2,310 research outputs found
Towards real-world complexity: an introduction to multiplex networks
Many real-world complex systems are best modeled by multiplex networks of
interacting network layers. The multiplex network study is one of the newest
and hottest themes in the statistical physics of complex networks. Pioneering
studies have proven that the multiplexity has broad impact on the system's
structure and function. In this Colloquium paper, we present an organized
review of the growing body of current literature on multiplex networks by
categorizing existing studies broadly according to the type of layer coupling
in the problem. Major recent advances in the field are surveyed and some
outstanding open challenges and future perspectives will be proposed.Comment: 20 pages, 10 figure
Functional modulation of AMP-activated protein kinase by cereblon
AbstractMutations in cereblon (CRBN), a substrate binding component of the E3 ubiquitin ligase complex, cause a form of mental retardation in humans. However, the cellular proteins that interact with CRBN remain largely unknown. Here, we report that CRBN directly interacts with the α1 subunit of AMP-activated protein kinase (AMPK α1) and inhibits the activation of AMPK activation. The ectopic expression of CRBN reduces phosphorylation of AMPK α1 and, thus, inhibits the enzyme in a nutrient-independent manner. Moreover, AMPK α1 can be potently activated by suppressing endogenous CRBN using CRBN-specific small hairpin RNAs. Thus, CRBN may act as a negative modulator of the AMPK signaling pathway in vivo
Hydrated copper and gold monovalent cations: Ab initio study
To understand the hydration phenomena of noble transition metals, we investigated the structures, hydration energies, electronic properties, and spectra of the Cu+(H3O)(1-6) and Au+ (H2O)(1-6) clusters using ab initio calculations. The coordination numbers of these clusters are found to be only two, which is highly contrasted to those of Ag+ (H2O)(n) (which have the coordination numbers of 3-4) as well as the hydrated alkali metal ions (which have the coordination numbers of similar to6). For the possible identification of their interesting hydration structures, we predict their IR spectra for the OH stretch modes. (C) 2005 American Institute of Physics.open384
Direction of Arrival Estimation Algorithm: Direction Lock Loop
In this paper, a new direction of arrival (DOA)
estimation algorithm, direction lock loop (DiLL), is proposed.
It has a similar concept to the delay lock loop (DLL) that is
used for synchronization. It estimates the DOA of a signal by
iterations, and can track the DOA of a moving source. The
DiLL scheme is found to track better than the DOA
estimation scheme based on the PASTd, and its performance
is less sensitive to the DOA of a signal than that of the DOA
estimation scheme based on the PASTd. The DOA estimation
accuracy and the tracking capability are demonstrated by
analysis and computer simulations
Comparative lipidomics of 5-Fluorouracil-sensitive and -resistant colorectal cancer cells reveals altered sphingomyelin and ceramide controlled by acid sphingomyelinase (SMPD1).
5-Fluorouracil (5-FU) is a chemotherapeutic drug widely used to treat colorectal cancer. 5-FU is known to gradually lose its efficacy in treating colorectal cancer following the acquisition of resistance. We investigated the mechanism of 5-FU resistance using comprehensive lipidomic approaches. We performed lipidomic analysis on 5-FU-resistant (DLD-1/5-FU) and -sensitive (DLD-1) colorectal cancer cells using MALDI-MS and LC-MRM-MS. In particular, sphingomyelin (SM) species were significantly up-regulated in 5-FU-resistant cells in MALDI-TOF analysis. Further, we quantified sphingolipids including SM and Ceramide (Cer) using Multiple Reaction Monitoring (MRM), as they play a vital role in drug resistance. We found that 5-FU resistance in DLD-1/5-FU colorectal cancer cells was mainly associated with SM increase and Cer decrease, which are controlled by acid sphingomyelinase (SMPD1). In addition, reduction of SMPD1 expression was confirmed by LC-MRM-MS analysis and the effect of SMPD1 in drug resistance was assessed by treating DLD-1 cells with siRNA-SMPD1. Furthermore, clinical colorectal cancer data set analysis showed that down-regulation of SMPD1 was associated with resistance to chemotherapy regimens that include 5-FU. Thus, from our study, we propose that SM/Cer and SMPD1 are new potential target molecules for therapeutic strategies to overcome 5-FU resistance
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