An experimental study of clearance of inhaled particles from the human nose

Smith, Jennifer; Bailey, Michael R.; Etherington, G.; Shutt, A. L.; Youngman, M. J.

doi:10.3109/01902148.2010.518301

Cited by 11 publications

(7 citation statements)

References 19 publications

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“…It was assumed (Fig. A.1) that of material deposited in the ET airways, approximately 50% deposits in ET 1 , which is cleared by nose blowing at a rate of 1 d −1 , and the rest deposits in ET 2 , which clears to the gastrointestinal tract at a rate of 100 d −1 . (A12) In experiments intended to address this deficiency, subjects inhaled 1.5-, 3- or 6-µm aerodynamic diameter ( d ae ) radiolabelled insoluble particles through the nose while sitting at rest or performing light exercise (Smith et al., 2002, 2011). Retention in the nasal airways and clearance by voluntary nose blowing were followed until at least 95% of the initial ET deposit had cleared (typically approximately 2 d).…”

Section: Annex a Revision Of The Human Respiratory Tract Modelmentioning

confidence: 99%

“… (A15) In the original HRTM, it was assumed that particles deposited in the nasal passages during inhalation are partitioned equally between ET 1 and the posterior nasal passage, which is part of ET 2 [however, because of the way the deposition efficiencies were calculated for polydispersed aerosols during inhalation and exhalation, for most aerosol sizes of interest in radiological protection, the deposition fractions given in Publication 66 (ICRP, 1994a) are somewhat higher for ET 2 than for ET 1 ]. In the revised HRTM, based on the recent experiments (Smith et al., 2011), it is assumed that for nose breathing, the deposit in the ET airways is distributed 65% to ET 1 and 35% to ET 2 . To calculate the fractions of inhaled material deposited in ET 1 and ET 2 in the revised HRTM, the fractions deposited in ET 1 and ET 2 (calculated using the original HRTM) were summed to give the total deposit in the ET airways, and then repartitioned 65% to ET 1 and 35% to ET 2 (for mouth breathing, there is no deposition in ET 1 , and the fraction deposited in ET 2 remains as calculated using the original HRTM). (A16) Table A.2 gives values of fractional deposition in each region of the respiratory tract as a function of aerosol size for (a) an adult male sitting at rest, (b) an adult male undertaking light exercise, and (c) the Reference Worker.…”

Section: Annex a Revision Of The Human Respiratory Tract Modelmentioning

confidence: 99%

“…(A12) In experiments intended to address this deficiency, subjects inhaled 1.5-, 3or 6-mm aerodynamic diameter (d ae ) radiolabelled insoluble particles through the nose while sitting at rest or performing light exercise (Smith et al, 2002(Smith et al, , 2011. Retention in the nasal airways and clearance by voluntary nose blowing were followed until at least 95% of the initial ET deposit had cleared (typically approximately 2 d).…”

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ICRP Publication 130: Occupational Intakes of Radionuclides: Part 1

Paquet¹,

et al. 2015

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This report is the first in a series of reports replacing Publications 30 and 68 to provide revised dose coefficients for occupational intakes of radionuclides by inhalation and ingestion. The revised dose coefficients have been calculated using the Human Alimentary Tract Model (Publication 100) and a revision of the Human Respiratory Tract Model (Publication 66) that takes account of more recent data. In addition, information is provided on absorption into blood following inhalation and ingestion of different chemical forms of elements and their radioisotopes. In selected cases, it is judged that the data are sufficient to make material-specific recommendations. Revisions have been made to many of the models that describe the systemic biokinetics of radionuclides absorbed into blood, making them more physiologically realistic representations of uptake and retention in organs and tissues, and excretion. The reports in this series provide data for the interpretation of bioassay measurements as well as dose coefficients, replacing Publications 54 and 78. In assessing bioassay data such as measurements of whole-body or organ content, or urinary excretion, assumptions have to be made about the exposure scenario, including the pattern and mode of radionuclide intake, physical and chemical characteristics of the material involved, and the elapsed time between the exposure(s) and measurement. This report provides some guidance on monitoring programmes and data interpretation.

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Section: Annex a Revision Of The Human Respiratory Tract Modelmentioning

confidence: 99%

Section: Annex a Revision Of The Human Respiratory Tract Modelmentioning

confidence: 99%

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ICRP Publication 130: Occupational Intakes of Radionuclides: Part 1

Paquet¹,

et al. 2015

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“…Evidence from previous studies measured the percentage of inhaled particles in the lungs and characterized the translocation of particles from the respiratory tract ( Semmler et al. 2004 ; Smith et al. 2011 , 2014 ; U.S. EPA 2019 ).…”

Section: Introductionmentioning

confidence: 99%

PM2.5 and Serum Metabolome and Insulin Resistance, Potential Mediation by the Gut Microbiome: A Population-Based Panel Study of Older Adults in China

Zhao

Fang

Tang

et al. 2022

Environ Health Perspect

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Background: Insulin resistance (IR) affects the development of type 2 diabetes mellitus (T2DM), which is also influenced by accumulated fine particle air pollution [particulate matter (PM) with aerodynamic diameter of ( )] exposure. Previous experimental and epidemiological studies have proposed several potential mechanisms by which contributes to IR/T2DM, including inflammation imbalance, oxidative stress, and endothelial dysfunction. Recent evidence suggests that the imbalance of the gut microbiota affects the metabolic process and may precede IR. However, the underlying mechanisms of , gut microbiota, and metabolic diseases are unclear. Objectives: We investigated the associations between personal exposure to and fasting blood glucose and insulin levels, the IR index, and other related biomarkers. We also explored the potential underlying mechanisms (systemic inflammation and sphingolipid metabolism) between and insulin resistance and the mediating effects between and sphingolipid metabolism. Methods: We recruited 76 healthy seniors to participate in a repeated-measures panel study and conducted clinical examinations every month from September 2018 to January 2019. Linear mixed-effects (LME) models were used to analyze the associations between and health data (e.g., functional factors, the IR index, inflammation and other IR-related biomarkers, metabolites, and gut microbiota). We also performed mediation analyses to evaluate the effects of mediators (gut microbiota) on the associations between exposures ( ) and featured metabolism outcomes. Results: Our prospective panel study illustrated that exposure to was associated with an increased risk of higher IR index and functional biomarkers, and our study provided mechanistic evidence suggesting that exposure may contribute to systemic inflammation and altered sphingolipid metabolism. Discussion: Our findings demonstrated that was associated with the genera of the gut microbiota, which partially mediated the association between and sphingolipid metabolism. These findings may extend our current understanding of the pathways of and IR. https://doi.org/10.1289/EHP9688

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“…Undisturbed nasal breathing is essential for normal breathing physiology as a whole and the effects of nasal obstruction on the respiratory and cardiovascular systems have been well studied: right ventricle problems 1,2 , ischemic heart diseases 3,4,5,,6,7,8,9 , sleep disorders 10,11,12,13 , mucociliary clearance system disturbances 14,15 , paranasal sinus pathology 16,17 , have all been described as a result of impaired nasal breathing. The connection between the upper and lower respiratory systems has been recognized in allergic rhinitis and asthma as well, resulting in united airways concept.…”

Section: Introductionmentioning

confidence: 99%