RESUMO
Mechanoluminescent (ML) materials can directly convert external mechanical stimulation into light without the need for excitation from other forms of energy, such as light or electricity. This alluring characteristic makes ML materials potentially applicable in a wide range of areas, including dynamic imaging of force, advanced displays, information code, storage, and anti-counterfeiting encryption. However, current reproducible ML materials are restricted to sulfide- and oxide-based materials. In addition, most of the reported ML materials require pre-irradiation with ultraviolet (UV) lamps or other light sources, which seriously hinders their practical applications. Here, we report a novel ML material, MgF2:Mn2+, which emits bright red light under an external dynamic force without the need for pre-charging with UV light. The luminescence properties were systematically studied, and the piezophotonic application was demonstrated. More interestingly, unlike the well-known zinc sulfide ML complexes reported previously, a highly transparent ML film was successfully fabricated by incorporating MgF2:Mn2+ into polydimethylsiloxane (PDMS) matrices. This film is expected to find applications in advanced flexible optoelectronics such as integrated piezophotonics, artificial skin, athletic analytics in sports science, among others.
Assuntos
Luz , Luminescência , Raios Ultravioleta , IluminaçãoRESUMO
The microalgae Haematococcus pluvialis attracts attention for its ability to accumulate astaxanthin up to its 4% dry weight under stress conditions, such as high light, salt stress, and nitrogen starvation. Previous researches indicated that the regulation of astaxanthin synthesis might happen at the transcriptional level. However, the transcription regulatory mechanism of astaxanthin synthesis is still unknown in H. pluvialis. Lacking studies on transcription factors (TFs) further hindered from discovering this mechanism. Hence, the transcriptome analysis of H. pluvialis under the high light-sodium acetate stress for 1.5 h was performed in this study, aiming to discover TFs and the regulation on astaxanthin synthesis. In total, 83,869 unigenes were obtained and annotated based on seven databases, including NR, NT, Kyoto Encyclopedia of Genes and Genomes Orthology, SwissProt, Pfam, Eukaryotic Orthologous Groups, and Gene Ontology. Moreover, 476 TFs belonging to 52 families were annotated by blasting against the PlantTFDB database. By comparing with the control group, 4,367 differentially expressed genes composing of 2,050 upregulated unigenes and 2,317 downregulated unigenes were identified. Most of them were involved in metabolic process, catalytic activity, single-organism process, single-organism cellular process, and single-organism metabolic process. Among them, 28 upregulated TFs and 41 downregulated TFs belonging to 27 TF families were found. The transcription analysis showed that TFs had different transcription modules responding to the high light and sodium acetate stress. Interestingly, six TFs belonging to MYB, MYB_related, NF-YC, Nin-like, and C3H families were found to be involved in the transcription regulation of 27 astaxanthin synthesis-related genes according to the regulatory network. Moreover, these TFs might affect astaxanthin synthesis by directly regulating CrtO, showing that CrtO was the hub gene in astaxanthin synthesis. The present study provided new insight into a global view of TFs and their correlations to astaxanthin synthesis in H. pluvialis.
RESUMO
Chest X-ray is a "golden standard" for the diagnosis and severity assessment of community-acquired pneumonia (CAP). However, it cannot be used as routine examination of CAP in children. The present study aims to investigate the roles of prealbumin (PA) in CAP in children and further determine the usefulness of PA in diagnosis and severity assessment of CAP in children.This was a retrospective analysis of 174 cases of hospitalized children with CAP. The following indicators were recorded: vital sign, inflammatory indexes, PA, and respiratory pathogens immunoglobulin M antibody test results. A total of 33 healthy children were selected as the control group. The results of laboratory tests between CAP and control groups were compared. CAP group was further divided into mild CAP and severe CAP groups, and vital signs and laboratory examination results of 2 groups were compared.The total positive rate of Mycoplasma pneumoniae in this study was 27.4%, and there was no significant difference in different seasons (Pâ=â0.356). Compared with controls, there was no significant difference between procalcitonin and C-reactive protein in CAP group (Pâ=â0.355, 0.061). The white blood cell count, percentage of neutrophils, neutrophil count, and erythrocyte sedimentation rate in the CAP group were significantly higher than those in control group, and PA was significantly lower than that in the control group (all Pâ<â0.05). In the traditional cutoff value (<170âmg/L), the sensitivity of PA for the diagnosis of CAP was 0.847, which was significant higher than traditional inflammatory indicators. Moreover, it was found that PA was an independent protective factor for CAP in children based on multivariate analysis (odds ratio: 0.974; 95% confidence interval: 0.956-0.993; Pâ=â0.008). PA level in severe CAP group was significantly lower than in mild CAP group (Pâ=â0.001). With a cutoff value of 125âmg/L, the sensitivity and specificity of PA for the severity assessment of CAP were 0.703 and 0.714, respectively.Combined with traditional inflammatory markers, PA may improve the diagnostic efficacy of CAP in children. PA can be used as a reference marker to complement the chest X-rays for severity assessment of children CAP.
