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543 results on '"Finkelstein, Dianne M."'

1. Early Detection of Ovarian Cancer using the Risk of Ovarian Cancer Algorithm with Frequent CA125 Testing in Women at Increased Familial Risk – Combined Results from Two Screening Trials

Author

Skates, Steven J, Greene, Mark H, Buys, Saundra S, Mai, Phuong L, Brown, Powel, Piedmonte, Marion, Rodriguez, Gustavo, Schorge, John O, Sherman, Mark, Daly, Mary B, Rutherford, Thomas, Brewster, Wendy R, O'Malley, David M, Partridge, Edward, Boggess, John, Drescher, Charles W, Isaacs, Claudine, Berchuck, Andrew, Domchek, Susan, Davidson, Susan A, Edwards, Robert, Elg, Steven A, Wakeley, Katie, Phillips, Kelly-Anne, Armstrong, Deborah, Horowitz, Ira, Fabian, Carol J, Walker, Joan, Sluss, Patrick M, Welch, William, Minasian, Lori, Horick, Nora K, Kasten, Carol H, Nayfield, Susan, Alberts, David, Finkelstein, Dianne M, and Lu, Karen H

Subjects
Cancer, Ovarian Cancer, Prevention, Genetic Testing, Rare Diseases, Clinical Research, Genetics, Detection, screening and diagnosis, 4.4 Population screening, Adult, Aged, Algorithms, Breast Neoplasms, CA-125 Antigen, Early Detection of Cancer, Female, Humans, Membrane Proteins, Middle Aged, Neoplasm Staging, Ovarian Neoplasms, Risk Factors, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

Purpose: Women at familial/genetic ovarian cancer risk often undergo screening despite unproven efficacy. Research suggests each woman has her own CA125 baseline; significant increases above this level may identify cancers earlier than standard 6- to 12-monthly CA125 > 35 U/mL.Experimental Design: Data from prospective Cancer Genetics Network and Gynecologic Oncology Group trials, which screened 3,692 women (13,080 woman-screening years) with a strong breast/ovarian cancer family history or BRCA1/2 mutations, were combined to assess a novel screening strategy. Specifically, serum CA125 q3 months, evaluated using a risk of ovarian cancer algorithm (ROCA), detected significant increases above each subject's baseline, which triggered transvaginal ultrasound. Specificity and positive predictive value (PPV) were compared with levels derived from general population screening (specificity 90%, PPV 10%), and stage-at-detection was compared with historical high-risk controls.Results: Specificity for ultrasound referral was 92% versus 90% (P = 0.0001), and PPV was 4.6% versus 10% (P > 0.10). Eighteen of 19 malignant ovarian neoplasms [prevalent = 4, incident = 6, risk-reducing salpingo-oophorectomy (RRSO) = 9] were detected via screening or RRSO. Among incident cases (which best reflect long-term screening performance), three of six invasive cancers were early-stage (I/II; 50% vs. 10% historical BRCA1 controls; P = 0.016). Six of nine RRSO-related cases were stage I. ROCA flagged three of six (50%) incident cases before CA125 exceeded 35 U/mL. Eight of nine patients with stages 0/I/II ovarian cancer were alive at last follow-up (median 6 years).Conclusions: For screened women at familial/genetic ovarian cancer risk, ROCA q3 months had better early-stage sensitivity at high specificity, and low yet possibly acceptable PPV compared with CA125 > 35 U/mL q6/q12 months, warranting further larger cohort evaluation. Clin Cancer Res; 23(14); 3628-37. ©2017 AACR.

Published
2017

2. A Pilot Investigation of an iOS-Based App for Toilet Training Children with Autism Spectrum Disorder

Author

Mruzek, Daniel W., McAleavey, Stephen, Loring, Whitney A., Butter, Eric, Smith, Tristram, McDonnell, Erin, Levato, Lynne, Aponte, Courtney, Travis, Rebekah P., Aiello, Rachel E., Taylor, Cora M., Wilkins, Jonathan W., Corbett-Dick, Patricia, Finkelstein, Dianne M., York, Alyssa M., and Zanibbi, Katherine

Abstract

We developed an iOS-based app with a transmitter/disposable sensor and corresponding manualized intervention for children with autism spectrum disorder. The app signaled the onset of urination, time-stamped accidents for analysis, reminded parents to reinforce intervals of continence, provided a visual outlet for parents to communicate reinforcement, and afforded opportunity for timely feedback from clinicians. We compared this intervention with an intervention that uses standard behavioral treatment in a pilot randomized controlled trial of 33 children with autism spectrum disorder aged 3-6 years with urinary incontinence. Parents in both groups received initial training and four booster consultations over 3 months. Results support the feasibility of parent-mediated toilet training studies (e.g., 84% retention rate, 92% fidelity of parent-implemented intervention). Parents used the app and related technology with few difficulties or malfunctions. There were no statistically significant group differences for rate of urine accidents, toilet usage, or satisfaction at close of intervention or 3-month follow-up; however, the alarm group trended toward greater rate of skill acquisition with significantly less day-to-day intervention. Further development of alarm and related technology and future comparative studies with a greater number of participants are warranted.

Published
2019
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5. Evaluating Academic Scientists Collaborating in Team-Based Research

Author

Mazumdar, Madhu, Messinger, Shari, Finkelstein, Dianne M, Goldberg, Judith D, Lindsell, Christopher J, Morton, Sally C, Pollock, Brad H, Rahbar, Mohammad H, Welty, Leah J, and Parker, Robert A

Subjects
Curriculum and Pedagogy, Health Services and Systems, Health Sciences, Education, Prevention, Academic Medical Centers, Authorship, Cooperative Behavior, Employee Performance Appraisal, Faculty, Faculty, Medical, Humans, Research, Teaching, Biostatistics, Epidemiology, and Research Design (BERD) Key Function Committee of the Clinical and Translational Science Awards (CTSA) Consortium, Clinical Sciences, General & Internal Medicine, Curriculum and pedagogy, Health services and systems
Abstract

Criteria for evaluating faculty are traditionally based on a triad of scholarship, teaching, and service. Research scholarship is often measured by first or senior authorship on peer-reviewed scientific publications and being principal investigator on extramural grants. Yet scientific innovation increasingly requires collective rather than individual creativity, which traditional measures of achievement were not designed to capture and, thus, devalue. The authors propose a simple, flexible framework for evaluating team scientists that includes both quantitative and qualitative assessments. An approach for documenting contributions of team scientists in team-based scholarship, nontraditional education, and specialized service activities is also outlined. Although biostatisticians are used for illustration, the approach is generalizable to team scientists in other disciplines.The authors offer three key recommendations to members of institutional promotion committees, department chairs, and others evaluating team scientists. First, contributions to team-based scholarship and specialized contributions to education and service need to be assessed and given appropriate and substantial weight. Second, evaluations must be founded on well-articulated criteria for assessing the stature and accomplishments of team scientists. Finally, mechanisms for collecting evaluative data must be developed and implemented at the institutional level. Without these three essentials, contributions of team scientists will continue to be undervalued in the academic environment.

Published
2015

6. TBCRC009: A Multicenter Phase II Clinical Trial of Platinum Monotherapy With Biomarker Assessment in Metastatic Triple-Negative Breast Cancer

Author

Isakoff, Steven J, Mayer, Erica L, He, Lei, Traina, Tiffany A, Carey, Lisa A, Krag, Karen J, Rugo, Hope S, Liu, Minetta C, Stearns, Vered, Come, Steven E, Timms, Kirsten M, Hartman, Anne-Renee, Borger, Darrel R, Finkelstein, Dianne M, Garber, Judy E, Ryan, Paula D, Winer, Eric P, Goss, Paul E, and Ellisen, Leif W

Subjects
Genetics, Cancer, Clinical Research, Clinical Trials and Supportive Activities, Breast Cancer, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Good Health and Well Being, Adult, Aged, Antineoplastic Agents, BRCA1 Protein, BRCA2 Protein, Biomarkers, Tumor, Carboplatin, Cisplatin, Class I Phosphatidylinositol 3-Kinases, Drug Administration Schedule, Female, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Genomic Instability, Heterozygote, Humans, Loss of Heterozygosity, Middle Aged, Mutation, Neoplasm Staging, Phosphatidylinositol 3-Kinases, Treatment Outcome, Triple Negative Breast Neoplasms, Clinical Sciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeThe identification of patients with metastatic triple-negative breast cancer (mTNBC) who are expected to benefit from platinum-based chemotherapy is of interest. We conducted a single-arm phase II clinical trial of single-agent platinum for mTNBC with biomarker correlates.Patients and methodsPatients with mTNBC received first- or second-line cisplatin (75 mg/m(2)) or carboplatin (area under the concentration-time curve 6) by physician's choice once every 3 weeks. Coprimary end points were objective response rate (RR) and response prediction by p63/p73 gene expression. Secondary and exploratory end points included toxicity assessment, RR in cisplatin versus carboplatin, and RR in molecularly defined subgroups, including BRCA1/2 mutation carriers.ResultsPatients (N = 86; 69 as first-line therapy) received cisplatin (n = 43) or carboplatin (n = 43). RR was 25.6% (95% CI, 16.8% to 36%) and was numerically higher with cisplatin (32.6%) than with carboplatin (18.7%). RR was 54.5% in patients with germline BRCA1/2 mutations (n = 11). In patients without BRCA1/2 mutations (n = 66), exploratory analyses showed that a BRCA-like genomic instability signature (n = 32) discriminated responding and nonresponding tumors (mean homologous recombination deficiency-loss of heterozygosity/homologous recombination deficiency-large-scale state transitions [HRD-LOH/HRD-LST] scores were 12.68 and 5.11, respectively), whereas predefined analysis by p63/p73 expression status (n = 61), p53 and PIK3CA mutation status (n = 53), or PAM50 gene expression subtype (n = 55) did not. Five of the six long-term responders alive at a median of 4.5 years lacked germline BRCA1/2 mutations, and two of them had increased tumor HRD-LOH/HRD-LST scores.ConclusionPlatinum agents are active in mTNBC, especially in patients with germline BRCA1/2 mutations. A measure of tumor DNA repair function may identify patients without mutations who could benefit from platinum therapy agents. Prospective controlled confirmatory trials are warranted.

Published
2015

7. Long-term risk of medical conditions associated with breast cancer treatment

Author

Hill, Deirdre A, Horick, Nora K, Isaacs, Claudine, Domchek, Susan M, Tomlinson, Gail E, Lowery, Jan T, Kinney, Anita Y, Berg, Jonathan S, Edwards, Karen L, Moorman, Patricia G, Plon, Sharon E, Strong, Louise C, Ziogas, Argyrois, Griffin, Constance A, Kasten, Carol H, and Finkelstein, Dianne M

Subjects
Osteoporosis, Clinical Research, Prevention, Breast Cancer, Aging, Rehabilitation, Cancer, Cardiovascular, Heart Disease, Heart Disease - Coronary Heart Disease, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies, Adult, Aged, Antineoplastic Agents, Bone Diseases, Metabolic, Breast Neoplasms, Female, Heart Diseases, Humans, Lymph Node Excision, Lymphedema, Middle Aged, Prevalence, Radiotherapy, Risk Factors, Surveys and Questionnaires, Survivors, Breast neoplasms, Heart disease, Chemotherapy, Clinical Sciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

Early and late effects of cancer treatment are of increasing concern with growing survivor populations, but relevant data are sparse. We sought to determine the prevalence and hazard ratio of such effects in breast cancer cases. Women with invasive breast cancer and women with no cancer history recruited for a cancer research cohort completed a mailed questionnaire at a median of 10 years post-diagnosis or matched reference year (for the women without cancer). Reported medical conditions including lymphedema, osteopenia, osteoporosis, and heart disease (congestive heart failure, myocardial infarction, coronary heart disease) were assessed in relation to breast cancer therapy and time since diagnosis using Cox regression. The proportion of women currently receiving treatment for these conditions was calculated. Study participants included 2,535 women with breast cancer and 2,428 women without cancer (response rates 66.0 % and 50.4 %, respectively) Women with breast cancer had an increased risk of lymphedema (Hazard ratio (HR) 8.6; 95 % confidence interval (CI) 6.3-11.6), osteopenia (HR 2.1; 95 % CI 1.8-2.4), and osteoporosis (HR 1.5; 95 % CI 1.2-1.9) but not heart disease, compared to women without cancer Hazard ratios varied by treatment and time since diagnosis. Overall, 49.3 % of breast cancer cases reported at least one medical condition, and at 10 or more years post-diagnosis, 37.7 % were currently receiving condition-related treatment. Responses from survivors a decade following cancer diagnosis demonstrate substantial treatment-related morbidity, and emphasize the need for continued medical surveillance and follow-up care into the second decade post-diagnosis.

Published
2014

14. Analysis of Co-Aggregation of Cancer Based on Registry Data

Author

Matthews, Abigail G, Betensky, Rebecca A, Anton-Culver, Hoda, Bowen, Deborah, Griffin, Constance, Isaacs, Claudine, Kasten, Carol, Mineau, Geraldine, Nayfield, Susan, Schildkraut, Joellen, Strong, Louise, Weber, Barbara, and Finkelstein, Dianne M

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Ovarian Cancer, Colo-Rectal Cancer, Rare Diseases, Cancer, Digestive Diseases, Clinical Research, Pancreatic Cancer, 2.1 Biological and endogenous factors, Aetiology, Female, Humans, Male, Neoplasms, Registries, familial aggregation, association, family study, Cancer Genetics Network, Medical Biotechnology, Clinical Sciences, Public Health and Health Services, Genetics & Heredity, Clinical sciences, Public health
Abstract

ObjectiveAn exploratory analysis of co-aggregation of cancers using registry-based data.MethodsWe utilized sibships from over 18,000 families who had been recruited to the NCI-sponsored multi-institutional Cancer Genetics Network. The analysis assesses co-aggregation at the individual and family level and adjusts for ascertainment.ResultsWe found statistically significant familial co-aggregation of lung cancer with pancreatic (adjusted p < 0.001), prostate (adjusted p < 0.003), and colorectal cancers (adjusted p = 0.004). In addition, we found significant familial co-aggregation of pancreatic and colorectal cancers (adjusted p = 0.018), and co-aggregation of hematopoietic and (non-ovarian) gynecologic cancers (adjusted p = 0.01).ConclusionThis analysis identified familial aggregation of cancers for which a genetic component has yet to be established.

Published
2006

17. Supplementary Figures and Tables from Expressed Gene Fusions as Frequent Drivers of Poor Outcomes in Hormone Receptor–Positive Breast Cancer

Author

Matissek, Karina J., primary, Onozato, Maristela L., primary, Sun, Sheng, primary, Zheng, Zongli, primary, Schultz, Andrew, primary, Lee, Jesse, primary, Patel, Kristofer, primary, Jerevall, Piiha-Lotta, primary, Saladi, Srinivas Vinod, primary, Macleay, Allison, primary, Tavallai, Mehrad, primary, Badovinac-Crnjevic, Tanja, primary, Barrios, Carlos, primary, Beşe, Nuran, primary, Chan, Arlene, primary, Chavarri-Guerra, Yanin, primary, Debiasi, Marcio, primary, Demirdögen, Elif, primary, Egeli, Ünal, primary, Gökgöz, Sahsuvar, primary, Gomez, Henry, primary, Liedke, Pedro, primary, Tasdelen, Ismet, primary, Tolunay, Sahsine, primary, Werutsky, Gustavo, primary, St. Louis, Jessica, primary, Horick, Nora, primary, Finkelstein, Dianne M., primary, Le, Long Phi, primary, Bardia, Aditya, primary, Goss, Paul E., primary, Sgroi, Dennis C., primary, Iafrate, A. John, primary, and Ellisen, Leif W., primary

Published
2023
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18. Supplementary Materials from Early Detection of Ovarian Cancer using the Risk of Ovarian Cancer Algorithm with Frequent CA125 Testing in Women at Increased Familial Risk – Combined Results from Two Screening Trials

Author

Skates, Steven J., primary, Greene, Mark H., primary, Buys, Saundra S., primary, Mai, Phuong L., primary, Brown, Powel, primary, Piedmonte, Marion, primary, Rodriguez, Gustavo, primary, Schorge, John O., primary, Sherman, Mark, primary, Daly, Mary B., primary, Rutherford, Thomas, primary, Brewster, Wendy R., primary, O'Malley, David M., primary, Partridge, Edward, primary, Boggess, John, primary, Drescher, Charles W., primary, Isaacs, Claudine, primary, Berchuck, Andrew, primary, Domchek, Susan, primary, Davidson, Susan A., primary, Edwards, Robert, primary, Elg, Steven A., primary, Wakeley, Katie, primary, Phillips, Kelly-Anne, primary, Armstrong, Deborah, primary, Horowitz, Ira, primary, Fabian, Carol J., primary, Walker, Joan, primary, Sluss, Patrick M., primary, Welch, William, primary, Minasian, Lori, primary, Horick, Nora K., primary, Kasten, Carol H., primary, Nayfield, Susan, primary, Alberts, David, primary, Finkelstein, Dianne M., primary, and Lu, Karen H., primary

Published
2023
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19. Data from A Randomized Trial to Increase Colonoscopy Screening in Members of High-Risk Families in the Colorectal Cancer Family Registry and Cancer Genetics Network

Author

Lowery, Jan T., primary, Horick, Nora, primary, Kinney, Anita Y., primary, Finkelstein, Dianne M., primary, Garrett, Kathleen, primary, Haile, Robert W., primary, Lindor, Noralane M., primary, Newcomb, Polly A., primary, Sandler, Robert S., primary, Burke, Carol, primary, Hill, Deirdre A., primary, and Ahnen, Dennis J., primary

Published
2023
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21. FHPP Baseline Survey from A Randomized Trial to Increase Colonoscopy Screening in Members of High-Risk Families in the Colorectal Cancer Family Registry and Cancer Genetics Network

Author

Lowery, Jan T., primary, Horick, Nora, primary, Kinney, Anita Y., primary, Finkelstein, Dianne M., primary, Garrett, Kathleen, primary, Haile, Robert W., primary, Lindor, Noralane M., primary, Newcomb, Polly A., primary, Sandler, Robert S., primary, Burke, Carol, primary, Hill, Deirdre A., primary, and Ahnen, Dennis J., primary

Published
2023
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22. Supplementary Data from Bcl2 and Human Papilloma Virus 16 as Predictors of Outcome following Concurrent Chemoradiation for Advanced Oropharyngeal Cancer

Author

Nichols, Anthony C., primary, Finkelstein, Dianne M., primary, Faquin, William C., primary, Westra, William H., primary, Mroz, Edmund A., primary, Kneuertz, Peter, primary, Begum, Shahnaz, primary, Michaud, William A., primary, Busse, Paul M., primary, Clark, John R., primary, and Rocco, James W., primary

Published
2023
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23. Supplementary Figure 4 from Common Familial Colorectal Cancer Linked to Chromosome 7q31: A Genome-Wide Analysis

Author

Neklason, Deborah W., primary, Kerber, Richard A., primary, Nilson, David B., primary, Anton-Culver, Hoda, primary, Schwartz, Ann G., primary, Griffin, Constance A., primary, Lowery, Jan T., primary, Schildkraut, Joellen M., primary, Evans, James P., primary, Tomlinson, Gail E., primary, Strong, Louise C., primary, Miller, Alexander R., primary, Stopfer, Jill E., primary, Finkelstein, Dianne M., primary, Nadkarni, Prakash M., primary, Kasten, Carol H., primary, Mineau, Geraldine P., primary, and Burt, Randall W., primary

Published
2023
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24. Supplementary Figure 1 from Common Familial Colorectal Cancer Linked to Chromosome 7q31: A Genome-Wide Analysis

Author

Neklason, Deborah W., primary, Kerber, Richard A., primary, Nilson, David B., primary, Anton-Culver, Hoda, primary, Schwartz, Ann G., primary, Griffin, Constance A., primary, Lowery, Jan T., primary, Schildkraut, Joellen M., primary, Evans, James P., primary, Tomlinson, Gail E., primary, Strong, Louise C., primary, Miller, Alexander R., primary, Stopfer, Jill E., primary, Finkelstein, Dianne M., primary, Nadkarni, Prakash M., primary, Kasten, Carol H., primary, Mineau, Geraldine P., primary, and Burt, Randall W., primary

Published
2023
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25. Supplementary Figure 2 from Common Familial Colorectal Cancer Linked to Chromosome 7q31: A Genome-Wide Analysis

Author

Neklason, Deborah W., primary, Kerber, Richard A., primary, Nilson, David B., primary, Anton-Culver, Hoda, primary, Schwartz, Ann G., primary, Griffin, Constance A., primary, Lowery, Jan T., primary, Schildkraut, Joellen M., primary, Evans, James P., primary, Tomlinson, Gail E., primary, Strong, Louise C., primary, Miller, Alexander R., primary, Stopfer, Jill E., primary, Finkelstein, Dianne M., primary, Nadkarni, Prakash M., primary, Kasten, Carol H., primary, Mineau, Geraldine P., primary, and Burt, Randall W., primary

Published
2023
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26. Data from Common Familial Colorectal Cancer Linked to Chromosome 7q31: A Genome-Wide Analysis

Author

Neklason, Deborah W., primary, Kerber, Richard A., primary, Nilson, David B., primary, Anton-Culver, Hoda, primary, Schwartz, Ann G., primary, Griffin, Constance A., primary, Lowery, Jan T., primary, Schildkraut, Joellen M., primary, Evans, James P., primary, Tomlinson, Gail E., primary, Strong, Louise C., primary, Miller, Alexander R., primary, Stopfer, Jill E., primary, Finkelstein, Dianne M., primary, Nadkarni, Prakash M., primary, Kasten, Carol H., primary, Mineau, Geraldine P., primary, and Burt, Randall W., primary

Published
2023
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27. Supplementary Figure 3 from Common Familial Colorectal Cancer Linked to Chromosome 7q31: A Genome-Wide Analysis

Author

Neklason, Deborah W., primary, Kerber, Richard A., primary, Nilson, David B., primary, Anton-Culver, Hoda, primary, Schwartz, Ann G., primary, Griffin, Constance A., primary, Lowery, Jan T., primary, Schildkraut, Joellen M., primary, Evans, James P., primary, Tomlinson, Gail E., primary, Strong, Louise C., primary, Miller, Alexander R., primary, Stopfer, Jill E., primary, Finkelstein, Dianne M., primary, Nadkarni, Prakash M., primary, Kasten, Carol H., primary, Mineau, Geraldine P., primary, and Burt, Randall W., primary

Published
2023
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28. Supplementary Figure Legends 1-4 from Common Familial Colorectal Cancer Linked to Chromosome 7q31: A Genome-Wide Analysis

Author

Neklason, Deborah W., primary, Kerber, Richard A., primary, Nilson, David B., primary, Anton-Culver, Hoda, primary, Schwartz, Ann G., primary, Griffin, Constance A., primary, Lowery, Jan T., primary, Schildkraut, Joellen M., primary, Evans, James P., primary, Tomlinson, Gail E., primary, Strong, Louise C., primary, Miller, Alexander R., primary, Stopfer, Jill E., primary, Finkelstein, Dianne M., primary, Nadkarni, Prakash M., primary, Kasten, Carol H., primary, Mineau, Geraldine P., primary, and Burt, Randall W., primary

Published
2023
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33. Breast cancer in China

Author

Fan, Lei, Strasser-Weippl, Kathrin, Li, Jun-Jie, St Louis, Jessica, Finkelstein, Dianne M, Yu, Ke-Da, Chen, Wan-Qing, Shao, Zhi-Ming, and Goss, Paul E

Published
2014
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36. Adjuvant lapatinib for women with early-stage HER2-positive breast cancer: a randomised, controlled, phase 3 trial

Author

Goss, Paul E, Smith, Ian E, O'Shaughnessy, Joyce, Ejlertsen, Bent, Kaufmann, Manfred, Boyle, Frances, Buzdar, Aman U, Fumoleau, Pierre, Gradishar, William, Martin, Miguel, Moy, Beverly, Piccart-Gebhart, Martine, Pritchard, Kathleen I, Lindquist, Deborah, Chavarri-Guerra, Yanin, Aktan, Gursel, Rappold, Erica, Williams, Lisa S, and Finkelstein, Dianne M

Published
2013
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42. Analysis of Co-Aggregation of Cancer Based on Registry Data

Author

Matthews, Abigail G., Betensky, Rebecca A., Anton-Culver, Hoda, Bowen, Deborah, Griffin, Constance, Isaacs, Claudine, Kasten, Carol, Mineau, Geraldine, Nayfield, Susan, Schildkraut, Joellen, Strong, Louise, Weber, Barbara, and Finkelstein, Dianne M.

Published
2006

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