Your search keyword '"June Feng"' showing total 9 results

1. Automated Solid Phase Extraction and Polarity-Switching Tandem Mass Spectrometry Technique for High Throughput Analysis of Urine Biomarkers for 14 Tobacco-related Compounds

Author

Sujeewa C. Piyankarage, Ernest McGahee, June Feng, Benjamin C. Blount, and Lanqing Wang

Subjects

Chemistry, QD1-999

Published

2021

2. Method for the Determination of Ammonia in Mainstream Cigarette Smoke Using Ion Chromatography.

Author

Christina Vaughan Watson, June Feng, Liza Valentin-Blasini, Rayman Stanelle, and Clifford H Watson

Subjects

Medicine, Science

Abstract

Ammonia in mainstream smoke is present in both the particulate and vapor phases. The presence of ammonia in the cigarette filler material and smoke is of significance because of the potential role ammonia could have in raising the "smoke pH." An increased smoke pH could shift a fraction of total nicotine to free-base nicotine, which is reportedly more rapidly absorbed by the smoker. Methods measuring ammonia in smoke typically employ acid filled impingers to trap the smoke. We developed a fast, reliable method to measure ammonia in mainstream smoke without the use of costly and time consuming impingers to examine differences in ammonia delivery. The method uses both a Cambridge filter pad and a Tedlar bag to capture particulate and vapor phases of the smoke. We quantified ammonia levels in the mainstream smoke of 50 cigarette brands from 5 manufacturers. Ammonia levels ranged from approximately 1μg to 23μg per cigarette for ISO smoking conditions and 38μg to 67μg per cigarette for Canadian intense smoking conditions and statistically significance differences were observed between brands and manufacturers. Our findings suggest that ammonia levels vary by brand and are higher under Canadian intense smoking conditions.

Published

2016

3. Validating Wave 1 (2014) Urinary Cotinine and TNE-2 Cut-points for Differentiating Wave 4 (2017) Cigarette Use from Non-use in the United States Using Data from the PATH Study.

Author

Edwards, Kathryn C., Khan, Asia, Sharma, Eva, Lanqing Wang, June Feng, Blount, Benjamin C., Sosnoff, Connie S., Smith, Danielle M., Goniewicz, Maciej L., Pearson, Jennifer, Villanti, Andrea C., Delnevo, Cristine D., Bover-Manderski, Michelle T., Hatsukami, Dorothy K., Niaura, Raymond, Everard, Colm, Kimmel, Heather L., Duffy, Kara, Rostron, Brian L., and Del Valle-Pinero, Arseima Y.

Abstract

Background: Sex and racial/ethnic identity-specific cut-points for validating tobacco use using Wave 1 (W1) of the Population Assessment of Tobacco and Health (PATH) Study were published in 2020. The current study establishes predictive validity of the W1 (2014) urinary cotinine and total nicotine equivalents-2 (TNE-2) cut-points on estimating Wave 4 (W4; 2017) tobacco use. Methods: For exclusive and polytobacco cigarette use, weighted prevalence estimates based on W4 self-report alone and with exceeding the W1 cut-point were calculated to identify the percentage missed without biochemical verification. Sensitivity and specificity of W1 cut-points on W4 self-reported tobacco use status were examined. ROC curves were used to determine the optimal W4 cut-points to distinguish past 30-day users from non-users, and evaluate whether the cut-points significantly differed from W1. Results: Agreement between W4 self-reported use and exceeding the W1 cut-points was high overall and when stratified by demographic subgroups (0.7%-4.4% of use was missed if relying on self-report alone). The predictive validity of using the W1 cut-points to classify exclusive cigarette and polytobacco cigarette use at W4 was high (>90% sensitivity and specificity, except among polytobacco Hispanic smokers). Cut-points derived using W4 data did not significantly differ from the W1-derived cut-points [e.g., W1 exclusive = 40.5 ng/mL cotinine (95% confidence interval, CI: 26.1-62.8), W4 exclusive = 29.9 ng/mL cotinine (95% CI: 13.5-66.4)], among most demographic subgroups. Conclusions: The W1 cut-points remain valid for biochemical verification of self-reported tobacco use in W4. Impact: Findings from can be used in clinical and epidemiologic studies to reduce misclassification of cigarette smoking status. [ABSTRACT FROM AUTHOR]

Published

2023

4. Urinary Cotinine and Cotinine + Trans-3'-Hydroxycotinine (TNE-2) Cut-points for Distinguishing Tobacco Use from Nonuse in the United States: PATH Study (2013-2014).

Author

Edwards, Kathryn C., Naz, Tasmia, Stanton, Cassandra A., Goniewicz, Maciej L., Hatsukami, Dorothy K., Smith, Danielle M., Lanqing Wang, Villanti, Andrea, Pearson, Jennifer, Blount, Benjamin C., Bansal-Travers, Maansi, June Feng, Niaura, Raymond, Manderski, Michelle T. Bover, Sosnoff, Connie S., Delnevo, Cristine D., Duffy, Kara, Del Valle-Pinero, Arseima Y., Rostron, Brian L., and Everard, Colm

Abstract

Background: Determine the overall, sex-, and racially/ethnically-appropriate population-level cotinine and total nicotine equivalents (TNE-2, the molar sum of the two major nicotine metabolites) cut-points to distinguish tobacco users from nonusers across multiple definitions of use (e.g., exclusive vs. polytobacco, and daily vs. non-daily). Methods: Using Wave 1 (2013-2014) of the U.S. Population Assessment of Tobacco and Health (PATH) Study, we conducted weighted Receiver Operating Characteristic (ROC) analysis to determine the optimal urinary cotinine and TNE-2 cut-points, stratified by sex and race/ethnicity. Results: For past 30-day exclusive cigarette users, the cotinine cut-point that distinguished them from nonusers was 40.5 ng/mL, with considerable variation by sex (male: 22.2 ng/mL; female: 43.1 ng/mL) and between racial/ethnic groups (non-Hispanic other: 5.2 ng/mL; non-Hispanic black: 297.0 ng/mL). A similar, but attenuated, pattern emerged when assessing polytobacco cigarette users (overall cut-point = 39.1 ng/mL, range = 5.5 ng/mL-80.4 ng/mL) and any tobacco users (overall cut-point = 39.1 ng/mL, range = 4.8 ng/mL-40.0 ng/mL). Using TNE-2, which is less impacted by racial differences in nicotine metabolism, produced a comparable pattern of results although reduced the range magnitude. Conclusions: Because of similar frequency of cigarette use among polytobacco users, overall cut-points for exclusive cigarette use were not substantially different from cut-points that included polytobacco cigarette use or any tobacco use. Results revealed important differences in sex and race/ethnicity appropriate cut-points when evaluating tobacco use status and established novel urinary TNE-2 cut-points. [ABSTRACT FROM AUTHOR]

Published

2021

5. Collaborative Method Performance Study of the Measurement of Nicotine, Its Metabolites, and Total Nicotine Equivalents in Human Urine.

Author

Lanqing Wang, Bernert, John T., Benowitz, Neal L., June Feng, Jacob III, Peyton, McGahee, Ernest, Caudill, Samuel P., Scherer, Gerhard, Scherer, Max, Pluym, Nikola, Doig, Mira V., Newland, Kirk, Murphy, Sharon E., Caron, Nicolas J., Sander, Lane C., Makiko Shimizu, Hiroshi Yamazaki, Sung Kim, Langman, Loralie J., and Pritchett, Jeanita S.

Abstract

Background: Biomarkers of tobacco exposure have a central role in studies of tobacco use and nicotine intake. The most significant exposure markers are nicotine itself and its metabolites in urine. Therefore, it is important to evaluate the performance of laboratories conducting these biomarker measurements. Methods: This report presents the results from a method performance study involving 11 laboratories from 6 countries that are currently active in this area. Each laboratory assayed blind replicates of seven human urine pools at various concentrations on three separate days. The samples included five pools blended from smoker and nonsmoker urine sources, and two additional blank urine samples fortified with pure nicotine, cotinine, and hydroxycotinine standards. All laboratories used their own methods, and all were based on some form of liquid chromatography/tandem mass spectrometry. Results: Overall, good agreement was found among the laboratories in this study. Intralaboratory precision was good, and in the fortified pools, the mean bias observed was < + 3.5% for nicotine, approximately 1.2% for hydroxycotinine, and less than 1% for cotinine (1 outlier excluded in each case). Both indirect and direct methods for analyzing the glucuronides gave comparable results. Conclusions: This evaluation indicates that the experienced laboratories participating in this study can produce reliable and comparable human urinary nicotine metabolic profiles in samples from people with significant recent exposure to nicotine. Impact: This work supports the reliability and agreement of an international group of established laboratories measuring nicotine and its metabolites in urine in support of nicotine exposure studies. [ABSTRACT FROM AUTHOR]

Published

2018

6. Nicotine, Carcinogen, and Toxin Exposure in Long-Term E-Cigarette and Nicotine Replacement Therapy Users: A Cross-sectional Study.

Author

Shahab, Lion, Goniewicz, Maciej L., Blount, Benjamin C., Brown, Jamie, McNeill, Ann, Alwis, Udeni, June Feng, Lanqing Wang, West, Robert, Alwis, K Udeni, Feng, June, and Wang, Lanqing

Subjects

ELECTRONIC cigarettes, NICOTINE replacement therapy, PHYSIOLOGICAL effects of nicotine, CARCINOGENS, NITROSOAMINES, BIOMARKERS, ORGANIC compound analysis, NICOTINE, ORGANIC compounds, PLANTS, RESEARCH funding, SMOKING cessation, TIME, CROSS-sectional method, EQUIPMENT & supplies

Abstract

Background: Given the rapid increase in the popularity of e-cigarettes and the paucity of associated longitudinal health-related data, the need to assess the potential risks of long-term use is essential.Objective: To compare exposure to nicotine, tobacco-related carcinogens, and toxins among smokers of combustible cigarettes only, former smokers with long-term e-cigarette use only, former smokers with long-term nicotine replacement therapy (NRT) use only, long-term dual users of both combustible cigarettes and e-cigarettes, and long-term users of both combustible cigarettes and NRT.Design: Cross-sectional study.Setting: United Kingdom.Participants: The following 5 groups were purposively recruited: combustible cigarette-only users, former smokers with long-term (≥6 months) e-cigarette-only or NRT-only use, and long-term dual combustible cigarette-e-cigarette or combustible cigarette-NRT users (n = 36 to 37 per group; total n = 181).Measurements: Sociodemographic and smoking characteristics were assessed. Participants provided urine and saliva samples and were analyzed for biomarkers of nicotine, tobacco-specific N-nitrosamines (TSNAs), and volatile organic compounds (VOCs).Results: After confounders were controlled for, no clear between-group differences in salivary or urinary biomarkers of nicotine intake were found. The e-cigarette-only and NRT-only users had significantly lower metabolite levels for TSNAs (including the carcinogenic metabolite 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanol [NNAL]) and VOCs (including metabolites of the toxins acrolein; acrylamide; acrylonitrile; 1,3-butadiene; and ethylene oxide) than combustible cigarette-only, dual combustible cigarette-e-cigarette, or dual combustible cigarette-NRT users. The e-cigarette-only users had significantly lower NNAL levels than all other groups. Combustible cigarette-only, dual combustible cigarette-NRT, and dual combustible cigarette-e-cigarette users had largely similar levels of TSNA and VOC metabolites.Limitation: Cross-sectional design with self-selected sample.Conclusion: Former smokers with long-term e-cigarette-only or NRT-only use may obtain roughly similar levels of nicotine compared with smokers of combustible cigarettes only, but results varied. Long-term NRT-only and e-cigarette-only use, but not dual use of NRTs or e-cigarettes with combustible cigarettes, is associated with substantially reduced levels of measured carcinogens and toxins relative to smoking only combustible cigarettes.Primary Funding Source: Cancer Research UK. [ABSTRACT FROM AUTHOR]

Published

2017

7. Simultaneous Determination of Multiple Drugs of Abuse and Relevant Metabolites in Urine by LC-MS-MS.

Author

June Feng, Lanqing Wang, Dai, Ingrid, Harmon, Tia, and Bennert, John T.

Subjects

*DRUGS of abuse, *METABOLITES, *URINE, *HIGH performance liquid chromatography, *ATMOSPHERIC pressure, *ATMOSPHERIC ionization, *MASS spectrometry, *ANALYTICAL toxicology, *RESEARCH, *QUALITATIVE chemical analysis

Abstract

The article presents analytical toxicology research into the simultaneous determination of multiple drugs of abuse and metabolites in human urine by high performance liquid chromatography-atmospheric pressure ionization-tandem mass spectrometry (HPLC-API-MS-MS). Drugs of abuse include benzodiazepines, opiates, methadone, barbiturates, phencyclidine, amphetamines, cannabinoids, and cocaine. Results suggest that HPLC-API-MS-MS is suitable for the qualitative analysis of drug categories in urine without requiring prior derivatization.

Published

2007

8. Properties of Mixed-Mode Parameters of Cascaded Balanced Networks and Their Applications in Modeling of Differential Interconnects.

Author

Hao Shi, Beyene, Wendemagegnehu T., June Feng, Ben Chia, and Xingchao Yuan

Subjects

INTEGRATED circuit interconnections, FERROELECTRIC RAM, FERROELECTRIC crystals, FERROELECTRIC devices, INTEGRATED circuits, SCATTERING (Physics)

Abstract

The cascading properties of general four-port networks are explored with respect to the standard to mixed-mode transformation of scattering matrices. Rigorous proofs are given to show that, for balanced networks, the odd-/even-mode scattering matrix of two cascaded networks equals the scattering matrix of the cascade of the respective odd-/even-mode networks. This concept is used to extract physical equivalent-circuit models for coupled backplane vias, differential package traces, and differentially routed data pins of XDR memory devices. [ABSTRACT FROM AUTHOR]

Published

2006

9. Performance Analysis and Model-to -Hardware Correlation of Multigigahertz Parallel Bus With Transmit Pre-Emphasis Equalization.

Author

Beyene, Wendemagegnehu T., June Feng, Cheng, Newton, and Xingchao Yuan

Subjects

*MICROWAVE attenuation, *CROSSTALK, *ELECTRIC impedance, *ELECTRIC interference, *ATTENUATION (Physics), *ELECTROACOUSTICS

Abstract

The performance of multigigahertz systems is adversely impacted by nonideal physical effects such as attenuation, crosstalk, impedance mismatches, intersymbol interference, and component and parameter variations. Many of these nonideal physical effects can be mitigated by selecting proper signaling topologies and techniques, by using judicious design rules, and by applying advanced circuitry and signal processing techniques. However, the component and parameter variations due to process and environmental conditions are more difficult to overcome, and their impact on a multigigahertz system needs to be quantified in order to ensure robust system operation under worst case operating conditions. This paper investigates the sensitivity of the performance of multigigahertz systems to component and paramaeter variations using simulations. The modeling accuracy of the equalized channel is correlated with a prototype system operating at data rates of up to 8 Gb/s. The sensitivity of equalization taps to variations in channel parameters is also studied. Finally, a measurement-based simulation method of evaluating the impact of transmitter and receiver jitter on the system timing margin is presented. [ABSTRACT FROM AUTHOR]

Published

2005