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Dive into the research topics where Krishnendu Saha is active.

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Featured researches published by Krishnendu Saha.


Chemical Reviews | 2012

Gold Nanoparticles in Chemical and Biological Sensing

Krishnendu Saha; Sarit S. Agasti; Chaekyu Kim; Xiaoning Li; Vincent M. Rotello

Detection of chemical and biological agents plays a fundamental role in biomedical, forensic and environmental sciences1–4 as well as in anti bioterrorism applications.5–7 The development of highly sensitive, cost effective, miniature sensors is therefore in high demand which requires advanced technology coupled with fundamental knowledge in chemistry, biology and material sciences.8–13 In general, sensors feature two functional components: a recognition element to provide selective/specific binding with the target analytes and a transducer component for signaling the binding event. An efficient sensor relies heavily on these two essential components for the recognition process in terms of response time, signal to noise (S/N) ratio, selectivity and limits of detection (LOD).14,15 Therefore, designing sensors with higher efficacy depends on the development of novel materials to improve both the recognition and transduction processes. Nanomaterials feature unique physicochemical properties that can be of great utility in creating new recognition and transduction processes for chemical and biological sensors15–27 as well as improving the S/N ratio by miniaturization of the sensor elements.28 Gold nanoparticles (AuNPs) possess distinct physical and chemical attributes that make them excellent scaffolds for the fabrication of novel chemical and biological sensors (Figure 1).29–36 First, AuNPs can be synthesized in a straightforward manner and can be made highly stable. Second, they possess unique optoelectronic properties. Third, they provide high surface-to-volume ratio with excellent biocompatibility using appropriate ligands.30 Fourth, these properties of AuNPs can be readily tuned varying their size, shape and the surrounding chemical environment. For example, the binding event between recognition element and the analyte can alter physicochemical properties of transducer AuNPs, such as plasmon resonance absorption, conductivity, redox behavior, etc. that in turn can generate a detectable response signal. Finally, AuNPs offer a suitable platform for multi-functionalization with a wide range of organic or biological ligands for the selective binding and detection of small molecules and biological targets.30–32,36 Each of these attributes of AuNPs has allowed researchers to develop novel sensing strategies with improved sensitivity, stability and selectivity. In the last decade of research, the advent of AuNP as a sensory element provided us a broad spectrum of innovative approaches for the detection of metal ions, small molecules, proteins, nucleic acids, malignant cells, etc. in a rapid and efficient manner.37 Figure 1 Physical properties of AuNPs and schematic illustration of an AuNP-based detection system. In this current review, we have highlighted the several synthetic routes and properties of AuNPs that make them excellent probes for different sensing strategies. Furthermore, we will discuss various sensing strategies and major advances in the last two decades of research utilizing AuNPs in the detection of variety of target analytes including metal ions, organic molecules, proteins, nucleic acids, and microorganisms.


Accounts of Chemical Research | 2013

The Role of Surface Functionality in Determining Nanoparticle Cytotoxicity

Sung Tae Kim; Krishnendu Saha; Chaekyu Kim; Vincent M. Rotello

Surface properties dictate the behavior of nanomaterials in vitro, in vivo, and in the environment. Such properties include surface charge and hydrophobicity. Also key are more complex supramolecular interactions such as aromatic stacking and hydrogen bonding, and even surface topology from the structural to the atomic level. Surface functionalization of nanoparticles (NPs) provides an effective way to control the interface between nanomaterials and the biological systems they are designed to interact with. In medicine, for instance, proper control of surface properties can maximize therapeutic or imaging efficacy while minimizing unfavorable side effects. Meanwhile, in environmental science, thoughtful choice of particle coating can minimize the impact of manufactured nanomaterials on the environment. A thorough knowledge of how NP surfaces with various properties affect biological systems is essential for creating NPs with such useful therapeutic and imaging properties as low toxicity, stability, biocompatibility, favorable distribution throughout cells or tissues, and favorable pharmacokinetic profiles--and for reducing the potential environmental impact of manufactured nanomaterials, which are becoming increasingly prominent in the marketplace. In this Account, we discuss our research and that of others into how NP surface properties control interactions with biomolecules and cells at many scales, including the role the particle surface plays in determining in vivo behavior of nanomaterials. These interactions can be benign, beneficial, or lead to dysfunction in proteins, genes and cells, resulting in cytotoxic and genotoxic responses. Understanding these interactions and their consequences helps us to design minimally invasive imaging and delivery agents. We also highlight in this Account how we have fabricated nanoparticles to act as therapeutic agents via tailored interactions with biomacromolecules. These particles offer new therapeutic directions from traditional small molecule therapies, and with potentially greater versatility than is possible with proteins and nucleic acids.


ACS Nano | 2014

Functional Gold Nanoparticles as Potent Antimicrobial Agents against Multi-Drug-Resistant Bacteria

Xiaoning Li; Sandra M. Robinson; Akash Gupta; Krishnendu Saha; Ziwen Jiang; Daniel F. Moyano; Ali Sahar; Margaret A. Riley; Vincent M. Rotello

We present the use of functionalized gold nanoparticles (AuNPs) to combat multi-drug-resistant pathogenic bacteria. Tuning of the functional groups on the nanoparticle surface provided gold nanoparticles that were effective against both Gram-negative and Gram-positive uropathogens, including multi-drug-resistant pathogens. These AuNPs exhibited low toxicity to mammalian cells, and bacterial resistance was not observed after 20 generations. A strong structure–activity relationship was observed as a function of AuNP functionality, providing guidance to activity prediction and rational design of effective antimicrobial nanoparticles.


Small | 2010

The Role of Surface Functionality on Acute Cytotoxicity, ROS Generation and DNA Damage by Cationic Gold Nanoparticles

Apiwat Chompoosor; Krishnendu Saha; Partha Ghosh; Dylan J. Macarthy; Oscar R. Miranda; Zheng-Jiang Zhu; Kathleen F. Arcaro; Vincent M. Rotello

Gold nanoparticles (AuNPs) are promising materials for biomedical applications [1,2] due to their tunable surface properties [3] and extraordinary stability.[4] Additionally, the inert core material reduces the potential for toxicity issues arising from particle degradation.[5] The size regime and concomitant geometrical outcomes including high degree of curvature, however, generates the potential for toxicity.[6,7] Generally, the toxicity of AuNPs depends on size, shape, the degree to which they aggregate, and their surface properties[8,9] Recently, several studies on the short-term cytotoxicity of AuNPs[10] and quantum dots[11] have focused on size,[12,13] shape,[14,15] and charge.[16] To date, however, issues such as ligand hydrophobicity have not been systematically explored.


Molecular Therapy | 2014

Gold Nanoparticles for Nucleic Acid Delivery

Ya Ding; Ziwen Jiang; Krishnendu Saha; Chang Soo Kim; Sung Tae Kim; Ryan F. Landis; Vincent M. Rotello

Gold nanoparticles provide an attractive and applicable scaffold for delivery of nucleic acids. In this review, we focus on the use of covalent and noncovalent gold nanoparticle conjugates for applications in gene delivery and RNA-interference technologies. We also discuss challenges in nucleic acid delivery, including endosomal entrapment/escape and active delivery/presentation of nucleic acids in the cell.


ACS Nano | 2014

Fabrication of Corona-Free Nanoparticles with Tunable Hydrophobicity

Daniel F. Moyano; Krishnendu Saha; Gyan Prakash; Bo Yan; Hao Kong; Mahdieh Yazdani; Vincent M. Rotello

A protein corona is formed at the surface of nanoparticles in the presence of biological fluids, masking the surface properties of the particle and complicating the relationship between chemical functionality and biological effects. We present here a series of zwitterionic NPs of variable hydrophobicity that do not adsorb proteins at moderate levels of serum protein and do not form hard coronas at physiological serum concentrations. These particles provide platforms to evaluate nanobiological behavior such as cell uptake and hemolysis dictated directly by chemical motifs at the nanoparticle surface.


Journal of the American Chemical Society | 2012

Aggregation and Interaction of Cationic Nanoparticles on Bacterial Surfaces

Steven C. Hayden; Gengxiang Zhao; Krishnendu Saha; Ronnie L. Phillips; Xiaoning Li; Oscar R. Miranda; Vincent M. Rotello; Mostafa A. El-Sayed; Ingeborg Schmidt-Krey; Uwe H. F. Bunz

Cationic monolayer-protected gold nanoparticles (AuNPs) with sizes of 6 or 2 nm interact with the cell membranes of Escherichia coli (Gram-) and Bacillus subtilis (Gram+), resulting in the formation of strikingly distinct AuNP surface aggregation patterns or lysis depending upon the size of the AuNPs. The aggregation phenomena were investigated by transmission electron microscopy and UV-vis spectroscopy. Upon proteolytic treatment of the bacteria, the distinct aggregation patterns disappeared.


Small | 2013

Surface functionality of nanoparticles determines cellular uptake mechanisms in mammalian cells.

Krishnendu Saha; Sung Tae Kim; Bo Yan; Oscar R. Miranda; Felix S. Alfonso; Denis Shlosman; Vincent M. Rotello

Nanoparticles (NPs) are versatile scaffolds for numerous biomedical applications including drug delivery and bioimaging. The surface functionality of NPs essentially dictates intracellular NP uptake and controls their therapeutic action. Using several pharmacological inhibitors, it is demonstrated that the cellular uptake mechanisms of cationic gold NPs in both cancer (HeLa) and normal cells (MCF10A) strongly depend on the NP surface monolayer, and mostly involve caveolae and dynamin-dependent pathways as well as specific cell surface receptors (scavenger receptors). Moreover, these NPs show different uptake mechanisms in cancer and normal cells, providing an opportunity to develop NPs with improved selectivity for delivery applications.


Angewandte Chemie | 2015

Acylsulfonamide‐Functionalized Zwitterionic Gold Nanoparticles for Enhanced Cellular Uptake at Tumor pH

Tsukasa Mizuhara; Krishnendu Saha; Daniel F. Moyano; Chang Soo Kim; Bo Yan; Young-Kwan Kim; Vincent M. Rotello

A nanoparticle design featuring pH-responsive alkoxyphenyl acylsulfonamide ligands is reported herein. As a result of ligand structure, this nanoparticle is neutral at pH 7.4, becoming positively charged at tumor pH (<6.5). The particle uptake and cytotoxicity increase over this pH range. This pH-controlled uptake and toxicity makes this particle a promising tool for tumor selective therapy.


Advanced Materials | 2014

25th Anniversary Article: Interfacing Nanoparticles and Biology: New Strategies for Biomedicine

Gulen Yesilbag Tonga; Krishnendu Saha; Vincent M. Rotello

The exterior surface of nanoparticles (NPs) dictates the behavior of these systems with the outside world. Understanding the interactions of the NP surface functionality with biosystems enables the design and fabrication of effective platforms for therapeutics, diagnostics, and imaging agents. In this review, we highlight the role of chemistry in the engineering of nanomaterials, focusing on the fundamental role played by surface chemistry in controlling the interaction of NPs with proteins and cells.

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Vincent M. Rotello

University of Massachusetts Amherst

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Daniel F. Moyano

University of Massachusetts Amherst

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Bo Yan

University of Massachusetts Amherst

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Sung Tae Kim

University of Massachusetts Amherst

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Gulen Yesilbag Tonga

University of Massachusetts Amherst

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Rubul Mout

University of Massachusetts Amherst

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Oscar R. Miranda

University of Massachusetts Amherst

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Yi-Cheun Yeh

University of Massachusetts Amherst

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Bradley Duncan

University of Massachusetts Amherst

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Chandramouleeswaran Subramani

University of Massachusetts Amherst

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