Your search keyword '"Goren, K"' showing total 6 results

1. Heterogeneity and Gaps in Reporting Primary Outcomes From Neonatal Trials

Author

Baba, A, Webbe, J, Butcher, NJ, Rodrigues, C, Stallwood, E, Goren, K, Monsour, A, Chang, ASM, Trivedi, A, Manley, BJ, McCall, E, Bogossian, F, Namba, F, Schmölzer, GM, Harding, J, Nguyen, KA, Doyle, LW, Jardine, L, Rysavy, MA, Konstantinidis, M, Meyer, M, Helmi, MAM, Lai, NM, Hay, S, Onland, W, Choo, YM, Gale, C, Soll, RF, Offringa, M, Core Outcome Reporting in Neonatal Trials Study Group, Baba, A, Webbe, J, Butcher, NJ, Rodrigues, C, Stallwood, E, Goren, K, Monsour, A, Chang, ASM, Trivedi, A, Manley, BJ, McCall, E, Bogossian, F, Namba, F, Schmölzer, GM, Harding, J, Nguyen, KA, Doyle, LW, Jardine, L, Rysavy, MA, Konstantinidis, M, Meyer, M, Helmi, MAM, Lai, NM, Hay, S, Onland, W, Choo, YM, Gale, C, Soll, RF, Offringa, M, and Core Outcome Reporting in Neonatal Trials Study Group

Abstract

OBJECTIVES: Clear outcome reporting in clinical trials facilitates accurate interpretation and application of findings and improves evidence-informed decision-making. Standardized core outcomes for reporting neonatal trials have been developed, but little is known about how primary outcomes are reported in neonatal trials. Our aim was to identify strengths and weaknesses of primary outcome reporting in recent neonatal trials. METHODS: Neonatal trials including ≥100 participants/arm published between 2015 and 2020 with at least 1 primary outcome from a neonatal core outcome set were eligible. Raters recruited from Cochrane Neonatal were trained to evaluate the trials' primary outcome reporting completeness using relevant items from Consolidated Standards of Reporting Trials 2010 and Consolidated Standards of Reporting Trials-Outcomes 2022 pertaining to the reporting of the definition, selection, measurement, analysis, and interpretation of primary trial outcomes. All trial reports were assessed by 3 raters. Assessments and discrepancies between raters were analyzed. RESULTS: Outcome-reporting evaluations were completed for 36 included neonatal trials by 39 raters. Levels of outcome reporting completeness were highly variable. All trials fully reported the primary outcome measurement domain, statistical methods used to compare treatment groups, and participant flow. Yet, only 28% of trials fully reported on minimal important difference, 24% on outcome data missingness, 66% on blinding of the outcome assessor, and 42% on handling of outcome multiplicity. CONCLUSIONS: Primary outcome reporting in neonatal trials often lacks key information needed for interpretability of results, knowledge synthesis, and evidence-informed decision-making in neonatology. Use of existing outcome-reporting guidelines by trialists, journals, and peer reviewers will enhance transparent reporting of neonatal trials.

Published

2023

2. Strengthening Reporting of Neonatal Trials.

Author

Webbe, J, Baba, A, Butcher, NJ, Rodrigues, C, Stallwood, E, Goren, K, Monsour, A, Chang, ASM, Trivedi, A, Manley, BJ, McCall, E, Bogossian, F, Namba, F, Schmölzer, GM, Popat, H, Nguyen, KA, Doyle, LW, Jardine, L, Rysavy, MA, Konstantinidis, M, Muhd Helmi, MA, Lai, NM, Hay, S, Onland, W, Choo, YM, Gale, C, Soll, RF, Offringa, M, CORE OUTCOME REPORTING IN NEONATAL TRIALS (CORINT) STUDY GROUP, Webbe, J, Baba, A, Butcher, NJ, Rodrigues, C, Stallwood, E, Goren, K, Monsour, A, Chang, ASM, Trivedi, A, Manley, BJ, McCall, E, Bogossian, F, Namba, F, Schmölzer, GM, Popat, H, Nguyen, KA, Doyle, LW, Jardine, L, Rysavy, MA, Konstantinidis, M, Muhd Helmi, MA, Lai, NM, Hay, S, Onland, W, Choo, YM, Gale, C, Soll, RF, Offringa, M, and CORE OUTCOME REPORTING IN NEONATAL TRIALS (CORINT) STUDY GROUP

Abstract

BACKGROUND AND OBJECTIVES: There is variability in the selection and reporting of outcomes in neonatal trials with key information frequently omitted. This can impact applicability of trial findings to clinicians, families, and caregivers, and impair evidence synthesis. The Neonatal Core Outcomes Set describes outcomes agreed as clinically important that should be assessed in all neonatal trials, and Consolidated Standards of Reporting Trials (CONSORT)-Outcomes 2022 is a new, harmonized, evidence-based reporting guideline for trial outcomes. We reviewed published trials using CONSORT-Outcomes 2022 guidance to identify exemplars of neonatal core outcome reporting to strengthen description of outcomes in future trial publications. METHODS: Neonatal trials including >100 participants per arm published between 2015 to 2020 with a primary outcome included in the Neonatal Core Outcome Set were identified. Primary outcome reporting was reviewed using CONSORT 2010 and CONSORT-Outcomes 2022 guidelines by assessors recruited from Cochrane Neonatal. Examples of clear and complete outcome reporting were identified with verbatim text extracted from trial reports. RESULTS: Thirty-six trials were reviewed by 39 assessors. Examples of good reporting for CONSORT 2010 and CONSORT-Outcomes 2022 criteria were identified and subdivided into 3 outcome categories: "survival," "short-term neonatal complications," and "long-term developmental outcomes" depending on the core outcomes to which they relate. These examples are presented to strengthen future research reporting. CONCLUSIONS: We have identified examples of good trial outcome reporting. These illustrate how important neonatal outcomes should be reported to meet the CONSORT 2010 and CONSORT-Outcomes 2022 guidelines. Emulating these examples will improve the transmission of information relating to outcomes and reduce associated research waste.

Published

2023

3. Regeneration of injured articular cartilage using the recombinant human amelogenin protein.

Author

Helwa-Shalom O, Saba F, Spitzer E, Hanhan S, Goren K, Markowitz SI, Shilo D, Khaimov N, Gellman YN, Deutsch D, Blumenfeld A, Nevo H, and Haze A

Abstract

Aims: Cartilage injuries rarely heal spontaneously and often require surgical intervention, leading to the formation of biomechanically inferior fibrous tissue. This study aimed to evaluate the possible effect of amelogenin on the healing process of a large osteochondral injury (OCI) in a rat model., Methods: A reproducible large OCI was created in the right leg femoral trochlea of 93 rats. The OCIs were treated with 0.1, 0.5, 1.0, 2.5, or 5.0 μg/μl recombinant human amelogenin protein (rHAM + ) dissolved in propylene glycol alginate (PGA) carrier, or with PGA carrier alone. The degree of healing was evaluated 12 weeks after treatment by morphometric analysis and histological evaluation. Cell recruitment to the site of injury as well as the origin of the migrating cells were assessed four days after treatment with 0.5 μg/μl rHAM + using immunohistochemistry and immunofluorescence., Results: A total of 12 weeks after treatment, 0.5 μg/μl rHAM + brought about significant repair of the subchondral bone and cartilage. Increased expression of proteoglycan and type II collagen and decreased expression of type I collagen were revealed at the surface of the defect, and an elevated level of type X collagen at the newly developed tide mark region. Conversely, the control group showed osteoarthritic alterations. Recruitment of cells expressing the mesenchymal stem cell (MSC) markers CD105 and STRO-1, from adjacent bone marrow toward the OCI, was noted four days after treatment., Conclusion: We found that 0.5 μg/μl rHAM + induced in vivo healing of injured articular cartilage and subchondral bone in a rat model, preventing the destructive post-traumatic osteoarthritic changes seen in control OCIs, through paracrine recruitment of cells a few days after treatment., Competing Interests: The authors declare that they have no competing interests., (© 2023 Author(s) et al.)

Published

2023

4. The impact of music, play, and pet therapies in managing pain and anxiety in paediatric patients in hospital: a rapid systematic review.

Author

Goren K, Cen Y, Montemurri V, Moodley D, Sutton A, Ahmed A, Alphonsus L, Denezis P, Fleming C, Guertin H, Hyland K, Kalim A, Kim HH, Krause S, Liang A, Maclean E, Neocleous P, Patel A, Pritchard S, Purcell V, Qaqish M, Ryall S, Shum K, Suwary K, Vucetic A, Skinner J, Woolsey A, and Marcotte E

Abstract

Background: Hospitalized children face pain and anxiety associated with the environment and procedures., Objective: This review aimed to assess the impact of music, play, pet and art therapies on pain and anxiety in hospitalized paediatric patients. RCTs assessing the impact of music, play, pet, and/or art therapies on pain and/or anxiety in hospitalized paediatric patients were eligible., Methods: Database searching and citation screening was completed to identify studies. A narrative synthesis was used to summarize study findings and certainty of evidence was assessed using GRADE. Of the 761 documents identified, 29 were included spanning music (n = 15), play (n = 12), and pet (n = 3) therapies., Results: A high certainty of evidence supported play in reducing pain and moderate certainty for music and pet. A moderate certainty of evidence supported music and play in reducing anxiety., Conclusion: Complementary therapies utilized alongside conventional medical treatment may mitigate pain and anxiety in hospitalized paediatric patients., Competing Interests: The authors have no conflicts of interest to declare., (© The Author(s) 2023. Published by Oxford University Press on behalf of the Canadian Paediatric Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2023

5. Pharmacological and neurosurgical interventions for individuals with cerebral palsy and dystonia: a systematic review update and meta-analysis.

Author

Bohn E, Goren K, Switzer L, Falck-Ytter Y, and Fehlings D

Subjects

Baclofen administration & dosage, Baclofen therapeutic use, Botulinum Toxins adverse effects, Botulinum Toxins therapeutic use, Cerebral Palsy drug therapy, Cerebral Palsy surgery, Clonidine adverse effects, Clonidine therapeutic use, Deep Brain Stimulation adverse effects, Dystonia drug therapy, Dystonia surgery, Humans, Injections, Spinal adverse effects, Levodopa therapeutic use, Trihexyphenidyl adverse effects, Trihexyphenidyl therapeutic use, Cerebral Palsy therapy, Dystonia therapy, Neurosurgical Procedures

Abstract

Aim: To update a systematic review of evidence published up to December 2015 for pharmacological/neurosurgical interventions among individuals with cerebral palsy (CP) and dystonia., Method: Searches were updated (January 2016 to May 2020) for oral baclofen, trihexyphenidyl, benzodiazepines, clonidine, gabapentin, levodopa, botulinum neurotoxin (BoNT), intrathecal baclofen (ITB), and deep brain stimulation (DBS), and from database inception for medical cannabis. Eligible studies included at least five individuals with CP and dystonia and reported on dystonia, goal achievement, motor function, pain/comfort, ease of caregiving, quality of life (QoL), or adverse events. Evidence certainty was evaluated using GRADE., Results: Nineteen new studies met inclusion criteria (two trihexyphenidyl, one clonidine, two BoNT, nine ITB, six DBS), giving a total of 46 studies (four randomized, 42 non-randomized) comprising 915 participants when combined with those from the original systematic review. Very low certainty evidence supported improved dystonia (clonidine, ITB, DBS) and goal achievement (clonidine, BoNT, ITB, DBS). Low to very low certainty evidence supported improved motor function (DBS), pain/comfort (clonidine, BoNT, ITB, DBS), ease of caregiving (clonidine, BoNT, ITB), and QoL (ITB, DBS). Trihexyphenidyl, clonidine, BoNT, ITB, and DBS may increase adverse events. No studies were identified for benzodiazepines, gabapentin, oral baclofen, and medical cannabis., Interpretation: Evidence evaluating the use of pharmacological and neurosurgical management options for individuals with CP and dystonia is limited to between low and very low certainty. What this paper adds Meta-analysis suggests that intrathecal baclofen (ITB) and deep brain stimulation (DBS) may improve dystonia and pain. Meta-analysis suggests that DBS may improve motor function. Clonidine, botulinum neurotoxin, ITB, and DBS may improve achievement of individualized goals. ITB and DBS may improve quality of life. No direct evidence is available for oral baclofen, benzodiazepines, gabapentin, or medical cannabis., (© 2021 The Authors. Developmental Medicine & Child Neurology published by John Wiley & Sons Ltd on behalf of Mac Keith Press.)

Published

2021

6. Skeletal ligament healing using the recombinant human amelogenin protein.

Author

Hanhan S, Ejzenberg A, Goren K, Saba F, Suki Y, Sharon S, Shilo D, Waxman J, Spitzer E, Shahar R, Atkins A, Liebergall M, Blumenfeld A, Deutsch D, and Haze A

Subjects

Alginates administration & dosage, Animals, Biomarkers metabolism, Cell Movement drug effects, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Carriers, Female, Humans, Medial Collateral Ligament, Knee injuries, Medial Collateral Ligament, Knee innervation, Mesenchymal Stem Cells cytology, Mesenchymal Stem Cells metabolism, Nerve Endings drug effects, Rats, Recombinant Proteins pharmacology, Tensile Strength, Wound Healing physiology, Amelogenin pharmacology, Medial Collateral Ligament, Knee drug effects, Mesenchymal Stem Cells drug effects, Proprioception drug effects, Wound Healing drug effects

Abstract

Injuries to ligaments are common, painful and debilitating, causing joint instability and impaired protective proprioception sensation around the joint. Healing of torn ligaments usually fails to take place, and surgical replacement or reconstruction is required. Previously, we showed that in vivo application of the recombinant human amelogenin protein (rHAM(+)) resulted in enhanced healing of the tooth-supporting tissues. The aim of this study was to evaluate whether amelogenin might also enhance repair of skeletal ligaments. The rat knee medial collateral ligament (MCL) was chosen to prove the concept. Full thickness tear was created and various concentrations of rHAM(+), dissolved in propylene glycol alginate (PGA) carrier, were applied to the transected MCL. 12 weeks after transection, the mechanical properties, structure and composition of transected ligaments treated with 0.5 μg/μl rHAM(+) were similar to the normal un-transected ligaments, and were much stronger, stiffer and organized than control ligaments, treated with PGA only. Furthermore, the proprioceptive free nerve endings, in the 0.5 μg/μl rHAM(+) treated group, were parallel to the collagen fibres similar to their arrangement in normal ligament, while in the control ligaments the free nerve endings were entrapped in the scar tissue at different directions, not parallel to the axis of the force. Four days after transection, treatment with 0.5 μg/μl rHAM(+) increased the amount of cells expressing mesenchymal stem cell markers at the injured site. In conclusion application of rHAM(+) dose dependently induced mechanical, structural and sensory healing of torn skeletal ligament. Initially the process involved recruitment and proliferation of cells expressing mesenchymal stem cell markers., (© 2016 The Authors. Journal of Cellular and Molecular Medicine published by John Wiley & Sons Ltd and Foundation for Cellular and Molecular Medicine.)

Published

2016