DNA-Directed Artificial Light-Harvesting Antenna

Dutta, Prasun; Varghese, Reji; Nangreave, Jeanette; Lin, Su; Yan, Hao; Liu, Yan

doi:10.1021/ja1115138

Cited by 268 publications

(262 citation statements)

References 85 publications

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“…Similarly, the method for crystal replication we have demonstrated could also be applied to the discovery of functional materials: DNA crystals can serve as templates for proteins, small molecules, and nanoparticles (42), allowing the use of this system for the exploration via directed evolution of photonic or plasmonic nanostructures (43,44) or of how the specific nanoscale arrangements of proteins gives rise to specific biological function (45). And while DNA crystals are more complex than most natural crystals, crystal growth processes and strong mechanical forces are varied and ubiquitous, suggesting the plausibility of a natural crystal growth process and environment that together support crystal information replication.…”

Section: Discussionmentioning

confidence: 99%

Robust self-replication of combinatorial information via crystal growth and scission

Schulman

Yurke²,

Winfree³

2012

Proc. Natl. Acad. Sci. U.S.A.

118

110

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Understanding how a simple chemical system can accurately replicate combinatorial information, such as a sequence, is an important question for both the study of life in the universe and for the development of evolutionary molecular design techniques. During biological sequence replication, a nucleic acid polymer serves as a template for the enzyme-catalyzed assembly of a complementary sequence. Enzymes then separate the template and complement before the next round of replication. Attempts to understand how replication could occur more simply, such as without enzymes, have largely focused on developing minimal versions of this replication process. Here we describe how a different mechanism, crystal growth and scission, can accurately replicate chemical sequences without enzymes. Crystal growth propagates a sequence of bits while mechanically-induced scission creates new growth fronts. Together, these processes exponentially increase the number of crystal sequences. In the system we describe, sequences are arrangements of DNA tile monomers within ribbon-shaped crystals. 99.98% of bits are copied correctly and 78% of 4-bit sequences are correct after two generations; roughly 40 sequence copies are made per growth front per generation. In principle, this process is accurate enough for 1,000-fold replication of 4-bit sequences with 50% yield, replication of longer sequences, and Darwinian evolution. We thus demonstrate that neither enzymes nor covalent bond formation are required for robust chemical sequence replication. The form of the replicated information is also compatible with the replication and evolution of a wide class of materials with precise nanoscale geometry such as plasmonic nanostructures or heterogeneous protein assemblies.algorithmic self-assembly | DNA nanotechnology | self-assembly I n cells, long genomes are accurately replicated via a complex replication process involving tens or sometimes hundreds of enzymes. Nearer to life's origins, a much simpler system must have been responsible for genome replication; evolution of this information then produced more and more complex forms. How a chemical system could be capable of sustained replication and evolution and yet be simple enough to arise spontaneously is an open question.Enzyme-free autocatalytic systems, which are generally simpler than those with enzymes, are known to exponentially replicate one or a small set of species (1-5), but none of these systems replicate an arrangement of subunits defining a combinatorial sequence of information. Without the capacity for combinatorial information replication, open-ended evolution, in which complexity increases without bound (6), cannot occur. Some RNA sequences have been shown to act as RNA polymerases that can assemble a general RNA sequence given a template (7). If such an RNA sequence polymerized a copy of itself, the required enzyme would be produced by the replication process, making it self-sustaining. However, fidelity sufficient for RNA-mediated RNA self-replication has not yet been observe...

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Section: Discussionmentioning

confidence: 99%

Robust self-replication of combinatorial information via crystal growth and scission

Schulman

Yurke²,

Winfree³

2012

Proc. Natl. Acad. Sci. U.S.A.

118

110

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“…[1][2][3][4][5] In the endeavor to harvest the sun light by mimicking the natural photosynthesis, articial light harvesting systems have been created, in which the excitation energy is channeled from multiple donor molecules to just a few or a single acceptor. [6][7][8][9][10] These articial light harvesting systems have been designed in one, 11 two 12 and three 13 dimensions. Apart from photosynthesis the concept of light harvesting is also exploited for analytical purposes to enhance the uorescence emission of luminescent probes and in this way improve the sensitivity of sensors.…”

Section: Introductionmentioning

confidence: 99%

“…DNA origami structures have been used to create highly sensitive SERS substrates by attaching gold nanoparticle dimers, [23][24][25] to analyze DNA strand breaks induced by low energy electrons 26,27 and UV photons 28 and to arrange different uo-rophores 29,29,30 at precise distances to create nanoscale photonic devices which can be used for example as photonic wires, 15,18 to resolve conformational changes of biomolecules, [31][32][33][34] as logic gates 35,36 and articial light harvesting complexes. 8,10,18 The light harvesting efficiency is in this context typically expressed as an antenna effect (AE), i.e. the intensity of A emission when D is excited compared to the A intensity when it is directly excited.…”

Section: Introductionmentioning

confidence: 99%

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FRET efficiency and antenna effect in multi-color DNA origami-based light harvesting systems

Olejko

Bald

2017

RSC Adv.

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“…Extended DNA nanostructures have shown promise as structural scaffolds that can organize patterned arrays of cargo, with potential in plasmonics 25 , catalysis 26,27 , artificial light harvesting 28 and nanoelectronics 29,30 . These applications require fine control over the placement and order of specific functional groups, which can be challenging at the nanometre scale.…”

Section: Resultsmentioning

confidence: 99%

Sequential growth of long DNA strands with user-defined patterns for nanostructures and scaffolds

2015

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DNA strands of well-defined sequence are valuable in synthetic biology and nanostructure assembly. Drawing inspiration from solid-phase synthesis, here we describe a DNA assembly method that uses time, or order of addition, as a parameter to define structural complexity. DNA building blocks are sequentially added with in-situ ligation, then enzymatic enrichment and isolation. This yields a monodisperse, single-stranded long product (for example, 1,000 bases) with user-defined length and sequence pattern. The building blocks can be repeated with different order of addition, giving different DNA patterns. We organize DNA nanostructures and quantum dots using these backbones. Generally, only a small portion of a DNA structure needs to be addressable, while the rest is purely structural. Scaffolds with specifically placed unique sites in a repeating motif greatly minimize the number of components used, while maintaining addressability. This combination of symmetry and site-specific asymmetry within a DNA strand is easily accomplished with our method.

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DNA-Directed Artificial Light-Harvesting Antenna

Cited by 268 publications

References 85 publications

Robust self-replication of combinatorial information via crystal growth and scission

Robust self-replication of combinatorial information via crystal growth and scission

FRET efficiency and antenna effect in multi-color DNA origami-based light harvesting systems

Sequential growth of long DNA strands with user-defined patterns for nanostructures and scaffolds

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