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Lizhong He

Researcher at Monash University, Clayton campus

Publications -  87
Citations -  2706

Lizhong He is an academic researcher from Monash University, Clayton campus. The author has contributed to research in topics: Adsorption & Chemistry. The author has an hindex of 24, co-authored 77 publications receiving 2351 citations. Previous affiliations of Lizhong He include Tianjin University & University of Queensland.

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Nanoparticle synthesis in microreactors

TL;DR: In this paper, a review of recent achievements in the synthesis of nanoparticles in microfluidic reactors is presented and compared, including continuous flow, gas-liquid segmented flow and droplet-based microreactors.
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Poly-L-lysine functionalized large pore cubic mesostructured silica nanoparticles as biocompatible carriers for gene delivery.

TL;DR: Large pore mesoporous silica nanoparticles functionalized with poly-L-lysine were designed as a new carrier material for gene delivery applications and demonstrated great potential for efficient gene transfer into cancer cells as a decrease of the cellular viability of the osteosarcoma cancer cells was induced.
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Computational Study of MoN2 Monolayer as Electrochemical Catalysts for Nitrogen Reduction

TL;DR: In this article, a computational study of molybdenum nitride (MoN2) nanosheet as a catalyst for ammonia synthesis at room temperature under the scheme of density functional theory is presented.
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A Novel Correlation for Protein Diffusion Coefficients Based on Molecular Weight and Radius of Gyration

TL;DR: A new correlation is proposed for the prediction of protein diffusion coefficients in free solution that works well for diverse proteins with different shapes and extensive molecular weight and radius of gyration.
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Molecular insight into conformational transition of amyloid β-peptide 42 inhibited by (-)-epigallocatechin-3-gallate probed by molecular simulations.

TL;DR: The work has elucidated the molecular mechanism of the inhibition effect of EGCG on the conformational transition of Aβ(42), and the findings are considered critical for exploring more effective agents for the inhibition of A β(42) fibrillogenesis.