Your search keyword '"Areej A. Alhareeri"' showing total 15 results

1. Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Kellie J. Archer, Han Fu, Debra E. Lyon, R. K. Elswick, Debra L. Kelly, Angela R. Starkweather, Lynne W. Elmore, Yahya A. Bokhari, and Colleen K. Jackson-Cook

Subjects

Telomere, Breast cancer, Chemotherapy-related cognitive dysfunction, Psychoneurologic symptoms, Chromosome-specific telomere lengths, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Survival rates for breast cancer (BC) have improved, but quality of life post-diagnosis/treatment can be adversely affected, with survivors reporting a constellation of psychoneurological symptoms (PNS) including stress, anxiety, depression, pain, fatigue, sleep disturbance, and cognitive dysfunction. Methods To assess a potential relationship between telomere length (TL) and the development/persistence of PNS, we longitudinally studied 70 women (ages 23–71) with early stage BC (I-IIIA) at 5 time-points: prior to treatment (baseline), the mid-point of their chemotherapy cycle, 6 months, 1 year, and 2 years following the initiation of chemotherapy. Measures quantified included assessments of each of the PNS noted above and TL [using both a multiplex qPCR assay and a chromosome-specific fluorescence in situ hybridization (FISH) assay]. Results Variables associated with qPCR mean TLs were age (p = 0.004) and race (T/S ratios higher in Blacks than Whites; p = 0.019). Significant differences (mostly decreases) in chromosome-specific TLs were identified for 32 of the 46 chromosomal arms at the mid-chemo time-point (p = 0.004 to 0.049). Unexpectedly, the sequential administration of doxorubicin [Adriamycin], cyclophosphamide [Cytoxan], and docetaxel [Taxotere] (TAC regimen) was consistently associated with higher TLs, when compared to TLs in women receiving a docetaxel [Taxotere], Carboplatin [Paraplatin], and trastuzumab [Herceptin] [TCH] chemotherapy regimen [association was shown with both the qPCR and FISH assays (p = 0.036)]. Of the PNS, pain was significantly negatively associated with TL (higher pain; shorter telomeres) for a subset of chromosomal arms (5q, 8p, 13p, 20p, 22p, Xp, Xq) (p = 0.014–0.047). Chromosomal TLs were also associated with 7 of the 8 cognitive domains evaluated, with the strongest relationship being noted for chromosome 17 and the visual memory domain (shorter telomeres; lower scores). Conclusions We showed that race and age were significantly associated with telomere length in women treated for early stage BC and that acquired telomere alterations differed based on the woman’s treatment regimen. Our study also demonstrated that pain and cognitive domain measures were significantly related to telomere values in this study cohort. Expanding upon the knowledge gained from this longitudinal study could provide insight about the biological cascade of events that contribute to PNS related to BC and/or its treatment.

Published

2020

2. Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Debra E. Lyon, Angela Starkweather, Ronald K. Elswick, Han Fu, Yahya A. Bokhari, Kellie J. Archer, Debra Lynch Kelly, Colleen Jackson-Cook, Lynne W. Elmore, and Areej A. Alhareeri

Subjects

Oncology, Aging, Longitudinal study, Time Factors, medicine.medical_treatment, Psychoneurologic symptoms, chemistry.chemical_compound, Breast cancer, 0302 clinical medicine, Cancer Survivors, Antineoplastic Combined Chemotherapy Protocols, Medicine, Longitudinal Studies, Pain Measurement, 0303 health sciences, Age Factors, Telomere, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Chemotherapy regimen, Docetaxel, 030220 oncology & carcinogenesis, Female, Research Article, medicine.drug, Adult, medicine.medical_specialty, Cyclophosphamide, Pain, Breast Neoplasms, lcsh:RC254-282, Young Adult, 03 medical and health sciences, Internal medicine, Humans, Cognitive Dysfunction, Aged, 030304 developmental biology, Chemotherapy, business.industry, Telomere Homeostasis, medicine.disease, Carboplatin, chemistry, Karyotyping, Quality of Life, TAC Regimen, Chromosome-specific telomere lengths, Chemotherapy-related cognitive dysfunction, business

Abstract

Background Survival rates for breast cancer (BC) have improved, but quality of life post-diagnosis/treatment can be adversely affected, with survivors reporting a constellation of psychoneurological symptoms (PNS) including stress, anxiety, depression, pain, fatigue, sleep disturbance, and cognitive dysfunction. Methods To assess a potential relationship between telomere length (TL) and the development/persistence of PNS, we longitudinally studied 70 women (ages 23–71) with early stage BC (I-IIIA) at 5 time-points: prior to treatment (baseline), the mid-point of their chemotherapy cycle, 6 months, 1 year, and 2 years following the initiation of chemotherapy. Measures quantified included assessments of each of the PNS noted above and TL [using both a multiplex qPCR assay and a chromosome-specific fluorescence in situ hybridization (FISH) assay]. Results Variables associated with qPCR mean TLs were age (p = 0.004) and race (T/S ratios higher in Blacks than Whites; p = 0.019). Significant differences (mostly decreases) in chromosome-specific TLs were identified for 32 of the 46 chromosomal arms at the mid-chemo time-point (p = 0.004 to 0.049). Unexpectedly, the sequential administration of doxorubicin [Adriamycin], cyclophosphamide [Cytoxan], and docetaxel [Taxotere] (TAC regimen) was consistently associated with higher TLs, when compared to TLs in women receiving a docetaxel [Taxotere], Carboplatin [Paraplatin], and trastuzumab [Herceptin] [TCH] chemotherapy regimen [association was shown with both the qPCR and FISH assays (p = 0.036)]. Of the PNS, pain was significantly negatively associated with TL (higher pain; shorter telomeres) for a subset of chromosomal arms (5q, 8p, 13p, 20p, 22p, Xp, Xq) (p = 0.014–0.047). Chromosomal TLs were also associated with 7 of the 8 cognitive domains evaluated, with the strongest relationship being noted for chromosome 17 and the visual memory domain (shorter telomeres; lower scores). Conclusions We showed that race and age were significantly associated with telomere length in women treated for early stage BC and that acquired telomere alterations differed based on the woman’s treatment regimen. Our study also demonstrated that pain and cognitive domain measures were significantly related to telomere values in this study cohort. Expanding upon the knowledge gained from this longitudinal study could provide insight about the biological cascade of events that contribute to PNS related to BC and/or its treatment.

Published

2020

3. Additional file 2 of Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Archer, Kellie J., Fu, Han, Lyon, Debra E., R. K. Elswick, Kelly, Debra L., Starkweather, Angela R., Elmore, Lynne W., Bokhari, Yahya A., and Jackson-Cook, Colleen K.

Abstract

Additional file 2. a. Mixed Effects Linear Model Fitting Assessment of Associations of Variables with MMqPCR Telomere Length and b. Mixed Effects Linear Model Fitting Assessment for Variables NOT Showing Significant MMqPCR Telomere Length Associations. Tables show least square means and p values for variables evaluated in the mixed effects linear model.

Published

2020

4. Additional file 9 of Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Archer, Kellie J., Fu, Han, Lyon, Debra E., R. K. Elswick, Kelly, Debra L., Starkweather, Angela R., Elmore, Lynne W., Bokhari, Yahya A., and Jackson-Cook, Colleen K.

Subjects

carbohydrates (lipids), polycyclic compounds

Abstract

Additional file 9. Studies on the Effect of Doxorubicin (Adriamycin) on Telomere Biology. Literature review of previous reports assessing the biological response/mechanism of Doxorubincin (also called Adriamycin) on telomeres.

Published

2020

5. Additional file 4 of Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Archer, Kellie J., Fu, Han, Lyon, Debra E., R. K. Elswick, Kelly, Debra L., Starkweather, Angela R., Elmore, Lynne W., Bokhari, Yahya A., and Jackson-Cook, Colleen K.

Abstract

Additional file 4. a. Breast Tumor Characteristics for Subset of 50 Study Participants Evaluated using the Chromosome-Specific FISH Method and b. Demographics and Chemotherapy Regimens for Subset of 50 Study Participants Evaluated using the Chromosome-Specific FISH Method. List pathology and treatment findings for the subset of 50 participants evaluated with the chromosome-specific analysis at time-points 1 and 2.

Published

2020

6. Additional file 8 of Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Archer, Kellie J., Fu, Han, Lyon, Debra E., R. K. Elswick, Kelly, Debra L., Starkweather, Angela R., Elmore, Lynne W., Bokhari, Yahya A., and Jackson-Cook, Colleen K.

Abstract

Additional file 8. Chromosome-Specific Telomere Length and Cancer Risk. Literature review of previous reports of chromosome-specific telomere lengths related to cancer.

Published

2020

7. Additional file 5 of Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Archer, Kellie J., Fu, Han, Lyon, Debra E., R. K. Elswick, Kelly, Debra L., Starkweather, Angela R., Elmore, Lynne W., Bokhari, Yahya A., and Jackson-Cook, Colleen K.

Abstract

Additional file 5. Comparisons of Chromosome-Specific Telomere Values Between Baseline and Mid-Chemo Specimens. List of the means, standard deviations, mean of difference between baseline and time-point 2 and the p values for each individual telomere (short arm 1, long arm 1, etc) calculated using the FISH chromosome-specific assay.

Published

2020

8. Additional file 3 of Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Archer, Kellie J., Fu, Han, Lyon, Debra E., R. K. Elswick, Kelly, Debra L., Starkweather, Angela R., Elmore, Lynne W., Bokhari, Yahya A., and Jackson-Cook, Colleen K.

Abstract

Additional file 3. Differences in Baseline (T1) Compared to Mid-Chemotherapy (T2) Time-points for FISH-based Chromosome-Specific Telomere Values. Heatmap showing differences in individual telomere values for each participant.

Published

2020

9. Additional file 10 of Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Archer, Kellie J., Fu, Han, Lyon, Debra E., R. K. Elswick, Kelly, Debra L., Starkweather, Angela R., Elmore, Lynne W., Bokhari, Yahya A., and Jackson-Cook, Colleen K.

Abstract

Additional file 10. Hypothesized Biological Cascade Contributing to Psychoneurological Symptoms in Women Receiving Chemotherapy for Breast Cancer. Schematic representation of inter-relationships between telomeres and inflammation, which lead to psychoneurological symptoms via alterations in epigenetic patterns/gene expression, and/or senescence.

Published

2020

10. Additional file 6 of Telomere lengths in women treated for breast cancer show associations with chemotherapy, pain symptoms, and cognitive domain measures: a longitudinal study

Author

Areej A. Alhareeri, Archer, Kellie J., Fu, Han, Lyon, Debra E., R. K. Elswick, Kelly, Debra L., Starkweather, Angela R., Elmore, Lynne W., Bokhari, Yahya A., and Jackson-Cook, Colleen K.

Abstract

Additional file 6. Mixed Effects Linear Model Fitting Assessment of Mid-Chemo Timepoint as a Variable Associated with Chromosome-Specific Telomere Length. List of least square values, standard errors, and p values for results of mixed effects linear model fitting of chromosome-specific data.

Published

2020

11. Telomere length: a review of methods for measurement

Author

Lathika Mohanraj, Colleen Jackson-Cook, Victoria Menzies, Debra E. Lyon, Angela Starkweather, Candace W. Burton, Lynne W. Elmore, Marty Montpetit, Kristin Filler, Areej A. Alhareeri, and Alison J. Montpetit

Subjects

Alternative methods, Telomere biology, Extramural, Clinical study design, Chromosome Mapping, Computational biology, Biology, Multiple methods, Telomere, Weights and Measures, Polymerase Chain Reaction, Article, Genetic Techniques, Humans, General Nursing, Biomarkers, In Situ Hybridization, Fluorescence, Polymorphism, Restriction Fragment Length, Fluorescent Dyes

Abstract

Background: The exciting discovery that telomere shortening is associated with many health conditions and that telomere lengths can be altered in response to social and environmental exposures has underscored the need for methods to accurately and consistently quantify telomere length. Objectives: The purpose of this article is to provide a comprehensive summary that compares and contrasts the current technologies used to assess telomere length. Discussion: Multiple methods have been developed for the study of telomeres. These techniques include quantification of telomere length by terminal restriction fragmentation—which was one of the earliest tools used for length assessment—making it the gold standard in telomere biology. Quantitative polymerase chain reaction provides the advantage of being able to use smaller amounts of DNA, thereby making it amenable to epidemiology studies involving large numbers of people. An alternative method uses fluorescent probes to quantify not only mean telomere lengths but also chromosome-specific telomere lengths; however, the downside of this approach is that it can only be used on mitotically active cells. Additional methods that permit assessment of the length of a subset of chromosome-specific telomeres or the subset of telomeres that demonstrate shortening are also reviewed. Conclusion: Given the increased utility for telomere assessments as a biomarker in physiological, psychological, and biobehavioral research, it is important that investigators become familiar with the methodological nuances of the various procedures used for measuring telomere length. This will ensure that they are empowered to select an optimal assessment approach to meet the needs of their study designs. Gaining a better understanding of the benefits and drawbacks of various measurement techniques is important not only in individual studies, but also to further establish the science of telomere associations with biobehavioral phenomena.

Published

2014

12. Higher Proportion of at Least Pentaploidy for Chromosomes X, Y, and 18 Is Present in Myocytes of Patients Having a Good Outcome After Receiving a Left-Ventricular Assist Device

Author

Lauren N. Huddle, Areej A. Alhareeri, Valentina Robila, Michael O. Idowu, Margaret M. Grimes, and Colleen Jackson-Cook

Subjects

Cardiac function curve, medicine.medical_specialty, medicine.medical_treatment, Aneuploidy, General Medicine, Biology, medicine.disease, Surgery, Transplantation, Ventricular assist device, Internal medicine, cardiovascular system, medicine, Cardiology, Myocyte, Myocyte hypertrophy, Good outcome, Ploidy

Abstract

Myocyte hypertrophy and ploidy status have been proposed as predictive factors for cardiac function improvement of patients following left-ventricular assist device (LVAD) explantation and outcome of cardiac transplantation, but there is a paucity of data testing this hypothesis. The primary aim of this study was to determine if ploidy status correlates with myocyte size and/or outcome. Aneuploidy/polyploidy patterns …

Published

2012

13. ChromoEnhancer: An Artificial-Intelligence-Based Tool to Enhance Neoplastic Karyograms as an Aid for Effective Analysis.

Author

Bokhari Y, Alhareeri A, Aljouie A, Alkhaldi A, Rashid M, Alawad M, Alhassnan R, Samargandy S, Panahi A, Heidrich W, and Arodz T

Subjects

Cytogenetics, Humans, Intelligence, Karyotyping, Chromosome Aberrations, Image Processing, Computer-Assisted methods

Abstract

Cytogenetics laboratory tests are among the most important procedures for the diagnosis of genetic diseases, especially in the area of hematological malignancies. Manual chromosomal karyotyping methods are time consuming and labor intensive and, hence, expensive. Therefore, to alleviate the process of analysis, several attempts have been made to enhance karyograms. The current chromosomal image enhancement is based on classical image processing. This approach has its limitations, one of which is that it has a mandatory application to all chromosomes, where customized application to each chromosome is ideal. Moreover, each chromosome needs a different level of enhancement, depending on whether a given area is from the chromosome itself or it is just an artifact from staining. The analysis of poor-quality karyograms, which is a difficulty faced often in preparations from cancer samples, is time consuming and might result in missing the abnormality or difficulty in reporting the exact breakpoint within the chromosome. We developed ChromoEnhancer, a novel artificial-intelligence-based method to enhance neoplastic karyogram images. The method is based on Generative Adversarial Networks (GANs) with a data-centric approach. GANs are known for the conversion of one image domain to another. We used GANs to convert poor-quality karyograms into good-quality images. Our method of karyogram enhancement led to robust routine cytogenetic analysis and, therefore, to accurate detection of cryptic chromosomal abnormalities. To evaluate ChromoEnahancer, we randomly assigned a subset of the enhanced images and their corresponding original (unenhanced) images to two independent cytogeneticists to measure the karyogram quality and the elapsed time to complete the analysis, using four rating criteria, each scaled from 1 to 5. Furthermore, we compared the enhanced images with our method to the original ones, using quantitative measures (PSNR and SSIM metrics).

Published

2022

14. QuaDMutNetEx: a method for detecting cancer driver genes with low mutation frequency.

Author

Bokhari Y, Alhareeri A, and Arodz T

Subjects

Humans, Mutation, Algorithms, Computational Biology methods, Neoplasms genetics

Abstract

Background: Cancer is caused by genetic mutations, but not all somatic mutations in human DNA drive the emergence or growth of cancers. While many frequently-mutated cancer driver genes have already been identified and are being utilized for diagnostic, prognostic, or therapeutic purposes, identifying driver genes that harbor mutations occurring with low frequency in human cancers is an ongoing endeavor. Typically, mutations that do not confer growth advantage to tumors - passenger mutations - dominate the mutation landscape of tumor cell genome, making identification of low-frequency driver mutations a challenge. The leading approach for discovering new putative driver genes involves analyzing patterns of mutations in large cohorts of patients and using statistical methods to discriminate driver from passenger mutations., Results: We propose a novel cancer driver gene detection method, QuaDMutNetEx. QuaDMutNetEx discovers cancer drivers with low mutation frequency by giving preference to genes encoding proteins that are connected in human protein-protein interaction networks, and that at the same time show low deviation from the mutual exclusivity pattern that characterizes driver mutations occurring in the same pathway or functional gene group across a cohort of cancer samples., Conclusions: Evaluation of QuaDMutNetEx on four different tumor sample datasets show that the proposed method finds biologically-connected sets of low-frequency driver genes, including many genes that are not found if the network connectivity information is not considered. Improved quality and interpretability of the discovered putative driver gene sets compared to existing methods shows that QuaDMutNetEx is a valuable new tool for detecting driver genes. QuaDMutNetEx is available for download from https://github.com/bokhariy/QuaDMutNetExunder the GNU GPLv3 license.

Published

2020

15. Telomere length: a review of methods for measurement.

Author

Montpetit AJ, Alhareeri AA, Montpetit M, Starkweather AR, Elmore LW, Filler K, Mohanraj L, Burton CW, Menzies VS, Lyon DE, and Jackson-Cook CK

Subjects

Fluorescent Dyes, Humans, In Situ Hybridization, Fluorescence, Polymerase Chain Reaction, Polymorphism, Restriction Fragment Length, Weights and Measures, Biomarkers analysis, Chromosome Mapping methods, Genetic Techniques, Telomere classification

Abstract

Background: The exciting discovery that telomere shortening is associated with many health conditions and that telomere lengths can be altered in response to social and environmental exposures has underscored the need for methods to accurately and consistently quantify telomere length., Objectives: The purpose of this article is to provide a comprehensive summary that compares and contrasts the current technologies used to assess telomere length., Discussion: Multiple methods have been developed for the study of telomeres. These techniques include quantification of telomere length by terminal restriction fragmentation-which was one of the earliest tools used for length assessment-making it the gold standard in telomere biology. Quantitative polymerase chain reaction provides the advantage of being able to use smaller amounts of DNA, thereby making it amenable to epidemiology studies involving large numbers of people. An alternative method uses fluorescent probes to quantify not only mean telomere lengths but also chromosome-specific telomere lengths; however, the downside of this approach is that it can only be used on mitotically active cells. Additional methods that permit assessment of the length of a subset of chromosome-specific telomeres or the subset of telomeres that demonstrate shortening are also reviewed., Conclusion: Given the increased utility for telomere assessments as a biomarker in physiological, psychological, and biobehavioral research, it is important that investigators become familiar with the methodological nuances of the various procedures used for measuring telomere length. This will ensure that they are empowered to select an optimal assessment approach to meet the needs of their study designs. Gaining a better understanding of the benefits and drawbacks of various measurement techniques is important not only in individual studies, but also to further establish the science of telomere associations with biobehavioral phenomena.

Published

2014