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2. Atypical RhoUV GTPases in development and disease

Author

Woo, Stephanie and Strasser, Leesa

Subjects
Biochemistry and Cell Biology, Biological Sciences, 2.1 Biological and endogenous factors, Generic health relevance, GTP-Binding Proteins, rho GTP-Binding Proteins, Signal Transduction, Cell Adhesion, EMT, Rho GTPases, RhoU, RhoV, cancer, embryogenesis, Medical Biochemistry and Metabolomics, Biochemistry & Molecular Biology, Biochemistry and cell biology
Abstract

RhoU and RhoV are members of the Rho family of small GTPases that comprise their own subfamily. RhoUV GTPases are classified as atypical due to the kinetics of their GTP/GDP binding cycles. They also possess unique N- and C-termini that regulate their subcellular localization and activity. RhoU and RhoV have been linked to cytoskeletal regulation, cell adhesion, and cell migration. They each exhibit distinct expression patterns during embryonic development and diseases such as cancer metastasis, suggesting they have specialized functions. In this review, we will discuss the known functions of RhoU and RhoV, with a focus on their roles in early development, organogenesis, and disease.

Published
2024

3. Effects of N-glycans on the structure of human IgA2

Author

Ruocco, Valentina, Grünwald-Gruber, Clemens, Rad, Behzad, Tscheliessnig, Rupert, Hammel, Michal, and Strasser, Richard

Subjects
Biochemistry and Cell Biology, Biological Sciences, Cancer, Biotechnology, 2.1 Biological and endogenous factors, IgA antibodies, N-linked glycan, SAXS, flexibility, protein assembly, protein stability, Biochemistry and cell biology, Medical biochemistry and metabolomics
Abstract

The transition of IgA antibodies into clinical development is crucial because they have the potential to create a new class of therapeutics with superior pathogen neutralization, cancer cell killing, and immunomodulation capacity compared to IgG. However, the biological role of IgA glycans in these processes needs to be better understood. This study provides a detailed biochemical, biophysical, and structural characterization of recombinant monomeric human IgA2, which varies in the amount/locations of attached glycans. Monomeric IgA2 antibodies were produced by removing the N-linked glycans in the CH1 and CH2 domains. The impact of glycans on oligomer formation, thermal stability, and receptor binding was evaluated. In addition, we performed a structural analysis of recombinant IgA2 in solution using Small Angle X-Ray Scattering (SAXS) to examine the effect of glycans on protein structure and flexibility. Our results indicate that the absence of glycans in the Fc tail region leads to higher-order aggregates. SAXS, combined with atomistic modeling, showed that the lack of glycans in the CH2 domain results in increased flexibility between the Fab and Fc domains and a different distribution of open and closed conformations in solution. When binding with the Fcα-receptor, the dissociation constant remains unaltered in the absence of glycans in the CH1 or CH2 domain, compared to the fully glycosylated protein. These results provide insights into N-glycans' function on IgA2, which could have important implications for developing more effective IgA-based therapeutics in the future.

Published
2024

4. Tender Topics: Exploring Sensitive Issues with Pre-K through First Grade Children through Read-Alouds

Author

Mankiw, Sue and Strasser, Janis

Abstract

The topics including bullying, family diversity, homelessness, disabilities, and incarceration are often referred to as "tender topics." They can be difficult for teachers to explain to or discuss with children. In their work with children, families, and teachers, the authors have seen that it is not necessarily the topic that makes conversations difficult, but who they are as individuals that determines their comfort level in addressing these subjects. It is important to view tender topics not as problems, but as subjects that are part of the everyday lives of children and families. However, some might see these topics as problems because children and adults don't know how to approach them, and are uncomfortable talking about them. In this article the authors offer some storybook suggestions that they have used to explain to children about tender topics. (Contains 4 resources and 10 online resources.)

Published
2013

5. Apposition of Fibroblasts With Metaplastic Gastric Cells Promotes Dysplastic Transition

Author

Lee, Su-Hyung, Panta, Ela W Contreras, Gibbs, David, Won, Yoonkyung, Min, Jimin, Zhang, Changqing, Roland, Joseph T, Hong, Se-Hoon, Sohn, Yoojin, Krystofiak, Evan, Jang, Bogun, Ferri, Lorenzo, Sangwan, Veena, Ragoussis, Jiannis, Camilleri-Broët, Sophie, Caruso, Joseph, Chen-Tanyolac, Chira, Strasser, Michael, Gascard, Philippe, Tlsty, Thea D, Huang, Sui, Choi, Eunyoung, and Goldenring, James R

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Stomach Cancer, Rare Diseases, Clinical Research, Digestive Diseases, 2.1 Biological and endogenous factors, Humans, Gastric Mucosa, Stomach Neoplasms, Hyperplasia, Metaplasia, Fibroblasts, Gastric Carcinogenesis, SPEM, PDGFRA, Clinical Sciences, Neurosciences, Paediatrics and Reproductive Medicine, Gastroenterology & Hepatology, Clinical sciences, Nutrition and dietetics
Abstract

Background & aimsElements of field cancerization, including atrophic gastritis, metaplasia, and dysplasia, promote gastric cancer development in association with chronic inflammation. However, it remains unclear how stroma changes during carcinogenesis and how the stroma contributes to progression of gastric preneoplasia. Here we investigated heterogeneity of fibroblasts, one of the most important elements in the stroma, and their roles in neoplastic transformation of metaplasia.MethodsWe used single-cell transcriptomics to evaluate the cellular heterogeneity of mucosal cells from patients with gastric cancer. Tissue sections from the same cohort and tissue microarrays were used to identify the geographical distribution of distinct fibroblast subsets. We further evaluated the role of fibroblasts from pathologic mucosa in dysplastic progression of metaplastic cells using patient-derived metaplastic gastroids and fibroblasts.ResultsWe identified 4 subsets of fibroblasts within stromal cells defined by the differential expression of PDGFRA, FBLN2, ACTA2, or PDGFRB. Each subset was distributed distinctively throughout stomach tissues with different proportions at each pathologic stage. The PDGFRα+ subset expanded in metaplasia and cancer compared with normal, maintaining a close proximity with the epithelial compartment. Co-culture of metaplasia- or cancer-derived fibroblasts with gastroids showing the characteristics of spasmolytic polypeptide-expressing metaplasia-induced disordered growth, loss of metaplastic markers, and increases in markers of dysplasia. Culture of metaplastic gastroids with conditioned media from metaplasia- or cancer-derived fibroblasts also promoted dysplastic transition.ConclusionsThese findings indicate that fibroblast associations with metaplastic epithelial cells can facilitate direct transition of metaplastic spasmolytic polypeptide-expressing metaplasia cell lineages into dysplastic lineages.

Published
2023

6. Concerted epithelial and stromal changes during progression of Barrett’s Esophagus to invasive adenocarcinoma exposed by multi-scale, multi-omics analysis

Author

Strasser, Michael K, Gibbs, David L, Gascard, Philippe, Bons, Joanna, Hickey, John W, Schürch, Christian M, Tan, Yuqi, Black, Sarah, Chu, Pauline, Ozkan, Alican, Basisty, Nathan, Sangwan, Veena, Rose, Jacob, Shah, Samah, Camilleri-Broet, Sophie, Fiset, Pierre-Oliver, Bertos, Nicolas, Berube, Julie, Djambazian, Haig, Li, Rui, Oikonomopoulos, Spyridon, Fels-Elliott, Daffolyn Rachael, Vernovsky, Sarah, Shimshoni, Elee, Collyar, Deborah, Russell, Ann, Ragoussis, Ioannis, Stachler, Matthew, Goldenring, James R, McDonald, Stuart, Ingber, Donald E, Schilling, Birgit, Nolan, Garry P, Tlsty, Thea D, Huang, Sui, and Ferri, Lorenzo E

Subjects
Biomedical and Clinical Sciences, Engineering, Biomedical Engineering, Cancer, Biotechnology, Rare Diseases, Digestive Diseases, 2.1 Biological and endogenous factors
Abstract

Esophageal adenocarcinoma arises from Barrett's esophagus, a precancerous metaplastic replacement of squamous by columnar epithelium in response to chronic inflammation. Multi-omics profiling, integrating single-cell transcriptomics, extracellular matrix proteomics, tissue-mechanics and spatial proteomics of 64 samples from 12 patients' paths of progression from squamous epithelium through metaplasia, dysplasia to adenocarcinoma, revealed shared and patient-specific progression characteristics. The classic metaplastic replacement of epithelial cells was paralleled by metaplastic changes in stromal cells, ECM and tissue stiffness. Strikingly, this change in tissue state at metaplasia was already accompanied by appearance of fibroblasts with characteristics of carcinoma-associated fibroblasts and of an NK cell-associated immunosuppressive microenvironment. Thus, Barrett's esophagus progresses as a coordinated multi-component system, supporting treatment paradigms that go beyond targeting cancerous cells to incorporating stromal reprogramming.

Published
2023

7. Relationships between the Nicotine Metabolite Ratio and a Panel of Exposure and Effect Biomarkers: Findings from Two Studies of U.S. Commercial Cigarette Smokers

Author

Carroll, Dana M, Murphy, Sharon E, Benowitz, Neal L, Strasser, Andrew A, Kotlyar, Michael, Hecht, Stephen S, Carmella, Steve G, McClernon, Francis J, Pacek, Lauren R, Dermody, Sarah S, Vandrey, Ryan G, Donny, Eric C, and Hatsukami, Dorothy K

Subjects
Tobacco, Brain Disorders, Prevention, Cancer, Clinical Research, Tobacco Smoke and Health, Substance Misuse, Respiratory, Good Health and Well Being, Adult, Biomarkers, Cigarette Smoking, Cotinine, Cross-Sectional Studies, Datasets as Topic, Female, Humans, Inflammation, Longitudinal Studies, Male, Middle Aged, Nicotine, Randomized Controlled Trials as Topic, Self Report, Severity of Illness Index, Smokers, Tobacco Use Disorder, United States, Medical and Health Sciences, Epidemiology
Abstract

BackgroundWe examined the nicotine metabolite ratio's (NMR) relationship with smoking intensity, nicotine dependence, and a broad array of biomarkers of exposure and biological effect in commercial cigarette smokers.MethodsSecondary analysis was conducted on two cross-sectional samples of adult, daily smokers from Wave 1 (2013-2014) of the Population Assessment of Tobacco Use and Health (PATH) Study and baseline data from a 2014-2017 randomized clinical trial. Data were restricted to participants of non-Hispanic, white race. The lowest quartile of NMR (

Published
2020

8. Mouth-Level Nicotine Intake Estimates from Discarded Filter Butts to Examine Compensatory Smoking in Low Nicotine Cigarettes

Author

Smith, Tracy T, Koopmeiners, Joseph S, Hatsukami, Dorothy K, Tessier, Katelyn M, Benowitz, Neal L, Murphy, Sharon E, Strasser, Andrew A, Tidey, Jennifer W, Blount, Benjamin C, Valentin, Liza, Bravo Cardenas, Roberto, Watson, Clifford, Pirkle, James L, and Donny, Eric C

Subjects
Tobacco, Substance Misuse, Prevention, Tobacco Smoke and Health, Drug Abuse (NIDA only), Clinical Research, Brain Disorders, Cardiovascular, Cancer, Respiratory, Good Health and Well Being, Adult, Cigarette Smoking, Female, Humans, Male, Middle Aged, Mouth, Nicotine, Smokers, Smoking Reduction, Terpenes, Tobacco Products, Medical and Health Sciences, Epidemiology
Abstract

BackgroundA mandated reduction in the nicotine content of cigarettes could reduce smoking rate and prevalence. However, one concern is that smokers may compensate by increasing the intensity with which they smoke each cigarette to obtain more nicotine. This study assessed whether smokers engage in compensatory smoking by estimating the mouth-level nicotine intake of low nicotine cigarettes smoked during a clinical trial.MethodsSmokers were randomly assigned to receive cigarettes with one of five nicotine contents for 6 weeks. An additional group received a cigarette with the lowest nicotine content, but an increased tar yield. The obtained mouth-level nicotine intake from discarded cigarette butts for a subset of participants (51-70/group) was estimated using solanesol as described previously. A compensation index was calculated for each group to estimate the proportion of nicotine per cigarette recovered through changes in smoking intensity.ResultsThere was no significant increase in smoking intensity for any of the reduced nicotine cigarettes as measured by the compensation index (an estimated 0.4% of the nicotine lost was recovered in the lowest nicotine group; 95% confidence interval, -0.1 to 1.2). There was a significant decrease in smoking intensity for very low nicotine content cigarettes with increased tar yield.ConclusionsReductions in nicotine content did not result in compensatory changes in how intensively participants smoked research cigarettes.ImpactCombined with data from clinical trials showing a reduction in cigarettes smoked per day, these data suggest that a reduction in nicotine content is unlikely to result in increased smoke exposure.

Published
2020

9. Effects of immediate versus gradual nicotine reduction in cigarettes on biomarkers of biological effects

Author

Hatsukami, Dorothy K, Luo, Xianghua, Heskin, Alisa K, Tang, Mei Kuen, Carmella, Steven G, Jensen, Joni, Robinson, Jason D, Vandrey, Ryan, Drobes, David J, Strasser, Andrew A, al'Absi, Mustafa, Leischow, Scott, Cinciripini, Paul M, Koopmeiners, Joseph, Ikuemonisan, Joshua, Benowitz, Neal L, Donny, Eric C, and Hecht, Stephen S

Subjects
Clinical and Health Psychology, Public Health, Health Sciences, Psychology, Clinical Trials and Supportive Activities, Cancer, Tobacco Smoke and Health, Prevention, Tobacco, Drug Abuse (NIDA only), Substance Misuse, Clinical Research, Respiratory, Cardiovascular, Good Health and Well Being, Adult, Bayes Theorem, Biomarkers, C-Reactive Protein, Cigarette Smoking, Dinoprost, Dinoprostone, Erythrocyte Count, Erythrocyte Indices, Female, Humans, Inflammation, Leukocyte Count, Male, Middle Aged, Nicotine, Nicotinic Agonists, Oxidative Stress, Platelet Count, Smoking Reduction, Tobacco Products, Biomarkers of biological effects, hematological parameters, immediate versus gradual nicotine reduction, inflammation, oxidative stress, reduced nicotine content cigarettes, Medical and Health Sciences, Psychology and Cognitive Sciences, Substance Abuse, Public health, Clinical and health psychology
Abstract

AimA previous study showed significantly greater reductions in number of cigarettes smoked and biomarkers of toxicant and carcinogen exposure in smokers assigned to immediate reduction of nicotine in cigarettes to very low levels versus gradually over time or continued smoking of normal nicotine content cigarettes. This study examines the effects of these approaches on selected biomarkers associated with harmful biological effects.DesignThree-arm, randomized controlled trial.SettingTen United States academic institutional sites.ParticipantsDaily smokers uninterested in quitting smoking with a mean age of 45.1 [standard deviation (SD) = 13.4)] years and smoking 17.1 (SD = 8.5) cigarettes/day; 43.9% (549 of 1250) female; 60.6% (758 of 1250) white ethnicity.Interventions(1) Smoking cigarettes where nicotine content was immediately reduced to very low levels (n = 503); (2) smoking cigarettes where nicotine content was gradually reduced, with dose changes occurring monthly (n = 498); and (3) continued smoking with normal nicotine content cigarettes (n = 249).MeasurementsSmokers were assessed at baseline while smoking their usual brand cigarettes, and again at 4, 8, 12, 16 and 20 weeks. Outcomes were areas under the concentration time curve (AUC) for the period of study of biomarkers of inflammation, oxidative stress and hematological parameters.FindingsNo consistent significant differences were observed across groups (Bayes factors showing data to be insensitive), with the only exception being red blood cell size variability, which was observed to be lower in the immediate versus gradual nicotine reduction [mean difference =  -0.11; 95% confidence interval (CI) = -0.18, -0.04, P = 0.004] and normal nicotine control groups (mean difference = - 0.15, 95% CI = -0.23, -0.06, P = 0.001).ConclusionIt remains unclear whether switching to very low nicotine cigarettes leads to a short-term reduction in biomarkers of tobacco-related harm.

Published
2019

11. Longitudinal stability in cigarette smokers of urinary biomarkers of exposure to the toxicants acrylonitrile and acrolein

Author

Chen, Menglan, Carmella, Steven G, Sipe, Chistopher, Jensen, Joni, Luo, Xianghua, Le, Chap T, Murphy, Sharon E, Benowitz, Neal L, McClernon, F Joseph, Vandrey, Ryan, Allen, Sharon S, Denlinger-Apte, Rachel, Cinciripini, Paul M, Strasser, Andrew A, al’Absi, Mustafa, Robinson, Jason D, Donny, Eric C, Hatsukami, Dorothy, and Hecht, Stephen S

Subjects
Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Substance Misuse, Tobacco Smoke and Health, Clinical Trials and Supportive Activities, Prevention, Pediatric Research Initiative, Clinical Research, Tobacco, Cancer, Good Health and Well Being, Acetylcysteine, Acrolein, Acrylonitrile, Adult, Biomarkers, Cigarette Smoking, Female, Hazardous Substances, Humans, Longitudinal Studies, Male, Middle Aged, Randomized Controlled Trials as Topic, Smokers, Tobacco Products, Toxicology, General Science & Technology
Abstract

The urinary metabolites cyanoethyl mercapturic acid (CEMA) and 3-hydroxypropyl mercapturic acid (3-HPMA) have been widely used as biomarkers of exposure to acrylonitrile and acrolein, respectively, but there are no published data on their consistency over time in the urine of cigarette smokers. We provided, free of charge over a 20 week period, Spectrum NRC600/601 research cigarettes to cigarette smokers in the control arm of a randomized clinical trial of the reduced nicotine cigarette. Urine samples were collected at weeks 4, 8, 12, 16, and 20 and analyzed for CEMA and 3-HPMA, and total nicotine equivalents (TNE) using validated methods. Creatinine-corrected intra-class correlation coefficients for CEMA, 3-HPMA, and TNE were 0.67, 0.46, and 0.68, respectively, indicating good longitudinal consistency for CEMA, while that of 3-HPMA was fair. A strong correlation between CEMA and TNE values was observed. These data support the use of CEMA as a reliable biomarker of tobacco smoke exposure. This is the first report of the longitudinal stability of the biomarkers of acrylonitrile and acrolein exposure in smokers. The data indicate that CEMA, the biomarker of acrylonitrile exposure, is consistent over time in cigarette smokers, supporting its use. While 3-HPMA levels were less stable over time, this biomarker is nevertheless a useful monitor of human acrolein exposure because of its specificity to this toxicant.

Published
2019

12. Longitudinal stability in cigarette smokers of urinary eicosanoid biomarkers of oxidative damage and inflammation

Author

Carmella, Steven G, Heskin, Alisa K, Tang, Mei Kuen, Jensen, Joni, Luo, Xianghua, Le, Chap T, Murphy, Sharon E, Benowitz, Neal L, McClernon, F Joseph, Vandrey, Ryan, Allen, Sharon S, Denlinger-Apte, Rachel, Cinciripini, Paul M, Strasser, Andrew A, al’Absi, Mustafa, Robinson, Jason D, Donny, Eric C, Hatsukami, Dorothy K, and Hecht, Stephen S

Subjects
Analytical Chemistry, Biomedical and Clinical Sciences, Chemical Sciences, Tobacco Smoke and Health, Tobacco, Prevention, Cancer, Clinical Research, Good Health and Well Being, Biomarkers, Body Mass Index, Cigarette Smoking, Dinoprost, Eicosanoids, F2-Isoprostanes, Female, Humans, Inflammation, Male, Metabolome, Middle Aged, Oxidative Stress, General Science & Technology
Abstract

The urinary metabolites (Z)-7-[1R,2R,3R,5S)-3,5-dihydroxy-2-[(E,3S)-3-hydroxyoct-1-enyl]cyclopentyl]hept-5-enoic acid (8-iso-PGF2α), an F2-isoprostane and biomarker of oxidative damage, and "prostaglandin E2 metabolite" (PGE-M), a biomarker of inflammation, are elevated in cigarette smokers. However, there is little information in the literature on the longitudinal stability of these widely used biomarkers. In a large clinical trial involving 10 institutional sites, smokers were given, free of charge over a period of 20 weeks, Spectrum NRC600/601 research cigarettes containing 15.5 mg nicotine/g tobacco. All participants were instructed to smoke these cigarettes for the duration of the study. At weeks 4, 8, 12, 16, and 20, first morning urine voids were collected and analyzed for 8-iso-PGF2α and PGE-M using validated liquid chromatography-electrospray ionization-tandem mass spectrometry methods. The mean level of 8-iso-PGF2α at Week 4 was 1.34 ± 1.08 (S.D.) pmol/mg creatinine (N = 226) while that of PGE-M was 73.7 ± 113 (S.D.) pmol/mg creatinine (N = 232). The corresponding levels at Week 20 were 1.35 ± 0.93 (S.D.) pmol/mg creatinine (N = 209) for 8-iso-PGF2α and 74.2 ± 142 (S.D.) pmol/mg creatinine (N = 210) for PGE-M. There was variation in these values in the intervening weeks. The intra-class correlation coefficients (ICC) were 0.51 (95% CI, 0.45, 0.57) and 0.36 (0.30, 0.43), for 8-iso-PGF2α and PGE-M, respectively, indicating fair longitudinal stability for 8-iso-PGF2α and poorer longitudinal stability for PGE-M in cigarette smokers. Males had higher ICC values than females for both 8-iso-PGF2α and PGE-M. These results indicate that, in addition to cigarette smoking, endogenous processes of oxidative damage and inflammation influence the levels of these biomarkers over time among current smokers.

Published
2019

13. Whether to push or pull? Nicotine reduction and non-combusted alternatives - Two strategies for reducing smoking and improving public health

Author

Smith, Tracy T, Hatsukami, Dorothy K, Benowitz, Neal L, Colby, Suzanne M, McClernon, F Joseph, Strasser, Andrew A, Tidey, Jennifer W, White, Cassidy M, and Donny, Eric C

Subjects
Public Health, Health Sciences, Prevention, Drug Abuse (NIDA only), Tobacco, Substance Misuse, Brain Disorders, Tobacco Smoke and Health, 3.1 Primary prevention interventions to modify behaviours or promote wellbeing, Prevention of disease and conditions, and promotion of well-being, Respiratory, Cancer, Good Health and Well Being, Behavior, Addictive, Electronic Nicotine Delivery Systems, Humans, Nicotine, Smoking Reduction, Tobacco Smoking, Nicotine reduction, Alternative nicotine delivery systems, E-cigarettes, Endgame, Human Movement and Sports Sciences, Public Health and Health Services, Epidemiology, Public health
Abstract

Combustible cigarettes remain the most harmful and addictive tobacco product, and reducing the prevalence of smoking continues to be a critical public health goal. While nicotine is the constituent primarily responsible for addiction to cigarettes, most of the harm associated with smoking comes from byproducts of tobacco combustion. Recently, two different approaches for reducing the harms of smoking have emerged, both of which focus on breaking the link between the addiction to nicotine and the harms caused by smoking. First, the addictive potential of cigarettes could be minimized by requiring a large reduction in the nicotine content of cigarettes. Evidence for a nicotine reduction policy thus far shows that the use of very low nicotine content cigarettes results in a reduction in the number of cigarettes people smoke per day and a reduction in cigarette dependence. Second, emerging alternative nicotine delivery systems (ANDS) like electronic cigarettes may provide sufficient nicotine to act as substitutes for cigarettes while delivering much lower levels of toxicants. Evidence suggests that the emergence of ANDS has increased the percentage of smokers who are able to quit. The present paper will briefly review the evidence for each of these approaches, and consider what contemporary reinforcement and addiction theories can tell us about their likely success. We argue that the most effective endgame approach is one that pursues both nicotine reduction and alternative nicotine delivery systems as complementary.

Published
2018

14. Effect of Immediate vs Gradual Reduction in Nicotine Content of Cigarettes on Biomarkers of Smoke Exposure: A Randomized Clinical Trial

Author

Hatsukami, Dorothy K, Luo, Xianghua, Jensen, Joni A, al’Absi, Mustafa, Allen, Sharon S, Carmella, Steven G, Chen, Menglan, Cinciripini, Paul M, Denlinger-Apte, Rachel, Drobes, David J, Koopmeiners, Joseph S, Lane, Tonya, Le, Chap T, Leischow, Scott, Luo, Kai, McClernon, F Joseph, Murphy, Sharon E, Paiano, Viviana, Robinson, Jason D, Severson, Herbert, Sipe, Christopher, Strasser, Andrew A, Strayer, Lori G, Tang, Mei Kuen, Vandrey, Ryan, Hecht, Stephen S, Benowitz, Neal L, and Donny, Eric C

Subjects
Cancer, Clinical Trials and Supportive Activities, Prevention, Clinical Research, Tobacco, Tobacco Smoke and Health, 3.1 Primary prevention interventions to modify behaviours or promote wellbeing, Prevention of disease and conditions, and promotion of well-being, Respiratory, Good Health and Well Being, Acetylcysteine, Adult, Area Under Curve, Biomarkers, Breath Tests, Carbon Monoxide, Creatinine, Double-Blind Method, Female, Humans, Male, Middle Aged, Nicotine, Phenanthrenes, Smoke, Smoking Cessation, Substance Withdrawal Syndrome, Tobacco Products, Tobacco Use Disorder, Medical and Health Sciences, General & Internal Medicine
Abstract

ImportanceThe optimal temporal approach for reducing nicotine to minimally or nonaddictive levels in all cigarettes sold in the United States has not been determined.ObjectivesTo determine the effects of immediate vs gradual reduction in nicotine content to very low levels and as compared with usual nicotine level cigarettes on biomarkers of toxicant exposure.Design, setting, and participantsA double-blind, randomized, parallel-design study with 2 weeks of baseline smoking and 20 weeks of intervention was conducted at 10 US sites. A volunteer sample of daily smokers with no intention to quit within 30 days was recruited between July 2014 and September 2016, with the last follow-up completed in March 2017.Interventions(1) Immediate reduction to 0.4 mg of nicotine per gram of tobacco cigarettes; (2) gradual reduction from 15.5 mg to 0.4 mg of nicotine per gram of tobacco cigarettes with 5 monthly dose changes; or (3) maintenance on 15.5 mg of nicotine per gram of tobacco cigarettes.Main outcomes and measuresBetween-group differences in 3 co-primary biomarkers of smoke toxicant exposure: breath carbon monoxide (CO), urine 3-hydroxypropylmercapturic acid (3-HPMA, metabolite of acrolein), and urine phenanthrene tetraol (PheT, indicator of polycyclic aromatic hydrocarbons) calculated as area under the concentration-time curve over the 20 weeks of intervention.ResultsAmong 1250 randomized participants (mean age, 45 years; 549 women [44%]; 958 [77%] completed the trial), significantly lower levels of exposure were observed in the immediate vs gradual reduction group for CO (mean difference, -4.06 parts per million [ppm] [95% CI, -4.89 to -3.23]; P

Published
2018

15. Association of Reduced Nicotine Content Cigarettes With Smoking Behaviors and Biomarkers of Exposure Among Slow and Fast Nicotine Metabolizers: A Nonrandomized Clinical Trial.

Author

Mercincavage, Melissa, Lochbuehler, Kirsten, Wileyto, E Paul, Benowitz, Neal L, Tyndale, Rachel F, Lerman, Caryn, and Strasser, Andrew A

Subjects
Humans, Tobacco Use Disorder, Carbon Monoxide, Nicotine, Creatinine, Nicotinic Agonists, Linear Models, Smoking, Adult, Aged, Middle Aged, Academic Medical Centers, Philadelphia, Female, Male, Young Adult, Tobacco Products, Biomarkers, Substance Abuse, Tobacco, Clinical Research, Tobacco Smoke and Health, Prevention, 3.1 Primary prevention interventions to modify behaviours or promote well-being, Cancer
Abstract

ImportanceThe US Food and Drug Administration (FDA) has announced its intention to reduce the nicotine content in combustible cigarettes but must base regulation on public health benefits. Fast nicotine metabolizers may be at risk for increased smoking following a national nicotine reduction policy. We hypothesized that using reduced nicotine content (RNC) cigarettes would be associated with increases in smoking behaviors and exposure among smokers with a fast-but not slow-nicotine-metabolite ratio (NMR).ObjectivesTo examine the association of RNC cigarettes with smoking behaviors and biomarkers of exposure and to compare these associations in fast and slow metabolizers of nicotine based on the NMR.Design setting and participantsA 35-day, 3-period, within-participant nonrandomized clinical trial was conducted at an academic medical center in Philadelphia, Pennsylvania. A 5-day baseline period using the smokers' preferred brand of cigarettes was followed by 2 consecutive 15-day periods using free investigational RNC cigarettes. A total of 100 daily, non-treatment-seeking, nonmenthol cigarette smokers (59 fast, 41 slow metabolizers) were recruited from December 24, 2013, to December 2, 2015. Data analysis was performed from December 12, 2016, to January 3, 2018.InterventionsTwo 15-day periods using cigarettes containing 5.2 mg (RNC1) and 1.3 mg (RNC2) of nicotine per gram of tobacco.Main outcomes and measuresSmoking behaviors (number of cigarettes per day [CPD], total puff volume) and biomarkers of exposure (carbon monoxide [CO], urine total nicotine equivalents [TNE], and 4-[methylnitrosamino]-1-[3-pyridyl]-1-butanol [NNAL]).ResultsSmokers (73 [73.0%] men; 74 [74.0%] white; mean [SD] age, 43.02 [12.13] years; mean [SD] CPD, 17.31 [5.72]) consumed 2.62 (95% CI, 1.54-3.70) more CPD during the RNC1 period vs their preferred brand during baseline (P < .001) and approximated baseline CPD during the RNC2 period (mean difference, 0.96 [95% CI, -0.36 to 2.28]; P = .24). Additional outcome measures were lower during both RNC periods vs baseline (total puff volume, mean [95% CI]: RNC1, 537 mL [95% CI, 479-595 mL]; RNC2, 598 mL [95% CI, 547-649 mL] vs baseline, 744 mL [95% CI, 681-806 mL]; TNE, mean [95% CI]: RNC1, 30.9 nmoL/mg creatinine [95% CI, 26.0-36.6 nmoL/mg]; RNC2, 22.8 nmoL/mg creatinine [95% CI, 17.8-29.0 nmoL/mg] vs baseline, 54.6 nmoL/mg creatinine [95% CI, 48.1-62.1 nmoL/mg]; and NNAL, mean [95% CI]: RNC1, 229 pg/mg creatinine [95% CI, 189-277 pg/mg]; RNC2, 190 pg/mg creatinine [95% CI, 157-231 pg/mg] vs baseline, 280 pg/mg creatinine [95% CI, 231-339 pg/mg]; all P < .001). Carbon monoxide measures were similar across study periods (CO boost [SD], RNC1, 4.6 ppm [4.1-5.1 ppm]; RNC2, 4.2 ppm [3.7-4.6 ppm]; and baseline, 4.4 ppm [3.8-4.9 ppm]). The RNC cigarette associations did not differ by NMR.Conclusions and relevanceBoth RNC cigarettes were associated with decreased puffing and urinary biomarker exposure but not with decreased daily cigarette consumption or CO levels. The NMR did not moderate associations at the nicotine levels tested, suggesting that fast metabolizers may not be at greater risk of increasing use or exposure from these products should the FDA mandate an RNC standard for cigarettes.

Published
2018

16. Estimations and predictors of non‐compliance in switchers to reduced nicotine content cigarettes

Author

Nardone, Natalie, Donny, Eric C, Hatsukami, Dorothy K, Koopmeiners, Joseph S, Murphy, Sharon E, Strasser, Andrew A, Tidey, Jennifer W, Vandrey, Ryan, and Benowitz, Neal L

Subjects
Biological Psychology, Psychology, Clinical Trials and Supportive Activities, Tobacco, Clinical Research, Tobacco Smoke and Health, 3.1 Primary prevention interventions to modify behaviours or promote wellbeing, Cancer, Good Health and Well Being, Adult, Biomarkers, Double-Blind Method, Female, Ganglionic Stimulants, Healthy Volunteers, Humans, Male, Nicotine, Patient Compliance, Saliva, Smoking Reduction, Tobacco Products, Urinalysis, cigarette smoking, cotinine, nicotine reduction, reduced nicotine content cigarettes, total nicotine equivalents, Medical and Health Sciences, Psychology and Cognitive Sciences, Substance Abuse, Public health, Clinical and health psychology
Abstract

Background and aimsClinical trials on the impact and safety of reduced nicotine content cigarettes (RNCs) are ongoing, and an important methodological concern is participant compliance with smoking only RNCs. Our aims were to measure non-compliance biochemically with urine cotinine (COT) and total nicotine equivalents (TNEs), compare with self-reported non-compliance and identify associated covariates.DesignSecondary analysis of a double-blind, parallel, randomized clinical trial.SettingResearch centers from the United States, enrolling participants from June 2013 to July 2014.ParticipantsVolunteer sample of 242 participants (55% Caucasian), average age of 41.2 years, smoking at least five cigarettes per day (CPD).InterventionSmoking very low nicotine cigarettes (VLNCs; 0.4 mg nicotine/g tobacco) for 6 weeks.MeasurementsThe primary outcome was biochemically verified non-compliance, measured as thresholds of COT/CPD and TNE/CPD ratios, considering changes in nicotine content from conventional levels to VLNCs, and as an absolute threshold of week 6 TNEs. Self-reported non-compliance was measured via daily phone calls. Key predictors included age, sex, race, menthol preference, nicotine metabolite ratio, time to first cigarette, dependence, CPD, TNEs, tar level and cigarette evaluation.FindingsEstimates of non-compliance with smoking the VLNCs exclusively include: the biochemical ratios (both 78%), the week 6 TNE threshold (76%) and self-report (39%). Of the key covariates, age, dependence and cigarette evaluations of satisfaction were significant; for age, younger participants more likely to be non-compliant [P = 0.01; odds ratio (OR) = 0.98, 95% confidence interval (CI) = 0.96-0.99]. Dependence was associated significantly with self-reported non-compliance (P = 0.01; OR = 1.28, 95% CI = 1.06-1.55). Cigarette evaluations of satisfaction were associated significantly with non-compliance (P = 0.001; OR = 0.71, 95% CI = 0.61-0.82).ConclusionsAmong smokers volunteering to smoke only very low nicotine cigarettes for 6 weeks, non-compliance was common and biochemical assessments detected more cases of non-compliance than self-report. Despite high levels of non-compliance, smokers reduced their intake of nicotine by an average of 60%.

Published
2016

17. Nicotine Replacement, Topography, and Smoking Phenotypes of E-cigarettes

Author

Strasser, Andrew A, Souprountchouk, Valentina, Kaufmann, Amanda, Blazekovic, Sonja, Leone, Frank, Benowitz, Neal L, and Schnoll, Robert A

Subjects
Epidemiology, Health Sciences, Tobacco, Substance Misuse, Tobacco Smoke and Health, Cancer, Good Health and Well Being, cotinine, e-cigarette, nicotine craving, nicotine withdrawal, smoking behavior, vaping
Abstract

ObjectivesLittle is known about the degree of nicotine replacement across first-generation e-cigarette brands, how e-cigarettes are used, and if there is variation across brands in relevant smoking phenotypes. The objective of this project was to collect data that are critical to better understanding, use, and exposure when using e-cigarettes, which may then inform clinical trials and tobacco regulatory policy.MethodsTwenty-eight cigarette smokers were randomized to use one of 5 popular brands of e-cigarettes for a 10-day study. Day 1 (own cigarette brand) data established baseline levels for cotinine, carbon monoxide (CO), topography, cigarette liking, withdrawal, and craving. Participants returned on Days 5 and 10 to reassess these measures while exclusively using e-cigarettes.ResultsCompared to cigarette smoking, e-cigarettes provided significantly lower nicotine levels (25%-50%), reduced CO exposure, and lower ratings of liking (p < .05). Topography significantly differed between cigarette and e-cigarette sessions (p < .05). All brands significantly reduced withdrawal and craving (p < .05). There were no significant brand differences in outcome measures associated with exposure or use.ConclusionsE-cigarettes are not liked as much as cigarettes, provide significantly lower nicotine replacement, reduce CO exposure, and mitigate withdrawal and craving. The patterns of use significantly differ compared to cigarette smoking.

Published
2016

18. Randomized Trial of Reduced-Nicotine Standards for Cigarettes

Author

Donny, Eric C, Denlinger, Rachel L, Tidey, Jennifer W, Koopmeiners, Joseph S, Benowitz, Neal L, Vandrey, Ryan G, al'Absi, Mustafa, Carmella, Steven G, Cinciripini, Paul M, Dermody, Sarah S, Drobes, David J, Hecht, Stephen S, Jensen, Joni, Lane, Tonya, Le, Chap T, McClernon, F Joseph, Montoya, Ivan D, Murphy, Sharon E, Robinson, Jason D, Stitzer, Maxine L, Strasser, Andrew A, Tindle, Hilary, and Hatsukami, Dorothy K

Subjects
Clinical Trials and Supportive Activities, Substance Misuse, Tobacco Smoke and Health, Clinical Research, Drug Abuse (NIDA only), Brain Disorders, Tobacco, Prevention, Prevention of disease and conditions, and promotion of well-being, Evaluation of treatments and therapeutic interventions, 3.1 Primary prevention interventions to modify behaviours or promote wellbeing, 6.1 Pharmaceuticals, Cancer, Good Health and Well Being, Biomarkers, Creatinine, Double-Blind Method, Humans, Inhalation Exposure, Linear Models, Nicotine, Substance Withdrawal Syndrome, Tars, Tobacco Products, Tobacco Use Disorder, United States, United States Food and Drug Administration, Medical and Health Sciences, General & Internal Medicine
Abstract

BackgroundThe Food and Drug Administration can set standards that reduce the nicotine content of cigarettes.MethodsWe conducted a double-blind, parallel, randomized clinical trial between June 2013 and July 2014 at 10 sites. Eligibility criteria included an age of 18 years or older, smoking of five or more cigarettes per day, and no current interest in quitting smoking. Participants were randomly assigned to smoke for 6 weeks either their usual brand of cigarettes or one of six types of investigational cigarettes, provided free. The investigational cigarettes had nicotine content ranging from 15.8 mg per gram of tobacco (typical of commercial brands) to 0.4 mg per gram. The primary outcome was the number of cigarettes smoked per day during week 6.ResultsA total of 840 participants underwent randomization, and 780 completed the 6-week study. During week 6, the average number of cigarettes smoked per day was lower for participants randomly assigned to cigarettes containing 2.4, 1.3, or 0.4 mg of nicotine per gram of tobacco (16.5, 16.3, and 14.9 cigarettes, respectively) than for participants randomly assigned to their usual brand or to cigarettes containing 15.8 mg per gram (22.2 and 21.3 cigarettes, respectively; P

Published
2015

24. Australian recommendations for the management of hepatocellular carcinoma: a consensus statement.

Author

Lubel, John S, Roberts, Stuart K, Strasser, Simone I, Thompson, Alexander J, Philip, Jennifer, Goodwin, Mark, Clarke, Stephen, Crawford, Darrell HG, Levy, Miriam T, and Shackel, Nick

Abstract

Introduction: Hepatocellular carcinoma (HCC) is a leading cause of cancer deaths both globally and in Australia. Surveillance for HCC in at‐risk populations allows diagnosis at an early stage, when potentially curable. However, most Australians diagnosed with HCC die of the cancer or of liver disease. In the changing landscape of HCC management, unique challenges may lead to clinical practice variation. As a result, there is a need to identify best practice management of HCC in an Australian context. This consensus statement has been developed for health professionals involved in the care of adult patients with HCC in Australia. It is applicable to specialists, general medical practitioners, nurses, health coordinators and hospital administrators. Methods and recommendations: This statement has been developed by specialists in hepatology, radiology, surgery, oncology, palliative care, and primary care, including medical practitioners and nurses. The statement addresses four main areas relevant to HCC management: epidemiology and incidence, diagnosis, treatment, and patient management. A modified Delphi process was used to reach consensus on 31 recommendations. Principal recommendations include the adoption of surveillance strategies, use of multidisciplinary meetings, diagnosis, treatment options and patient management. Changes in management as a result of this statement: This consensus statement will simplify HCC patient management and reduce clinical variation. Ultimately, this should result in better outcomes for patients with HCC. [ABSTRACT FROM AUTHOR]

Published
2021
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25. ESPEN practical guideline: Clinical Nutrition in cancer.

Author

Muscaritoli, Maurizio, Arends, Jann, Bachmann, Patrick, Baracos, Vickie, Barthelemy, Nicole, Bertz, Hartmut, Bozzetti, Federico, Hütterer, Elisabeth, Isenring, Elizabeth, Kaasa, Stein, Krznaric, Zeljko, Laird, Barry, Larsson, Maria, Laviano, Alessandro, Mühlebach, Stefan, Oldervoll, Line, Ravasco, Paula, Solheim, Tora S., Strasser, Florian, and de van der Schueren, Marian

Abstract

This practical guideline is based on the current scientific ESPEN guidelines on nutrition in cancer patients. ESPEN guidelines have been shortened and transformed into flow charts for easier use in clinical practice. The practical guideline is dedicated to all professionals including physicians, dieticians, nutritionists and nurses working with patients with cancer. A total of 43 recommendations are presented with short commentaries for the nutritional and metabolic management of patients with neoplastic diseases. The disease-related recommendations are preceded by general recommendations on the diagnostics of nutritional status in cancer patients. This practical guideline gives guidance to health care providers involved in the management of cancer patients to offer optimal nutritional care. [ABSTRACT FROM AUTHOR]

Published
2021
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26. Hepatitis B management during immunosuppression for haematological and solid organ malignancies: an Australian consensus statement.

Author

Doyle, Joseph, Raggatt, Michelle, Slavin, Monica, McLachlan, Sue‐Anne, Strasser, Simone I, Sasadeusz, Joseph J, Howell, Jessica, Hajkowicz, Krispin, Nandurkar, Harshal, Johnston, Anna, Bak, Narin, Thompson, Alexander J, and McLachlan, Sue-Anne

Abstract

Introduction: Individuals with chronic hepatitis B virus (HBV) infection or past exposure to HBV infection have a substantial risk of reactivation during immunosuppressive cancer therapy. HBV reactivation can lead to liver failure, cancer treatment interruption or death. Clinical concordance with screening and treatment guidelines is inconsistent in practice, and existing international guidelines are not specific to the Australian context. We developed an Australian consensus statement with infectious diseases, hepatology, haematology and oncology specialists to inform hepatitis B screening and antiviral management for immunocompromised patients with haematological and solid organ malignancies in Australia.Main Recommendations: Recommendations address four key areas of HBV infection management for immunocompromised patients with haematological and solid organ malignancies: who to test for HBV infection, when to start antiviral agents, when to stop antiviral agents, and how to monitor patients during cancer therapy. We recommend testing all patients undergoing cancer treatment for hepatitis B (including HBV surface antigen [HBsAg], HBV core antibody [anti-HBc], and HBV surface antibody) before cancer treatment. Individuals with chronic HBV infection (HBsAg positive) or past exposure (HBsAg negative and anti-HBc positive) receiving higher risk chemotherapy require antiviral prophylaxis using entecavir or tenofovir.Changes in Management AsA Result Of This Statement: This consensus statement will simplify the approach to testing and prophylaxis for HBV infection during cancer therapy, and harmonise approaches to discontinuing and monitoring individuals which have been highly variable in practice. We advocate for broader Medicare Benefits Schedule and Pharmaceutical Benefits Scheme access to HBV testing and treatment for patients undergoing cancer therapy. [ABSTRACT FROM AUTHOR]

Published
2019
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27. ESPEN expert group recommendations for action against cancer-related malnutrition.

Author

Arends, J., Baracos, V., Bertz, H., Bozzetti, F., Calder, P.C., Deutz, N.E.P., Erickson, N., Laviano, A., Lisanti, M.P., Lobo, D.N., McMillan, D.C., Muscaritoli, M., Ockenga, J., Pirlich, M., Strasser, F., de van der Schueren, M., Van Gossum, A., Vaupel, P., and Weimann, A.

Abstract

Summary Patients with cancer are at particularly high risk for malnutrition because both the disease and its treatments threaten their nutritional status. Yet cancer-related nutritional risk is sometimes overlooked or under-treated by clinicians, patients, and their families. The European Society for Clinical Nutrition and Metabolism (ESPEN) recently published evidence-based guidelines for nutritional care in patients with cancer. In further support of these guidelines, an ESPEN oncology expert group met for a Cancer and Nutrition Workshop in Berlin on October 24 and 25, 2016. The group examined the causes and consequences of cancer-related malnutrition, reviewed treatment approaches currently available, and built the rationale and impetus for clinicians involved with care of patients with cancer to take actions that facilitate nutrition support in practice. The content of this position paper is based on presentations and discussions at the Berlin meeting. The expert group emphasized 3 key steps to update nutritional care for people with cancer: (1) screen all patients with cancer for nutritional risk early in the course of their care, regardless of body mass index and weight history; (2) expand nutrition-related assessment practices to include measures of anorexia, body composition, inflammatory biomarkers, resting energy expenditure, and physical function; (3) use multimodal nutritional interventions with individualized plans, including care focused on increasing nutritional intake, lessening inflammation and hypermetabolic stress, and increasing physical activity. [ABSTRACT FROM AUTHOR]

Published
2017
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28. ESPEN guidelines on nutrition in cancer patients.

Author

Arends, Jann, Bachmann, Patrick, Baracos, Vickie, Barthelemy, Nicole, Bertz, Hartmut, Bozzetti, Federico, Fearon, Ken, Hütterer, Elisabeth, Isenring, Elizabeth, Kaasa, Stein, Krznaric, Zeljko, Laird, Barry, Larsson, Maria, Laviano, Alessandro, Mühlebach, Stefan, Muscaritoli, Maurizio, Oldervoll, Line, Ravasco, Paula, Solheim, Tora, and Strasser, Florian

Abstract

Summary Cancers are among the leading causes of morbidity and mortality worldwide, and the number of new cases is expected to rise significantly over the next decades. At the same time, all types of cancer treatment, such as surgery, radiation therapy, and pharmacological therapies are improving in sophistication, precision and in the power to target specific characteristics of individual cancers. Thus, while many cancers may still not be cured they may be converted to chronic diseases. All of these treatments, however, are impeded or precluded by the frequent development of malnutrition and metabolic derangements in cancer patients, induced by the tumor or by its treatment. These evidence-based guidelines were developed to translate current best evidence and expert opinion into recommendations for multi-disciplinary teams responsible for identification, prevention, and treatment of reversible elements of malnutrition in adult cancer patients. The guidelines were commissioned and financially supported by ESPEN and by the European Partnership for Action Against Cancer (EPAAC), an EU level initiative. Members of the guideline group were selected by ESPEN to include a range of professions and fields of expertise. We searched for meta-analyses, systematic reviews and comparative studies based on clinical questions according to the PICO format. The evidence was evaluated and merged to develop clinical recommendations using the GRADE method. Due to the deficits in the available evidence, relevant still open questions were listed and should be addressed by future studies. Malnutrition and a loss of muscle mass are frequent in cancer patients and have a negative effect on clinical outcome. They may be driven by inadequate food intake, decreased physical activity and catabolic metabolic derangements. To screen for, prevent, assess in detail, monitor and treat malnutrition standard operating procedures, responsibilities and a quality control process should be established at each institution involved in treating cancer patients. All cancer patients should be screened regularly for the risk or the presence of malnutrition. In all patients – with the exception of end of life care – energy and substrate requirements should be met by offering in a step-wise manner nutritional interventions from counseling to parenteral nutrition. However, benefits and risks of nutritional interventions have to be balanced with special consideration in patients with advanced disease. Nutritional care should always be accompanied by exercise training. To counter malnutrition in patients with advanced cancer there are few pharmacological agents and pharmaconutrients with only limited effects. Cancer survivors should engage in regular physical activity and adopt a prudent diet. [ABSTRACT FROM AUTHOR]

Published
2017
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29. Addiction and Eyes on Screen: How Smokers Process Smoking-Related PSAs.

Author

Sanders-Jackson, Ashley N., Cappella, Joseph, Linebarger, Deborah, Taylor-Piotrowski, Jessica, O'Keeffe, Moira, Strasser, Andrew, and Lerman, Caryn

Subjects
SMOKING, CIGARETTE smokers, PUBLIC service advertising, TOBACCO use, SUBSTANCE abuse
Abstract

The purpose of this study is to understand how addicted smokers process smoking-related PSAs by looking at fixation duration of eyes on screen, which may suggest resources allocated to visual attention. Smokers (like all addicts) are appetatively activated by images of their addicted substance (in this case smoking and cigarettes). However, with complex stimuli, like PSAs, it is possible that smoking cues will elicit avoidance responses in accordance with the fear appeal literature or that they will elicit overload. Smoking cues in PSAs should be processed similarly to complex stimuli (operationalized in this case as high in Information Introduced (I-squared)) due to the emotional nature of these cues which should call forth significant resources for processing. It is also likely that individual difference variables in addiction to tobacco and sensation seeking will moderate effects. This is research is funded by the National Cancer Institute's Effects of Public Information in Cancer (EPIC) Center of Excellence in Cancer Communication Research, reference number 5P50CA095856-05. ..PAT.-Unpublished Manuscript [ABSTRACT FROM AUTHOR]

Published
2008

30. Patient-focused endpoints in advanced cancer: Criterion-based validation of accelerometer-based activity monitoring.

Author

Skipworth, Richard J.E., Stene, Guro B., Dahele, Max, Hendry, Paul O., Small, Alexandra C., Blum, David, Kaasa, Stein, Trottenberg, Peter, Radbruch, Lukas, Strasser, Florian, Preston, Tom, Fearon, Kenneth C.H., and Helbostad, Jorunn L.

Abstract

Summary: Background & aims: Objective assessment of daily physical activity (PA) by body-worn accelerometers offers potential as a novel endpoint in the clinical management of advanced cancer patients. This study aimed to assess criterion-based validity of an accelerometer-based activity monitoring system (AM-system), ActivPAL™, using two different methods. Methods: Advanced cancer in patients and outpatients (Karnofsky Performance Status (KPS) 40–100). ActivPAL™ measurements were validated against (i) observations and (ii) energy expenditure (EE) measured by 2-week doubly-labelled water (DLW) protocol. Results: Absolute errors for mean time spent in different body positions (<0.1%) and number of transfers (0%) were low. Step count error was significantly higher in patients with KPS 40–60 (non-self caring) compared to KPS 70–100 (self-caring) (33 vs. 24%, p = 0.006). Post-hoc mathematical analysis demonstrated that absolute errors for the mean energy expenditure of activity (EEA) (1.4%) and mean total EE (0.4%) were low, but agreement was also low. Conclusions: AM-systems provide valid estimates of body positions and transfers, but not step count, especially in non-self caring patients. ActivPAL™ can derive estimates of EE but there is considerable variability in results, which is consistent, in part, with the inaccuracy in step count. Further studies are required to assess the validity of different endpoints derived from AM-systems in advanced cancer patients. [Copyright &y& Elsevier]

Published
2011
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