 24 months to assess changes in pain, physical function, and health-related quality of life using validated patient-reported outcome measures. The primary objective is to determine the proportion of treated joints achieving a clinically meaningful response at 6 months based on OMERACT-OARSI criteria. Secondary outcomes include long-term clinical response, safety, retreatment rates, and healthcare utilisation outcomes associated with LDRT. The registry aims to generate the first prospective Australian dataset to inform clinical practice, treatment standardisation, and future research on LDRT for osteoarthritis.

  • Island Study Linking Ageing and Neurodegenerative Disease: Investigating the impact of a public health approach to dementia prevention

    ISLAND hypothesises that a public health approach to dementia prevention can reduce modifiable risk factors in the Tasmanian community. Our novel approach to dementia prevention involves a combination of education with positive lifestyle change. We have shown that our public health approach has efficacy to reduce modifiable risk factors in the Tasmanian community.

  • Does pre-prandial (before meals) compared to prandial (with meals) ingestion of metformin optimise glucose lowering in people with type 2 diabetes?

    Metformin is the first-line glucose-lowering medicine in most clinical guidelines on the management of type 2 diabetes. Standard advice has been to take metformin with meals. However, recent evidence suggests that taking metformin an interval before each meal may work better for lowering blood glucose after the meal. In this study, we will test whether taking metformin 60 min before meals improves glucose-lowering after each meal, compared to taking it with meals in people with type 2 diabetes.

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