Improved broadband and quasi-omnidirectional anti-reflection properties with biomimetic silicon nanostructures
Nature routinely produces nanostructured surfaces with useful properties, such as the self-cleaning lotus leaf, the colour of the butterfly wing, the photoreceptor in brittlestar and the anti-reflection observed in the moth eye. Scientists and engineers have been able to mimic some of these natural structures in the laboratory and in real-world applications. Here, we report a simple aperiodic array of silicon nanotips on a 6-inch wafer with a sub-wavelength structure that can suppress the reflection of light at a range of wavelengths from the ultraviolet, through the visible part of the spectrum, to the terahertz region. Reflection is suppressed for a wide range of angles of incidence and for both s- and p-polarized light. The antireflection properties of the silicon result from changes in the refractive index caused by variations in the height of the silicon nanotips, and can be simulated with models that have been used to explain the low reflection from moth eyes. The improved anti-reflection properties of the surfaces could have applications in renewable energy and electro-optical devices for the military.
Raman spectroscopy, which is based on the inelastic scattering of photons by chemical entities, has been successfully utilized for the investigation of adsorbed molecules on surfaces, [1][2][3] although the low cross section limits its applications.Surface-enhanced Raman scattering (SERS) has drawn a lot of attention since its discovery in 1974, [4] primarily because it can greatly enhance the normally weak Raman signal and thereby facilitate the convenient identification of the vibrational signatures of molecules in chemical and biological systems. [5] Recently, the observation of single-molecule Raman scattering has further enhanced the Raman detection sensitivity limit and widened the scope of SERS for sensor applications. [6,7] Although SERS effects can be achieved simply by exploiting the electromagnetic resonance properties of roughened surfaces or nanoparticles of Au or Ag, the fabrication of reliable SERS substrates with uniformly high enhancement factors remains the focus of much research. Spraying Au or Ag colloids on a substrate leads to an extremely high SERS signal at some local 'hot-junctions'; [6][7][8] however, it is not easy to achieve a reliable, stable, and uniform SERS signal spanning a wide dynamical range using this method. Van Duyne and coworkers have used nanosphere lithography, [9] while Liu andLee exploited soft lithography, [10] in order to fabricate Ag nanoparticle arrays with high SERS activity and improved uniformity. Käll and co-workers have shown theoretically that the effective Raman cross section of a molecule placed between two metal nanoparticles can be enhanced by more than 12 orders of magnitude.[11] Such enhancement is likely to be related to the 'hot-junctions' observed in some SERS experiments. Several theoretical groups have also investigated field enhancement for SERS from metal nanoparticle arrays. [12][13][14] Specifically, García-Vidal and Pendry proposed that very localized plasmon modes, created by strong electromagnetic coupling between two adjacent metallic objects, dominate the SERS response in an array of nanostructures.[12] The interparticle-coupling-induced enhancement was attributed to the broadening of the plasmon resonance peak because the probability of the resonance covering both the excitation wavelength and the Raman peak increases with its width. They calculated the average enhancement factor over the surfaces of an array of infinitely long Ag nanorods with semicircular cross sections, and showed that significant near-field interaction occurs between adjacent nanorods when the gap between the nanorods reaches half the value of their diameter. Other groups have studied the dependence of the enhancement factor on the gap between adjacent nanoparticles on a SERS active substrate. For example, Gunnarsson et al. investigated SERS on ordered Ag nanoparticle arrays with an interparticle gap above 75 nm. [15] Lee and co-workers were able to achieve the temperature-controlled variation of interparticle gaps between Ag nanoparticles embedded in a polymer membra...
BackgroundThe study of speciation in the marine realm is challenging because of the apparent absence of physical barriers to dispersal, which are one of the main drivers of genetic diversity. Although phylogeographic studies using mitochondrial DNA (mtDNA) information often reveal significant genetic heterogeneity within marine species, the evolutionary significance of such diversity is difficult to interpret with these markers. In the northwestern (NW) Pacific, several studies have emphasised the potential importance of sea-level regression during the most recent glaciations as a driver of genetic diversity in marine species. These studies have failed, however, to determine whether the period of isolation was long enough for divergence to attain speciation. Among these marine species, the cosmopolitan estuarine-dependent fish Mugil cephalus represents an interesting case study. Several divergent allopatric mtDNA lineages have been described in this species worldwide, and three occur in sympatry in the NW Pacific.ResultsTen nuclear microsatellites were surveyed to estimate the level of genetic isolation of these lineages and determine the role of sea-level fluctuation in the evolution of NW Pacific M. cephalus. Three cryptic species of M. cephalus were identified within this region (NWP1, 2 and 3) using an assignment test on the microsatellite data. Each species corresponds with one of the three mtDNA lineages in the COI phylogenetic tree. NWP3 is the most divergent species, with a distribution range that suggests tropical affinities, while NWP1, with a northward distribution from Taiwan to Russia, is a temperate species. NWP2 is distributed along the warm Kuroshio Current. The divergence of NWP1 from NWP2 dates back to the Pleistocene epoch and probably corresponds to the separation of the Japan and China Seas when sea levels dropped. Despite their subsequent range expansion since this period of glaciation, no gene flow was observed among these three lineages, indicating that speciation has been achieved.ConclusionsThis study successfully identified three cryptic species in M. cephalus inhabiting the NW Pacific, using a combination of microsatellites and mitochondrial genetic markers. The current genetic architecture of the M. cephalus species complex in the NW Pacific is the result of a complex interaction of contemporary processes and historical events. Sea level and temperature fluctuations during Plio-Pleistocene epochs probably played a major role in creating the marine species diversity of the NW Pacific that is found today.
BackgroundColibactin is a nonribosomal peptide-polyketide synthesized by multi-enzyme complexes encoded by the pks gene cluster. Colibactin-producing Escherichia coli have been demonstrated to induce host DNA damage and promote colorectal cancer (CRC) development. In Taiwan, the occurrence of pyogenic liver abscess (PLA) has been suggested to correlate with an increasing risk of CRC, and Klebsiella pneumoniae is the predominant PLA pathogen in TaiwanMethodology/Principal FindingsAt the asn tRNA loci of the newly sequenced K. pneumoniae 1084 genome, we identified a 208-kb genomic island, KPHPI208, of which a module identical to the E. coli pks colibactin gene cluster was recognized. KPHPI208 consists of eight modules, including the colibactin module and the modules predicted to be involved in integration, conjugation, yersiniabactin production, microcin production, and unknown functions. Transient infection of BALB/c normal liver cells with K. pneumoniae 1084 increased the phosphorylation of histone H2AX, indicating the induction of host DNA damage. Colibactin was required for the genotoxicity of K. pneumoniae 1084, as it was diminished by deletion of clbA gene and restored to the wild type level by trans-complementation with a clbA coding plasmid. Besides, BALB/c mice infected with K. pneumoniae 1084 exhibited enhanced DNA damage in the liver parenchymal cells when compared to the isogenic clbA deletion mutant. By PCR detection, the prevalence of pks-positive K. pneumoniae in Taiwan is 25.6%, which is higher than that reported in Europe (3.5%), and is significantly correlated with K1 type, which predominantly accounted for PLA in Taiwan.ConclusionsOur knowledge regarding how bacteria contribute to carcinogenesis has just begun. The identification of genotoxic K. pneumoniae and its genetic components will facilitate future studies to elucidate the molecular basis underlying the link between K. pneumoniae, PLA, and CRC.
Candida spp. are part of the natural human microbiota, but they also represent important opportunistic human pathogens. Biofilm-associated Candida albicans infections are clinically relevant due to their high levels of resistance to traditional antifungal agents. In this study, we investigated the ability of linalool to inhibit the formation of C. albicans biofilms and reduce existing C. albicans biofilms. Linalool exhibited antifungal activity against C. albicans ATCC 14053, with a minimum inhibitory concentration (MIC) of 8 mM. Sub-MIC concentrations of linalool also inhibited the formation of germ tubes and biofilms in that strain. The defective architecture composition of C. albicans biofilms exposed to linalool was characterized by scanning electron microscopy. The expression levels of the adhesin genes HWP1 and ALS3 were downregulated by linalool, as assessed by real-time RT-PCR. The expression levels of CYR1 and CPH1, which encode components of the cAMP-PKA and MAPK hyphal formation regulatory pathways, respectively, were also suppressed by linalool, as was the gene encoding their upstream regulator, Ras1. The expression levels of long-term hyphae maintenance associated genes, including UME6, HGC1, and EED1, were all suppressed by linalool. These results indicate that linalool may have therapeutic potential in the treatment of candidiasis associated with medical devices because it interferes with the morphological switch and biofilm formation of C. albicans.
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