Nanoparticle Mass Transfer From Lung Airways to Systemic Regions—Part I: Whole-Lung Aerosol Dynamics

Kolanjiyil, Arun V.; Kleinstreuer, Clement

doi:10.1115/1.4025332

Cited by 44 publications

(33 citation statements)

References 41 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In contrast, nanoaerosols in the range of 50 nm deposit primarily by Brownian motion (84), with particle charge also potentially playing a role. Deposition by Brownian motion in an airway becomes directly proportional to residence time and inversely proportional to particle velocity (85–87), which is reversed for microparticles. Airflow velocities are known to decrease with depth into the bifurcating airway tree.…”

Section: Discussionmentioning

confidence: 99%

Small Airway Absorption and Microdosimetry of Inhaled Corticosteroid Particles after Deposition

Longest

Hindle

2017

Pharm Res

View full text Add to dashboard Cite

Purpose To predict the cellular-level epithelial absorbed dose from deposited inhaled corticosteroid (ICS) particles in a model of an expanding and contracting small airway segment for different particle forms. Methods A computational fluid dynamics (CFD)-based model of drug dissolution, absorption and clearance occurring in the surface liquid of a representative small airway generation (G13) was developed and used to evaluate epithelial dose for the same deposited drug mass of conventional microparticles, nanoaggregates and a true nanoaerosol. The ICS medications considered were budesonide (BD) and fluticasone propionate (FP). Within G13, total epithelial absorption efficiency (AE) and dose uniformity (microdosimetry) were evaluated. Results Conventional microparticles resulted in very poor AE of FP (0.37%) and highly nonuniform epithelial absorption, such that <5% of cells received drug. Nanoaggregates improved AE of FP by a factor of 57-fold and improved dose delivery to reach approximately 40% of epithelial cells. True nanoaerosol resulted in near 100% AE for both drugs and uniform drug delivery to all cells. Conclusions Current ICS therapies are absorbed by respiratory epithelial cells in a highly nonuniform manner that may partially explain poor clinical performance in the small airways. Both nanoaggregates and nanoaerosols can significantly improve ICS absorption efficiency and uniformity.

show abstract

Section: Discussionmentioning

confidence: 99%

Small Airway Absorption and Microdosimetry of Inhaled Corticosteroid Particles after Deposition

Longest

Hindle

2017

Pharm Res

View full text Add to dashboard Cite

show abstract

“…During the smoking of tobacco, some constituents on the nano-scale penetrate the pulmonary alveoli and enter via lymph and/or blood circulation other organs [138]. Thus, a realistic and accurate multi-compartment model for deposited constituent mass transfer into systemic regions is a valuable and cost-effective tool for toxicologists and others to establish dose-response-effect relationships and generate new physical insight and reliable, quantitative data sets [14,15]. …”

Section: Discussionmentioning

confidence: 99%

“…It should be able to predict inhaled tobacco smoke droplet/vapor and toxicant deposition for a set of realistic inlet conditions on a subject-specific basis. Furthermore, in conjunction with a multi-compartment model [14,15] for deposited constituent mass transfer into organs, it is a valuable and cost-effective tool for toxicologists and others to establish dose-response relationships and generate new physical insight and reliable, quantitative data sets. …”

Section: Introductionmentioning

confidence: 99%

Lung Deposition Analyses of Inhaled Toxic Aerosols in Conventional and Less Harmful Cigarette Smoke: A Review

Kleinstreuer

Feng

2013

IJERPH

Self Cite

View full text Add to dashboard Cite

Inhaled toxic aerosols of conventional cigarette smoke may impact not only the health of smokers, but also those exposed to second-stream smoke, especially children. Thus, less harmful cigarettes (LHCs), also called potential reduced exposure products (PREPs), or modified risk tobacco products (MRTP) have been designed by tobacco manufacturers to focus on the reduction of the concentration of carcinogenic components and toxicants in tobacco. However, some studies have pointed out that the new cigarette products may be actually more harmful than the conventional ones due to variations in puffing or post-puffing behavior, different physical and chemical characteristics of inhaled toxic aerosols, and longer exposure conditions. In order to understand the toxicological impact of tobacco smoke, it is essential for scientists, engineers and manufacturers to develop experiments, clinical investigations, and predictive numerical models for tracking the intake and deposition of toxicants of both LHCs and conventional cigarettes. Furthermore, to link inhaled toxicants to lung and other diseases, it is necessary to determine the physical mechanisms and parameters that have significant impacts on droplet/vapor transport and deposition. Complex mechanisms include droplet coagulation, hygroscopic growth, condensation and evaporation, vapor formation and changes in composition. Of interest are also different puffing behavior, smoke inlet conditions, subject geometries, and mass transfer of deposited material into systemic regions. This review article is intended to serve as an overview of contributions mainly published between 2009 and 2013, focusing on the potential health risks of toxicants in cigarette smoke, progress made in different approaches of impact analyses for inhaled toxic aerosols, as well as challenges and future directions.

show abstract

“…A higher percentage of blood is habitually present in the veins, therefore, a significant proportion of ENM may exist here (Venous settling, Figure 1) (11). …”

Section: The Cardiovascular Systemmentioning

confidence: 99%

Metal Nanomaterial Toxicity Variations Within the Vascular System

Abukabda

Stapleton

Nurkiewicz

2016

Curr Envir Health Rpt

View full text Add to dashboard Cite

Engineered nanomaterials (ENM) are anthropogenic materials with at least one dimension less than 100 nm. Their ubiquitous employment in biomedical and industrial applications in the absence of full toxicological assessments raises significant concerns over their safety on human health. This is a significant concern, especially for metal and metal oxide ENM as they may possess the greatest potential to impair human health. A large body of literature has developed that reflects adverse systemic effects associated with exposure to these materials, but an integrated mechanistic framework for how ENM exposure influences morbidity remains elusive. This may be due in large part to the tremendous diversity of existing ENM and the rate at which novel ENM are produced. In this review, the influence of specific ENM physicochemical characteristics and hemodynamic factors on cardiovascular toxicity are discussed. Additionally, the toxicity of metallic, and metal oxide ENM is presented in the context of the cardiovascular system and its discrete anatomical and functional components. Finally, future directions and understudied topics are presented. While it is clear that the nanotechnology boom has increased our interest in ENM toxicity, it is also evident that the field of cardiovascular nanotoxicology remains in its infancy and continued, expansive research is necessary in order to determine the mechanisms via which ENM exposure contributes to cardiovascular morbidity.

show abstract

Nanoparticle Mass Transfer From Lung Airways to Systemic Regions—Part I: Whole-Lung Aerosol Dynamics

Cited by 44 publications

References 41 publications

Small Airway Absorption and Microdosimetry of Inhaled Corticosteroid Particles after Deposition

Small Airway Absorption and Microdosimetry of Inhaled Corticosteroid Particles after Deposition

Lung Deposition Analyses of Inhaled Toxic Aerosols in Conventional and Less Harmful Cigarette Smoke: A Review

Metal Nanomaterial Toxicity Variations Within the Vascular System

Contact Info

Product

Resources

About