Your search keyword '"Merone, Lea"' showing total 5 results

1. A systematic review and meta-analysis of published research data on COVID-19 infection fatality rates.

Author

Meyerowitz-Katz, Gideon and Merone, Lea

Subjects

*COVID-19, *GOVERNMENT report writing, *PANDEMICS, *COMORBIDITY, *GREY literature

Abstract

• COVID-19 infection fatality rate (IFR) is an important statistic for policy about the disease. • Published estimates vary, with a 'true' fatality rate hard to calculate. • Systematically reviewing the literature and meta-analysing the results show an IFR of 0.68% (0.53%–0.82%). • This rate varied from place to place, with a lower range of 0.17% and a highest estimate of 1.7%. • Serology studies with a lower risk of bias appeared to demonstrate a higher IFR than those at a higher risk of bias. An important unknown during the coronavirus disease-2019 (COVID-19) pandemic has been the infection fatality rate (IFR). This differs from the case fatality rate (CFR) as an estimate of the number of deaths and as a proportion of the total number of cases, including those who are mild and asymptomatic. While the CFR is extremely valuable for experts, IFR is increasingly being called for by policy makers and the lay public as an estimate of the overall mortality from COVID-19. Pubmed, Medline, SSRN, and Medrxiv were searched using a set of terms and Boolean operators on 25/04/2020 and re-searched on 14/05/2020, 21/05/2020 and 16/06/2020. Articles were screened for inclusion by both authors. Meta-analysis was performed in Stata 15.1 by using the metan command, based on IFR and confidence intervals extracted from each study. Google/Google Scholar was used to assess the grey literature relating to government reports. After exclusions, there were 24 estimates of IFR included in the final meta-analysis, from a wide range of countries, published between February and June 2020. The meta-analysis demonstrated a point estimate of IFR of 0.68% (0.53%–0.82%) with high heterogeneity (p < 0.001). Based on a systematic review and meta-analysis of published evidence on COVID-19 until July 2020, the IFR of the disease across populations is 0.68% (0.53%–0.82%). However, due to very high heterogeneity in the meta-analysis, it is difficult to know if this represents a completely unbiased point estimate. It is likely that, due to age and perhaps underlying comorbidities in the population, different places will experience different IFRs due to the disease. Given issues with mortality recording, it is also likely that this represents an underestimate of the true IFR figure. More research looking at age-stratified IFR is urgently needed to inform policymaking on this front. [ABSTRACT FROM AUTHOR]

Published

2020

2. Primary Prevention of Cardiovascular Disease in Minority Indigenous Populations: A Systematic Review.

Author

Merone, Lea, McDermott, Robyn, Mein, Jacki, Clarke, Philip, and McDonald, Malcolm

Subjects

*INDIGENOUS peoples, *TORRES Strait Islanders, *PREVENTIVE medicine, *CARDIOVASCULAR diseases, *META-analysis, *RISK assessment -- Law & legislation, *CARDIOVASCULAR disease prevention, *PUBLIC health surveillance, *SYSTEMATIC reviews, *PREVENTIVE health services, *DISEASE prevalence, *MEDICAL care of indigenous peoples

Abstract

Introduction: Cardiovascular disease (CVD) is the commonest cause of death across the globe; incidence and prevalence rates are increasing. Together, CVD and diabetes mellitus are responsible for a quarter of the health gap observed between Aboriginal Australians and Torres Strait Islanders, and non-Indigenous Australians. Numerous programs have been proposed and implemented to Close the Gap; ideally, these should be evidence-based.Objective: The aim of this review is to evaluate primary prevention measures and programs that aim to reduce CVD risk in minority Indigenous populations around the world.Methods: A search of PubMed, the Cochrane Library and the Elsevier Scopus Database was initially conducted using the terms "cardiovascular disease", "population groups", "primary prevention", "health services, indigenous", "indigenous health", "risk assessment" and "risk management". Results were then assessed per inclusion/exclusion criteria. A second reviewer independently evaluated the publications and review process to ensure agreement.Results: The initial search produced 37 publications; 19 met the inclusion criteria and were incorporated into a comparative table. Most were descriptive, mixed-methods, audit or intervention studies. Heterogeneity of study design prevented statistical analysis.Conclusion: Addressing CVD risk in minority Indigenous populations is a multifactorial challenge; there is substantial room for improvement in routine risk assessment and management. Holistic approaches need to embrace local cultural perceptions of health and wellbeing. Validated risk reduction tools, individualised management plans, polypills and computer based decision support tools are promising to improve outcomes for those at risk. [ABSTRACT FROM AUTHOR]

Published

2020

3. Safety and tolerability of experimental hookworm infection in humans with metabolic disease: study protocol for a phase 1b randomised controlled clinical trial.

Author

Pierce, Doris, Merone, Lea, Lewis, Chris, Rahman, Tony, Croese, John, Loukas, Alex, McDonald, Malcolm, Giacomin, Paul, and McDermott, Robyn

Subjects

*TYPE 2 diabetes risk factors, *FECAL analysis, *OBESITY complications, *HUMAN microbiota, *DIET, *HOOKWORM disease, *MEDICAL care costs, *METABOLIC disorders, *TYPE 2 diabetes, *PHYSICAL diagnosis, *QUESTIONNAIRES, *TIME, *DISEASE management, *TREATMENT effectiveness, *PHYSICAL activity, *DISEASE risk factors

Abstract

Background: Abdominal obesity and presence of the metabolic syndrome (MetS) significantly increase the risk of developing diseases such as Type 2 diabetes mellitus (T2DM) with escalating emergence of MetS and T2DM constituting a significant public health crisis worldwide. Lower prevalence of inflammatory and metabolic diseases such as T2DM in countries with higher incidences of helminth infections suggested a potential role for these parasites in the prevention and management of certain diseases. Recent studies confirmed the potential protective nature of helminth infection against MetS and T2DM via immunomodulation or, potentially, alteration of the intestinal microbiota. This Phase 1b safety and tolerability trial aims to assess the effect of inoculation with helminths on physical and metabolic parameters, immune responses, and the microbiome in otherwise healthy women and men. Methods: Participants eligible for inclusion are adults aged 18–50 with central obesity and a minimum of one additional feature of MetS recruited from the local community with a recruitment target of 54. In a randomised, double-blind, placebo-controlled design, three groups will receive either 20 or 40 stage three larvae of the human hookworm Necator americanus or a placebo. Eligible participants will provide blood and faecal samples at their baseline and 6-monthly assessment visits for a total of 24 months with an optional extension to 36 months. During each scheduled visit, participants will also undergo a full physical examination and complete diet (PREDIMED), physical activity, and patient health (PHQ-9) questionnaires. Outcome measurements include tolerability and safety of infection with Necator americanus, changes in metabolic and immunological parameters, and changes in the composition of the faecal microbiome. Discussion: Rising cost of healthcare associated with obesity-induced metabolic diseases urgently calls for new approaches in disease prevention. Findings from this trial will provide valuable information regarding the potential mechanisms by which hookworms, potentially via alterations in the microbiota, may positively influence metabolic health. Trial registration: The protocol was registered on ANZCTR.org.au on 05 June 2017 with identifier ACTRN12617000818336. Alternatively, a Google search using the above trial registration number will yield a direct link to the trial protocol within the ANZCTR website. [ABSTRACT FROM AUTHOR]

Published

2019

4. Nutritional anti-inflammatories in the treatment and prevention of type 2 diabetes mellitus and the metabolic syndrome.

Author

Merone, Lea and McDermott, Robyn

Subjects

*TYPE 2 diabetes treatment, *METABOLIC syndrome, *BIOMARKERS, *ANTI-inflammatory agents, *EVIDENCE-based medicine, *FISH oils, *PHYSIOLOGICAL effects of vitamins, *PREVENTION

Abstract

Aims: Obesity-fuelled metabolic syndrome and diabetes is now a global epidemic. There is increasing evidence that these and other chronic conditions have common inflammatory antecedents. There is an interest in nutritionally based anti-inflammatory treatments for type 2 diabetes and metabolic syndrome. The aim of this review is to examine the evidence from a 5-year period; 2011-2016, for nutritionally based anti-inflammatory treatments for the Metabolic Syndrome and Type 2 Diabetes Mellitus.Methods: A literature search produced a total number of 1377 records, of which 26 papers were evaluated.Results: Literature was analysed and tabulated according to date, outcome measures and results.Conclusion: The evidence is strong for use of polyphenolic compounds, fish oils and vitamins in reducing inflammation biomarkers, however the impact on metabolic control is less evident. [ABSTRACT FROM AUTHOR]

Published

2017

5. Outbreak of multi-drug-resistant (MDR) Shigella flexneri in northern Australia due to an endemic regional clone acquiring an IncFII plasmid.

Author

Guglielmino, Christine J. D., Kakkanat, Asha, Forde, Brian M., Rubenach, Sally, Merone, Lea, Stafford, Russell, Graham, Rikki M. A., Beatson, Scott A., and Jennison, Amy V.

Subjects

*SHIGELLOSIS, *SHIGELLA flexneri, *INDIGENOUS Australians, *PUBLIC health surveillance, *MULTIDRUG resistance, *MEN who have sex with men

Abstract

Epidemiological surveillance of Shigella spp. in Australia is conducted to inform public health response. Multi-drug resistance has recently emerged as a contributing factor to sustained local transmission of Shigella spp. All data were collected as part of routine public health surveillance, and strains were whole-genome sequenced for further molecular characterisation. 108 patients with an endemic regional Shigella flexneri strain were identified between 2016 and 2019. The S. flexneri phylogroup 3 strain endemic to northern Australia acquired a multi-drug resistance conferring blaDHA plasmid, which has an IncFII plasmid backbone with virulence and resistance elements typically found in IncR plasmids. This is the first report of multi-drug resistance in Shigella sp. in Australia that is not associated with men who have sex with men. This strain caused an outbreak of multi-drug-resistant S. flexneri in northern Australia that disproportionality affects Aboriginal and Torres Strait Islander children. Community controlled public health action is recommended. [ABSTRACT FROM AUTHOR]

Published

2021