Chunquan Yu scite author profile

To discern whether the characteristics and outcome of invasive aspergillosis in liver transplant recipients have evolved during the past decade, 26 patients who underwent transplantation during 1990-1995 (known as "the earlier cohort") were compared with 20 patients who underwent transplantation during 1998-2001 (known as "the later cohort"). Twenty-three percent of the Aspergillus infections in the earlier cohort occurred у90 days after transplantation, compared with 55% of such infections in the later cohort ( ). The earlier cohort P p .026 was significantly more likely to have disseminated infection ( ) and central nervous system (CNS) in-P p .034 volvement ( ) than was the later cohort. The mortality rate was significantly higher for the earlier cohort P p .0004 (92%) than for the later cohort (60%;). Only disseminated infection (not the year of transplantation) P p .012 approached statistical significance as an independent predictor of outcome. In the current era, invasive aspergillosis occurs later in the posttransplantation period, is less likely to be associated with CNS infection, and is associated with a lower mortality rate, compared with invasive aspergillosis in the early 1990s.Invasive aspergillosis has long been recognized as one of the most significant opportunistic fungal infections in liver transplant recipients [1][2][3][4]. The frequency of invasive aspergillosis among liver transplant recipients ranges from 1% to 6% [2]. However, the mortality rate for these patients exceeds 90% [1,5]; an estimated 16.9% of all deaths that have occurred among liver

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Opportunistic Mycelial Fungal Infections in Organ Transplant Recipients: Emerging Importance of Non-Aspergillus Mycelial Fungi

Husain

Alexander

Muñóz

et al. 2003

Clinical Infectious Diseases

312

200

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To determine the spectrum and impact of mycelial fungal infections, particularly those due to non-Aspergillus molds, 53 liver and heart transplant recipients with invasive mycelial infections were prospectively identified in a multicenter study. Invasive mycelial infections were due to Aspergillus species in 69.8% of patients, to non-Aspergillus hyalohyphomycetes in 9.4%, to phaeohyphomycetes in 9.4%, to zygomycetes in 5.7%, and to other causes in 5.7%. Infections due to mycelial fungi other than Aspergillus species were significantly more likely to be associated with disseminated (P=.005) and central nervous system (P=.07) infection than were those due to Aspergillus species. Overall mortality at 90 days was 54.7%. The associated mortality rate was 100% for zygomycosis, 80% for non-Aspergillus hyalohyphomycosis, 54% for aspergillosis, and 20% for phaeohyphomycosis. Thus, non-Aspergillus molds have emerged as significant pathogens in organ transplant recipients. These molds are more likely to be associated with disseminated infections and to be associated with poorer outcomes than is aspergillosis.

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Deep learning analysis in coronary computed tomographic angiography imaging for the assessment of patients with coronary artery stenosis

Han

Liu

Sun

et al. 2020

Computer Methods and Programs in Biomedicine

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Identification of essential hypertension biomarkers in human urine by non-targeted metabolomics based on UPLC-Q-TOF/MS

Zhao

Liu

Zhu

et al. 2018

Clinica Chimica Acta

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Tetrandrine exerts antidepressant-like effects in animal models: Role of brain-derived neurotrophic factor

Gao

Cui

et al. 2013

Behavioural Brain Research

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Chunquan Yu

Trends in Risk Profiles for and Mortality Associated with Invasive Aspergillosis among Liver Transplant Recipients

Opportunistic Mycelial Fungal Infections in Organ Transplant Recipients: Emerging Importance of Non-Aspergillus Mycelial Fungi

Deep learning analysis in coronary computed tomographic angiography imaging for the assessment of patients with coronary artery stenosis

Identification of essential hypertension biomarkers in human urine by non-targeted metabolomics based on UPLC-Q-TOF/MS

Tetrandrine exerts antidepressant-like effects in animal models: Role of brain-derived neurotrophic factor

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