2,621 research outputs found

    Nitrate Leaching in Irrigated Corn and Soybean in a Semi-Arid Climate

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    Nitrate-nitrogen leached from the root zone of land in intensive corn production is a major groundwater contaminant in some of the intensively irrigated regions of the western Cornbelt, including central and western Nebraska. To obtain a clearer understanding of the amount and timing of nitrate leaching losses from irrigated crops, 14 monolithic percolation lysimeters were installed in 1989-1990 in sprinkler irrigated plots at the University of Nebraskaโ€™s West Central Research and Extension Center near North Platte, Nebraska. The lysimeters were used to provide a direct measure of leachate depth from continuous corn and a corn-soybean rotation. Both cropping systems were sprinkler irrigated and used current best management practices (BMPs) in the region for water and nitrogen management. Leachate was collected from 1990 through 1998 and analyzed for nitrate-N concentration. Results for the period 1993- 1998 are reported here. In the semi-arid climate of West-Central Nebraska, the interaction of rainfall patterns with the period of active uptake of water by crops played a major role in defining leaching patterns. Careful irrigation scheduling did not eliminate leaching during the growing season. There was no significant difference in drainage depth between continuous corn and the corn-soybean rotation. The average drainage depth among the lysimeters was 218 mm yr-1. This was more than expected, and in part resulted from above normal precipitation during several years of the study. No water quality benefit was found for the corn-soybean rotation as compared to continuous corn. Nitrate-N concentration in the leachate from continuous corn averaged 24 mg L-1, while that from the corn-soybean rotation averaged 42 mg L-1. Total yearly nitrate leaching loss averaged 52 kg ha-1 for continuous corn and 91 kg ha-1 for the rotation. This represents the equivalent of 27% and 105% of the amount of N fertilizer applied over the six years of study. In calculating N fertilizer needs for corn in Nebraska, the recommended legume N credit of 50 kg ha-1 for a preceding crop of soybean may be too low under irrigated production

    Recruitment of latent pools of high-avidity CD8+ T cells to the antitumor immune response

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    A major barrier to successful antitumor vaccination is tolerance of high-avidity T cells specific to tumor antigens. In keeping with this notion, HER-2/neu (neu)-targeted vaccines, which raise strong CD8+ T cell responses to a dominant peptide (RNEU420-429) in WT FVB/N mice and protect them from a neu-expressing tumor challenge, fail to do so in MMTV-neu (neu-N) transgenic mice. However, treatment of neu-N mice with vaccine and cyclophosphamide-containing chemotherapy resulted in tumor protection in a proportion of mice. This effect was specifically abrogated by the transfer of neu-Nโ€“derived CD4+CD25+ T cells. RNEU420-429-specific CD8+ T cells were identified only in neu-N mice given vaccine and cyclophosphamide chemotherapy which rejected tumor challenge. Tetramer-binding studies demonstrated that cyclophosphamide pretreatment allowed the activation of high-avidity RNEU420-429-specific CD8+ T cells comparable to those generated from vaccinated FVB/N mice. Cyclophosphamide seemed to inhibit regulatory T (T reg) cells by selectively depleting the cycling population of CD4+CD25+ T cells in neu-N mice. These findings demonstrate that neu-N mice possess latent pools of high-avidity neu-specific CD8+ T cells that can be recruited to produce an effective antitumor response if T reg cells are blocked or removed by using approaches such as administration of cyclophosphamide before vaccination

    Book Reviews

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    Reviews of the following books: The Long Argument: English Puritanism and the Shaping of New England Culture, 1570-1700 by Stephen Foster; The Salem Witch Crisis by Larry Gragg; A Home for Everyman: The Greek Revival and Maine Domestic Architecture by Joyce K. Bibber; The Gunpowder Mills of Maine by Maurice W. Hitten; In the Hands of Providence: Joshua L. Chamberlain And The American Civil War by Alice Rains Trulock; Hurricane Island: The Town That Disappeared by Eleanor Motley Richardson; Home Front On Penobscot Bay: Rockland During The War Years, 1940-1945by Paul G. Merriam, Thomas J. Molloy, and Theodore W. Sylvester, Jr.; The History of Broadcasting in Maine: The First Fifty Yearsby Ellie Thompson; New Compass Points by Roy P. Fairfiel

    Efficacy of Carraguardยฎ-Based Microbicides In Vivo Despite Variable In Vitro Activity

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    Anti-HIV microbicides are being investigated in clinical trials and understanding how promising strategies work, coincident with demonstrating efficacy in vivo, is central to advancing new generation microbicides. We evaluated Carraguardยฎ and a new generation Carraguard-based formulation containing the non-nucleoside reverse transcriptase inhibitor (NNRTI) MIV-150 (PC-817). Since dendritic cells (DCs) are believed to be important in HIV transmission, the formulations were tested for the ability to limit DC-driven infection in vitro versus vaginal infection of macaques with RT-SHIV (SIVmac239 bearing HIV reverse transcriptase). Carraguard showed limited activity against cell-free and mature DC-driven RT-SHIV infections and, surprisingly, low doses of Carraguard enhanced infection. However, nanomolar amounts of MIV-150 overcame enhancement and blocked DC-transmitted infection. In contrast, Carraguard impeded infection of immature DCs coincident with DC maturation. Despite this variable activity in vitro, Carraguard and PC-817 prevented vaginal transmission of RT-SHIV when applied 30 min prior to challenge. PC-817 appeared no more effective than Carraguard in vivo, due to the limited activity of a single dose of MIV-150 and the dominant barrier effect of Carraguard. However, 3 doses of MIV-150 in placebo gel at and around challenge limited vaginal infection, demonstrating the potential activity of a topically applied NNRTI. These data demonstrate discordant observations when comparing in vitro and in vivo efficacy of Carraguard-based microbicides, highlighting the difficulties in testing putative anti-viral strategies in vitro to predict in vivo activity. This work also underscores the potential of Carraguard-based formulations for the delivery of anti-viral drugs to prevent vaginal HIV infection

    The transcriptional profile of coronary arteritis in Kawasaki disease

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    BackgroundKawasaki Disease (KD) can cause potentially life-threatening coronary arteritis in young children, and has a likely infectious etiology. Transcriptome profiling is a powerful approach to investigate gene expression in diseased tissues. RNA sequencing of KD coronary arteries could elucidate the etiology and the host response, with the potential to improve KD diagnosis and/or treatment.MethodsDeep RNA sequencing was performed on KD (nโ€‰=โ€‰8) and childhood control (nโ€‰=โ€‰7) coronary artery tissues, revealing 1074 differentially expressed mRNAs. Non-human RNA sequences were subjected to a microbial discovery bioinformatics platform, and microbial sequences were analyzed by Metastats for association with KD.ResultsT lymphocyte activation, antigen presentation, immunoglobulin production, and type I interferon response were significantly upregulated in KD arteritis, while the tumor necrosis factor ฮฑ pathway was not differentially expressed. Transcripts from known infectious agents were not specifically associated with KD coronary arteritis.ConclusionsThe immune transcriptional profile in KD coronary artery tissues has features of an antiviral immune response such as activated cytotoxic T lymphocyte and type I interferon-induced gene upregulation. These results provide new insights into the pathogenesis of KD arteritis that can guide selection of new immunomodulatory therapies for high-risk KD patients, and provide direction for future etiologic studies

    Changing Preferences for Survival After Hospitalization With Advanced Heart Failure

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    ObjectivesThis study was designed to analyze how patient preferences for survival versus quality-of-life change after hospitalization with advanced heart failure (HF).BackgroundAlthough patient-centered care is a priority, little is known about preferences to trade length of life for quality among hospitalized patients with advanced HF, and it is not known how those preferences change after hospitalization.MethodsThe time trade-off utility, symptom scores, and 6-min walk distance were measured in 287 patients in the ESCAPE (Evaluation Study of Congestive Heart Failure and Pulmonary Artery Catheter Effectiveness) trial at hospitalization and again during 6 months after therapy to relieve congestion.ResultsWillingness to trade was bimodal. At baseline, the median trade for better quality was 3 months' survival time, with a modest relation to symptom severity. Preference for survival time was stable for most patients, but increase after discharge occurred in 98 of 145 (68%) patients initially willing to trade survival time, and was more common with symptom improvement and after therapy guided by pulmonary artery catheters (p = 0.034). Adjusting days alive after hospital discharge for patients' survival preference reduced overall days by 24%, with the largest reduction among patients dying early after discharge (p = 0.0015).ConclusionsPreferences remain in favor of survival for many patients despite advanced HF symptoms, but increase further after hospitalization. The bimodal distribution and the stability of patient preference limit utility as a trial end point, but support its relevance in design of care for an individual patient

    Challenges facing early career academic cardiologists

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    Early career academic cardiologists currently face unprecedented challenges that threaten a highly valued career path. A team consisting of early career professionals and senior leadership members of American College of Cardiology completed this white paper to inform the cardiovascular medicine profession regarding the plight of early career cardiologists and to suggest possible solutions. This paper includes: 1) definition of categories of early career academic cardiologists; 2) general challenges to all categories and specific challenges to each category; 3) obstacles as identified by a survey of current early career members of the American College of Cardiology; 4) major reasons for the failure of physician-scientists to receive funding from National Institute of Health/National Heart Lung and Blood Institute career development grants; 5) potential solutions; and 6) a call to action with specific recommendations
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