Assembly and melting of DNA nanotubes from single-sequence tiles

2008 ◽  
Vol 21 (3) ◽  
pp. 034112 ◽  
Author(s):  
T L Sobey ◽  
S Renner ◽  
F C Simmel
Author(s):  
Chris Köcher

AbstractWe study the reachability problem for queue automata and lossy queue automata. Concretely, we consider the set of queue contents which are forwards resp. backwards reachable from a given set of queue contents. Here, we prove the preservation of regularity if the queue automaton loops through some special sets of transformation sequences. This is a generalization of the results by Boigelot et al. and Abdulla et al. regarding queue automata looping through a single sequence of transformations. We also prove that our construction is possible in polynomial time.


Nanomaterials ◽  
2021 ◽  
Vol 11 (8) ◽  
pp. 2003
Author(s):  
Samet Kocabey ◽  
Aslihan Ekim Kocabey ◽  
Roger Schneiter ◽  
Curzio Rüegg

DNA nanotechnology offers to build nanoscale structures with defined chemistries to precisely position biomolecules or drugs for selective cell targeting and drug delivery. Owing to the negatively charged nature of DNA, for delivery purposes, DNA is frequently conjugated with hydrophobic moieties, positively charged polymers/peptides and cell surface receptor-recognizing molecules or antibodies. Here, we designed and assembled cholesterol-modified DNA nanotubes to interact with cancer cells and conjugated them with cytochrome c to induce cancer cell apoptosis. By flow cytometry and confocal microscopy, we observed that DNA nanotubes efficiently bound to the plasma membrane as a function of the number of conjugated cholesterol moieties. The complex was taken up by the cells and localized to the endosomal compartment. Cholesterol-modified DNA nanotubes, but not unmodified ones, increased membrane permeability, caspase activation and cell death. Irreversible inhibition of caspase activity with a caspase inhibitor, however, only partially prevented cell death. Cytochrome c-conjugated DNA nanotubes were also efficiently taken up but did not increase the rate of cell death. These results demonstrate that cholesterol-modified DNA nanotubes induce cancer cell death associated with increased cell membrane permeability and are only partially dependent on caspase activity, consistent with a combined form of apoptotic and necrotic cell death. DNA nanotubes may be further developed as primary cytotoxic agents, or drug delivery vehicles, through cholesterol-mediated cellular membrane interactions and uptake.


2019 ◽  
Vol 626 ◽  
pp. A16 ◽  
Author(s):  
A. Rojas-Arriagada ◽  
M. Zoccali ◽  
M. Schultheis ◽  
A. Recio-Blanco ◽  
G. Zasowski ◽  
...  

Context. The Galactic bulge has a bimodal metallicity distribution function: different kinematic, spatial, and, potentially, age distributions characterize the metal-poor and metal-rich components. Despite this observed dichotomy, which argues for different formation channels for those stars, the distribution of bulge stars in the α-abundance versus metallicity plane has been found so far to be a rather smooth single sequence. Aims. We use data from the fourteenth data release of the APOGEE spectroscopic survey (DR14) to investigate the distribution in the Mg abundance (as tracer of the α-elements)-versus-metallicity plane of a sample of stars selected to be in the inner region of the bulge. Methods. A clean sample has been selected from the DR14 using a set of data- and pipeline-flags to ensure the quality of their fundamental parameters and elemental abundances. An additional selection made use of computed spectro-photometric distances to select a sample of likely bulge stars as those with RGC ≤ 3.5 kpc. We adopt magnesium abundance as an α-abundance proxy for our clean sample as it has been proven to be the most accurate α-element as determined by ASPCAP, the pipeline for data products from APOGEE spectra. Results. From the distribution of our bulge sample in the [Mg/Fe]-versus-[Fe/H] plane, we found that the sequence is bimodal. This bimodality is given by the presence of a low-Mg sequence of stars parallel to the main high-Mg sequence over a range of ∼0.5 dex around solar metallicity. The two sequences merge above [Fe/H] ∼ 0.15 dex into a single sequence whose dispersion in [Mg/Fe] is larger than either of the two sequences visible at lower metallicity. This result is confirmed when we consider stars in our sample that are inside the bulge region according to trustworthy Gaia DR2 distances.


ACS Nano ◽  
2016 ◽  
Vol 10 (8) ◽  
pp. 7780-7791 ◽  
Author(s):  
Himanshu Joshi ◽  
Atul Kaushik ◽  
Nadrian C. Seeman ◽  
Prabal K. Maiti

1998 ◽  
Vol 41 (5) ◽  
pp. 1052-1060 ◽  
Author(s):  
Peter J. Fitzgibbons ◽  
Sandra Gordon-Salant

This investigation examined the abilities of younger and older listeners to discriminate and identify temporal order of sounds presented in tonal sequences. It was hypothesized that older listeners would exhibit greater difficulty than younger listeners on both temporal processing tasks, particularly for complex stimulus patterns. It was also anticipated that tone order discrimination would be easier than tone order identification for all listeners. Listeners were younger and older adults with either normal hearing or mild-to-moderate sensorineural hearing losses. Stimuli were temporally contiguous three-tone sequences within a 1/3 octave frequency range centered at 4000 Hz. For the discrimination task, listeners discerned differences between standard and comparison stimulus sequences that varied in tonal temporal order. For the identification task, listeners identified tone order of a single sequence using labels of relative pitch. Older listeners performed more poorly than younger listeners on the discrimination task for the more complex pitch patterns and on the identification task for faster stimulus presentation rates. The results also showed that order discrimination is easier than order identification for all listeners. The effects of hearing loss on the ordering tasks were minimal.


2013 ◽  
Vol 135 (7) ◽  
pp. 2864-2864 ◽  
Author(s):  
Paul W. K. Rothemund ◽  
Axel Ekani-Nkodo ◽  
Nick Papadakis ◽  
Ashish Kumar ◽  
Deborah Kuchnir Fygenson ◽  
...  
Keyword(s):  

2014 ◽  
Vol 998-999 ◽  
pp. 1532-1535
Author(s):  
Yu Ming Zhao

The optimal scheduling of crude-oil operation in refineries has been studied by various groups during the past decade leading to different mixed integer linear programming or mixed nonlinear programming formulations. This paper presents a new formulation with oil residency time constraint based on single-operation sequencing (SOS). It is different from previous formulations as it considers oil residency time constraint and pipeline transfer and does not require to postulate the number of priority-slots in which operations take place. This model is also based on the representation of a crude-oil scheduling by a single sequence of transfer operations. A simple MILP procedure has been used to solve this model leading to an satisfactory optimal result.


Genetics ◽  
2000 ◽  
Vol 154 (2) ◽  
pp. 869-884 ◽  
Author(s):  
Tim Langdon ◽  
Charlotte Seago ◽  
R Neil Jones ◽  
Helen Ougham ◽  
Howard Thomas ◽  
...  

Abstract The most distinctive region of the rye B chromosome is a subtelomeric domain that contains an exceptional concentration of B-chromosome-specific sequences. At metaphase this domain appears to be the physical counterpart of the subtelomeric heterochromatic regions present on standard rye chromosomes, but its conformation at interphase is less condensed. In this report we show that the two sequence families that have been previously found to make up the bulk of the domain have been assembled from fragments of a variety of sequence elements, giving rise to their ostensibly foreign origin. A single mechanism, probably based on synthesis-dependent strand annealing (SDSA), is responsible for their assembly. We provide evidence for sequential evolution of one family on the B chromosome itself. The extent of these rearrangements and the complexity of the higher-order organization of the B-chromosome-specific families indicate that instability is a property of the domain itself, rather than of any single sequence. Indirect evidence suggests that particular fragments may have been selected to confer different properties on the domain and that rearrangements are frequently selected for their effect on DNA structure. The current organization appears to represent a transient stage in the evolution of a conventional heterochromatic region from complex sequences.


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