Your search keyword '"N. Burger"' showing total 12 results

1. Methylated DNA markers for monitoring palliative chemotherapy response in advanced colorectal cancer

Author

Graham P. Lidgard, Sara S. Then, Michael W. Kaiser, Hatim T. Allawi, Hao Xie, Joleen M. Hubbard, Douglas W. Mahoney, Kelli N. Burger, John B. Kisiel, Karen A. Doering, Mojun Zhu, William R. Taylor, and Patrick H. Foote

Subjects

Advanced colorectal cancer, Oncology, Cancer Research, medicine.medical_specialty, business.industry, Colorectal cancer, Genetic marker, Internal medicine, medicine, Palliative chemotherapy, business, medicine.disease

Abstract

e15511 Background: Aberrantly methylated DNA marker (MDM) candidates are strongly associated with primary colorectal cancer (CRC) before treatment and detect CRC recurrence with high sensitivity when assayed from plasma. The relationship of these MDMs in association to chemotherapy treatment response is unknown. Methods: In a prospective cohort of patients receiving systemic therapy for advanced CRC, peripheral blood was collected serially during restaging visits. 15 patients were retrospectively identified to have partial response (PR), stable disease (SD) and progressive disease (PD) to treatment (n=5 for each group) based on the Response Evaluation Criteria in Solid Tumors (RECIST) version 1.1. Using paired samples from each patient before and after response assessment, we analyzed 11 MDMs ( GRIN2D, ZNF671, ANKRD13B, QKI, VAV3, JAM3, SFMBT2, CHST2, ZNF568, FER1L4 and CNNM1) to assess correlation with treatment response. Cell-free DNA was extracted and bisulfite treated before MDMs were quantified by target enrichment long-probe quantitative-amplified signal assay and normalized to a methylated sequence of B3GALT6. Continuous variables are summarized as a median with corresponding interquartile ranges (IQR) and comparisons between subgroups were based on the Wilcox Rank Sums test. Results: The median interval between pre- and post-response assessment visits was 69 days (IQR: 63-83 days) and the level of tumor burden at pre-assessment was similar across all response types (Table 1). Patients with PD had higher levels of methylated GRIN2D, ZNF671 and ANKRD13B than those with PR or SD at baseline and may offer additional prognostic value over CEA which was similar in the PR and PD groups before treatment (Table 1). Elevation of pre-assessment MDMs preceded radiographic evidence of disease progression by 82 days (IQR 69-83 days). Conclusions: Three MDMs, GRIN2D, ZNF671 and ANKRD13B, were found to reflect treatment response (PD vs. PR + SD) as shown in the table. Although this pilot study was limited by a small sample size, it demonstrated the feasibility of using plasma-based MDMs in monitoring treatment response to systemic therapy for advanced CRC and should be compared to CEA in a larger study.[Table: see text]

Published

2021

2. Discovery and validation of novel methylated DNA markers of cervical cancer

Author

William R. Taylor, Xiaoming Cao, Maureen A. Lemens, Rondell P. Graham, Kelli N. Burger, Seth W. Slettedahl, Calise K. Berger, Maria O'Connell, Mark E. Sherman, Brendan T. Broderick, Karen A. Doering, John B. Kisiel, Jamie N. Bakkum-Gamez, Douglas W. Mahoney, J. Kenneth Schoolmeester, Sarah E. Kerr, and Patrick H. Foote

Subjects

Oncology, Cervical cancer, Cancer Research, medicine.medical_specialty, business.industry, Genetic marker, Internal medicine, medicine, Cervical cytology, business, Dna testing, medicine.disease

Abstract

5526 Background: HR-HPV DNA testing, with or without cervical cytology, provides excellent sensitivity for detection of cervical cancer (CC) and its precursors; negative test results indicate that risk of disease is extremely low and enable women to undergo reduced screening with safety. However, management of women who screen positive remains challenging as many will prove to have self-limited HR-HPV infections. DNA methylation is an early event in carcinogenesis that could enhance CC screening specificity. Methods: For discovery, DNA from 70 FFPE CC (36 squamous, 34 adenocarcinoma) tissues that were reviewed microscopically, 18 fresh frozen benign cervicovaginal (BCV) tissues collected at the time of benign hysterectomy, and 18 buffy coats from cancer-free women underwent reduced representation bisulfite sequencing (RRBS) to identify MDMs associated with CC. Candidate MDM selection was based on area under the receiver operating characteristic curve (AUC) discrimination, methylation fold change, and low background methylation among benign controls. Candidate MDMs were re-tested using methylation-specific PCR (MSP) to confirm performance. Blinded biological validation was performed using MSP on DNA extracted from independent FFPE CC (38 squamous, 43 adenocarcinoma) and BCV (40) tissues. The performance of CC MDMs was also tested in DNA extracted from cervical dysplasia (36 adenocarcinoma in situ (AIS), 32 cervical intraepithelial neoplasia (CIN) 2/3, 11 CIN 1) FFPE tissues. Results: From RRBS discovery and technical validation via MSP, 30 candidate MDMs showed marked methylation fold changes (10 to >1000) across both CC histologies compared to BCV tissue from cancer-free women. Each of the 30 MDMs highly discriminated CC from BCV tissue with 9 MDMs having an AUC >0.90 (Table). CC MDMs also highly discriminated AIS from BCV but did not perform well in CIN 2/3 and CIN 1 (Table). Conclusions: Whole methylome sequencing, stringent filtering criteria, and biological validation have yielded outstanding candidate MDMs for CC that highly discriminate CC from BCV, notably with high specificity. Performance in cervical dysplasias varied with higher positivity rates in AIS than in CIN 2/3 and CIN 1. Translation to testing these novel MDMs in lower genital tract biospecimens and the addition of HR-HPV to the CC panel are warranted.[Table: see text]

Published

2021

3. Novel methylated DNA markers in plasma detect distant recurrence of colorectal cancer

Author

David A. Ahlquist, Calise K. Berger, Karen A. Doering, Hao Xie, John B. Kisiel, Douglas W. Mahoney, Kelli N. Burger, Patrick H. Foote, Joleen M. Hubbard, Graham P. Lidgard, Hatim T. Allawi, Maria McGlinch, William R. Taylor, and Xiaoming Cao

Subjects

Cancer Research, Colorectal cancer, business.industry, Distant recurrence, Early detection, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Oncology, Genetic marker, 030220 oncology & carcinogenesis, medicine, Cancer research, business, 030215 immunology

Abstract

4088 Background: Methylated DNA markers (MDMs) are broadly informative for early detection of colorectal cancer (CRC) but have not been extensively studied for post-treatment surveillance and disease monitoring. We aimed to assess the feasibility of novel CRC-associated MDMs for detection of distant recurrent CRC (rCRC) in plasma. Methods: A panel of 13 MDMs previously identified to be discriminant for primary CRC was selected. In a cross-sectional analysis of plasma samples, MDMs were assayed blindly (by target enrichment long-probe quantitative amplified signal assay) from 160 age/sex-balanced patients (60 healthy controls, 60 with resected CRC and no evidence of disease (NED), and 40 rCRC after primary tumor resection). Plasma-derived carcinoembryonic antigen (CEA) was measured on all patients. Random forest modeling was used to derive a prediction algorithm of MDMs (with and without CEA) for the endpoint of rCRC relative to healthy controls. The accuracy of the algorithm was summarized as sensitivity, specificity, and area under the receiver operating characteristic curve (AUC) with 95% confidence intervals (CI) in the test set. Results: Median patient age was 55 (interquartile range: 49-64) years. As shown in the Table below, a single MDM with the highest AUC was significantly better than CEA ( p= 0.02). On cross validation, CEA provided no additional improvement to the performance of the panel of 13 MDMs ( p= 0.2). The cross-validated panel of MDMs detected rCRC liver metastases with 96% (79-100%) sensitivity, lung metastases with 78% (40-97%) sensitivity, and peritoneal/nodal metastases with 57% (18-90%) sensitivity. Lesions with Response Evaluation Criteria in Solid Tumors sum > 4 cm were detected with 94% (73-100%) sensitivity and ≤4 cm with 78% (52-94%) sensitivity. Conclusions: Novel MDMs in plasma detect rCRC with promising accuracy. The clinical utility of MDMs for non-invasive post-treatment surveillance and treatment monitoring in CRC warrants further evaluation in longitudinal studies with sufficient follow-up to exclude sub-clinical recurrence in those with NED. [Table: see text]

Published

2020

4. Methylated DNA markers for plasma detection of ovarian cancer: Discovery, validation, and clinical feasibility

Author

Viji Shridhar, William R. Taylor, David A. Ahlquist, Maria Giakoumopoulos, Maureen A. Lemens, Jamie N. Bakkum-Gamez, Sarah E. Kerr, Hannah Berg, Calise K. Berger, Mark E. Sherman, John B. Kisiel, Douglas W. Mahoney, Lisa Marinelli, Hatim T. Allawi, Michael W. Kaiser, Kelli N. Burger, Seth W. Slettedahl, J. Kenneth Schoolmeester, and Karen A. Doering

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Poor prognosis, Screening test, business.industry, Advanced stage, medicine.disease, medicine.disease_cause, Genetic marker, Internal medicine, DNA methylation, Medicine, business, Ovarian cancer, Carcinogenesis

Abstract

6072 Background: Effective screening tests for ovarian cancer (OC) are lacking; most cases present at advanced stage and portend poor prognosis. DNA methylation is an early event in carcinogenesis and can be detected in blood plasma samples from cancer patients. In DNA extracted from tissues, we first discovered, then validated discriminant methylated DNA marker (MDM) candidates for OC and subsequently tested independent plasma from women with and without OC. Methods: For discovery, DNA from 67 frozen tissues (18 high grade serous (HGS), 18 endometrioid, 15 clear cell (CC), 6 mucinous OCs; 10 benign fallopian tube epithelium (FT); and 19 buffy coats from cancer-free women underwent reduced representation bisulfite sequencing (RRBS) to identify MDMs associated with OC. Candidate MDM selection was based on receiver operating characteristic (ROC) discrimination, methylation fold change, and low background methylation among controls. Blinded biological validation was performed using methylated specific PCR on DNA extracted from independent FFPE tissues from OCs (36 HGS, 22 endometrioid, 21 CC, and 14 mucinous) and 29 FT. Top performing MDMs in tissue were tested using long-probe quantitative amplified signal assays in independent pre-treatment plasma samples from women newly-diagnosed with OC and population-sampled healthy women. A random forest modeling analysis was performed to generate predictive probability of disease; results were 500-fold in silico cross-validated. Results: After RRBS discovery and biological validation, 33 MDMs showed marked methylation fold changes (10 to > 1000) across all OC histologies vs FT. The top 11 MDMs ( GPRIN1, CDO1, SRC, SIM2, AGRN, FAIM2, CELF2, DSCR6, GYPC, CAPN2, BCAT1) were tested on plasma from 91 women with OC (76 (84%) HGS) and 91 without OC; the cross-validated 11-MDM panel highly discriminated OC from controls (96% (95%CI 89-99%) specificity; 79% (69-87%) sensitivity, and AUC 0.91 (0.86 - 0.96)). Among HGS, the panel correctly identified 83%, including 5/6 stage I/II, and the majority of other subtypes (Table). Conclusions: Whole methylome sequencing, stringent filtering criteria, and biological validation yielded outstanding candidate MDMs for OC that performed with promisingly high sensitivity and specificity in plasma. Larger plasma-based OC MDM testing studies, with larger numbers of non-HGS histologies are warranted. [Table: see text]

Published

2020

5. Methylated DNA marker panel for metastatic melanoma: Discovery and tissue validation

Author

David A. Ahlquist, William R. Bamlet, Enrica Quattrocchi, Alexander Meves, Kelli N. Burger, Karen A. Doering, Patrick H. Foote, William R. Taylor, John B. Kisiel, Julia S. Lehman, and Douglas W. Mahoney

Subjects

Oncology, Cancer Research, Disease surveillance, medicine.medical_specialty, Metastatic melanoma, business.industry, Genetic marker, Melanoma, Internal medicine, medicine, business, medicine.disease

Abstract

e22024 Background: Disease surveillance in high risk melanoma patients using PET/CT is recommended every 6 months, an algorithm that is extremely expensive and often difficult to access. Biomarkers capable of detecting recurrence and low volume metastasis have application in tools to improve the cost effectiveness of surveillance. Towards this long term goal, our aim was to discover melanoma-specific methylated DNA markers (MDMs). Methods: Candidate MDMs were identified by reduced representation bisulfite sequencing of selected age- and sex-balanced snap frozen metastatic melanoma, benign control skin and white blood cells. Sequences were filtered for highest methylation difference, lowest control methylation background ( < 1%), and highest discrimination by variance inflated logistic regression. Using formalin-fixed tissues, the top 32 MDMs were further evaluated in metastatic melanoma from 35 patients, primary melanoma from 26 patients, and 73 control samples (47 benign precursor lesions or normal skin, and 26 healthy buffy coat samples to assess for background DNA in circulation). Candidate markers were blindly assayed by quantitative methylation specific PCR. After normalization by within sample ACTB level, random forest modeling with cross-validation identified marker combinations with greatest predictive accuracy. Results: On receiver operator characteristics analyses of individual marker candidates, areas under the curve (AUCs) ranged from 0.43 to 0.97. Median AUC was 0.835. At 100% specificity, a cross-validated panel of five MDMs (see Table), yielded a sensitivity of 33/35 cases (94.3%; 95% CI, 86.6-100%) for metastatic melanoma and 22/26 cases (84.6%; 95% CI, 70.7-98.5%) for primary melanoma. Furthermore, none of the 5 markers were detected in normal buffy coat samples. Conclusions: A panel of five novel MDMs assayed on tissue and undetectable in normal buffy coat achieves very high discrimination between melanoma and benign control tissues. This panel can be assessed in blood or other bodily fluids for application in melanoma surveillance. [Table: see text]

Published

2020

6. Paclitaxel-associated acute pain syndrome (P-APS) and its association on the development of peripheral neuropathy: NCCTG trial N08C1

Author

Daniel H. Lachance, Kelli N. Burger, C. L. Loprinzi, S. R. Dakhil, Gamini S. Soori, Anthony J. Jaslowski, J. A. Sloan, Brandi N. Reeves, Nguyet A. Le-Lindqwister, and Joseph Kelaghan

Subjects

musculoskeletal diseases, Cancer Research, medicine.medical_specialty, business.industry, virus diseases, medicine.disease, body regions, chemistry.chemical_compound, Peripheral neuropathy, Oncology, Paclitaxel, chemistry, Internal medicine, medicine, business, Acute pain

Abstract

9047 Background: Paclitaxel is well known to cause an acute pain syndrome that has been referred to as arthralgias and myalgias. It has been hypothesized that this pain might actually be neurologic...

Published

2011

7. Using the Skindex-16 and CTCAE to assess rash symptoms: Results of a pooled-analysis (N0993)

Author

Robert C. Miller, Charles L. Loprinzi, Kelli N. Burger, Aminah Jatoi, Jeff A. Sloan, and Pamela J. Atherton

Subjects

Clinical trial, Cancer Research, medicine.medical_specialty, Pooled analysis, Oncology, business.industry, medicine, Cancer, medicine.symptom, medicine.disease, business, Dermatology, Rash

Abstract

9018 Background: Historically, symptoms of rash have been measured in prospective clinical trials using the clinician- reported National Cancer Institute Common Terminology Criteria for Adverse Eve...

Published

2010

8. Natural history of paclitaxel-associated acute pain syndrome (P-APS): NCCTG trial N08C1

Author

Kelli N. Burger, C. L. Loprinzi, Gamini S. Soori, Anthony J. Jaslowski, Arif H. Kamal, S. R. Dakhil, Brandi N. Reeves, J. A. Sloan, Nguyet A. Le-Lindqwister, and Sherry L. Wolf

Subjects

musculoskeletal diseases, Cancer Research, medicine.medical_specialty, business.industry, virus diseases, body regions, Natural history, chemistry.chemical_compound, Oncology, Paclitaxel, chemistry, Internal medicine, medicine, business, Acute pain

Abstract

9135 Background: Paclitaxel is well known to cause an acute pain syndrome that has, in the past, been referred to as arthralgias and myalgias. It has been hypothesized that this pain might actually...

Published

2010

9. A phase I study of tumor treating fields (TTFields) in combination with pemetrexed for pretreated advanced non-small cell lung cancer

Author

Daniel Betticher, Yoram Palti, N. Burger, Miklos Pless, Eilon D. Kirson, J. Studt, Natalie Fischer, R. von Moos, Uri Weinberg, and Martin Buess

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Kidney, Pathology, Lung, business.industry, Cell, medicine.disease, Clinical trial, medicine.anatomical_structure, Pemetrexed, Internal medicine, Toxicity, Medicine, Stage (cooking), business, Lung cancer, medicine.drug

Abstract

e18500 Background: TTFields (tumor treating fields) are low intensity, intermediate frequency, alternating electric fields which slow the growth of solid tumors in-vivo, and have shown promise in pilot clinical trials in patients with advanced solid tumors. TTFields are a regional treatment which acts both by interfering with microtubules polymerization and by physical disruption of the cell structure during cytokinesis. It has been shown previously that TTFields sensitize non-small cell lung cultures to Pemetrexed. In-Vivo, TTFields did not increase pemetrexed related toxicity. Methods: A prospective trial was performed in 14, pretreated, stage IIIb-IV, NSCLC patients. Patients with brain metastases were excluded, as were patients with abnormal marrow, kidney, liver or cardiac functions. Patients with history of clinically significant arrhythmias or those having pacemakers were excluded as well. Patients received Pemetrexed 500mg/m2 IV q3w together with daily TTFields (12 h/day) using a portable medical device (NovoTTF-100L). The device generated 2 direction (AP and Lat), 150 kHz TTFields. Patients were followed every three weeks and had a lung CT every 9 weeks. The primary endpoint was the safety and tolerability of the NovoTTF-100L device in combination with pemetrexed. Results: The 14 patients received an average of 4 courses of pemetrexed (Range 1–9) and a cumulative TTFields treatment time of 182 weeks. The device was well tolerated as indicated in the device log files which showed an average daily use of 11±1 hours. There were no device-related, nor pemetrexed-related SAEs. In addition, no unexpected abnormalities were evident in the lab tests or EKGs, done every 3 weeks for all patients. There were no reports of arrhythmias. The only device related AE seen in all patients was dermatitis under the electrodes. This improved with meticulous skin care, topical steroid use and in extreme cases oral steroids. One patient (7.6%) had a CR, 1 a PR (7.6%), 9 SD (69.2%) and 3 PD (23%). 77% of patients were progression free at 12 weeks and the 6 month survival was 89%. Conclusions: TTFields are well tolerated when given together with pemetrexed. The excellent safety profile and initial efficacy results reported here justify further clinical testing. [Table: see text]

Published

2009

10. Pregabalin for hot flashes in women: NCCTG trial N07C1

Author

David L. Graham, R. Qin, C. L. Loprinzi, P. J. Stella, S. R. Dakhil, Kendrith M. Rowland, Kelli N. Burger, Donald J. Jurgens, and N. Erwin

Subjects

Cancer Research, genetic structures, Oncology, Gabapentin, business.industry, Anesthesia, Pregabalin, Treatment options, Medicine, business, medicine.drug

Abstract

9513 Background: Hot flashes are a major problem in many women for which better treatment options are needed. Given the known efficacy of gabapentin for decreasing hot flashes, it was decided to evaluate pregabalin, with hopes that it would work better and/or with fewer toxicities. Methods: A three-arm, double-blinded, placebo-controlled randomized trial was developed. Women with bothersome hot flashes (at least 28/week) were randomized to receive either a placebo or target pregabalin oral doses of 75 mg bid or 150 mg bid (starting at 50 mg/d and then increasing the dose at weekly intervals to 50 mg bid, then 75 mg bid, and then, in the higher dose arm, 150 mg bid); patients were treated for 6 weeks. Hot flash numbers and scores (hot flash number times mean severity) were measured using a validated daily hot flash diary. A one-week baseline period preceded initiation of study tablets. The primary endpoint was the average intra-patient difference in hot flash score between baseline and week six, comparing the higher dose pregabalin arm and the placebo arm. With the planned sample size of 55 patients per arm, there was an 80% power and two-sided 5% Type I error rate to detect a difference of 0.54 standard deviations, or 1.08 hot flashes per day, or 2.7 units of hot flash score per day. Results: 207 patients were randomized between 6/20/2008 and 8/21/2008. The study arms were well balanced. Mean/median daily hot flash scores and frequencies for all pts at baseline were 15.7/13.4 and 8.3/7.7, respectively. The table shows the decreases in hot flashes from the baseline to the sixth treatment week. Larger numbers illustrate greater hot flash reductions. Toxicity information, quality of life information, and information regarding the effects of hot flashes on subjective symptoms will be available at the meeting time. Conclusions: Pregabalin reduces hot flashes in women. There appears to be similar effects with both studied doses. [Table: see text] No significant financial relationships to disclose.

Published

2009

11. Compliance issues in completion of patient-reported outcomes in a series of NCCTG/Mayo clinical trials

Author

Michele Y. Halyard, Pamela J. Atherton, Kelli N. Burger, J. A. Sloan, and Paul L. Schaefer

Subjects

Gerontology, Clinical trial, Cancer Research, medicine.medical_specialty, Oncology, business.industry, Physical therapy, Medicine, Patient compliance, business, humanities, Compliance (psychology)

Abstract

17506 Background: The use of Patient Reported Outcomes (PROs) as measures of primary and secondary endpoints in clinical trials has increased, thus study results rely on patient compliance. This st...

Published

2008

12. Endpoint comparison for osteoporosis assessment in cancer control studies (N02C1 and N03CC)

Author

Brent Diekmann, Xinghua Zhao, Stephanie L. Hines, Kelli N. Burger, C. L. Loprinzi, E. A. Perez, Angelina Tan, J. A. Sloan, Amylou C. Dueck, Heshan Liu, and Pamela J. Atherton

Subjects

Oncology, Bone mineral, Cancer Research, medicine.medical_specialty, business.industry, Osteoporosis, food and beverages, Cancer, medicine.disease, Cancer control, Internal medicine, medicine, business

Abstract

6627 Background: Methodological issues hamper efficacy assessment of agents to prevent osteoporosis in cancer survivors. The diagnosis of osteoporosis can vary depending upon which bone mineral den...

Published

2008