12 results on '"Ward, Catherine"'
Search Results
2. Prevention of child mental health problems through parenting interventions in Southeastern Europe (RISE): study protocol for a multi-site randomised controlled trial
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Tăut, Diana, Băban, Adriana, Frantz, Inga, Dănilă, Ingrid, Lachman, Jamie M., Heinrichs, Nina, Ward, Catherine L., Gardner, Frances, Fang, Xiangming, Hutchings, Judy, Raleva, Marija, Lesco, Galina, Murphy, Hugh, and Foran, Heather
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- 2021
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3. Feasibility pilot of an adapted parenting program embedded within the Thai public health system
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McCoy, Amalee, Lachman, Jamie M., Ward, Catherine L., Tapanya, Sombat, Poomchaichote, Tassawan, Kelly, Jane, Mukaka, Mavuto, Cheah, Phaik Yeong, and Gardner, Frances
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- 2021
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4. Evaluating the dissemination and scale-up of two evidence-based parenting interventions to reduce violence against children: study protocol
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Shenderovich, Yulia, Ward, Catherine L., Lachman, Jamie M., Wessels, Inge, Sacolo-Gwebu, Hlengiwe, Okop, Kufre, Oliver, Daniel, Ngcobo, Lindokuhle L., Tomlinson, Mark, Fang, Zuyi, Janowski, Roselinde, Hutchings, Judy, Gardner, Frances, and Cluver, Lucie
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- 2020
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5. The association between neighbourhood-level deprivation and depression: evidence from the south african national income dynamics study.
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Dowdall, Nicholas, Ward, Catherine L., and Lund, Crick
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DEPRIVATION (Psychology) , *MENTAL depression , *MENTAL health , *POVERTY reduction , *PUBLIC health - Abstract
Background: Depression contributes substantially to the burden of disease in South Africa. Little is known about how neighbourhoods affect the mental health of the people living in them. Methods: Using nationally representative data (N=11,955) from the South African National Income Dynamics Study and the South African Indices of Multiple Deprivation (SAIMD) modelled at small-area level, this study tested associations between neighbourhood-level deprivation and depression, after controlling for individual-level covariates. Results: Results showed a significant positive association between neighbourhood-level deprivation and depression using the composite SAIMD (β = 0.31 (0.15); p=0.04) as well as the separate deprivation domains. Living environment deprivation (β =0.53 (0.16); p=0.001) and employment deprivation (β = 0.38 (0.13); p=0.004), respectively, were the two most salient domains in predicting this relationship. Conclusions: Findings supported the hypothesis that there is a positive association between living in a more deprived neighbourhood and depression, even after controlling for individual-level covariates. This study suggests that alleviating structural poverty could reduce the burden of depression in South Africa. [ABSTRACT FROM AUTHOR]
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- 2017
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6. Impairment of early fracture healing by skeletal muscle trauma is restored by FK506.
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Hurtgen, Brady J., Henderson, Beth E. P., Ward, Catherine L., Goldman, Stephen M., Garg, Koyal, McKinley, Todd O., Greising, Sarah M., Wenke, Joseph C., and Corona, Benjamin T.
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INFLAMMATION treatment ,BONE regeneration ,OSTEOTOMY ,SKELETAL muscle injuries ,ANIMAL experimentation ,ANIMALS ,BIOLOGICAL models ,BIOPSY ,CALLUS ,FRACTURE fixation ,TACROLIMUS ,IMMUNITY ,IMMUNOSUPPRESSIVE agents ,MACROPHAGES ,MUSCLE diseases ,ORTHOPEDIC implants ,RATS ,SOFT tissue injuries ,T cells ,TIBIA injuries ,TORQUE ,SKELETAL muscle ,FRACTURE healing ,DISEASE complications ,PHARMACODYNAMICS ,THERAPEUTICS - Abstract
Background: Heightened local inflammation due to muscle trauma or disease is associated with impaired bone regeneration.Methods: We hypothesized that FK506, an FDA approved immunomodulatory compound with neurotrophic and osteogenic effects, will rescue the early phase of fracture healing which is impaired by concomitant muscle trauma in male (~4 months old) Lewis rats. FK506 (1 mg/kg; i.p.) or saline was administered systemically for 14 days after an endogenously healing tibia osteotomy was created and fixed with an intermedullary pin, and the overlying tibialis anterior (TA) muscle was either left uninjured or incurred volumetric muscle loss injury (6 mm full thickness biopsy from middle third of the muscle).Results: The salient observations of this study were that 1) concomitant TA muscle trauma impaired recovery of tibia mechanical properties 28 days post-injury, 2) FK506 administration rescued the recovery of tibia mechanical properties in the presence of concomitant TA muscle trauma but did not augment mechanical recovery of an isolated osteotomy (no muscle trauma), 3) T lymphocytes and macrophage presence within the traumatized musculature were heightened by trauma and attenuated by FK506 3 days post-injury, and 4) T lymphocyte but not macrophage presence within the fracture callus were attenuated by FK506 at 14 days post-injury. FK506 did not improve TA muscle isometric torque production CONCLUSION: Collectively, these findings support the administration of FK506 to ameliorate healing of fractures with severe muscle trauma comorbidity. The results suggest one potential mechanism of action is a reduction in local T lymphocytes within the injured musculoskeletal tissue, though other mechanisms to include direct osteogenic effects of FK506 require further investigation. [ABSTRACT FROM AUTHOR]- Published
- 2017
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7. A parenting programme to prevent abuse of adolescents in South Africa: study protocol for a randomised controlled trial.
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Cluver, Lucie, Meinck, Franziska, Shenderovich, Yulia, Ward, Catherine L., Romero, Rocio Herrero, Redfern, Alice, Lombard, Carl, Doubt, Jenny, Steinert, Janina, Catanho, Ricardo, Wittesaele, Camille, De Stone, Sachin, Salah, Nasteha, Mpimpilashe, Phelisa, Lachman, Jamie, Loening, Heidi, Gardner, Frances, Blanc, Daphnee, Nocuza, Mzuvekile, and Lechowicz, Meryn
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TEENAGER abuse ,PARENTING ,PREVENTION of child abuse ,BEHAVIOR disorders in adolescence ,MENTAL health of teenagers ,ABUSED teenagers ,YOUTH services ,COMPARATIVE studies ,RESEARCH methodology ,MEDICAL cooperation ,RESEARCH protocols ,RESEARCH ,STATISTICAL sampling ,EVALUATION research ,RANDOMIZED controlled trials - Abstract
Background: An estimated one billion children experience child abuse each year, with the highest rates in low- and middle-income countries. The Sinovuyo Teen programme is part of Parenting for Lifelong Health, a WHO/UNICEF initiative to develop and test violence-prevention programmes for implementation in low-resource contexts. The objectives of this parenting support programme are to prevent the abuse of adolescents, improve parenting and reduce adolescent behavioural problems. This trial aims to evaluate the effectiveness of Sinovuyo Teen compared to an attention-control group of a water hygiene programme.Methods/design: This is a pragmatic cluster randomised controlled trial, with stratified randomisation of 37 settlements (rural and peri-urban) with 40 study clusters in the Eastern Cape of South Africa. Settlements receive either a 14-session parenting support programme or a 1-day water hygiene programme. The primary outcomes are child abuse and parenting practices, and secondary outcomes include adolescent behavioural problems, mental health and social support. Concurrent process evaluation and qualitative research are conducted. Outcomes are reported by both primary caregivers and adolescents. Brief follow-up measures are collected immediately after the intervention, and full follow-up measures collected at 3-8 months post-intervention. A 15-24-month follow-up is planned, but this will depend on the financial and practical feasibility given delays related to high levels of ongoing civil and political violence in the research sites.Discussion: This is the first known trial of a parenting programme to prevent abuse of adolescents in a low- or middle-income country. The study will also examine potential mediating pathways and moderating factors.Trial Registration: Pan-African Clinical Trials Registry PACTR201507001119966. Registered on 27 April 2015. It can be found by searching for the key word 'Sinovuyo' on their website or via the following link: http://www.pactr.org/ATMWeb/appmanager/atm/atmregistry?_nfpb=true&_windowLabel=BasicSearchUpdateController_1&BasicSearchUpdateController_1_actionOverride=%2Fpageflows%2Ftrial%2FbasicSearchUpdate%2FviewTrail&BasicSearchUpdateController_1id=1119. [ABSTRACT FROM AUTHOR]- Published
- 2016
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8. Soluble factors from biofilms of wound pathogens modulate human bone marrow-derived stromal cell differentiation, migration, angiogenesis, and cytokine secretion.
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Ward, Catherine L., Sanchez Jr., Carlos J., Pollot, Beth E., Romano, Desiree R., Hardy, Sharanda K., Becerra, Sandra C., Rathbone, Christopher R., and Wenke, Joseph C.
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BIOFILMS , *STAPHYLOCOCCUS aureus , *PSEUDOMONAS aeruginosa , *MESENCHYMAL stem cells , *CELL differentiation , *CELL survival , *PARACRINE mechanisms , *WOUND healing - Abstract
Background: Chronic, non-healing wounds are often characterized by the persistence of bacteria within biofilms - aggregations of cells encased within a self-produced polysaccharide matrix. Biofilm bacteria exhibit unique characteristics from planktonic, or culture-grown, bacterial phenotype, including diminished responses to antimicrobial therapy and persistence against host immune responses. Mesenchymal stromal cells (MSCs) are host cells characterized by their multifunctional ability to undergo differentiation into multiple cell types and modulation of host-immune responses by secreting factors that promote wound healing. While these characteristics make MSCs an attractive therapeutic for wounds, these pro-healing activities may be differentially influenced in the context of an infection (i.e., biofilm related infections) within chronic wounds. Herein, we evaluated the effect of soluble factors derived from biofilms of clinical isolates of Staphylococcus aureus and Pseudomonas aeruginosa on the viability, differentiation, and paracrine activity of human MSCs to evaluate the influence of biofilms on MSC activity in vitro. Results: Exposure of MSCs to biofilm-conditioned medias of S. aureus and P. aeruginosa resulted in reductions in cell viability, in part due to activation of apoptosis. Similarly, exposure to soluble factors from biofilms was also observed to diminish the migration ability of cells and to hinder multi-lineage differentiation of MSCs. In contrast to these findings, exposure of MSCs to soluble factors from biofilms resulted in significant increases in the release of paracrine factors involved in inflammation and wound healing. Conclusions: Collectively, these findings demonstrate that factors produced by biofilms can negatively impact the intrinsic properties of MSCs, in particular limiting the migratory and differentiation capacity of MSCs. Consequently, these studies suggest use/application of stem-cell therapies in the context of infection may have a limited therapeutic effect. [ABSTRACT FROM AUTHOR]
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- 2015
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9. Amyotrophic lateral sclerosis-linked FUS/TLS alters stress granule assembly and dynamics.
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Baron, Desiree M., Kaushansky, Laura J., Ward, Catherine L., Sama, Reddy Ranjith K., Chian, Ru-Ju, Boggio, Kristin J., Quaresma, Alexandre J. C., Nickerson, Jeffrey A., and Bosco, Daryl A.
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AMYOTROPHIC lateral sclerosis ,LIPOSARCOMA ,FRONTOTEMPORAL dementia ,OXIDATIVE stress ,CYTOPLASMIC granules ,GENETIC mutation - Abstract
Background: Amyotrophic lateral sclerosis (ALS)-linked fused in sarcoma/translocated in liposarcoma (FUS/TLS or FUS) is concentrated within cytoplasmic stress granules under conditions of induced stress. Since only the mutants, but not the endogenous wild-type FUS, are associated with stress granules under most of the stress conditions reported to date, the relationship between FUS and stress granules represents a mutant-specific phenotype and thus may be of significance in mutant-induced pathogenesis. While the association of mutant-FUS with stress granules is well established, the effect of the mutant protein on stress granules has not been examined. Here we investigated the effect of mutant-FUS on stress granule formation and dynamics under conditions of oxidative stress. Results: We found that expression of mutant-FUS delays the assembly of stress granules. However, once stress granules containing mutant-FUS are formed, they are more dynamic, larger and more abundant compared to stress granules lacking FUS. Once stress is removed, stress granules disassemble more rapidly in cells expressing mutant-FUS. These effects directly correlate with the degree of mutant-FUS cytoplasmic localization, which is induced by mutations in the nuclear localization signal of the protein. We also determine that the RGG domains within FUS play a key role in its association to stress granules. While there has been speculation that arginine methylation within these RGG domains modulates the incorporation of FUS into stress granules, our results demonstrate that this post-translational modification is not involved. Conclusions: Our results indicate that mutant-FUS alters the dynamic properties of stress granules, which is consistent with a gain-of-toxic mechanism for mutant-FUS in stress granule assembly and cellular stress response [ABSTRACT FROM AUTHOR]
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- 2013
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10. Staphylococcus aureus biofilms decrease osteoblast viability, inhibits osteogenic differentiation, and increases bone resorption in vitro.
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Sanchez, Carlos J., Ward, Catherine L., Romano, Desiree R., Hurtgen, Brady J., Hardy, Sharanda K., Woodbury, Ronald L., Trevino, Alex V., Rathbone, Christopher R., and Wenke, Joseph C.
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STAPHYLOCOCCUS aureus , *BIOFILMS , *OSTEOINDUCTION , *BONE resorption , *OSTEOMYELITIS , *ALKALINE phosphatase , *BONE growth - Abstract
Background: Osteomyelitis is a severe and often debilitating disease characterized by inflammatory destruction of bone. Despite treatment, chronic infection often develops which is associated with increased rates of treatment failure, delayed osseous-union, and extremity amputation. Within affected bone, bacteria exist as biofilms, however the impact of biofilms on osteoblasts during disease are unknown. Herein, we evaluated the effect of S. aureus biofilms on osteoblast viability, osteogenic potential, and the expression of the pro-osteoclast factor, receptor activator of NF-kB ligand (RANK-L). Methods: Osteoblasts were exposed to biofilm conditioned media (BCM) from clinical wound isolates of Staphylococcus aureus under normal growth and osteogenic conditions to assess cellular viability and osteoblast differentiation, respectively. Cell viability was evaluated using a live/dead assay and by quantifying total cellular DNA at days 0, 1, 3, 5, and 7. Apoptosis following treatment with BCM was measured by flow-cytometry using the annexin V-FITC/PI apoptosis kit. Osteogenic differentiation was assessed by measuring alkaline phosphatase activity and intracellular accumulation of calcium and osteocalcin for up to 21 days following exposure to BCM. Expression of genes involved in osteogenic differentiation and osteoclast regulation, were also evaluated by quantitative real-time PCR. Results: BCM from clinical strains of S. aureus reduced osteoblast viability which was accompanied by an increase in apoptosis. Osteogenic differentiation was significantly inhibited following treatment with BCM as indicated by decreased alkaline phosphatase activity, decreased intracellular accumulation of calcium and inorganic phosphate, as well as reduced expression of transcription factors and genes involved in bone mineralization in viable cells. Importantly, exposure of osteoblasts to BCM resulted in up-regulated expression of RANK-L and increase in the RANK-L/ OPG ratio compared to the untreated controls. Conclusions: Together these studies suggest that soluble factors produced by S. aureus biofilms may contribute to bone loss during chronic osteomyelitis simultaneously by: (1) reducing osteoblast viability and osteogenic potential thereby limiting new bone growth and (2) promoting bone resorption through increased expression of RANK-L by osteoblasts. To our knowledge these are the first studies to demonstrate the impact of staphylococcal biofilms on osteoblast function, and provide an enhanced understanding of the pathogenic role of staphylococcal biofilms during osteomyelitis. [ABSTRACT FROM AUTHOR]
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- 2013
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11. Reducing child abuse amongst adolescents in low- and middle-income countries: A pre-post trial in South Africa.
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Cluver, Lucie, Meinck, Franziska, Yakubovich, Alexa, Doubt, Jenny, Redfern, Alice, Ward, Catherine, Salah, Nasteha, De Stone, Sachin, Petersen, Tshiamo, Mpimpilashe, Phelisa, Romero, Rocio Herrero, Ncobo, Lulu, Lachman, Jamie, Tsoanyane, Sibongile, Shenderovich, Yulia, Loening, Heidi, Byrne, Jasmina, Sherr, Lorraine, Kaplan, Lauren, and Gardner, Frances
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PREVENTION of child abuse ,PREVENTION of mental depression ,CHILD abuse & psychology ,AGGRESSION (Psychology) ,PSYCHOLOGY of caregivers ,CHILD abuse ,CLINICAL trials ,COMPARATIVE studies ,DEVELOPING countries ,EMOTIONS ,INCOME ,RESEARCH methodology ,MEDICAL cooperation ,MENTAL health ,PARENTING ,PSYCHOLOGY of parents ,RESEARCH ,SUBSTANCE abuse ,TEENAGERS' conduct of life ,SOCIAL support ,SOCIOECONOMIC factors ,EVALUATION research ,INTIMATE partner violence ,EVALUATION of human services programs - Abstract
Background: No known studies have tested the effectiveness of child abuse prevention programmes for adolescents in low- or middle-income countries. 'Parenting for Lifelong Health' ( http://tiny.cc/whoPLH ) is a collaborative project to develop and rigorously test abuse-prevention parenting programmes for free use in low-resource contexts. Research aims of this first pre-post trial in South Africa were: i) to identify indicative effects of the programme on child abuse and related outcomes; ii) to investigate programme safety for testing in a future randomised trial, and iii) to identify potential adaptations.Methods: Two hundred thirty participants (adolescents and their primary caregivers) were recruited from schools, welfare services and community-sampling in rural, high-poverty South Africa (no exclusion criteria). All participated in a 12-week parenting programme, implemented by local NGO childcare workers to ensure real-world external validity. Standardised pre-post measures with adolescents and caregivers were used, and paired t-tests were conducted for primary outcomes: abuse (physical, emotional abuse and neglect), adolescent behaviour problems and parenting (positive and involved parenting, poor monitoring and inconsistent discipline), and secondary outcomes: mental health, social support and substance use.Results: Participants reported high levels of socio-economic deprivation, e.g. 60 % of adolescents had either an HIV-positive caregiver or were orphaned by AIDS, and 50 % of caregivers experienced intimate partner violence. i) indicative effects: Primary outcomes comparing pre-test and post-test assessments showed reductions reported by adolescents and caregivers in child abuse (adolescent report 63.0 % pre-test to 29.5 % post-test, caregiver report 75.5 % pre-test to 36.5 % post-test, both p < 0.001) poor monitoring/inconsistent discipline (p < .001), adolescent delinquency/aggressive behaviour (both p < .001), and improvements in positive/involved parenting (p < .01 adolescent report, p < .001 caregiver report). Secondary outcomes showed improved social support (p < .001 adolescent and caregiver reports), reduced parental and adolescent depression (both p < .001), parenting stress (p < .001 caregiver report) and caregiver substance use (p < .002 caregiver report). There were no changes in adolescent substance use. No negative effects were detected. ii) Programme acceptability and attendance was high. There was unanticipated programme diffusion within some study villages, with families initiating parenting groups in churches, and diffusion through school assemblies and religious sermons. iii) potential adaptations identified included the need to strengthen components on adolescent substance use and to consider how to support spontaneous programme diffusion with fidelity.Conclusions: The programme showed no signs of harm and initial evidence of reductions in child abuse and improved caregiver and adolescent outcomes. It showed high acceptability and unexpected community-level diffusion. Findings indicate needs for adaptations, and suitability for the next research step of more rigorous testing in randomised trials, using cluster randomization to allow for diffusion effects. [ABSTRACT FROM AUTHOR]- Published
- 2016
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12. Association of Child Maltreatment with South African Adults' Wages: Evidence from the Cape Area Panel Study.
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Zheng X, Fang X, Fry DA, Ganz G, Casey T, Hsiao C, and Ward CL
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Child maltreatment is a prevalent public health problem in both developed and developing countries. While many studies have investigated the relationship between violence against children and health of the victims, little is known about the long term economic consequences of child maltreatment, especially in developing countries. Using data from the Cape Area Panel Study, this paper applies Heckman selection models to investigate the relationship between childhood maltreatment and young adults' wages in South Africa. The results show that, on average, any experience of physical or emotional abuse during childhood is associated with a later 12% loss of young adults' wages. In addition, the correlation between physical abuse and economic consequence (14%) is more significant than the relationship between emotional abuse and wages (8%) of young adults; and the higher the frequency of maltreatment, the greater the associations with wages. With respect to gender differences, wage loss due to the experience of childhood maltreatment is larger for females than males. Specifically, males' wages are more sensitive to childhood emotional abuse, while females' wages are more likely to be affected by childhood physical abuse. These results emphasize the importance of prioritizing investments in prevention and intervention programs to reduce the prevalence of child maltreatment and to help victims better overcome the long-term negative effect.
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- 2018
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