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1. Pre-treatment amino acids and risk of paclitaxel-induced peripheral neuropathy in SWOG S0221.

Author

Chen, Ciao-Sin, Zirpoli, Gary, Budd, G. Thomas, Barlow, William E., Pusztai, Lajos, Hortobagyi, Gabriel N., Albain, Kathy S., Godwin, Andrew K., Thompson, Alastair, Henry, N. Lynn, Ambrosone, Christine B., Stringer, Kathleen A., and Hertz, Daniel L.

Subjects
AMINO acids, BODY mass index, PHENYLALANINE, PERIPHERAL neuropathy, BONFERRONI correction, PACLITAXEL
Abstract

Background: Chemotherapy-induced peripheral neuropathy (CIPN) is a treatment-limiting and debilitating neurotoxicity of many commonly used anti-cancer agents, including paclitaxel. The objective of this study was to confirm the previously found inverse association between pre-treatment blood concentrations of histidine and CIPN occurrence and examine relationships of other amino acids with CIPN severity. Methods: Pre-treatment serum concentrations of 20 amino acids were measured in the SWOG S0221 (NCT00070564) trial of patients with early-stage breast cancer receiving paclitaxel. The associations between amino acids and CIPN severity were tested in regression analysis adjusted for paclitaxel schedule, age, self-reported race, and body mass index with Bonferroni correction. The network of metabolic pathways of amino acids was analyzed using over-representation analysis. The partial correlation network of amino acids was evaluated using a debiased sparse partial correlation algorithm. Results: In the primary analysis, histidine concentration was not associated with CIPN occurrence (odds ratio (OR) = 0.97 [0.83, 1.13], p = 0.72). In secondary analyses, higher concentrations of four amino acids, glutamate (β = 0.58 [0.23, 0.93], p = 0.001), phenylalanine (β = 0.54 [0.19, 0.89], p = 0.002), tyrosine (β = 0.57 [0.23, 0.91], p = 0.001), and valine (β = 0.58 [0.24, 0.92], p = 0.001) were associated with more severe CIPN, but none of these associations retained significance after adjustment. In the over-representation analysis, no amino acid metabolic pathways were significantly enriched (all FDR > 0.05). In the network of enriched pathways, glutamate metabolism had the highest centrality. Conclusions: This analysis showed that pre-treatment serum amino acid concentrations are not strongly predictive of CIPN severity. Prospectively designed studies that assess non-amino acid metabolomics predictors are encouraged. [ABSTRACT FROM AUTHOR]

Published
2024
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3. Impact of early detection on cancer curability: A modified Delphi panel study.

Author

Schwartzberg, Lee, Broder, Michael S., Ailawadhi, Sikander, Beltran, Himisha, Blakely, L. Johnetta, Budd, G. Thomas, Carr, Laurie, Cecchini, Michael, Cobb, Patrick, Kansal, Anuraag, Kim, Ashley, Monk, Bradley J., Wong, Deborah J., Campos, Cynthia, and Yermilov, Irina

Subjects
EARLY detection of cancer, PANEL analysis, INTRAHEPATIC bile ducts, BREAST, MEDICAL screening, BLOOD testing, PANCREAS
Abstract

Expert consensus on the potential benefits of early cancer detection does not exist for most cancer types. We convened 10 practicing oncologists using a RAND/UCLA modified Delphi panel to evaluate which of 20 solid tumors, representing >40 American Joint Committee on Cancer (AJCC)-identified cancer types and 80% of total cancer incidence, would receive potential clinical benefits from early detection. Pre-meeting, experts estimated how long cancers take to progress and rated the current curability and benefit (improvement in curability) of an annual hypothetical multi-cancer screening blood test. Post-meeting, experts rerated all questions. Cancers had varying estimates of the potential benefit of early cancer detection depending on estimates of their curability and progression by stage. Cancers rated as progressing quickly and being curable in earlier stages (stomach, esophagus, lung, urothelial tract, melanoma, ovary, sarcoma, bladder, cervix, breast, colon/rectum, kidney, uterus, anus, head and neck) were estimated to be most likely to benefit from a hypothetical screening blood test. Cancer types rated as progressing quickly but having comparatively lower cure rates in earlier stages (liver/intrahepatic bile duct, gallbladder, pancreas) were estimated to have medium likelihood of benefit from a hypothetical screening blood test. Cancer types rated as progressing more slowly and having higher curability regardless of stage (prostate, thyroid) were estimated to have limited likelihood of benefit from a hypothetical screening blood test. The panel concluded most solid tumors have a likelihood of benefit from early detection. Even among difficult-to-treat cancers (e.g., pancreas, liver/intrahepatic bile duct, gallbladder), early-stage detection was believed to be beneficial. Based on the panel consensus, broad coverage of cancers by screening blood tests would deliver the greatest potential benefits to patients. [ABSTRACT FROM AUTHOR]

Published
2022
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5. Cardiac risk stratification in cancer patients: A longitudinal patient-patient network analysis.

Author

Hou, Yuan, Zhou, Yadi, Hussain, Muzna, Budd, G. Thomas, Tang, Wai Hong Wilson, Abraham, James, Xu, Bo, Shah, Chirag, Moudgil, Rohit, Popovic, Zoran, Watson, Chris, Cho, Leslie, Chung, Mina, Kanj, Mohamed, Kapadia, Samir, Griffin, Brian, Svensson, Lars, Collier, Patrick, and Cheng, Feixiong

Subjects
DISEASE risk factors, CARDIOVASCULAR diseases, CANCER patients, STROKE, CORONARY artery disease, HEART failure, CAUSES of death
Abstract

Background: Cardiovascular disease is a leading cause of death in general population and the second leading cause of mortality and morbidity in cancer survivors after recurrent malignancy in the United States. The growing awareness of cancer therapy-related cardiac dysfunction (CTRCD) has led to an emerging field of cardio-oncology; yet, there is limited knowledge on how to predict which patients will experience adverse cardiac outcomes. We aimed to perform unbiased cardiac risk stratification for cancer patients using our large-scale, institutional electronic medical records.Methods and Findings: We built a large longitudinal (up to 22 years' follow-up from March 1997 to January 2019) cardio-oncology cohort having 4,632 cancer patients in Cleveland Clinic with 5 diagnosed cardiac outcomes: atrial fibrillation, coronary artery disease, heart failure, myocardial infarction, and stroke. The entire population includes 84% white Americans and 11% black Americans, and 59% females versus 41% males, with median age of 63 (interquartile range [IQR]: 54 to 71) years old. We utilized a topology-based K-means clustering approach for unbiased patient-patient network analyses of data from general demographics, echocardiogram (over 25,000), lab testing, and cardiac factors (cardiac). We performed hazard ratio (HR) and Kaplan-Meier analyses to identify clinically actionable variables. All confounding factors were adjusted by Cox regression models. We performed random-split and time-split training-test validation for our model. We identified 4 clinically relevant subgroups that are significantly correlated with incidence of cardiac outcomes and mortality. Among the 4 subgroups, subgroup I (n = 625) has the highest risk of de novo CTRCD (28%) with an HR of 3.05 (95% confidence interval (CI) 2.51 to 3.72). Patients in subgroup IV (n = 1,250) had the worst survival probability (HR 4.32, 95% CI 3.82 to 4.88). From longitudinal patient-patient network analyses, the patients in subgroup I had a higher percentage of de novo CTRCD and a worse mortality within 5 years after the initiation of cancer therapies compared to long-time exposure (6 to 20 years). Using clinical variable network analyses, we identified that serum levels of NT-proB-type Natriuretic Peptide (NT-proBNP) and Troponin T are significantly correlated with patient's mortality (NT-proBNP > 900 pg/mL versus NT-proBNP = 0 to 125 pg/mL, HR = 2.95, 95% CI 2.28 to 3.82, p < 0.001; Troponin T > 0.05 μg/L versus Troponin T ≤ 0.01 μg/L, HR = 2.08, 95% CI 1.83 to 2.34, p < 0.001). Study limitations include lack of independent cardio-oncology cohorts from different healthcare systems to evaluate the generalizability of the models. Meanwhile, the confounding factors, such as multiple medication usages, may influence the findings.Conclusions: In this study, we demonstrated that the patient-patient network clustering methodology is clinically intuitive, and it allows more rapid identification of cancer survivors that are at greater risk of cardiac dysfunction. We believed that this study holds great promise for identifying novel cardiac risk subgroups and clinically actionable variables for the development of precision cardio-oncology. [ABSTRACT FROM AUTHOR]

Published
2021
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6. Physical Activity Before, During, and After Chemotherapy for High-Risk Breast Cancer: Relationships With Survival.

Author

Cannioto, Rikki A, Hutson, Alan, Dighe, Shruti, McCann, William, McCann, Susan E, Zirpoli, Gary R, Barlow, William, Kelly, Kara M, DeNysschen, Carol A, Hershman, Dawn L, Unger, Joseph M, Moore, Halle C F, Stewart, James A, Isaacs, Claudine, Hobday, Timothy J, Salim, Muhammad, Hortobagyi, Gabriel N, Gralow, Julie R, Albain, Kathy S, and Budd, G Thomas

Subjects
PHYSICAL activity, CANCER chemotherapy, CANCER-related mortality, DIAGNOSIS, GUIDELINES, BREAST tumor treatment, RESEARCH, RESEARCH methodology, CANCER relapse, PROGNOSIS, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, RANDOMIZED controlled trials, EXERCISE, DRUG therapy, BREAST, RESEARCH funding, COMBINED modality therapy, BREAST tumors, LONGITUDINAL method, PROPORTIONAL hazards models
Abstract

Background: Although physical activity has been consistently associated with reduced breast cancer mortality, evidence is largely based on data collected at one occasion. We examined how pre- and postdiagnosis physical activity was associated with survival outcomes in high-risk breast cancer patients.Methods: Included were 1340 patients enrolled in the Diet, Exercise, Lifestyle and Cancer Prognosis (DELCaP) Study, a prospective study of lifestyle and prognosis ancillary to a SWOG clinical trial (S0221). Activity before diagnosis, during treatment, and at 1- and 2-year intervals after enrollment was collected. Patients were categorized according to the Physical Activity Guidelines for Americans as meeting the minimum guidelines (yes/no) and incrementally as inactive, low active, moderately active (meeting the guidelines), or high active.Results: In joint-exposure analyses, patients meeting the guidelines before and 1 year after diagnosis experienced statistically significant reductions in hazards of recurrence (hazard ratio [HR] = 0.59, 95% confidence interval [CI] = 0.42 to 0.82) and mortality (HR = 0.51, 95% CI = 0.34-0.77); associations were stronger at 2-year follow-up for recurrence (HR = 0.45, 95% CI = 0.31 to 0.65) and mortality (HR = 0.32, 95% CI = 0.19 to 0.52). In time-dependent analyses, factoring in activity from all time points, we observed striking associations with mortality for low- (HR = 0.41, 95% CI = 0.24 to 0.68), moderate- (HR = 0.42, 95% CI = 0.23 to 0.76), and high-active patients (HR = 0.31, 95% CI = 0.18 to 0.53).Conclusions: Meeting the minimum guidelines for physical activity both before diagnosis and after treatment appears to be associated with statistically significantly reduced hazards of recurrence and mortality among breast cancer patients. When considering activity from all time points, including during treatment, lower volumes of regular activity were associated with similar overall survival advantages as meeting and exceeding the guidelines. [ABSTRACT FROM AUTHOR]

Published
2021
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9. Precision Oncology in Solid Tumors: A Longitudinal Tertiary Care Center Experience.

Author

Sadaps, Meena, Funchain, Pauline, Mahdi, Haider, Grivas, Petros, Pritchard, Amy, Klek, Stefan, Estfan, Bassam, Abraham, Jame, Budd, G. Thomas, Stevenson, James P., Pennell, Nathan A., Khorana, Alok A., Bolwell, Brian J., and Sohal, Davendra P.S.

Subjects
TUMOR treatment, TUMOR genetics, HUMAN genome, INDIVIDUALIZED medicine, ONCOLOGY, CLINICAL trials
Abstract

Purpose: Precision oncology is widely discussed, but cohort studies are limited. We previously reported our prospective experience of precision oncology in solid tumors, and here we report our longitudinal experience, focusing on therapeutic impact. Patients and Methods: We conducted a retrospective review of 600 consecutive patients seen at Cleveland Clinic from 2013 to 2016 for treatment of incurable solid tumor malignancies for whom tumor genomic profiling was ordered using FoundationOne (Cambridge, MA). Results were discussed at our multidisciplinary genomics tumor board. Data analyzed included subsequent therapy and overall survival (OS). Results: Median age was 59 years (range, 18 to 94 years), 308 (51.3%) were female, and 533 (88.8%) were white. Targeted therapy was recommended in 310 patients (51.7%). After results, 313 patients (52.2%) started any subsequent therapy; of these, 95 (30%; 15.8% overall) received genomics-driven therapy (G), and 218 (70%) received non–genomics-driven treatment (NG). For the G versus NG group, the on-label, off-label, and clinical trial therapy breakdowns were 23% versus 88%, 47% versus 3%, and 30% versus 9%, respectively. Median OS for patients receiving no therapy after tumor genomic profiling was 5.5 months; for the G and NG groups, it was 18 (P <.001) and 14.4 (P <.001) months, respectively (P = NS for G v NG). The use of G increased from 10% in the first 250-patient cohort (reported earlier) to 20% in the subsequent 350-patient cohort. Conclusion: Tumor genomic profiling influenced treatment in 15.8% of patients. More patients received treatment via clinical trials in the G cohort, and although not statistically significant, there was a trend toward increased OS in the G (v NG) group. These data can further guide real-world applications of precision oncology. [ABSTRACT FROM AUTHOR]

Published
2018
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10. Can CDK4/6 inhibitors cause fatal lung injury?

Author

Jazieh, Khalid A., Budd, G. Thomas, Dalpiaz, Nancy, and Abraham, Jame

Subjects
HORMONE receptor positive breast cancer, LUNG injuries, INTERSTITIAL lung diseases, EPIDERMAL growth factor receptors
Abstract

In two studies assessing pulmonary toxicity in lung cancer patients undergoing systemic antineoplastic therapy, about 6-7% of patients developed chemotherapy-induced lung disease, and about one-third of those patients died as a result [[5]]. The first patient in our clinical practice to develop pneumonitis while on a CDK4/6 inhibitor was a 74-year-old female with a history of hormone receptor-positive/HER2 negative breast cancer diagnosed in 2013. A - Baseline CT prior to Patient 1's symptoms - 27 August 2018; B - CT on presentation of Patient 1-23 November 2018; C - Follow-up CT for Patient 1-24 May 2019. [Extracted from the article]

Published
2019
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13. Adherence to Cancer Prevention Lifestyle Recommendations Before, During, and 2 Years After Treatment for High-risk Breast Cancer.

Author

Cannioto, Rikki A., Attwood, Kristopher M., Davis, Evan W., Mendicino, Lucas A., Hutson, Alan, Zirpoli, Gary R., Tang, Li, Nair, Nisha M., Barlow, William, Hershman, Dawn L., Unger, Joseph M., Moore, Halle C. F., Isaacs, Claudine, Hobday, Timothy J., Hortobagyi, Gabriel N., Gralow, Julie R., Albain, Kathy S., Budd, G. Thomas, and Ambrosone, Christine B.

Published
2023
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14. Osteoporosis therapy and outcomes for postmenopausal patients with hormone receptor-positive breast cancer: NCIC CTG MA.27.

Author

Lipton, Allan, Chapman, Judith‐Anne W., Leitzel, Kim, Garg, Ashwani, Pritchard, Kathleen I., Ingle, James N., Budd, G. Thomas, Ellis, Matthew J., Sledge, George W., Rabaglio, Manuela, Han, Lei, Elliott, Catherine R., Shepherd, Lois E., Goss, Paul E., Ali, Suhail M., and Chapman, Judith-Anne W

Subjects
OSTEOPOROSIS in women, HEALTH outcome assessment, MENOPAUSE, HORMONE receptor positive breast cancer, ANASTROZOLE, THERAPEUTICS, DIPHOSPHONATES, PROTEIN metabolism, STEROID drugs, HETEROCYCLIC compounds, ORGANIC compounds, AROMATASE inhibitors, BREAST tumors, COMBINED modality therapy, COMPARATIVE studies, MASTECTOMY, RESEARCH methodology, MEDICAL cooperation, MULTIVARIATE analysis, OSTEOPOROSIS, PROGNOSIS, RADIOTHERAPY, RESEARCH, RESEARCH funding, EVALUATION research, RANDOMIZED controlled trials, TREATMENT effectiveness, PROPORTIONAL hazards models, DISEASE complications
Abstract

Background: Breast cancer patients in the MA.27 trial had similar outcomes with steroidal aromatase inhibitor (AI) exemestane and nonsteroidal anastrozole. AIs increase the risk of osteoporosis. This study examined the effects of self-reported osteoporosis and osteoporosis therapy (OPT) on outcomes.Methods: The MA.27 phase 3 adjuvant trial enrolled 7576 postmenopausal women. The primary outcome was event-free survival (EFS), and the secondary outcome was distant disease-free survival (DDFS). Patients were permitted bisphosphonates to prevent or treat osteopenia/osteoporosis. In a multivariate, stratified Cox regression, factors were significant with a 2-sided Wald test P value ≤ .05.Results: Osteoporosis was reported at the baseline by 654 of the 7576 women (8.6%) and in total by 1294 patients. Oral OPT was received at the baseline by 815 of the 7576 women (10.8%) and in total by 2711 patients (36%). With a median follow-up of 4.1 years, 693 EFS events (9.15%) and 321 DDFS events (4.2%) occurred. Osteoporosis was not associated with EFS or DDFS. Few EFS events occurred before the initiation of OPT, with no substantive evidence of a time-differing effect on outcomes (nonproportional hazards). OPT (yes vs no) was significantly associated with improved EFS (hazard ratio [HR] for yes vs no, 0.67; 95% confidence interval [CI], 0.57-0.80; P < .001) and DDFS (HR, 0.57; 95% CI, 0.44-0.73; P <. 001). Time-differing (time-dependent) OPT was not (EFS; P = .45). OPT did not alter the incidence of visceral-only metastasis (P = .31).Conclusions: Oral OPT, administered to postmenopausal breast cancer patients receiving adjuvant AI therapy, was associated with improved EFS and DDFS; the time of OPT initiation (a time-dependent effect) did not affect the outcome. OPT did not alter the risk of visceral metastasis. Cancer 2017;123:2444-51. © 2017 American Cancer Society. [ABSTRACT FROM AUTHOR]

Published
2017
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15. Impact of an alternative chromosome 17 probe and the 2013 American Society of Clinical Oncology and College of American Pathologists guidelines on fluorescence in situ hybridization for the determination of HER2 gene amplification in breast cancer.

Author

Donaldson, Alana R., Shetty, Shashirekha, Wang, Zhen, Rivera, Christine L., Portier, Bryce P., Budd, G. Thomas, Downs‐Kelly, Erinn, Lanigan, Christopher P., and Calhoun, Benjamin C.

Subjects
IN situ hybridization, HER2 protein, BREAST cancer, CHROMOSOMES, HORMONE therapy, CANCER treatment
Abstract

Background: The dual-probe fluorescence in situ hybridization (FISH) assay for human epidermal growth factor receptor 2 (HER2) gene amplification in breast cancer provides an HER2:CEP17 (centromere enumeration probe for chromosome 17) ratio. Copy number alteration (CNA) in CEP17 may skew this ratio. The authors analyzed the impact of the 2013 American Society of Oncology/College of American Pathologists (ASCO/CAP) guidelines and an alternative chromosome 17 probe on HER2 status in tumor specimens with CEP17 CNA.Methods: Specimens with CEP17 CNA (n = 310) were selected from 3048 tumor samples that were received from January 2013 to June 2015 for testing with the alternative chromosome 17 probe D17S122. Reclassification of HER2 status was assessed using the 2007 and 2013 ASCO/CAP guidelines.Results: The alternative chromosome 17 probe reclassified 82 of 310 (26.5%) and 87 of 310 (28.1%) tumors using the 2007 and 2013 guidelines, respectively. Of the 41 of 310 tumors (13.2%) that were reclassified from nonamplified to amplified according to 2007 guidelines, 28 of 41 (68.3%) had an average HER2 copy number ≥4.0 and <6.0. The 39 of 310 tumors (12.6%) that were reclassified from equivocal to amplified according to 2013 guidelines had a mean HER2 copy number between ≥4.0 and <6.0. Most of these patients had stage I, hormone receptor-positive, lymph node-negative tumors, which is an unusual clinicopathologic profile for HER2-amplified tumors, and most received HER2-targeted therapy in addition to endocrine therapy.Conclusions: Reflex testing with an alternative chromosome 17 probe using the 2013 ASCO/CAP guidelines reclassified 28.1% of tumor samples that had CEP17 CNA, converting nearly one-half from equivocal to amplified. The benefit of HER2-targeted therapy in this patient population requires further study. Cancer 2017;123:2230-2239. © 2017 American Cancer Society. [ABSTRACT FROM AUTHOR]

Published
2017
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16. MET and PTEN gene copy numbers and Ki-67 protein expression associate with pathologic complete response in ERBB2-positive breast carcinoma patients treated with neoadjuvant trastuzumab-based therapy.

Author

Calhoun, Benjamin C., Portier, Bryce, Zhen Wang, Minca, Eugen C., Budd, G. Thomas, Lanigan, Christopher, Tubbs, Raymond R., Morrison, Larry E., and Wang, Zhen

Subjects
PROTEIN expression, KI-67 test, MET gene, PTEN protein, BREAST cancer patients, TRASTUZUMAB, ADJUVANT treatment of cancer, CANCER chemotherapy, THERAPEUTICS, ANTINEOPLASTIC agents, BREAST cancer chemotherapy, BREAST cancer, BREAST tumors, CELL receptors, COMBINED modality therapy, IMMUNOHISTOCHEMISTRY, IN situ hybridization, PHARMACOKINETICS, PHOSPHATASES, PROGNOSIS, TUMOR markers, TREATMENT effectiveness, RECEIVER operating characteristic curves, DUCTAL carcinoma, GENOTYPES
Abstract

Background: Pathologic complete response (pCR) after neoadjuvant chemotherapy for breast cancer is associated with improved prognosis in aggressive tumor subtypes, including ERBB2- positive tumors. Recent adoption of pCR as a surrogate endpoint for clinical trials in early stage breast cancer in the neoadjuvant setting highlights the need for biomarkers that, alone or in combination, help predict the likelihood of response to treatment.Methods: Biopsy specimens from 29 patients with invasive ductal carcinoma treated with trastuzumab-based therapy prior to definitive resection and pathologic staging were evaluated by dual color bright field in situ hybridization (dual ISH) using probes for MET, TOP2A, PTEN, and PIK3CA genes, each paired with centromeric probes to their respective chromosomes (chromosomes 7, 17, 10, and 3). Ki-67 expression was assessed by immunohistochemistry (IHC). Various parameters describing copy number alterations were evaluated for each gene and centromere probe to identify the optimal parameters for clinical relevance. Combinations of ISH parameters and IHC expression for Ki-67 were also evaluated.Results: Of the four genes and their respective chromosomes evaluated by ISH, two gene copy number parameters provided statistically significant associations with pCR: MET gain or loss relative to chromosome 7 (AUC = 0.791, sensitivity = 92 % and specificity = 67 % at optimal cutoff, p = 0.0032) and gain of PTEN (AUC = 0.674, sensitivity = 38 % and specificity = 100 % at optimal cutoff, p = 0.039). Ki-67 expression was also found to associate significantly with pCR (AUC = 0.726, sensitivity = 100 % and specificity = 42 % at optimal cutoff, p = 0.0098). Combining gain or loss of MET relative to chromosome 7 with Ki-67 expression further improved the association with pCR (AUC = 0.847, sensitivity = 92 % and specificity = 83 % at optimal cutoffs, p = 0.0006).Conclusions: An immunogenotypic signature of low complexity comprising MET relative copy number and Ki-67 expression generated by dual ISH and IHC may help predict pCR in ERBB2-positive breast cancer treated with neoadjuvant chemotherapy and trastuzumab. These findings require validation in additional patient cohorts. [ABSTRACT FROM AUTHOR]

Published
2016
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21. The expression of TRMT2A, a novel cell cycleregulated protein, identifies a subset of breastcancer patients with HER2 over-expression thatare at an increased risk of recurrence.

Author

Hicks, David G., Janarthanan, Bagi R., Vardarajan, Ramya, Kulkarni, Swati A., Khoury, Thaer, Dim, Daniel, Budd, G. Thomas, Yoder, Brian J., Tubbs, Raymond, Schreeder, Marshall T., Estopinal, Noel C., Beck, Rodney A., Yanling Wang, Ring, Brian Z., Seitz, Robert S., and Ross, Douglas T.

Subjects
CANCER patients, BREAST cancer, CANCER treatment, DRUG therapy, CELL cycle regulation
Abstract

Background: Over-expression of HER2 in a subset of breast cancers (HER2+) is associated with high histological grade and aggressive clinical course. Despite these distinctive features, the differences in response of HER2+ patients to both adjuvant cytotoxic chemotherapy and targeted therapy (e.g. trastuzumab) suggests that unrecognized biologic and clinical diversity is confounding treatment strategies. Furthermore, the small but established risk of cardiac morbidity with trastuzumab therapy compels efforts towards the identification of biomarkers that might help stratify patients. Methods: A single institution tissue array cohort assembled at the Clearview Cancer Institute of Huntsville (CCIH) was screened by immunohistochemistry staining using a large number of novel and commercially available antibodies to identify those with a univariate association with clinical outcome in HER2+ patients. Staining with antibody directed at TRMT2A was found to be strongly associated with outcome in HER2+ patients. This association with outcome was tested in two independent validation cohorts; an existing staining dataset derived from tissue assembled at the Cleveland Clinic Foundation (CCF), and in a new retrospective study performed by staining archived paraffin blocks available at the Roswell Park Cancer Institute (RPCI). Results: TRMT2A staining showed a strong correlation with likelihood of recurrence at five years in 67 HER2+ patients from the CCIH discovery cohort (HR 7.0; 95% CI 2.4 to 20.1, p < 0.0004). This association with outcome was confirmed using 75 HER2+ patients from the CCF cohort (HR 3.6; 95% CI 1.3 to 10.2, p < 0.02) and 64 patients from the RPCI cohort (HR 3.4; 95% CI 1.3-8.9, p < 0.02). In bivariable analysis the association with outcome was independent of grade, tumor size, nodal status and the administration of conventional adjuvant chemotherapy in the CCIH and RPCI cohorts. Conclusions: Studies from three independent single institution cohorts support TRMT2A protein expression as a biomarker of increased risk of recurrence in HER2+ breast cancer patients. These results suggest that TRMT2A expression should be further studied in the clinical trial setting to explore its predictive power for response to adjuvant cytotoxic chemotherapy in combination with HER2 targeted therapy. [ABSTRACT FROM AUTHOR]

Published
2010
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24. A phase II pharmacodynamic study of pyrazoloacridine in patients with metastatic colorectal cancer.

Author

Pelley, Robert, Ganapathi, Ram, Wood, Laura, Rybicki, Lisa, McLain, Denise, Budd, G. Thomas, Peereboom, David, Olencki, Thomas, and Bukowski, Ronald M.

Subjects
CANCER patients, GENES, NUCLEIC acids, THERAPEUTICS, COLON cancer, MEDICAL care
Abstract

Purpose: To perform a phase II trial of pyrazoloacridine (PZA), a novel DNA intercalator, in patients with metastatic colorectal carcinoma and no previous therapy. Methods: PZA was administered at a dose of 750 mg/m2 intravenously over 3 h every 21 days. Pharmacokinetic studies to determine PZA plasma concentrations were performed. Results: No responses were seen in 14 response-evaluable patients. Patients received a median of two cycles of PZA (range 1–6). Toxicity included neutropenia and neurologic side-effects, which were ≥ grade III in 73% and 14%, respectively. High plasma concentrations of PZA (Cmax) correlated with low neutrophil counts (P=0.04). Conclusions: PZA is inactive at this dose and schedule in colorectal cancer, and produces moderately severe toxicity. [ABSTRACT FROM AUTHOR]

Published
2000
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33. Primary Extraosseous Ewing Sarcoma of the Kidney With Level III Inferior Vena Cava Thrombus.

Author

Fergany, Amr F., Dhar, Nivedita, Budd, G. Thomas, Skacel, Marek, and Garcia, Jorge A.

Subjects
EWING'S sarcoma, KIDNEY tumors, SOFT tissue tumors, VENA cava inferior, BLOOD coagulation, TOMOGRAPHY, DIAGNOSIS
Abstract

Ewing sarcoma typically presents as a skeletal-based tumor, with rare instances of peripheral primitive neuroectodermal tumor (PNET) arising in the soft tissues. Few examples of organ-based PNETs have been previously described in the literature. These tumors are exceedingly rare as a primary renal neoplasm. To our knowledge, this is the first report documenting a primary extraskeletal Ewing sarcoma of the kidney with thrombus extending into the intrahepatic inferior vena cava thrombus (level III). [ABSTRACT FROM AUTHOR]

Published
2009
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34. Hypercalcemia caused by metastatic adamantinoma: response to radiotherapy.

Author

Lyons, Janice A., Budd, G. Thomas, and Crownover, Richard L.

Subjects
LUNG cancer, HYPERCALCEMIA
Abstract

Purpose . To describe successful palliation of a patient with metastatic adamantinoma presenting with lung metastases and hypercalcemia resulting from a parathormone-like substance released from the tumor. Methods and materials. The records of a patient with a history of a tibial adamantinoma who presented with symptoms of hypercalcemia 20 years after the original surgery, as well as the literature concerning hypercalcemia and adamantinoma were reviewed and summarized. Results. After thorough review of the literature we found no prior reports of radiation being used for palliation of hypercalcemia associated with metastatic adamantinoma. We report rapid improvement in symptoms and normalization of serum calcium levels following a course of radiation therapy.The patient remains asymptomatic 15 months following radiotherapy despite a gradual return of elevated serum calcium levels. Discussion. Radiation therapy should be considered as a palliative option for patients who are not surgical candidates presenting with medically refractory hypercalcemia. [ABSTRACT FROM AUTHOR]

Published
1999
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36. Supplement Use and Chemotherapy-Induced Peripheral Neuropathy in a Cooperative Group Trial (S0221): The DELCaP Study.

Author

Zirpoli, Gary R, McCann, Susan E, Sucheston-Campbell, Lara E, Hershman, Dawn L, Ciupak, Gregory, Davis, Warren, Unger, Joseph M, Moore, Halle C F, Stewart, James A, Isaacs, Claudine, Hobday, Timothy J, Salim, Muhammad, Hortobagyi, Gabriel N, Gralow, Julie R, Budd, G Thomas, Albain, Kathy S, and Ambrosone, Christine B

Abstract

Background: Chemotherapy-induced peripheral neuropathy (CIPN) can interfere with daily function and quality of life, and there are no known preventive approaches. In a cohort of breast cancer patients receiving paclitaxel as part of a clinical trial (SWOG 0221), we examined the use of dietary supplements both before diagnosis and during treatment in relation to CIPN.Methods: At registration to S0221, 1225 breast cancer patients completed questionnaires regarding the use of multivitamins and supplements before and at diagnosis. A second questionnaire at six months queried use during treatment. Supplement use was evaluated in relation to CIPN, assessed via the National Cancer Institute Common Terminology Criteria for Adverse Events (CTCAE v. 3.0) and the self-reported Functional Assessment of Cancer Therapy/Gynecologic Oncology Group Neurotoxicity (FACT/GOG-Ntx) subscale. Odds ratios (ORs) and 95% confidence intervals (CIs) were computed with logistic regression for the CTCAE analyses and ordinal regression for the FACT/GOG-Ntx analyses.Results: Multivitamin use before diagnosis was associated with reduced symptoms of CIPN (CTCAE-adjusted OR = 0.60, 95% CI = 0.42 to 0.87; FACT/GOG-Ntx-adjusted OR = 0.78, 95% CI = 0.61 to 1.00). Use during treatment was marginally inversely associated with CIPN (CTCAE-adjusted OR = 0.73, 95% CI = 0.49 to 1.08; FACT/GOG-Ntx-adjusted OR = 0.77, 95% CI = 0.60 to 0.99). Other supplement use, either before diagnosis or during treatment, was not statistically significantly associated with CIPN.Conclusions: Multivitamin use may be associated with reduced risk of CIPN, although individual dietary supplement use did not appreciably affect risk. Multivitamin use could be a surrogate for other related behaviors that are the actual drivers of the association with reduced CIPN. Without prospective randomized trials of vitamin supplementation, recommendations for use or changes to clinical practice are clearly not warranted. [ABSTRACT FROM AUTHOR]

Published
2017
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37. Palindromic amplification of the ERBB2 oncogene in primary HER2-positive breast tumors.

Author

Marotta, Michael, Onodera, Taku, Johnson, Jeffrey, Budd, G. Thomas, Watanabe, Takaaki, Cui, Xiaojiang, Giuliano, Armando E., Niida, Atsushi, and Tanaka, Hisashi

Abstract

Oncogene amplification confers a growth advantage to tumor cells for clonal expansion. There are several, recurrently amplified oncogenes throughout the human genome. However, it remains unclear whether this recurrent amplification is solely a manifestation of increased fitness resulting from random amplification mechanisms, or if a genomic locus-specific amplification mechanism plays a role. Here we show that the ERBB2 oncogene at 17q12 is susceptible to palindromic gene amplification, a mechanism characterized by the inverted (palindromic) duplication of genomic segments, in HER2-positive breast tumors. We applied two genomic approaches to investigate amplification mechanisms: sequencing of DNA libraries enriched with tumor-derived palindromic DNA (Genome-wide Analysis of Palindrome Formation) and whole genome sequencing (WGS). We observed significant enrichment of palindromic DNA within amplified ERBB2 genomic segments. Palindromic DNA was particularly enriched at amplification peaks and at boundaries between amplified and normal copy-number regions. Thus, palindromic gene amplification shaped the amplified ERBB2 locus. The enrichment of palindromic DNA throughout the amplified segments leads us to propose that the ERBB2 locus is amplified through the mechanism that repeatedly generates palindromic DNA, such as Breakage-Fusion-Bridge cycles. The genomic architecture surrounding ERBB2 in the normal genome, such as segmental duplications, could promote the locus-specific mechanism. [ABSTRACT FROM AUTHOR]

Published
2017
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40. A common copy-number breakpoint of ERBB2 amplification in breast cancer colocalizes with a complex block of segmental duplications.

Author

Marotta, Michael, Chen, Xiongfong, Inoshita, Ayako, Stephens, Robert, Thomas Budd, G, Crowe, Joseph P, Lyons, Joanne, Kondratova, Anna, Tubbs, Raymond, Tanaka, Hisashi, and Budd, G Thomas

Subjects
BREAST cancer research, HUMAN genome, HER2 protein, POLYMERASE chain reaction, GENE amplification
Abstract

Introduction: Segmental duplications (low-copy repeats) are the recently duplicated genomic segments in the human genome that display nearly identical (> 90%) sequences and account for about 5% of euchromatic regions. In germline, duplicated segments mediate nonallelic homologous recombination and thus cause both non-disease-causing copy-number variants and genomic disorders. To what extent duplicated segments play a role in somatic DNA rearrangements in cancer remains elusive. Duplicated segments often cluster and form genomic blocks enriched with both direct and inverted repeats (complex genomic regions). Such complex regions could be fragile and play a mechanistic role in the amplification of the ERBB2 gene in breast tumors, because repeated sequences are known to initiate gene amplification in model systems.Methods: We conducted polymerase chain reaction (PCR)-based assays for primary breast tumors and analyzed publically available array-comparative genomic hybridization data to map a common copy-number breakpoint in ERBB2-amplified primary breast tumors. We further used molecular, bioinformatics, and population-genetics approaches to define duplication contents, structural variants, and haplotypes within the common breakpoint.Results: We found a large (> 300-kb) block of duplicated segments that was colocalized with a common-copy number breakpoint for ERBB2 amplification. The breakpoint that potentially initiated ERBB2 amplification localized in a region 1.5 megabases (Mb) on the telomeric side of ERBB2. The region is very complex, with extensive duplications of KRTAP genes, structural variants, and, as a result, a paucity of single-nucleotide polymorphism (SNP) markers. Duplicated segments are varied in size and degree of sequence homology, indicating that duplications have occurred recurrently during genome evolution.Conclusions: Amplification of the ERBB2 gene in breast tumors is potentially initiated by a complex region that has unusual genomic features and thus requires rigorous, labor-intensive investigation. The haplotypes we provide could be useful to identify the potential association between the complex region and ERBB2 amplification. [ABSTRACT FROM AUTHOR]

Published
2012
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42. POINT / COUNTER.

Author

Hudis, Clifford and Budd, G. Thomas

Published
2009

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