Lingxin Chen

Recent advances in molecular imprinting technology: current status, challenges and highlighted applications

Molecular imprinting technology (MIT) concerns formation of selective sites in a polymer matrix with the memory of a template. Recently, molecularly imprinted polymers (MIPs) have aroused extensive attention and been widely applied in many fields, such as solid-phase extraction, chemical sensors and artificial antibodies owing to their desired selectivity, physical robustness, thermal stability, as well as low cost and easy preparation. With the rapid development of MIT as a research hotspot, it faces a number of challenges, involving biological macromolecule imprinting, heterogeneous binding sites, template leakage, incompatibility with aqueous media, low binding capacity and slow mass transfer, which restricts its applications in various aspects. This critical review briefly reviews the current status of MIT, particular emphasis on significant progresses of novel imprinting methods, some challenges and effective strategies for MIT, and highlighted applications of MIPs. Finally, some significant attempts in further developing MIT are also proposed (236 references).

SERS Tags: Novel Optical Nanoprobes for Bioanalysis

CONTENTS 1. Introduction 1.1. Fundamental Theory of Surface-Enhanced Raman Scattering 1.2. Optical Properties of SERS Tags 2. Synthesis of SERS Tags 2.1. Noble Metal Nanosubstrates 2.1.1. Single Particle-Based SERS Substrates 2.1.2. Nanoparticle Cluster-Based Substrates 2.2. Raman Reporter Molecules 2.2.1. Selection Principles and Reporter Types 2.2.2. Self-Assembled Monolayer Coverage Strategy 2.3. Surface Coating for Protection 2.3.1. Biomolecule Coating 2.3.2. Polymer Coating 2.3.3. Liposome Coating 2.3.4. Silica Coating 2.4. Attachment of Targeting Molecules 3. Bioanalysis Applications 3.1. Ionic and Molecular Detection 3.2. Pathogen Detection 3.3. Live-Cell Imaging 3.3.1. Cancer Marker Detection 3.3.2. Intercellular Microenvironment Sensing 3.4. Tissue SERS Imaging 3.5. In Vivo SERS Imaging 4. Challenges and Perspectives 4.1. Reproducible Signal of SERS Tags 4.1.1. Precisely Controlled Hot Spots for Nanosubstrates 4.1.2. Calibration of SERS Intensities and Enhancements 4.2. Improving Multiplexing Capability 4.3. Reduced Size for Subcellular Imaging 4.4. Development of Multifunctional Nanoplatforms 4.4.1. Magnetic SERS Dots 4.4.2. Multimodal Imaging Dots 4.4.3. SERS Tag-Based Therapeutic Systems 4.5. Biocompatibility 5. Conclusions and Remarks

Chemical basis of interactions between engineered nanoparticles and biological systems.

As defined by the European Commission, nanomaterial is a natural, incidental or manufactured material containing particles in an unbound state or as an aggregate or agglomerate in which ≥ 50% of the particles in the number size distribution have one or more external dimensions in the size range 1 to 100 nm. In specific cases and where warranted by concerns for the environment, health, safety or competition, the number size distribution threshold of 50% may be replaced with a threshold between 1 and 50%.1 Engineered nanomaterials (ENMs) refer to man-made nanomaterials. Materials in the nanometer range often possess unique physical, optical, electronic, and biological properties compared with larger particles, such as the strength of graphene,2 the electronic properties of carbon nanotubes (CNTs),3 the antibacterial activity of silver nanoparticles4 and the optical properties of quantum dots (QDs).5 The unique and advanced properties of ENMs have led to a rapid increase in their application. These applications include aerospace and airplanes, energy, architecture, chemicals and coatings, catalysts, environmental protection, computer memory, biomedicine and consumer products. Driven by these demands, the worldwide ENM production volume in 2016 is conservatively estimated in a market report by Future Markets to be 44,267 tons or ≥

Quantum dots, lighting up the research and development of nanomedicine

5 billion.6 As the production and applications of ENMs rapidly expand, their environmental impacts and effects on human health are becoming increasingly significant.7 Due to their small sizes, ENMs are easily made airborne.8 However, no accurate method to quantitatively measure their concentration in air currently exists. A recently reported incident of severe pulmonary fibrosis caused by inhaled polymer nanoparticles in seven female workers obtained much attention.9 In addition to the release of ENM waste from industrial sites, a major release of ENMs to environmental water occurs due to home and personal use of appliances, cosmetics and personal products, such as shampoo and sunscreen.10 Airborne and aqueous ENMs pose immediate danger to the human respiratory and gastrointestinal systems. ENMs may enter other human organs after they are absorbed into the bloodstream through the gastrointestinal or respiratory systems.11,12 Furthermore, ENMs in cosmetics and personal care products, such as lotion, sunscreen and shampoo may enter human circulation through skin penetration.13 ENMs are very persistent in the environment and are slowly degraded. The dissolved metal ions from ENMs can also revert back to nanoparticles under natural conditions.14 ENMs are stored in plants, microbes and animal organs and can be transferred and accumulated through the food chain.15,16 In addition to the accidental entry of ENMs into human and biological systems, ENMs are also purposefully injected into or enter humans for medicinal and diagnostic purposes.17 Therefore, interactions of ENMs with biological systems are inevitable. In addition to engineered nanomaterials, there are also naturally existing nanomaterials such as proteins and DNA molecules, which are key components of biological systems. These materials, combined with lipids and organic and inorganic small molecules, form the basic units of living systems –cells.18 To elucidate how nanomaterials affect organs and physiological functions, a thorough understanding of how nanomaterials perturb cells and biological molecules is required (Figure 1). Rapidly accumulating evidence indicates that ENMs interact with the basic components of biological systems, such as proteins, DNA molecules and cells.19-21 The driving forces for such interactions are quite complex and include the size, shape and surface properties (e.g., hydrophobicity, hydrogen-bonding capability, pi-bonds and stereochemical interactions) of ENMs.22-25 Figure 1 Interactions of nanoparticles with biological systems at different levels. Nanoparticles enter the human body through various pathways, reaching different organs and contacting tissues and cells. All of these interactions are based on nanoparticle-biomacromolecule ... Evidence also indicates that chemical modifications on a nanoparticle’s surface alter its interactions with biological systems.26-28 These observations not only support the hypothesis that basic nano-bio interactions are mainly physicochemical in nature but also provide a powerful approach to controlling the nature and strength of a nanoparticle’s interactions with biological systems. Practically, a thorough understanding of the fundamental chemical interactions between nanoparticles and biological systems has two direct impacts. First, this knowledge will encourage and assist experimental approaches to chemically modify nanoparticle surfaces for various industrial or medicinal applications. Second, a range of chemical information can be combined with computational methods to investigate nano-biological properties and predict desired nanoparticle properties to direct experiments.29-31 The literature regarding nanoparticle-biological system interactions has increased exponentially in the past decade (Figure 2). However, a mechanistic understanding of the chemical basis for such complex interactions is still lacking. This review intends to explore such an understanding in the context of recent publications. Figure 2 An analysis of literature statistics indicates growing concern for the topics that are the focus of this review. The number of publications and citations were obtained using the keywords “nanoparticles” and “biological systems” ... A breakthrough technology cannot prosper without wide acceptance from the public and society; that is, it must pose minimal harm to human health and the environment. Nanotechnology is now facing such a critical challenge. We must elucidate the effects of ENMs on biological systems (such as biological molecules, human cells, organs and physiological systems). Accumulating experimental evidence suggests that nanoparticles interact with biological systems at nearly every level, often causing unwanted physiological consequences. Elucidating these interactions is the goal of this review. This endeavor will help regulate the proper application of ENMs in various products and their release into the environment. A more significant mission of this review is to direct the development of “safe-by-design” ENMs, as their demands for and applications continue to increase.

Determination of 16 polycyclic aromatic hydrocarbons in environmental water samples by solid-phase extraction using multi-walled carbon nanotubes as adsorbent coupled with gas chromatography-mass spectrometry.

UNLABELLED Quantum dots (QDs) have proven themselves as powerful inorganic fluorescent probes, especially for long term, multiplexed imaging and detection. The newly developed QDs labeling techniques have facilitated the study of drug delivery on the level of living cells and small animals. Moreover, based on QDs and fluorescence imaging system, multifunctional nanocomplex integrated targeting, imaging and therapeutic functionalities have become effective materials for synchronous cancer diagnosis and treatment. In this review, we will summarize the recent advances of QDs in the research of drug delivery system from the following aspects: surface modification strategies of QDs for drug delivery, QDs as drug nanocarriers, QD-labeled drug nanocarriers, QD-based fluorescence resonance energy transfer (FRET) technique for drug release study as well as the development of multifunctional nanomedicines. Possible perspective in this field will also be discussed. FROM THE CLINICAL EDITOR This review discusses the role and significance of quantum dots (QDs) from the following aspects: surface modification strategies of QDs for drug delivery, QDs as drug nanocarriers, QD-labeled drug nanocarriers, QD-based fluorescence resonance energy transfer (FRET) technique for drug release study as well as the development of multifunctional nanomedicines.

Quercetin molecularly imprinted polymers: Preparation, recognition characteristics and properties as sorbent for solid-phase extraction

A solid-phase extraction (SPE) using multi-walled carbon nanotubes (MWCNTs) as adsorbent coupled with gas chromatography-mass spectrometry (GC-MS) method was developed for the determination of 16 polycyclic aromatic hydrocarbons (PAHs) in environmental water samples. Several condition parameters, such as extraction adsorbents, elution solvents and volumes, and sample loading flow rate and volume were optimized to obtain high SPE recoveries and extraction efficiency. 150mg MWCNTs as sorbent presented high extraction efficiency of 16 PAHs due to the large specific surface area and high adsorption capacity of MWCNTs compared with the commercial C18 column (250mg/2mL). The calibration curves of 16 PAHs extracted were linear in the range of 20-5000ngL(-1), with the correlation coefficients (r(2)) between 0.9848 and 0.9991. The method attained good precisions (relative standard deviation, RSD) from 1.2% to 12.1% for standard PAHs aqueous solutions; method recoveries ranged in 76.0-125.5%, 74.5-127.0%, and 70.0-122.0% for real spiked samples from river water, tap water and seawater, respectively. Limits of detection (LODs, S/N=3) of the method were determined from 2.0 to 8.5ngL(-1). The optimized method was successfully applied to the determination of 16 PAHs in real environmental water samples.

Recent advances in surface-enhanced Raman scattering detection technology for microfluidic chips.

Molecular imprinted polymers (MIPs) were prepared through thermal polymerization by using quercetin as the template molecule, acrylamide (AA) as the functional monomer and ethylene glycol dimethacrylate (EDMA) as the cross-linker in the porogen of tetrahydrofuran (THF). The synthesized MIPs were identified by both Fourier transform infrared (FTIR) and scanning electron microscope (SEM). Systematic investigations of the influences of key synthetic conditions, including functional monomers, porogens and cross-linkers, on the recognition properties of the MIPs were conducted. Scatchard analysis revealed that the homogeneous binding sites were formed in the polymers. Besides quercetin, two structurally similar compounds of rutin and catechol were employed for molecular recognition specificity tests of MIPs. It was observed that the MIPs exhibited the highest selective rebinding to quercetin. Accordingly, the MIPs were used as a solid-phase extraction (SPE) sorbent for the extraction and enrichment of quercetin in cacumen platycladi samples, followed by HPLC-UV analysis. The application of MIPs with high affinity and excellent stereo-selectivity toward quercetin in SPE might offer a novel method for the enrichment and determination of flavonoid compounds in the natural products.

Nanomaterial-assisted aptamers for optical sensing.

Microfluidic chip devices and their application to sensitive chemical and biological analyses have attracted significant attention over the past decade. The miniaturization of reaction systems offers practical advantages over conventional benchtop systems. In this case, however, a highly sensitive on‐chip detection method is important for the monitoring of chemical reactions as well as for the detection of analytes inside the channel because the detection volume in a micrometer‐size channel is extremely small. Recently, a surface‐enhanced Raman scattering (SERS) technique is being regarded as a potential candidate for the highly sensitive detection of analytes in a microfluidic chip. This review provides a general survey and an in‐depth look at recent developments in SERS techniques for the biological/environmental analysis of minute analytes in a microfluidic chip.

Molecularly imprinted core-shell nanoparticles for determination of trace atrazine by reversible addition-fragmentation chain transfer surface imprinting

Aptamers are single-strand DNA or RNA selected in vitro that bind specifically with a broad range of targets from metal ions, organic molecules, to proteins, cells and microorganisms. As an emerging class of recognition elements, aptamers offer remarkable convenience in the design and modification of their structures, which has motivated them to generate a great variety of aptamer sensors (aptasensors) that exhibit high sensitivity as well as specificity. On the other hand, the development of nanoscience and nanotechnology has generated nanomaterials with novel properties compared with their counterparts in macroscale. By integrating their strengths of both fields, recently, versatile aptamers coupling with novel nanomaterials for designing nanomaterial-assisted aptasensors (NAAs) make the combinations universal strategies for sensitive optical sensing. NAAs have been considered as an excellent sensing platform and found wide applications in analytical community. In this review, we summarize recent advances in the development of various optical NAAs, employing various detection techniques including colorimetry, fluorometry, surface-enhanced Raman scattering (SERS), magnetic resonance imaging (MRI) and surface plasmon resonance (SPR).

Dummy molecularly imprinted polymers-capped CdTe quantum dots for the fluorescent sensing of 2,4,6-trinitrotoluene.

A simple and effective method was proposed to prepare uniform surface-imprinted nanoparticles. This strategy was carried out by introducing vinyl groups to the surface of silica beads by a one-step modification, followed by copolymerization of functional monomers via reversible addition–fragmentation chain transfer (RAFT) precipitation polymerization. Owing to the intrinsic advantages of controlled/living polymerization and surface imprinting technology, the resultant RAFT surface-imprinted nano-sized polymers (RAFT-SINPs) demonstrated spherical shaped particles with excellent monodispersity, and improvements in imprinting efficiency and mass transfer in comparison to molecularly imprinted polymers (MIPs) prepared by traditional precipitation polymerization. Recoveries of 93.4% and 79.8% were achieved by one-step extraction when RAFT-SINPs were used for the preconcentration and selective separation of atrazine in spiked corn and lettuce samples, respectively. These results provided the possibility for the separation and enrichment of atrazine from complicated matrices by RAFT-SINPs.