Archive for month: December, 2024

A new study published in the Journal of Allergy and Clinical Immunology showed that effective therapy for chronic spontaneous urticaria (CSU) may lower mortality. Between 0.5% and 1% of people have chronic spontaneous urticaria which is a prevalent immunologic condition. It is linked to several negative patient outcomes, both direct and indirect that ranged from a decline in quality of life (QoL) to a rise in allergy misdiagnosis and mislabeling.

Complete disease control is the aim of treatment for CSU, and stepwise pharmacologic therapy is advised by recommendations. Omalizumab (licensed dose 300 mg monthly) is recommended for patients with uncontrolled symptoms even after receiving maximal doses of antihistamines (approximately 20% to 50% of all patients with CSU).

This is despite the fact that the first step is the regular use of second-generation H1-antihistamines, followed by doses increasing up to 4-fold. Therefore, this study was conducted to evaluate the influence of treatment recommendations for urticaria on mortality rates, risk for comorbidities that are major causes of death, and all-cause mortality in CSU patients.

The electronic medical data of 1,27,28,913 non-urticaria controls and 2,72,190 adult CSU patients from the US Collaborative TriNetx Analytics Network are the subjects of this retrospective population-based cohort research. A total of 2,64,680 propensity score-matched people suffering from CSU and an equal number of non-urticaria controls were included in the research.

The patients with CSU had greater 3-month, 1-year, and 5-year all-cause mortality. CSU patients had greater risk and incidence of the top causes of mortality in the US, such as malignant neoplasms and suicidal thoughts and attempts, than non-CSU controls.

White and younger patients seemed to be at a higher risk of death at CSU. When compared to patients who were not treated, CSU patients treated with second-generation H1-antihistamines had significantly reduced all-cause death rates at 5 years, as were patients treated with omalizumab as opposed to those treated with antihistamines.

Overall, chronic spontaneous urticaria patients had a 1.7-fold higher risk of all-cause death than the individuals without CSU. Mortality rates were reduced by CSU therapy with omalizumab and second-generation antihistamines by indicating that these risks might be reduced with appropriate care.

Source:

Kolkhir, P., Bieber, K., Hawro, T., Kridin, K., Ludwig, M. A., Olbrich, H., Metz, M., Vorobyev, A., Ludwig, R. J., & Maurer, M. (2024). Mortality in adult patients with chronic spontaneous urticaria: A real world cohort study. In Journal of Allergy and Clinical Immunology. Elsevier BV. https://doi.org/10.1016/j.jaci.2024.11.036

Researchers have identified that moderate to severe retinopathy of prematurity (ROP) is strongly related to the increased risk of autism spectrum disorder (ASD) in children born extremely premature. A recent study was conducted by Pia L. and colleagues which was published in the journal Acta Paediatrica.

A recent study published in the
journal BMC Surgery found that norepinephrine has protective effects on
intraoperative hemorrhage and postoperative pain and also helps to reduce
hospitalization in individuals undergoing resection of benign breast nodules.

Also Read: Cryoablation Safe for Breast Cancer Patients who are poor surgical candidates: Study

Also Read:AI Powered Blood Test Detects Earliest Stage of Breast Cancer: Study Finds

Giving more blood to anemic patients after a heart attack may save lives, according to a Rutgers Health-led study.

The study, published in NEJM Evidence, affirms research conducted in 2023 that suggested mortality rate or recurrent heart attacks were more frequent in anemic patients who received less blood.

Jeffrey L. Carson, provost and Distinguished Professor of medicine at Rutgers Robert Wood Johnson Medical School, led both studies. The 2023 trial – referred to as MINT (myocardium infarction and transfusion) – looked at transfusions in anemic patients following a heart attack.

After that 2023 trial, Carson planned a study on blood transfusions that combined data from similar trials to generate more precise estimates of treatment effects.

In cooperation with researchers in France and the United States, Carson acquired data from the four clinical trials evaluating blood transfusion in 4,311 patients with heart attacks. These trials included patients who had a heart attack and low blood count. Half the patients received less blood transfusions and the other half received more blood transfusions. The trials compared the frequency of death at 30 days or recurrent heart attacks and death at six months.

The results of this analysis, published recently in NEJM Evidence, didn’t definitively establish that giving less blood transfusions increased a patients’ risk of death or heart attack at 30 days, but did suggest that using less transfusions was associated with an increased risk of death at six months.

In the original clinical trial, a large percentage of patients had suffered a previous heart attack, heart failure, diabetes or kidney disease. The average age of participants was 72, with 45% women.

The researchers compared the frequency of the main outcome of death or recurrent heart attack at 30 days after enrollment into the trial. Although not statistically significant, the study found the frequency of mortality or recurrent heart attack was 2.4% lower when a liberal approach was used.

“The results of this analysis show that giving more blood to anemic patients with heart attacks can save lives at six months,” Carson said.

Both studies were funded through by the National Heart, Lung and Blood Institute, which is a part of the National Institutes of Health.

For nearly two decades, Carson has studied the implications of red blood cell transfusion strategies toward providing optimal treatment for patients. His work helped establish transfusion guidelines in 2012 used by physicians to inform patient care, updates to which were announced last year in the Journal of the American Medical Association emphasizing an individualized approach in adults and children that account for the patients underlying medical problems, patient preferences and symptoms.

Reference:

Jeffrey L. Carson, Dean A. Fergusson, Helaine Noveck, Ranjeeta Mallick, Tabassome Simon, Restrictive versus Liberal Transfusion in Myocardial Infarction — A Patient-Level Meta-Analysis, NEJM Evidence, DOI: 10.1056/EVIDoa2400223

High cardiorespiratory fitness is associated with better cognitive performance and lower risk of dementia long term, including in people with a genetic predisposition to dementia, show the findings of a study published online in the British Journal of Sports Medicine.

Cardiorespiratory fitness (CRF) is the capacity of the circulatory and respiratory systems to supply oxygen to muscles and declines increasingly with age as skeletal muscle is lost. CRF declines by around 3% to 6% per decade when people are in their 20s and 30s, but this accelerates to more than 20% per decade by the time people reach their 70s. Low CRF is a strong predictor of cardiovascular events such as strokes and heart attacks and mortality from all causes.

Most previous studies investigating the impact of CRF on cognitive function and dementia risk included a small number of participants. For this study, the authors looked at a much larger group by accessing data on 61,214 dementia-free people aged 39-70 years who enrolled in the UK Biobank study between 2009 and 2010 and were followed for up to 12 years.

At enrolment, a 6-minute submaximal exercise test on a stationary bike was completed to estimate CRF, cognitive function was estimated using neuropsychological tests, and genetic predisposition for dementia was estimated using the polygenic risk score for Alzheimer’s disease. During the follow-up period of up to 12 years, 553 people (0.9%) received a diagnosis of dementia.

Participants were divided into three equal-sized groups standardised by age and sex according to their CRF scores for the analysis which showed that people with high CRF had higher cognitive function and a lower risk of dementia.

Compared with people with low CRF, the incidence rate ratio (IRR) of all dementia was 0.6 for people with high CRF, and onset of dementia was delayed by 1.48 years. A high CRF also reduced all dementia risk by 35% among people with a moderate/high polygenic risk score.

This is an observational study, and as such, can’t establish cause and effect, and the researchers acknowledge various imitations to their findings.

Most importantly the number of dementia cases may have been underestimated because UK Biobank participants are generally healthier than the general population, plus individuals with certain health conditions were excluded from the exercise test making the population investigated ‘healthier’ still. The reliance on registries to identify dementia cases might have led to a further underestimation. Also, the submaximal exercise test used is considered less accurate than maximal exercise testing which requires participants to exercise to exhaustion, and any association between CRF change and dementia risk could not be examined due to the lack of repeat CRF measurements.

The authors conclude, “Our study shows that higher CRF is associated with better cognitive function and decreased dementia risk. Moreover, high CRF may buffer the impact of genetic risk of all dementia by 35%.”

They add that their findings suggest that, “Enhancing CRF could be a strategy for the prevention of dementia, even among people with a high genetic predisposition for Alzheimer’s disease.”

Further research on the relationship between CRF and brain health, especially in older adults, and on the mechanisms by which CRF modifies the relationship between genetic risk and dementia is needed, they say.