1,825 research outputs found
Airline Horizontal Mergers and Productivity: Empirical Evidence from a Natural Experiment in China
The identification of possible efficiency gains is a core issue in the analysis of mergers. However, empirical studies are generally subject to bias caused by merger endogeneity. In the early 2000s, the Chinese government pursued a strategy of merging small firms in key industries to create large enterprise groups. Mergers created by this policy provide a rare natural experiment to investigate the effect of mergers. We take the opportunity to apply the difference-in-differences approach to identify the effect of mergers on the efficiency of Chinese airlines. Overall, our analysis suggests that the mergers increased the productivity of Chinese airlines
Insights into high temperature pretreatment on cellulase processing of bamboo
Bamboo processing was performed with commercial cellulase. The properties of cellulase and the effect of high temperature pretreatment on cellulase hydrolysis of bamboo were investigated. Results indicated that cellulase hydrolysis performed fast and dramatically within 30 minutes, and then gradually reached its balance. It was found that pretreatment played an active role in cellulase processing, which enhanced the saccharification of bamboo and benefited high-molecular-weight lignin degradation and removal. Additionally, a better performance of bamboo processing was achieved under the cellulase concentration of 15IU in total reaction system of 100 ml at 50°C, pH 4.8, together with the high temperature pretreatment of 120°C for 15 minutes
Spin Fluctuation Induced Linear Magnetoresistance in Ultrathin Superconducting FeSe Films
The discovery of high-temperature superconductivity in FeSe/STO has trigged
great research interest to reveal a range of exotic physical phenomena in this
novel material. Here we present a temperature dependent magnetotransport
measurement for ultrathin FeSe/STO films with different thickness and
protection layers. Remarkably, a surprising linear magnetoresistance (LMR) is
observed around the superconducting transition temperatures but absent
otherwise. The experimental LMR can be reproduced by magnetotransport
calculations based on a model of magnetic field dependent disorder induced by
spin fluctuation. Thus, the observed LMR in coexistence with superconductivity
provides the first magnetotransport signature for spin fluctuation around the
superconducting transition region in ultrathin FeSe/STO films
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Strict Major Histocompatibility Complex Molecule Class-Specific Binding by Co-Receptors Enforces MHC-Restricted αβ TCR Recognition during T Lineage Subset Commitment
Since the discovery of co-receptor dependent αβTCR recognition, considerable effort has been spent on elucidating the basis of CD4 and CD8 lineage commitment in the thymus. The latter is responsible for generating mature CD4 helper and CD8αβ cytotoxic T cell subsets. Although CD4+ and CD8+ T cell recognition of peptide antigens is known to be MHC class II- and MHC class I-restricted, respectively, the mechanism of single positive (SP) thymocyte lineage commitment from bipotential double-positive (DP) progenitors is not fully elucidated. Classical models to explain thymic CD4 vs. CD8 fate determination have included a stochastic selection model or instructional models. The latter are based either on strength of signal or duration of signal impacting fate. More recently, differential co-receptor gene imprinting has been shown to be involved in expression of transcription factors impacting cytotoxic T cell development. Here, we address commitment from a structural perspective, focusing on the nature of co-receptor binding to MHC molecules. By surveying 58 MHC class II and 224 MHC class I crystal structures in the Protein Data Bank, it becomes clear that CD4 cannot bind to MHC I molecules, nor can CD8αβ or CD8αα bind to MHC II molecules. Given that the co-receptor delivers Lck to phosphorylate exposed CD3 ITAMs within a peptide/MHC (pMHC)-ligated TCR complex to initiate cell signaling, this strict co-receptor recognition fosters MHC class-restricted SP thymocyte lineage commitment at the DP stage even though both co-receptors are expressed on a single cell. In short, the binding preference of an αβTCR for a peptide complexed with an MHC molecule dictates which co-receptor subsequently binds, thereby supporting development of that subset lineage. How function within the lineage is linked further to biopotential fate determination is discussed
Association of Maternal Body Mass Index With Risk of Infant Mortality: A Dose-Response Meta-Analysis
Objective: This study presumed that a high or low bodymass index (BMI)might increase
the risk of infant mortality. Therefore, a meta-analysis was performed to systematically
assess the association between maternal BMI and the risk of infant mortality.
Methods: The electronic databases, including Pubmed, Embase database, and
Cochrane Library, were systemically searched by two investigators from inception
to November 26th, 2020, with no language restriction. In parallel, a dose-response
was assessed.
Results: Finally, 22 cohort studies involving 13,532,293 participants were included
into this paper, which showed that compared with normal BMI, maternal overweight
significantly increased the risks of infant mortality [risk ratio (RR), 1.16; 95% confidence
interval (CI), 1.13–1.19], neonatal mortality (RR, 1.23; 95% CI, 1.08–1.39), early neonatal
mortality (RR, 1.55; 95% CI, 1.26–1.92) and post-neonatal mortality (RR, 1.18; 95% CI,
1.07–1.29). Similarly, maternal obesity significantly increased the risk of infant mortality
(RR, 1.55; 95% CI, 1.41–1.70), neonatal mortality (RR, 1.55; 95% CI, 1.28–1.67), early
neonatal mortality (RR, 1.37; 95% CI, 1.13–1.67), and post-neonatal mortality (RR, 1.30;
95% CI, 1.03–1.65), whereas maternal underweight potentially decreased the risk of
infant mortality (RR, 0.93; 95% CI, 0.88–0.98). In the dose-response analysis, the risk of
infant mortality significantly increased when the maternal BMI was >25 kg/m2.
Conclusions: Maternal overweight or obesity significantly increases the risks of
infant mortality, neonatal mortality, early neonatal mortality, and post-neonatal mortality
compared with normal BMI in a dose-dependentmanner. Besides,maternal underweight
will not increase the risk of infant mortality, neonatal mortality, early neonatal mortality, or
postneonatal mortality; instead, it tends to decrease the risk of infant mortality. Early
weight management may provide potential benefits to infants, and more large-scale
prospective studies are needed to verify this finding in the future
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