A ternary-blend strategy is presented to surmount the shortcomings of both fullerene derivatives and nonfullerene small molecules as acceptors for the first time. The optimal ternary device shows a high power conversion efficiency (PCE) of 10.4%. Moreover, a significant enhancement in PCE (≈35%) relative to both of the binary reference devices, which has never been achieved before in high-efficiency ternary devices, is demonstrated.
Due to the attraction of optimizing the electronic structure beyond chemical synthesis, molecular doping has recently aroused wide interest in the field of organic solar cells. However, the selection of limited dopants confines its successful application. Inspired by the Lewis base characteristics of the photovoltaic materials, the Lewis acid as novel dopant is introduced in organic solar cells. In both fullerene and nonfullerene based blends, Lewis acid doping leads to increased photovoltaic performance. Detailed experiments reveal that Lewis acid doping has a synergistic effect on modifying the polymer's electronic properties and the acceptor's nanostructure even at low doping concentration, and these are simultaneously responsible for the device improvements. Based on the mechanism studies, it is proposed that the Lewis acid‐doped polymers anions produce induced dipole on the acceptor, this increases the intermolecular interaction and facilitates the morphology optimization. It is believed that the synergistic effect by Lewis acid doping greatly expands the application of doped organic solar cells, in concert with other existing methods to yield higher efficiency values.
A planar DPP-based polymer containing three regular alternating units exhibits a good photovoltaic performance with a high PCE of 9.02% and a large Voc of 0.86 V.
The power conversion efficiency of polymer solar cells (PSCs) is strongly affected by active layer morphology. Here, two solvent additives (ODT: octance‐1,8‐dithiol; DIO: 1,8‐diiodooctane) are used to optimize the bulk heterojunction morphology of FTAZ:ITIC‐Th based PSCs and ≈11% efficiency is obtained, which is 10% higher than the untreated device. Based on the morphological characterizations, the influence of binary solvent additives on manipulating molecular packing and phase separation of blend films is successfully revealed. More importantly, in situ grazing incidence wide‐angle X‐ray scattering characterization is adopted to explore the crucial role played by these two solvent additives at different stages of the film‐forming process, that is, ODT influences the initial stage of the film‐forming process, while DIO later establishes the ultimate photoactive film formation. Due to the impacts of two additives at different film processing stages, an optimal ratio of ODT:DIO (0.375%:0.125%) is obtained, which helps in realizing the optimized morphology.
Background/Aims: Matrix metalloproteinase 9 (MMP9), a potent endopeptidase degrading extracellular matrix, plays a pivotal role in the pathogenesis of ischaemic stroke (IS). The present study was undertaken to determine the association of MMP9 gene polymorphisms and the risk of IS in a southern Chinese population. Methods: A cohort of 1274 patients and 1258 age-matched healthy controls were genotyped to detect the four MMP9 polymorphisms (rs17156, rs3787268, rs3918241 and rs3918242) using SNaPshot. Results: Our study demonstrated a significant difference in the genotype and allele frequencies of the MMP9 rs3918242 polymorphism between the IS patients and the controls (P = 0.012 for the genotype and P = 0.0092 for the allele). Stratification by smoking status showed statistically significant differences in the frequency and allele of the rs3918242 polymorphism between IS patients and the controls (P = 0.0052 for the genotype and P = 0.0019 for the allele). Further stratification by IS subtypes revealed that the presence of the T allele of the MMP9 rs3918242 polymorphism confers a higher risk of the large artery atherosclerosis subtype of IS (P = 0.017). Moreover, IS patients with the rs3918242 T allele of MMP9 presented with increased serum MMP9 production, and this increase was more significant in smokers with IS (P = 0.022). Patients carrying the variant T allele of the MMP9 rs3918242 polymorphism exhibited significantly higher infarct volumes than those with the major CC genotype (P = 0.036). Conclusion: Our study provides preliminary evidence that the MMP9 rs3918242 polymorphism is linked to a higher risk of IS, confirming the role of MMP9 in the pathophysiology of IS, with potentially important therapeutic implications.
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