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1. Alternative dosing regimen of exemestane in a randomized presurgical trial: the role of obesity in biomarker modulation.

Author

Johansson, Harriet, Guerrieri-Gonzaga, Aliana, Gandini, Sara, Bertelsen, Bjørn-Erik, Macis, Debora, Serrano, Davide, Mellgren, Gunnar, Lazzeroni, Matteo, Thomas, Parijatham, Crew, Katherine, Kumar, Nagi, Briata, Irene, Galimberti, Viviana, Viale, Giuseppe, Vornik, Lana, Aristarco, Valentina, Buttiron Webber, Tania, Spinaci, Stefano, Brown, Powel, Heckman-Stoddard, Brandy, Szabo, Eva, Bonanni, Bernardo, and DeCensi, Andrea

Abstract

In a 3-arm presurgical trial, four-six weeks exemestane 25 mg three times/week (TIW) was non-inferior to 25 mg/day (QD) in suppressing circulating estradiol in postmenopausal women with ER-positive breast cancer. Since obesity may decrease exemestane efficacy, we analyzed changes in sex steroids, adipokines, Ki-67, and drug levels in relation to obesity. Postmenopausal women with early-stage ER-positive breast cancer were randomized to either exemestane 25 mg QD (n = 57), 25 mg TIW (n = 57), or 25 mg/week (QW, n = 62) for 4-6 weeks before breast surgery. Serum and tissue pre- and post-treatment biomarkers were stratified by body mass index (BMI)< or ≥30 kg/m2. Post-treatment median exemestane and 17-OH exemestane levels were 5-6 times higher in the QD arm compared to the TIW arm. For obese women, TIW maintained comparable reductions to QD in systemic estradiol levels, although the reduction in estrone was less with the TIW regimen. There was less suppression of SHBG with the TIW versus the QD dose schedule in obese women which should result in less systemic bioavailable estrogens. Metabolically, the effect of the TIW regimen was similar to the QD regimen for obese women in terms of leptin suppression and increase in the adiponectin-leptin ratio. Reduction in tissue Ki-67 was less for obese women on the TIW regimen than QD, although changes were similar for non-obese women. Our findings suggest that TIW exemestane should be explored further for primary cancer prevention in both normal weight and obese cohorts.

Published
2024

2. Naproxen chemoprevention induces proliferation of cytotoxic lymphocytes in Lynch Syndrome colorectal mucosa.

Author

Bowen, Charles M, Deng, Nan, Reyes-Uribe, Laura, Parra, Edwin Roger, Rocha, Pedro, Solis, Luisa M, Wistuba, Ignacio I, Sepeda, Valerie O, Vornik, Lana, Perloff, Marjorie, Szabo, Eva, Umar, Asad, Sinha, Krishna M, Brown, Powel H, and Vilar, Eduardo

Subjects
Intestinal Mucosa, Lymphocytes, Humans, Colorectal Neoplasms, Hereditary Nonpolyposis, Naproxen, Antineoplastic Agents, Cancer Vaccines, Immunotherapy, Chemoprevention, Lynch Syndrome, bioinformactics, cancer prevention, image mass cytometry, immunoprevention, Clinical Research, Cancer, Digestive Diseases, Colo-Rectal Cancer, Inflammatory and immune system, Immunology, Medical Microbiology
Abstract

BackgroundRecent clinical trial data from Lynch Syndrome (LS) carriers demonstrated that naproxen administered for 6-months is a safe primary chemoprevention that promotes activation of different resident immune cell types without increasing lymphoid cellularity. While intriguing, the precise immune cell types enriched by naproxen remained unanswered. Here, we have utilized cutting-edge technology to elucidate the immune cell types activated by naproxen in mucosal tissue of LS patients.MethodsNormal colorectal mucosa samples (pre- and post-treatment) from a subset of patients enrolled in the randomized and placebo-controlled 'Naproxen Study' were obtained and subjected to a tissue microarray for image mass cytometry (IMC) analysis. IMC data was processed using tissue segmentation and functional markers to ascertain cell type abundance. Computational outputs were then used to quantitatively compare immune cell abundance in pre- and post-naproxen specimens.ResultsUsing data-driven exploration, unsupervised clustering identified four populations of immune cell types with statistically significant changes between treatment and control groups. These four populations collectively describe a unique cell population of proliferating lymphocytes within mucosal samples from LS patients exposed to naproxen.ConclusionsOur findings show that daily exposure of naproxen promotes T-cell proliferation in the colonic mucosa, which paves way for developing combination of immunoprevention strategies including naproxen for LS patients.

Published
2023

7. Inhibition of mTOR signaling and clinical activity of metformin in oral premalignant lesions.

Author

Gutkind, J Silvio, Molinolo, Alfredo A, Wu, Xingyu, Wang, Zhiyong, Nachmanson, Daniela, Harismendy, Olivier, Alexandrov, Ludmil B, Wuertz, Beverly R, Ondrey, Frank G, Laronde, Denise, Rock, Leigha D, Rosin, Miriam, Coffey, Charles, Butler, Valerie D, Bengtson, Lisa, Hsu, Chiu-Hsieh, Bauman, Julie E, Hewitt, Stephen M, Cohen, Ezra Ew, Chow, H-H Sherry, Lippman, Scott M, and Szabo, Eva

Subjects
Clinical Trials, Head and neck cancer, Signal transduction, Clinical Research, Cancer, Prevention, Dental/Oral and Craniofacial Disease, 6.1 Pharmaceuticals
Abstract

BACKGROUNDThe aberrant activation of the PI3K/mTOR signaling circuitry is one of the most frequently dysregulated signaling events in head and neck squamous cell carcinoma (HNSCC). Here, we conducted a single-arm, open-label phase IIa clinical trial in individuals with oral premalignant lesions (OPLs) to explore the potential of metformin to target PI3K/mTOR signaling for HNSCC prevention.METHODSIndividuals with OPLs, but who were otherwise healthy and without diabetes, underwent pretreatment and posttreatment clinical exam and biopsy. Participants received metformin for 12 weeks (week 1, 500 mg; week 2, 1000 mg; weeks 3-12, 2000 mg daily). Pretreatment and posttreatment biopsies, saliva, and blood were obtained for biomarker analysis, including IHC assessment of mTOR signaling and exome sequencing.RESULTSTwenty-three participants were evaluable for response. The clinical response rate (defined as a ≥50% reduction in lesion size) was 17%. Although lower than the proposed threshold for favorable clinical response, the histological response rate (improvement in histological grade) was 60%, including 17% complete responses and 43% partial responses. Logistic regression analysis revealed that when compared with never smokers, current and former smokers had statistically significantly increased histological responses (P = 0.016). Remarkably, a significant correlation existed between decreased mTOR activity (pS6 IHC staining) in the basal epithelial layers of OPLs and the histological (P = 0.04) and clinical (P = 0.01) responses.CONCLUSIONTo our knowledge this is the first phase II trial of metformin in individuals with OPLs, providing evidence that metformin administration results in encouraging histological responses and mTOR pathway modulation, thus supporting its further investigation as a chemopreventive agent.TRIAL REGISTRATIONNCT02581137FUNDINGNIH contract HHSN261201200031I, grants R01DE026644 and R01DE026870.

Published
2021

10. Alternative dosing of exemestane in postmenopausal women with ER-positive breast cancer. Design and methods of a randomized presurgical trial

Author

Guerrieri-Gonzaga, Aliana, Serrano, Davide, Thomas, Parjhitham, Crew, Katherine D, Kumar, Nagi B, Gandini, Sara, Vornik, Lana A, Lee, Jack, Cagnacci, Sara, Vicini, Elisa, Accornero, Chiara A, D'Amico, Mauro, Guasone, Flavio, Spinaci, Stefano, Webber, Tania B, Brown, Powel H, Szabo, Eva, Heckman-Stoddard, Brandy, and Bonanni, Bernardo

Subjects
Health Services and Systems, Biomedical and Clinical Sciences, Health Sciences, Oncology and Carcinogenesis, Clinical Trials and Supportive Activities, Estrogen, Prevention, Patient Safety, Clinical Research, Cancer, Aging, Breast Cancer, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Androstadienes, Aromatase Inhibitors, Breast Neoplasms, Female, Humans, Postmenopause, Breast cancer, Drug schedule and alternative dose, Exemestane, Phase II study, Preventive medicine, Medical and Health Sciences, General Clinical Medicine, Public Health, Biomedical and clinical sciences, Health sciences
Abstract

IntroductionAromatase inhibitors are effective in lowering breast cancer incidence among postmenopausal women, but adverse events represent a barrier to their acceptability and adherence as a preventive treatment. This study aims to assess whether lowering exemestane schedule may retain biological activity while improving tolerability in breast cancer patients.Methods/designWe are conducting a, pre-surgical, non-inferiority phase IIb study in postmenopausal women with newly diagnosed estrogen receptor-positive breast cancer. Participants are randomized to receive either exemestane 25 mg/day or 25 mg/three times-week or once a week for 4 to 6 weeks prior to surgery. The primary endpoint is the percentage change of serum estradiol concentration between baseline and surgery comparing the three arms. Sample size of 180 women was calculated assuming a 6% non-inferiority of the percent change of estradiol in the lower dose arms compared with the 80% decrease predicted in the full dose arm, with 80% power and using a one-sided 5% significance level and a two-sample t-test. Main secondary outcomes are: safety; change in Ki-67 in cancer and adjacent pre-cancer tissue, circulating sex hormones, adipokines, lipid profile, insulin and glucose changes, in correlation with drug and metabolites concentrations.Results and discussionThe present paper is focused on methodology and operational aspects of the study. A total of 180 participants have ben enrolled. The trial is still blinded, and the analyses are ongoing. Despite the short term duration, results may have relevant implications for clinical management of women at increased risk of developing a ER positive breast cancer.

Published
2021

12. Naproxen chemoprevention promotes immune activation in Lynch syndrome colorectal mucosa

Author

Reyes-Uribe, Laura, Wu, Wenhui, Gelincik, Ozkan, Bommi, Prashant V, Francisco-Cruz, Alejandro, Solis, Luisa M, Lynch, Patrick M, Lim, Ramona, Stoffel, Elena M, Kanth, Priyanka, Samadder, N Jewel, Mork, Maureen E, Taggart, Melissa W, Milne, Ginger L, Marnett, Lawrence J, Vornik, Lana, Liu, Diane D, Revuelta, Maria, Chang, Kyle, You, Y Nancy, Kopelovich, Levy, Wistuba, Ignacio I, Lee, J Jack, Sei, Shizuko, Shoemaker, Robert H, Szabo, Eva, Richmond, Ellen, Umar, Asad, Perloff, Marjorie, Brown, Powel H, Lipkin, Steven M, and Vilar, Eduardo

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Biotechnology, Digestive Diseases, Colo-Rectal Cancer, Cancer, Prevention, Clinical Trials and Supportive Activities, Clinical Research, Genetics, Adult, Aged, Animals, Anti-Inflammatory Agents, Non-Steroidal, Chemoprevention, Colorectal Neoplasms, Hereditary Nonpolyposis, Dinoprostone, Disease Models, Animal, Female, Humans, Intestinal Mucosa, Male, Mice, Middle Aged, Naproxen, HNPCC syndrome, cancer syndromes, chemoprevention, gene expression, non-steroidal anti-inflammatory drugs, Clinical Sciences, Paediatrics and Reproductive Medicine, Gastroenterology & Hepatology, Clinical sciences, Nutrition and dietetics
Abstract

ObjectivePatients with Lynch syndrome (LS) are at markedly increased risk for colorectal cancer. It is being increasingly recognised that the immune system plays an essential role in LS tumour development, thus making an ideal target for cancer prevention. Our objective was to evaluate the safety, assess the activity and discover novel molecular pathways involved in the activity of naproxen as primary and secondary chemoprevention in patients with LS.DesignWe conducted a Phase Ib, placebo-controlled, randomised clinical trial of two dose levels of naproxen sodium (440 and 220 mg) administered daily for 6 months to 80 participants with LS, and a co-clinical trial using a genetically engineered mouse model of LS and patient-derived organoids (PDOs).ResultsOverall, the total number of adverse events was not different across treatment arms with excellent tolerance of the intervention. The level of prostaglandin E2 in the colorectal mucosa was significantly decreased after treatment with naproxen when compared with placebo. Naproxen activated different resident immune cell types without any increase in lymphoid cellularity, and changed the expression patterns of the intestinal crypt towards epithelial differentiation and stem cell regulation. Naproxen demonstrated robust chemopreventive activity in a mouse co-clinical trial and gene expression profiles induced by naproxen in humans showed perfect discrimination of mice specimens with LS and PDOs treated with naproxen and control.ConclusionsNaproxen is a promising strategy for immune interception in LS. We have discovered naproxen-induced gene expression profiles for their potential use as predictive biomarkers of drug activity.Trial registration numbergov Identifier: NCT02052908.

Published
2021

13. Low-Dose Aspirin in High-Risk Individuals With Screen-Detected Subsolid Lung Nodules: A Randomized Phase II Trial.

Author

Bonanni, Bernardo, Serrano, Davide, Maisonneuve, Patrick, Veronesi, Giulia, Johansson, Harriet, Aristarco, Valentina, Varricchio, Clara, Cazzaniga, Massimiliano, Lazzeroni, Matteo, Rampinelli, Cristiano, Bellomi, Massimo, Vecchi, Manuela, Spaggiari, Lorenzo, Vornik, Lana, Brown, Powel H, Beavers, Therese, Guerrieri-Gonzaga, Aliana, and Szabo, Eva

Abstract

Lung cancer screening by helical low-dose computed tomography detects nonsolid nodules that may be lung adenocarcinoma precursors. Aspirin's anti-inflammatory properties make it an attractive target for prevention of multiple cancers, including lung cancer. Therefore, we conducted a phase IIb trial (NCT02169271) to study the efficacy of low-dose aspirin to reduce the size of subsolid lung nodules (SSNs). A total of 98 current or former smokers (67.3% current) undergoing annual low-dose computed tomography screening with persistent SSNs were randomly assigned to receive aspirin 100 mg/day or placebo for 1 year. There was no difference in change in the sum of the longest diameters of target nodules in the placebo and aspirin arm after 12 months of treatment (-0.12 mm [SD = 1.55 mm] and +0.30 mm [SD= 2.54 mm], respectively; 2-sided P = .33 primary endpoint). There were no changes observed in subgroup analyses by individual characteristics or nodule type. One year of low-dose aspirin did not show any effect on lung SSNs. SSNs regression may not be the proper target for aspirin, and/or longer duration may be needed to see SSNs modifications.

Published
2020

16. A Phase IIa Trial of Metformin for Colorectal Cancer Risk Reduction among Individuals with History of Colorectal Adenomas and Elevated Body Mass Index

Author

Zell, Jason A, McLaren, Christine E, Morgan, Timothy R, Lawson, Michael J, Rezk, Sherif, Albers, C Gregory, Chen, Wen-Pin, Carmichael, Joseph C, Chung, Jinah, Richmond, Ellen, Rodriguez, LM, Szabo, Eva, Ford, Leslie G, Pollak, Michael N, and Meyskens, Frank L

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Nutrition, Colo-Rectal Cancer, Clinical Research, Cancer, Prevention, Digestive Diseases, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Adenoma, Administration, Oral, Aged, Biomarkers, Tumor, Biopsy, Body Mass Index, Colonic Polyps, Colonoscopy, Colorectal Neoplasms, Female, Humans, Intestinal Mucosa, Intestine, Large, Male, Metformin, Middle Aged, Obesity, Proctoscopy, Rectum, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis
Abstract

Obesity is associated with risk of colorectal adenoma (CRA) and colorectal cancer. The signaling pathway activated by metformin (LKB1/AMPK/mTOR) is implicated in tumor suppression in ApcMin/+ mice via metformin-induced reduction in polyp burden, increased ratio of pAMPK/AMPK, decreased pmTOR/mTOR ratio, and decreased pS6Ser235/S6Ser235 ratio in polyps. We hypothesized that metformin would affect colorectal tissue S6Ser235 among obese patients with recent history of CRA. A phase IIa clinical biomarker trial was conducted via the U.S. National Cancer Institute-Chemoprevention Consortium. Nondiabetic, obese subjects (BMI ≥30) ages 35 to 80 with recent history of CRA were included. Subjects received 12 weeks of oral metformin 1,000 mg twice every day. Rectal mucosa biopsies were obtained at baseline and end-of-treatment (EOT) endoscopy. Tissue S6Ser235 and Ki-67 immunostaining were analyzed in a blinded fashion using Histo score (Hscore) analysis. Among 32 eligible subjects, the mean baseline BMI was 34.9. Comparing EOT to baseline tissue S6Ser235 by IHC, no significant differences were observed. Mean (SD) Hscore at baseline was 1.1 (0.57) and 1.1 (0.51) at EOT; median Hscore change was 0.034 (P = 0.77). Similarly, Ki-67 levels were unaffected by the intervention. The adverse events were consistent with metformin's known side-effect profile. Among obese patients with CRA, 12 weeks of oral metformin does not reduce rectal mucosa pS6 or Ki-67 levels. Further research is needed to determine what effects metformin has on the target tissue of origin as metformin continues to be pursued as a colorectal cancer chemopreventive agent.

Published
2020

18. A prospective, single-arm, open-label, non-randomized, phase IIa trial of a nonavalent prophylactic HPV vaccine to assess immunogenicity of a prime and deferred-booster dosing schedule among 9-11 year-old girls and boys - clinical protocol.

Author

Zeng, Yi, Moscicki, Anna-Barbara, Sahasrabuddhe, Vikrant, Garcia, Francisco, Woo, Heide, Hsu, Chiu-Hsieh, Szabo, Eva, Dimond, Eileen, Vanzzini, Susan, Mondragon, Angelica, Butler, Valerie, DeRose, Hillary, and Chow, H-H

Subjects
Cervical cancer, Gardasil 9, HPV vaccine, Human papillomavirus, Nonavalent HPV vaccine, Serologic geometric mean titer, Antibodies, Viral, Child, Female, Humans, Immunization Schedule, Immunogenicity, Vaccine, Male, Papillomavirus Infections, Papillomavirus Vaccines, Prospective Studies, Treatment Outcome
Abstract

BACKGROUND: Human papillomavirus (HPV) vaccines are indicated for the prevention of cancers and genital warts caused by vaccine-covered HPV types. Although the standard regimen requires a two or three-dose vaccine series, there is emerging data suggesting that a single dose of the bivalent or quadrivalent HPV vaccine generates persistently positive antibody titers. No similar data is yet available for the nonavalent HPV vaccine, currently the only HPV vaccine available in the United States. The overall objective of our study is to assess the stability and kinetics of antibody titers for 24 months following a single dose of the nonavalent HPV vaccine among preteen girls and boys. METHODS: This is a prospective, single-arm, open-label, non-randomized, Phase IIa trial among 9-11 year-old girls and boys to determine the immunogenicity after a single dose of the nonavalent HPV vaccine (GARDASIL® 9) over 24 months, with a deferred booster dose at 24 months and an optional booster at 30 months after the first dose. Participants provide blood specimens at 6, 12, 18, 24, and 30 months after the first dose. Serologic geometric mean titers (GMT) of the nine vaccine types (HPV 16/18/ 6/11/31/33/45/52/58) will be measured at each time point. The primary objective is to determine the stability of type-specific serologic GMT of HPV16 and HPV18 between the 6- vs. 12-month, 12- vs. 18-month, and 18- vs. 24-month visits. Secondary objectives are to determine the stability of type-specific serologic GMT of the other HPV types (HPV 6/11/31/33/45/52/58) between the visits and to assess safety and reactogenicity after each vaccine dose. DISCUSSION: Single dose HPV vaccination could simplify the logistics and reduce costs of HPV vaccination in the US and across the world. This study will contribute important immunogenicity data on the stability and kinetics of type-specific antibody titers and inform feasibility of the single dose HPV vaccination paradigm. TRIAL REGISTRATION: ClinicalTrials.gov Identifier: NCT02568566 . Registered on October 6, 2015.

Published
2019

19. Inhibition of mTOR Signaling and Clinical Activity of Rapamycin in Head and Neck Cancer in a Window of Opportunity Trial

Author

Day, Terry A, Shirai, Keisuke, O'Brien, Paul E, Matheus, Maria Gisele, Godwin, Kristina, Sood, Amit J, Kompelli, Anvesh, Vick, Julie A, Martin, Daniel, Vitale-Cross, Lynn, Callejas-Varela, Juan Luis, Wang, Zhiyong, Wu, Xingyu, Harismendy, Olivier, Molinolo, Alfredo A, Lippman, Scott M, Van Waes, Carter, Szabo, Eva, and Gutkind, J Silvio

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Dental/Oral and Craniofacial Disease, Rare Diseases, Clinical Trials and Supportive Activities, Cancer, Orphan Drug, Digestive Diseases, Clinical Research, Health Disparities, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Animals, Apoptosis, Cell Line, Tumor, Class I Phosphatidylinositol 3-Kinases, Female, Gene Expression Regulation, Neoplastic, Head and Neck Neoplasms, Humans, Male, Mice, Middle Aged, Neoadjuvant Therapy, Neoplasm Staging, Phosphorylation, Positron Emission Tomography Computed Tomography, Proto-Oncogene Proteins c-akt, Signal Transduction, Sirolimus, Squamous Cell Carcinoma of Head and Neck, TOR Serine-Threonine Kinases, Exome Sequencing, Xenograft Model Antitumor Assays, Whole Exome Sequencing, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis
Abstract

PurposeWe studied the impact of mTOR signaling inhibition with rapamycin in head and neck squamous cell carcinoma (HNSCC) in the neoadjuvant setting. The goals were to evaluate the mTOR pathway as a therapeutic target for patients with advanced HNSCC, and the clinical safety, antitumor, and molecular activity of rapamycin administration on HNSCC.Patients and methodsPatients with untreated stage II-IVA HNSCC received rapamycin for 21 days (day 1, 15 mg; days 2-12, 5 mg) prior to definitive treatment with surgery or chemoradiation. Treatment responses were assessed clinically and radiographically with CT and FDG-PET. Pre- and posttreatment biopsies and blood were obtained for toxicity, immune monitoring, and IHC assessment of mTOR signaling, as well as exome sequencing.ResultsSixteen patients (eight oral cavity, eight oropharyngeal) completed rapamycin and definitive treatment. Half of patients were p16 positive. One patient had a pathologic complete response and four (25%) patients met RECIST criteria for response (1 CR, 3 PR, 12 SD). Treatment was well tolerated with no grade 4 or unexpected toxicities. No significant immune suppression was observed. Downstream mTOR signaling was downregulated in tumor tissues as measured by phosphorylation of S6 (P < 0.0001), AKT (P < 0.0001), and 4EBP (P = 0.0361), with a significant compensatory increase in phosphorylated ERK in most patients (P < 0.001). Ki67 was reduced in tumor biopsies in all patients (P = 0.013).ConclusionsRapamycin treatment was well tolerated, reduced mTOR signaling and tumor growth, and resulted in significant clinical responses despite the brief treatment duration, thus supporting the potential role of mTOR inhibitors in treatment regimens for HNSCC.

Published
2019

20. AACR White Paper: Shaping the Future of Cancer Prevention – A Roadmap for Advancing Science and Public Health

Author

Lippman, Scott M, Abate-Shen, Cory, Colbert Maresso, Karen L, Colditz, Graham A, Dannenberg, Andrew J, Davidson, Nancy E, Disis, Mary L, DuBois, Raymond N, Szabo, Eva, Giuliano, Anna R, Hait, William N, Lee, J Jack, Kensler, Thomas W, Kramer, Barnett S, Limburg, Paul, Maitra, Anirban, Martinez, Maria Elena, Rebbeck, Timothy R, Schmitz, Kathryn H, Vilar, Eduardo, and Hawk, Ernest T

Subjects
Genetics, Prevention, Cancer, Digestive Diseases, Human Genome, Good Health and Well Being, Biomedical Research, Congresses as Topic, Health Plan Implementation, Health Status Disparities, Humans, Neoplasms, Obesity, Primary Prevention, Public Health, Societies, Medical, Societies, Scientific, United States, Clinical Sciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

The recent pace, extent, and impact of paradigm-changing cancer prevention science has been remarkable. The American Association for Cancer Research (AACR) convened a 3-day summit, aligned with five research priorities: (i) Precancer Atlas (PCA). (ii) Cancer interception. (iii) Obesity-cancer linkage, a global epidemic of chronic low-grade inflammation. (iv) Implementation science. (v) Cancer disparities. Aligned with these priorities, AACR co-led the Lancet Commission to formally endorse and accelerate the NCI Cancer Moonshot program, facilitating new global collaborative efforts in cancer control. The expanding scope of creative impact is perhaps most startling-from NCI-funded built environments to AACR Team Science Awarded studies of Asian cancer genomes informing global primary prevention policies; cell-free epigenetic marks identifying incipient neoplastic site; practice-changing genomic subclasses in myeloproliferative neoplasia (including germline variant tightly linked to JAK2 V617F haplotype); universal germline genetic testing for pancreatic cancer; and repurposing drugs targeting immune- and stem-cell signals (e.g., IL-1β, PD-1, RANK-L) to cancer interception. Microbiota-driven IL-17 can induce stemness and transformation in pancreatic precursors (identifying another repurposing opportunity). Notable progress also includes hosting an obesity special conference (connecting epidemiologic and molecular perspectives to inform cancer research and prevention strategies), co-leading concerted national implementation efforts in HPV vaccination, and charting the future elimination of cancer disparities by integrating new science tools, discoveries and perspectives into community-engaged research, including targeted counter attacks on e-cigarette ad exploitation of children, Hispanics and Blacks. Following this summit, two unprecedented funding initiatives were catalyzed to drive cancer prevention research: the NCI Cancer Moonshot (e.g., PCA and disparities); and the AACR-Stand Up To Cancer bold "Cancer Interception" initiative.

Published
2018

23. Premalignant Progression in the Lung: Knowledge Gaps and Novel Opportunities for Interception of Non–Small Cell Lung Cancer. An Official American Thoracic Society Research Statement.

Author

Moghaddam, Seyed Javad, Savai, Rajkumar, Salehi-Rad, Ramin, Sengupta, Shreoshi, Kammer, Michael N., Massion, Pierre, Beane, Jennifer E., Ostrin, Edwin J., Priolo, Carmen, Tennis, Meredith A., Stabile, Laura P., Bauer, Alison K., Sears, Catherine R., Szabo, Eva, Rivera, M. Patricia, Powell, Charles A., Kadara, Humam, Jenkins, Brendan J., Dubinett, Steven M., and Houghton, A. McGarry

Subjects
NON-small-cell lung carcinoma, LUNGS, LUNG diseases, PRECANCEROUS conditions, LUNG cancer
Abstract

Rationale: Despite significant advances in precision treatments and immunotherapy, lung cancer is the most common cause of cancer death worldwide. To reduce incidence and improve survival rates, a deeper understanding of lung premalignancy and the multistep process of tumorigenesis is essential, allowing timely and effective intervention before cancer development. Objectives: To summarize existing information, identify knowledge gaps, formulate research questions, prioritize potential research topics, and propose strategies for future investigations into the premalignant progression in the lung. Methods: An international multidisciplinary team of basic, translational, and clinical scientists reviewed available data to develop and refine research questions pertaining to the transformation of premalignant lung lesions to advanced lung cancer. Results: This research statement identifies significant gaps in knowledge and proposes potential research questions aimed at expanding our understanding of the mechanisms underlying the progression of premalignant lung lesions to lung cancer in an effort to explore potential innovative modalities to intercept lung cancer at its nascent stages. Conclusions: The identified gaps in knowledge about the biological mechanisms of premalignant progression in the lung, together with ongoing challenges in screening, detection, and early intervention, highlight the critical need to prioritize research in this domain. Such focused investigations are essential to devise effective preventive strategies that may ultimately decrease lung cancer incidence and improve patient outcomes. [ABSTRACT FROM AUTHOR]

Published
2024
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25. Supplementary Figure S2 from Randomized, Double-Blind, Placebo-Controlled Trial of MUC1 Peptide Vaccine for Prevention of Recurrent Colorectal Adenoma

Author

Schoen, Robert E., primary, Boardman, Lisa A., primary, Cruz-Correa, Marcia, primary, Bansal, Ajay, primary, Kastenberg, David, primary, Hur, Chin, primary, Dzubinski, Lynda, primary, Kaufman, Sharon F., primary, Rodriguez, Luz M., primary, Richmond, Ellen, primary, Umar, Asad, primary, Szabo, Eva, primary, Salazar, Andres, primary, McKolanis, John, primary, Beatty, Pamela, primary, Pai, Reetesh K., primary, Singhi, Aatur D., primary, Jacqueline, Camille M., primary, Bao, Riyue, primary, Diergaarde, Brenda, primary, McMurray, Ryan P., primary, Strand, Carrie, primary, Foster, Nathan R., primary, Zahrieh, David M., primary, Limburg, Paul J., primary, and Finn, Olivera J., primary

Published
2024
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26. Supplementary Table S2 from Randomized, Double-Blind, Placebo-Controlled Trial of MUC1 Peptide Vaccine for Prevention of Recurrent Colorectal Adenoma

Author

Schoen, Robert E., primary, Boardman, Lisa A., primary, Cruz-Correa, Marcia, primary, Bansal, Ajay, primary, Kastenberg, David, primary, Hur, Chin, primary, Dzubinski, Lynda, primary, Kaufman, Sharon F., primary, Rodriguez, Luz M., primary, Richmond, Ellen, primary, Umar, Asad, primary, Szabo, Eva, primary, Salazar, Andres, primary, McKolanis, John, primary, Beatty, Pamela, primary, Pai, Reetesh K., primary, Singhi, Aatur D., primary, Jacqueline, Camille M., primary, Bao, Riyue, primary, Diergaarde, Brenda, primary, McMurray, Ryan P., primary, Strand, Carrie, primary, Foster, Nathan R., primary, Zahrieh, David M., primary, Limburg, Paul J., primary, and Finn, Olivera J., primary

Published
2024
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27. Supplementary Methods S2 from Randomized, Double-Blind, Placebo-Controlled Trial of MUC1 Peptide Vaccine for Prevention of Recurrent Colorectal Adenoma

Author

Schoen, Robert E., primary, Boardman, Lisa A., primary, Cruz-Correa, Marcia, primary, Bansal, Ajay, primary, Kastenberg, David, primary, Hur, Chin, primary, Dzubinski, Lynda, primary, Kaufman, Sharon F., primary, Rodriguez, Luz M., primary, Richmond, Ellen, primary, Umar, Asad, primary, Szabo, Eva, primary, Salazar, Andres, primary, McKolanis, John, primary, Beatty, Pamela, primary, Pai, Reetesh K., primary, Singhi, Aatur D., primary, Jacqueline, Camille M., primary, Bao, Riyue, primary, Diergaarde, Brenda, primary, McMurray, Ryan P., primary, Strand, Carrie, primary, Foster, Nathan R., primary, Zahrieh, David M., primary, Limburg, Paul J., primary, and Finn, Olivera J., primary

Published
2024
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30. Abstract A021: Pilot study of daily exemestane in patients with Endometrial Intraepithelial Neoplasia (EIN) or grade 1 endometrial cancer

Author

Erickson, Britt K., primary, Barrioullet, Lisa, additional, Arend, Rebecca C., additional, El-Rayes, Dina, additional, Khalifa, Mahmoud, additional, Skubitz, Amy, additional, Boylan, Kristin, additional, Nelson, Andrew, additional, Thyagarajan, Bharat, additional, Havighurst, Thomas, additional, Chappell, Richard, additional, Dimond, Eileen, additional, Deshong, Katina, additional, Samimi, Goli, additional, Szabo, Eva, additional, and Bailey, Howard, additional

Published
2024
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35. Randomized controlled trial of nasogastric tube use after esophagectomy : study protocol for the kinetic trial

Author

Hedberg, Jakob, Sundbom, Magnus, Edholm, David, Aahlin, Eirik Kjus, Szabo, Eva, Lindberg, Fredrik, Johnsen, Gjermund, Tidemann Førland, Dag, Johansson, Jan, Kauppila, Joonas H, Svendsen, Lars Bo, Nilsson, Magnus, Lindblad, Mats, Lagergren, Pernilla, Larsen, Michael Hareskov, Åkesson, Oscar, Löfdahl, Per, Mala, Tom, Achiam, Michael Patrick, Hedberg, Jakob, Sundbom, Magnus, Edholm, David, Aahlin, Eirik Kjus, Szabo, Eva, Lindberg, Fredrik, Johnsen, Gjermund, Tidemann Førland, Dag, Johansson, Jan, Kauppila, Joonas H, Svendsen, Lars Bo, Nilsson, Magnus, Lindblad, Mats, Lagergren, Pernilla, Larsen, Michael Hareskov, Åkesson, Oscar, Löfdahl, Per, Mala, Tom, and Achiam, Michael Patrick

Abstract

Esophagectomy is a complex and complication laden procedure. Despite centralization, variations in perioparative strategies reflect a paucity of evidence regarding optimal routines. The use of nasogastric (NG) tubes post esophagectomy is typically associated with significant discomfort for the patients. We hypothesize that immediate postoperative removal of the NG tube is non-inferior to current routines. All Nordic Upper Gastrointestinal Cancer centers were invited to participate in this open-label pragmatic randomized controlled trial (RCT). Inclusion criteria include resection for locally advanced esophageal cancer with gastric tube reconstruction. A pretrial survey was undertaken and was the foundation for a consensus process resulting in the Kinetic trial, an RCT allocating patients to either no use of a NG tube (intervention) or 5 days of postoperative NG tube use (control) with anastomotic leakage as primary endpoint. Secondary endpoints include pulmonary complications, overall complications, length of stay, health related quality of life. A sample size of 450 patients is planned (Kinetic trial: https://www.isrctn.com/ISRCTN39935085). Thirteen Nordic centers with a combined catchment area of 17 million inhabitants have entered the trial and ethical approval was granted in Sweden, Norway, Finland, and Denmark. All centers routinely use NG tube and all but one center use total or hybrid minimally invasive-surgical approach. Inclusion began in January 2022 and the first annual safety board assessment has deemed the trial safe and recommended continuation. We have launched the first adequately powered multi-center pragmatic controlled randomized clinical trial regarding NG tube use after esophagectomy with gastric conduit reconstruction.

Published
2024
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36. Randomized controlled trial of nasogastric tube use after esophagectomy:study protocol for the kinetic trial

Author

Hedberg, Jakob, Sundbom, Magnus, Edholm, David, Aahlin, Eirik Kjus, Szabo, Eva, Lindberg, Fredrik, Johnsen, Gjermund, Førland, Dag Tidemann, Johansson, Jan, Kauppila, Joonas H., Svendsen, Lars Bo, Nilsson, Magnus, Lindblad, Mats, Lagergren, Pernilla, Larsen, Michael Hareskov, Åkesson, Oscar, Löfdahl, Per, Mala, Tom, Achiam, Michael Patrick, Hedberg, Jakob, Sundbom, Magnus, Edholm, David, Aahlin, Eirik Kjus, Szabo, Eva, Lindberg, Fredrik, Johnsen, Gjermund, Førland, Dag Tidemann, Johansson, Jan, Kauppila, Joonas H., Svendsen, Lars Bo, Nilsson, Magnus, Lindblad, Mats, Lagergren, Pernilla, Larsen, Michael Hareskov, Åkesson, Oscar, Löfdahl, Per, Mala, Tom, and Achiam, Michael Patrick

Abstract

Esophagectomy is a complex and complication laden procedure. Despite centralization, variations in perioparative strategies reflect a paucity of evidence regarding optimal routines. The use of nasogastric (NG) tubes post esophagectomy is typically associated with significant discomfort for the patients. We hypothesize that immediate postoperative removal of the NG tube is non-inferior to current routines. All Nordic Upper Gastrointestinal Cancer centers were invited to participate in this open-label pragmatic randomized controlled trial (RCT). Inclusion criteria include resection for locally advanced esophageal cancer with gastric tube reconstruction. A pretrial survey was undertaken and was the foundation for a consensus process resulting in the Kinetic trial, an RCT allocating patients to either no use of a NG tube (intervention) or 5 days of postoperative NG tube use (control) with anastomotic leakage as primary endpoint. Secondary endpoints include pulmonary complications, overall complications, length of stay, health related quality of life. A sample size of 450 patients is planned (Kinetic trial: https://www.isrctn.com/ISRCTN39935085). Thirteen Nordic centers with a combined catchment area of 17 million inhabitants have entered the trial and ethical approval was granted in Sweden, Norway, Finland, and Denmark. All centers routinely use NG tube and all but one center use total or hybrid minimally invasive-surgical approach. Inclusion began in January 2022 and the first annual safety board assessment has deemed the trial safe and recommended continuation. We have launched the first adequately powered multi-center pragmatic controlled randomized clinical trial regarding NG tube use after esophagectomy with gastric conduit reconstruction.

Published
2024

39. Clinical and Genomic Characteristics of Small Cell Lung Cancer in Never Smokers: Results From a Retrospective Multicenter Cohort Study

Author

Thomas, Anish, Mian, Idrees, Tlemsani, Camille, Pongor, Lorinc, Takahashi, Nobuyuki, Maignan, Kathleen, Snider, Jeremy, Li, Gerald, Frampton, Garrett, Ali, Siraj, Kim, Sehyun, Nichols, Samantha, Rajapakse, Vinodh, Guha, Udayan, Sharon, Elad, Fujimoto, Junya, Moran, Cesar A., Wistuba, Ignacio I., Wei, Jun S., Khan, Javed, Szabo, Eva, Torres, Aracelis Z., and Carson, Kenneth R.

Published
2020
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43. NCI Resources for Cancer Immunoprevention Research

Author

Sei, Shizuko, primary, Srivastava, Sudhir, additional, Kelly, Halonna R., additional, Miller, Mark Steven., additional, Leitner, Wolfgang W., additional, Shoemaker, Robert H., additional, Szabo, Eva, additional, and Castle, Philip E., additional

Published
2024
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44. Transforming Cancer Prevention through Precision Medicine and Immune-oncology

Author

Kensler, Thomas W, Spira, Avrum, Garber, Judy E, Szabo, Eva, Lee, J Jack, Dong, Zigang, Dannenberg, Andrew J, Hait, William N, Blackburn, Elizabeth, Davidson, Nancy E, Foti, Margaret, and Lippman, Scott M

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Lung Cancer, Digestive Diseases, Clinical Research, Clinical Trials and Supportive Activities, Pancreatic Cancer, Prevention, Rare Diseases, Human Genome, Immunization, Cancer, Lung, Genetics, Good Health and Well Being, Animals, Biomarkers, Tumor, Biopsy, Cancer Vaccines, Disease Progression, Female, Genetic Predisposition to Disease, Germ-Line Mutation, Humans, Immune System, Immunosuppressive Agents, Male, Mice, Neoplasms, Precancerous Conditions, Precision Medicine, Randomized Controlled Trials as Topic, Sequence Analysis, DNA, Tumor Microenvironment, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis
Abstract

We have entered a transformative period in cancer prevention (including early detection). Remarkable progress in precision medicine and immune-oncology, driven by extraordinary recent advances in genome-wide sequencing, big-data analytics, blood-based technologies, and deep understanding of the tumor immune microenvironment (TME), has provided unprecedented possibilities to study the biology of premalignancy. The pace of research and discovery in precision medicine and immunoprevention has been astonishing and includes the following clinical firsts reported in 2015: driver mutations detected in circulating cell-free DNA in patients with premalignant lesions (lung); clonal hematopoiesis shown to be a premalignant state; molecular selection in chemoprevention randomized controlled trial (RCT; oral); striking efficacy in RCT of combination chemoprevention targeting signaling pathway alterations mechanistically linked to germline mutation (duodenum); molecular markers for early detection validated for lung cancer and showing promise for pancreatic, liver, and ovarian cancer. Identification of HPV as the essential cause of a major global cancer burden, including HPV16 as the single driver of an epidemic of oropharyngeal cancer in men, provides unique opportunities for the dissemination and implementation of public health interventions. Important to immunoprevention beyond viral vaccines, genetic drivers of premalignant progression were associated with increasing immunosuppressive TME; and Kras vaccine efficacy in pancreas genetically engineered mouse (GEM) model required an inhibitory adjuvant (Treg depletion). In addition to developing new (e.g., epigenetic) TME regulators, recent mechanistic studies of repurposed drugs (aspirin, metformin, and tamoxifen) have identified potent immune activity. Just as precision medicine and immune-oncology are revolutionizing cancer therapy, these approaches are transforming cancer prevention. Here, we set out a brief agenda for the immediate future of cancer prevention research (including a "Pre-Cancer Genome Atlas" or "PCGA"), which will involve the inter-related fields of precision medicine and immunoprevention - pivotal elements of a broader domain of personalized public health.

Published
2016

45. AB014. Bone marrow dyscrasias in autoimmune regulator deficiency: lessons from thymoma and autoimmune polyendocrinopathy-candidiasis ectodermal dystrophy

Author

DaSilva, Laercio, primary, Swift, Shannon, additional, Sansone, Susan, additional, Szabo, Eva, additional, Zhao, Chen, additional, Feierabend, Christine, additional, Patel, Nisha, additional, Ochoa, Sebastian, additional, Lionakis, Michail S., additional, Rajan, Arun, additional, and McAdams, Meredith, additional

Published
2023
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46. AB016. Phase 2 clinical trial of PT-112 in patients with thymic epithelial tumors

Author

McAdams, Meredith, primary, Swift, Shannon, additional, Donahue, Renee N., additional, Celades, Carolina, additional, Tsai, Yo-Ting, additional, Bingham, Molly, additional, Szabo, Eva, additional, Zhao, Chen, additional, Sansone, Susan, additional, Feierabend, Christine, additional, DaSilva, Laercio, additional, Shelat, Meenakshi, additional, O’Donnell, Joseph, additional, Ames, Tyler D., additional, Raphael, Brooke, additional, Steinberg, Seth M., additional, Gulley, James L., additional, Schlom, Jeffrey, additional, and Rajan, Arun, additional

Published
2023
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