Methods, apparatuses, and systems are provided for using laser ablation to manufacture nanoparticles. An example method includes steps of generating, by a laser beam generator, a laser beam, splitting, by a set of beam splitters, the laser beam into a plurality of derivative laser beams, and directing each derivative laser beam towards a plurality of targets. In this example method, the plurality of targets are submerged in corresponding synthesis solvents within corresponding synthesis chambers. Moreover, interaction of each derivative laser beam with its corresponding target releases nanoparticles into the corresponding synthesis solvent to create a nanoparticle solution including both the corresponding synthesis solvent and the released nanoparticles.

An apparatus and method for performing analysis and identification of molecules have been presented. In one embodiment, a portable molecule analyzer includes a sample input/output connection to receive a sample, a nanopore-based sequencing chip to perform analysis on the sample substantially in real-time, and an output interface to output result of the analysis.

An apparatus and method for performing analysis and identification of molecules have been presented. In one embodiment, a portable molecule analyzer includes a sample input/output connection to receive a sample, a nanopore-based sequencing chip to perform analysis on the sample substantially in real-time, and an output interface to output result of the analysis.

Compositions, devices, methods and systems are provided for differential functionalization of a surface of a structure to support biopolymer synthesis. Provided herein are processes which include use of lamps, lasers, and/or microcontact printing to add functional groups to surfaces for the efficient and uniform synthesis of oligonucleic acids.

An apparatus and method for performing analysis and identification of molecules have been presented. In one embodiment, a portable molecule analyzer includes a sample input/output connection to receive a sample, a nanopore-based sequencing chip to perform analysis on the sample substantially in real-time, and an output interface to output result of the analysis.

A high-throughput combinatorial materials experimental apparatus for in-situ synthesis and real-time characterization includes a composition spread device to prepare continuous or discrete composition distribution as precursor of the high-throughput experimental samples library, a low temperature diffusion mixing device to thoroughly mix the composition spread in the thickness direction through diffusion at a relatively low temperature to form an amorphous precursor, and an integrated synthesis-characterization unit for heat treatment of the material library precursor in either a parallel or point-by-point scanning mode at different thermodynamic conditions for phase formation and to characterize features or properties of the materials of interest in an in-situ and real-time manner. The integrated synthesis-characterization unit includes a chamber maintained at desired vacuum and atmosphere, a micro-heating source, an excitation source, a signal collector, and a sample holder.

Compositions, devices, methods and systems are provided for differential functionalization of a surface of a structure to support biopolymer synthesis. Provided herein are processes which include use of lamps, lasers, and/or microcontact printing to add functional groups to surfaces for the efficient and uniform synthesis of oligonucleic acids.

Provided is a method of isolating biochemical molecules on a microarray substrate, the method including providing a microarray substrate to which clusters of different kinds of biochemical molecules being classified by individual spot units are attached, the individual spots being regularly arranged thereon; obtaining location information of the individual spot in which a desired cluster among clusters of the biochemical molecules locates; locating an extraction tool for applying energy to isolate the desired cluster according to the location information; and isolating the desired cluster from the microarray substrate by applying energy in a contact or non-contact manner using the extraction tool.

Methods, apparatuses, and systems are provided for using laser ablation to manufacture nanoparticles. An example method includes steps of generating, by a laser beam generator, a laser beam, splitting, by a set of beam splitters, the laser beam into a plurality of derivative laser beams, and directing each derivative laser beam towards a plurality of targets. In this example method, the plurality of targets are submerged in corresponding synthesis solvents within corresponding synthesis chambers. Moreover, interaction of each derivative laser beam with its corresponding target releases nanoparticles into the corresponding synthesis solvent to create a nanoparticle solution including both the corresponding synthesis solvent and the released nanoparticles.

A method for producing a nucleic acid array which includes (a) a step of forming a layer (a PAG layer) made of a resin composition containing a photoacid generator (PAG) for generating an acid as a result of being exposed to light on a solid phase which has a molecule immobilized thereon and having a functional group protected by an acid-decomposable protective group; (b) a step of exposing a desired position of the PAG layer to light; (c) a step of removing the PAG layer which has been exposed to light; and (d) a step of bringing the solid phase from which the PAG layer has been removed into contact with a nucleotide derivative having an acid-decomposable protective group is provided.