Lung Deposition Analyses of Inhaled Toxic Aerosols in Conventional and Less Harmful Cigarette Smoke: A Review
Abstract
:1. Introduction
2. Cigarette Toxicity and Vulnerable Population Groups
2.1. Toxicants and Carcinogens in Conventional Cigarette Smoke
2.2. Less Harmful Cigarette Products
2.2.1. Manufacture Approaches
2.2.2. Typical LHC Products
Non-Burning Cigarettes
Electrical Heated Cigarettes (EHCs)
E-Cigarettes
2.2.3. Potential Health Risks of LHC Products
- (a)
- (b)
- Unknown reactions between some components in newly designed filters (or other new additives) may lead to the production of carcinogens or other toxicants.
Toxicants | Induced Cancer Type | Related Biomarkers |
---|---|---|
Acetaldehyde * | Lung, nasal | Leukocyte DNA adducts |
Acrolein * | Lung | 3-HPMA in urine |
Benzene * | Lung, leukemia | SPMA in urine |
Benzo[a]pyrene * | Lung | 1-hydroxypyrene in urine |
1,3-Butadiene * | Lung, leukemia, liver | MHBMA in urine |
Carbon monoxide * | N/A | Exhaled CO |
NNK, NNN * | Lung, nasal, oral cavity, liver, oesophageal, pancreatic, cervical | NNAL and NNN in urine |
PAH * | Lung, laryngeal, oral cavity, cervical | 1-HOP |
Formaldehyde | Lung, nasal | Leukocyte DNA adducts |
Nicotine * | N/A | Nicotine, cotinine, 3′-hydroxicotinine and other their glucuronides in urine |
Nickel * | Lung, nasal | N/A |
2.3. Children as the Vulnerable Population Group
3. Studies of Toxic Aerosols from Inhaled Cigarette Smoke
3.1. Experimental and Clinical Investigations
3.1.1. Experimental Studies
- (1)
- Cigarette Smoke Extract Exposure (CSEE) systems, which collect the CSPs using filters, traps, etc. [77].
- (2)
- A smoking machine to generate and dilute mainstream smoke samples to the experimental chamber, e.g., Walton Smoking Machine (WSM), Borgwaldt RM20S® smoking machine, TE-10z smoking machine, etc. [40,78,80,81,82]. The simulated puffing conditions were based on the International Organization for Standardization (ISO).
- An exposure chamber where the smoke and cell cultures (i.e., tissues or physiological fluids samples) interacts with each other [27,78]. Additionally, for clinical study, a human exposure chamber may be applied [40]. It is necessary to carefully regulate the conditions in the chamber, in order to mimic the environment in vivo.
3.1.2. Clinical Investigations
3.2. Computational Fluid-Particle Dynamics (CF-PD) Simulation Models
- (1)
- Multiphase flow models with relevant physical and bio-chemical processes. Considering the computational costs and accuracies, the multiphase flow models widely used for simulating tobacco smoke aerosol transport and deposition in human respiratory systems are mostly within the Euler-Lagrange and Euler-Euler frameworks [12,13,97,101]. Specifically, different approaches employed for particulate phases or vapors are as follows:
- (a)
- Lagrangian approaches employing the point force-and-moment method for transport and deposition simulations of tobacco smoke particulate phases, i.e., particles and droplets [12]. These approaches provide direct descriptions of the particulate flow by tracking the motion of individual particulate entities. The transient airflow field can be solved independently in the Eulerian frame in case of dilute aerosol suspensions.
- (b)
- Eulerian approaches with enhanced mass transfer for vapors and nanoparticles (less than 50 nm in diameter) in tobacco smoke [13]. Solution of the enhanced mass transfer equation, i.e., Euler-Euler approach, considering inhaled material convection, diffusion, coagulation/aggregation, wall-flux deposition, etc.
- (2)
- Initial and boundary conditions. Initial and boundary conditions include realistic airflow waveforms as part of smoking behavior, initial particle distribution at the mouth inlet, physical/chemical characteristics of inhaled particles, droplets and vapors, rigid or moving lung airway-wall boundary conditions, lung airway-outlet boundary conditions, etc.
- (3)
- Realistic human respiratory system geometries. Accurate and realistic human respiratory system models (see examples in Figure 1) compose the necessary precursor for experimental or computational airflow and particle transport/deposition analyses [100]. The human respiratory system ventilation path contains mouth, nose, pharynx, glottis, larynx, trachea, bronchi, bronchioles (including terminal bronchioles (Generation 16) and respiratory bronchioles (Generation 17–19)), and alveoli. Development of a subject-specific model for ventilation of a breathing lung can only be accomplished through multidisciplinary efforts that require expertise in medical imaging, airway geometric reconstruction, computational techniques, pulmonary physiology and medicine, and fluid mechanics [102].
3.3. Semi-Empirical Models
3.4. Parameters and Mechanisms Influencing the Deposition of Toxicants and Carcinogens
3.4.1. Variability in Smoking Behavior
- 31 to 86 mL in puff volume.
- 0.9 to 3.0 s in puff duration.
- 18 to 64 s for inter-puff interval.
- 2,100 to 3,800 mL/min in puff flow rate.
- 8 to 16 puffs per cigarette.
Cigarette | Smoking Condition | Puff Volume (mL) | Puff Duration (s) | Puff Frequency (min−1) |
---|---|---|---|---|
EHCSS-K6 | LOW4 | 40 | 1.2 | 4.0 |
EHCSS-K3 | LOW | 40 | 1.2 | 2.0 |
M6UK | LOW | 26 | 0.8 | 1.9 |
M6J | LOW | 15 | 0.7 | 0.9 |
PM1 | LOW | 29 | 0.9 | 3.6 |
Lark1 | LOW | 29 | 0.9 | 3.0 |
3.4.2. Mechanisms Influencing Time-Evolution of Aerosol Size
Evaporation or Hygroscopic Growth Effect
- Group 1: Assuming that the droplet surface temperature is uniform and does not change with time.
- Group 2: Assuming that no temperature gradient and species mass fraction gradient exist inside the droplets, i.e., infinite thermal conductivity and mass diffusivity in the liquid phase.
- Group 3: Taking into account the temperature gradient and mass fraction gradient inside droplets without considering the recirculation inside droplets (Hill’s vortex) which would enhance the effective thermal conductivity of the liquid.
- Group 4: Based on the Group 3 conditions, taking into account the recirculation effect by introducing a correction factor to the liquid thermal conductivity.
- Group 5: Describing the recirculation effect by simulation of the internal vortex dynamics.
- Group 6: Full solution of the multi-phase Navier-Stokes equations.
Particle-Particle Interactions
- (1)
- The initial acceleration phase: the cloud accelerate to its maximum velocity, during which the particles circulate in a toroidal vortex (Hill’s vortex) inside the cloud, in a manner similar to the heavy fluid inside a droplet descending in a lighter fluid. Chaotic fluctuations due to the particle-particle and particle-flow interactions will cause some particles to start cross the boundary of the closed surfaces (see Figure 6(a)).
- (2)
- The torus shape phase: The initial spherical shape cloud gradually evolves into a flattened oblate shape and eventually a torus due to the “leaking” of particles and the toroidal circulation motion (see Figure 6(b)).The torus expands until it reaches a critical aspect ratio.
- (3)
- The break-up phase: After the torus expands to the critical aspect ratio, it becomes instable and the cloud start to break into two and further four smaller particle clouds (see Figure 6(c) and (d)).
Charged-Particle Effect
4. Conclusions and Future Directions
4.1. Summary
- Inter-subject variability in respiratory tract geometry;
- Air-particle inlet conditions; and
- Type and properties of inhaled toxic aerosol.
4.2. Future Directions for Experimental Studies
- (1)
- High-resolution puff-by-puff measuring techniques for dense tobacco smoke. Present techniques and devices (e.g., Scanning Mobility Particle Sizer (SMPS), Optical Particle Counters (OPC), and Aerodynamic Particle Sizer (APS)) for measuring particle diameter time-evolution dynamics and deposition efficiency require diluted aerosol suspensions; thus, any influence of coagulation in the original dense suspensions is diminished [87]. Specifically, because most of the measurement techniques are low-time resolution, so that in order to capture aerosol particulate evolution, the high number concentration of the tobacco smoke need to be diluted [86]. Hence, high-time resolved, puff-by-puff measuring techniques have to be developed, and future work should focus on improving real-time quantitative measurements of key toxicants and nicotine inhaled and exhaled. This will allow improved estimates of regional depositions of toxic chemical species and particles to better improve dosimetry and quantitative risk assessment.
- (2)
- Pathological Biomarkers and Mechanisms. Although the causal relationship between smoking and several diseases has been well established, there is still little understanding of the underlying mechanisms. Furthermore, the health impact of the release of the volatile organic compounds from the “e-juice” and the release of e-cigarette particulate phase into the indoor environment are still mostly unknown [66]. Although many carcinogen biomarkers have been identified, difficulties exist in tracking them in the human lung airways and beyond. For example, amounts of strong carcinogens [31] are very limited per cigarette (i.e., 1–200 ng per cigarette). Therefore, available biomarkers need to be identified for further investigations.
4.3. Future Directions for CF-PD Simulations
- (1)
- Accurate Image Processing: Currently, 100% accurate realistic 3-D imaging and modeling of the entire human respiratory system is unrealistic for several reasons: (a) the resolution of CT/MRI is not sufficiently high to capture lung airway geometries on a small scale, i.e., airways exceeding generation 6 (G6); (b) the lung consists of 223 airways plus millions of alveoli; (c) in vivo measurements are difficult because the whole respiratory system geometry is time dependent according to the human respiratory movements [137]. Accurate and high-resolution image processing techniques of the future will be the cornerstone of CF-PD simulations of the transport and deposition of toxicants and carcinogens in the whole human respiratory system.
- (2)
- Realistic smoking inlet conditions. Most CF-PD simulations assumed that the aerosols are directly inhaled into the lung (e.g., without considering the closing of the soft palate during puffing). Thus, the following three steps of smoking, i.e., mouth hold, inhalation and exhalation must be accurately modeled due to their strong influences on aerosol size evolution [26,85]. Furthermore, the puffing strength is not constant during the consumption of one cigarette [11], i.e., it increases as the puff number increases.
- (3)
- Time-evolved aerosol size distribution release at the mouth inlet. Presently, assumed aerosol-size distributions at the mouth inlet, employed as boundary conditions for CF-PD simulations, are not time-developed. As it is evident from experiments, most smoke constituents feature a continuous increase from the first puff to the last puff. Also, for e-cigarettes (e.g., NJOY®), the aerosol concentration decreases rapidly as the puff number increases during smoking [11]. Furthermore, the transport of droplets probably suffers coalescence which would break the assumption of monodisperse particles. In this case the microscopic mechanism that lead to droplet coalescence need to be investigated and incorporated in the model, as well as the resulted polydisperse distribution. For accurate numerical prediction of the deposition patterns, time-evolved aerosol-size distributions of CSPs based on accurate experimental measurements are necessary.
- (4)
- Fluid-Structure Interaction. The assumption of rigid walls is a potentially misleading approximation considering that moving lung airway walls will influence the airflow characteristics and hence airflow-particle interaction in the near-wall region, thereby altering the deposition patterns of the particles. Thus, fluid-structure interaction (FSI) analysis should be introduced for the solution of airflow quantities (i.e., velocity, pressure and shear stress) impacted by continuously deforming geometries (i.e., near-mesh displacement and velocity), as well as the influence on the local DE of CSPs.
- (5)
- Coupled Droplet-Vapor Interaction. Currently, the vaporization of droplets with toxicants and vapor transport are uncoupled [62,63]. That is, except for water, the realistic vapor concentrations are ignored for the vaporization of officially identified toxicants in CSPs, while the vaporization mass is not considered in the mass transfer equation either. However, for more accurate modeling, the effect of coupled vaporization and vapor transfer should be investigated. Thus, the local vaporized mass of the objective toxicant has to be added to its vapor transport equation as a source term, while realistic vapor concentrations have to be employed in simulating the vaporization of species. In addition, the local and segmental mass loss due to wall deposition should be considered.
- (6)
- Nanoparticles/vapors in Tobacco Smoke. 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].
- (7)
- Particle Shape Effect. The filters of typical commercial cigarettes contain microscopic, needle-shaped shards of glass wool (like fiberglass insulation) which escape into the mouth and throat, and then lodge with tobacco tar in the lung tissue, surrounding the alveoli and lead to COPD, emphysema and eventually lung cancer. Numerous studies have demonstrated that the fiber aspect ratios as well as fiber durability are critical factors involved in pathogenicity [97]. Therefore, it is important to extend CF-PD modeling and accurately describe the orientation and transport of inhaled glass fibers.
Abbreviations
1-HOP | 1-Hydroxypyrene |
3-HPMA | 3-Hydroxypropylmercapturic Acid |
APS | Aerodynamic Particle Sizer |
CF-PD | Computational Fluid-Particle Dynamics |
COPD | Chronic Obstructive Pulmonary Disease |
CMD | Count Median Diameter |
CORESTA | Cooperation Centre for Scientific Research Relative to Tobacco |
CSEE | Cigarette Smoke Extract Exposure |
CSP | Cigarette Smoke Particles |
DE | Deposition Efficiency |
DEM | Discrete Element Method |
e-cigs | Electronic Cigarettes |
EHC | Electronic Heating Cigarettes |
ENDS | Electronic Nicotine Delivery Systems |
ETS | Environmental Tobacco Smoke |
FTC | Federal Trade Commission |
FSI | Fluid-Structure Interaction |
ISO | International Organization for Standardization |
LDE | Local Deposition Efficiency |
LHC | Less Harmful Cigarettes |
LLL | Left Lower Lung |
LUL | Left Upper Lung |
LUDEP | Lung Dose Evaluation Program |
MHBMA | Monohydroxy-3-Butenyl Mercapturic Acids |
MPPD | Multiple Path Particle Dosimetry |
MS | Mainstream Smoke |
NNAL | 4-(Methylnitrosamino)-1-(3-Pyridyl)-1-Butanol |
NNK | 4-(Methylnitrosamino)-1-(3-Pyridyl)-1-Butanone |
NNN | N'-Nitrosonornicotine |
OPC | Optical Particle Counters |
PAH | Polycyclic Aromatic Hydrocarbons |
PG | Propylene Glycol |
PREP | Potential Reduced Exposure Product |
PTR-MS | Proton-Transfer-Reaction Mass Spectrometry |
RH | Relative Humidity |
RLL | Right Lower Lung |
RML | Right Middle Lung |
RUL | Right Upper Lung |
SC | Safer Cigarettes |
SD | Standard Deviation |
SHS | Second-hand Smoke |
SMPS | Scanning Mobility Particle Sizer |
SPMA | S-Phenylmercapturic Acid |
TDE | Total Deposition Efficiency |
THR | Tobacco Harm Reduction |
TPM | Total Particulate Matter |
TSNA | Tobacco Specific Nitrosamines |
WSE | Whole Smoke Exposure |
WSM | Walton Smoking Machine |
Acknowledgements
Conflicts of Interest
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Kleinstreuer, C.; Feng, Y. Lung Deposition Analyses of Inhaled Toxic Aerosols in Conventional and Less Harmful Cigarette Smoke: A Review. Int. J. Environ. Res. Public Health 2013, 10, 4454-4485. https://doi.org/10.3390/ijerph10094454
Kleinstreuer C, Feng Y. Lung Deposition Analyses of Inhaled Toxic Aerosols in Conventional and Less Harmful Cigarette Smoke: A Review. International Journal of Environmental Research and Public Health. 2013; 10(9):4454-4485. https://doi.org/10.3390/ijerph10094454
Chicago/Turabian StyleKleinstreuer, Clement, and Yu Feng. 2013. "Lung Deposition Analyses of Inhaled Toxic Aerosols in Conventional and Less Harmful Cigarette Smoke: A Review" International Journal of Environmental Research and Public Health 10, no. 9: 4454-4485. https://doi.org/10.3390/ijerph10094454
APA StyleKleinstreuer, C., & Feng, Y. (2013). Lung Deposition Analyses of Inhaled Toxic Aerosols in Conventional and Less Harmful Cigarette Smoke: A Review. International Journal of Environmental Research and Public Health, 10(9), 4454-4485. https://doi.org/10.3390/ijerph10094454