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51. Integrative clinical genomics of metastatic cancer

Author

Robinson, Dan R., Wu, Yi-Mi, Lonigro, Robert J., Vats, Pankaj, Cobain, Erin, Everett, Jessica, Cao, Xuhong, Rabban, Erica, Kumar-Sinha, Chandan, Raymond, Victoria, Schuetze, Scott, Alva, Ajjai, Siddiqui, Javed, Chugh, Rashmi, Worden, Francis, Zalupski, Mark M., Innis, Jeffrey, Mody, Rajen J., Tomlins, Scott A., Lucas, David, Baker, Laurence H., Ramnath, Nithya, Schott, Ann F., Hayes, Daniel F., Vijai, Joseph, Offit, Kenneth, Stoffel, Elena M., Roberts, J. Scott, Smith, David C., Kunju, Lakshmi P., Talpaz, Moshe, Cielik, Marcin, and Chinnaiyan, Arul M.

Subjects
Cancer metastasis -- Genetic aspects, Gene expression -- Health aspects, Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Metastasis is the primary cause of cancer-related deaths. Although The Cancer Genome Atlas has sequenced primary tumour types obtained from surgical resections, much less comprehensive molecular analysis is available from clinically acquired metastatic cancers. Here we perform whole-exome and -transcriptome sequencing of 500 adult patients with metastatic solid tumours of diverse lineage and biopsy site. The most prevalent genes somatically altered in metastatic cancer included TP53, CDKN2A, PTEN, PIK3CA, and RB1. Putative pathogenic germline variants were present in 12.2% of cases of which 75% were related to defects in DNA repair. RNA sequencing complemented DNA sequencing to identify gene fusions, pathway activation, and immune profiling. Our results show that integrative sequence analysis provides a clinically relevant, multi-dimensional view of the complex molecular landscape and microenvironment of metastatic cancers., Author(s): Dan R. Robinson [1, 2]; Yi-Mi Wu [1, 2]; Robert J. Lonigro [1]; Pankaj Vats [1]; Erin Cobain [3]; Jessica Everett [3]; Xuhong Cao [1]; Erica Rabban [1]; Chandan [...]

Published
2017
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55. Assessment of Clinical Benefit of Integrative Genomic Profiling in Advanced Solid Tumors

Author

Cobain, Erin F., primary, Wu, Yi-Mi, additional, Vats, Pankaj, additional, Chugh, Rashmi, additional, Worden, Francis, additional, Smith, David C., additional, Schuetze, Scott M., additional, Zalupski, Mark M., additional, Sahai, Vaibhav, additional, Alva, Ajjai, additional, Schott, Anne F., additional, Caram, Megan E. V., additional, Hayes, Daniel F., additional, Stoffel, Elena M., additional, Jacobs, Michelle F., additional, Kumar-Sinha, Chandan, additional, Cao, Xuhong, additional, Wang, Rui, additional, Lucas, David, additional, Ning, Yu, additional, Rabban, Erica, additional, Bell, Janice, additional, Camelo-Piragua, Sandra, additional, Udager, Aaron M., additional, Cieslik, Marcin, additional, Lonigro, Robert J., additional, Kunju, Lakshmi P., additional, Robinson, Dan R., additional, Talpaz, Moshe, additional, and Chinnaiyan, Arul M., additional

Published
2021
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57. A Multi-Institutional Phase 2 Study of Neoadjuvant Gemcitabine and Oxaliplatin With Radiation Therapy in Patients With Pancreatic Cancer

Author

Kim, Edward J., Ben-Josef, Edgar, Herman, Joseph M., Bekaii-Saab, Tanios, Dawson, Laura A., Griffith, Kent A., Francis, Isaac R., Greenson, Joel K., Simeone, Diane M., Lawrence, Theodore S., Laheru, Daniel, Wolfgang, Christopher L., Williams, Terence, Bloomston, Mark, Moore, Malcolm J., Wei, Alice, and Zalupski, Mark M.

Published
2013
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61. Clinical Assessment of 5-Fluorouracil/Leucovorin, Nab-Paclitaxel, and Irinotecan (FOLFIRABRAX) in Untreated Patients with Gastrointestinal Cancer Using UGT1A1 Genotype–Guided Dosing

Author

Joshi, Smita S., primary, Catenacci, Daniel V.T., additional, Karrison, Theodore G., additional, Peterson, Jaclyn D., additional, Zalupski, Mark M., additional, Sehdev, Amikar, additional, Wade, James, additional, Sadiq, Ahad, additional, Picozzi, Vincent J., additional, Amico, Andrea, additional, Marsh, Robert, additional, Kozloff, Mark F., additional, Polite, Blase N., additional, Kindler, Hedy L., additional, and Sharma, Manish R., additional

Published
2020
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81. Dose Escalation Trial of the Wee1 Inhibitor Adavosertib (AZD1775) in Combination With Gemcitabine and Radiation for Patients With Locally Advanced Pancreatic Cancer

Author

Cuneo, Kyle C., primary, Morgan, Meredith A., additional, Sahai, Vaibhav, additional, Schipper, Matthew J., additional, Parsels, Leslie A., additional, Parsels, Joshua D., additional, Devasia, Theresa, additional, Al-Hawaray, Mahmoud, additional, Cho, Clifford S., additional, Nathan, Hari, additional, Maybaum, Jonathan, additional, Zalupski, Mark M., additional, and Lawrence, Theodore S., additional

Published
2019
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87. Cytogenetic findings in 19 malignant bone tumors

Author

Ozisik, Yavuz Y., Meloni, Aurelia M., Peier, Andrea, Altungoz, Oguz, Spanier, Suzanne S., Zalupski, Mark M., Leong, Stanley P.L., and Sandberg, Avery A.

Subjects
Bone cancer -- Genetic aspects, Human cytogenetics -- Analysis, Osteosarcoma -- Genetic aspects, Chondrosarcoma -- Genetic aspects, Health
Abstract

Background. The majority of karyotypes observed in osteosarcomas (OS) and chondrosarcomas (CS) are complex. Specific chromosomal abnormalities have not yet been characterized in either tumor except for a ring chromosome in parosteal OS. The purpose of this study was to determine recurrent chromosomal abnormalities and establish a possible correlation between the cytogenetic changes and the pathologic findings. Methods. Ten OS and nine CS were cytogenetically analyzed. Tumor samples were obtained from patients having a resection or incisional biopsy. Cytogenetic study of short term cell cultures included harvesting and G-banding, which were performed by routine methodologies. Results. Clonal abnormalities were observed in six OS and six CS. Modal chromosome numbers ranged from near diploid to near tetraploid in both types of tumors. The structural rearrangements observed in OS involved mostly chromosomes 1, 2, 6, 12, and 17. Nonreciprocal translocations were the most frequent event. Two OS had a single clonal abnormality involving 11p15 and 14q32, respectively. Double minute chromosomes were observed in three cases. In CS, the most frequent structural abnormalities were nonreciprocal translocations and deletions involving numerous chromosomes. Rearrangements of 1p together with other abnormalities were observed in four CS. Conclusions. The karyotypes were usually complex consisting of numerical and structural changes, particularly in high grade tumors. Rearrangements of 11p15 and 14q32 in OS and possibly 1p in CS were found as primary cytogenetic aberrations. Cytogenetic analysis in more cases of OS and CS together with molecular studies are necessary to characterize further the consistent genetic changes in these tumors. Cancer 1994; 74:2268-75.

Published
1994

88. A common cytogenetic abnormality and DNA content alterations in dedifferentiated chondrosarcoma

Author

Zalupski, Mark M., Ensley, John F., Ryan, James, Irish novelist, Selvaggi, Suzanne, Baker, Laurence H., and Wolman, Sandra R.

Subjects
Karyotypes -- Usage, Human chromosome abnormalities -- Health aspects, Chromosome deletion -- Health aspects, Flow cytometry -- Usage, Chondrosarcoma -- Genetic aspects, Chromosome abnormalities -- Health aspects, Health
Abstract

While flow cytometry is useful in screening human cancers for chromosome abnormalities, only karyotyping is the definitive test. Karyotyping requires the growth of living cells from a biopsy or blood sample. The test demands skill and patience, and is generally not suitable for mass screening. Nevertheless, the cases of two patients with dedifferentiated chondrosarcoma illustrate that the karyotype provides information that is not available by other techniques. Chondrosarcomas are the second most common form of bone cancer. They usually affect older patients and generally occur as slow-growing low-grade cartilaginous growths. However, about 10 percent of chondrosarcomas lose their differentiated state (dedifferentiation) and become poorly differentiated aggressive high-grade cancers with a poor prognosis. Fresh chondrosarcoma tissue was obtained from two patients at surgery. Flow cytometric analysis was performed on both specimens; one was found to have the normal diploid chromosome complement, while the other was found to have a pathological aneuploid complement. Karyotyping was performed on cells and revealed abnormalities within the cells of both specimens. While numerous abnormalities were observed in both specimens, the aneuploid specimen was cytogenetically more complex, as would be expected. However, one defect was common to the chondrosarcoma cells from both patients. This common feature consisted of breaks in the short arm of chromosome 1. These breaks revealed themselves as a deletion in one chromosome homolog and recombination in the other. In both patients, the deletion and recombination occurred at the same chromosome band, in the region of 1p36. This same region is lost in neuroblastoma (a malignant cancer that usually affects infants and children) and has been shown to be involved in myxoid chondrosarcoma. It is not yet known if the 1p36 break will prove to be a consistent finding in these tumors. However, the same break occurring in both patients cannot be attributed only to coincidence; investigation of the genes near the 1p36 point is likely to reveal interesting mechanisms of the malignant transformation of cells. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1990

90. HALO 202: Randomized Phase II Study of PEGPH20 Plus Nab-Paclitaxel/Gemcitabine Versus Nab-Paclitaxel/Gemcitabine in Patients With Untreated, Metastatic Pancreatic Ductal Adenocarcinoma

Author

Hingorani, Sunil R., primary, Zheng, Lei, additional, Bullock, Andrea J., additional, Seery, Tara E., additional, Harris, William P., additional, Sigal, Darren S., additional, Braiteh, Fadi, additional, Ritch, Paul S., additional, Zalupski, Mark M., additional, Bahary, Nathan, additional, Oberstein, Paul E., additional, Wang-Gillam, Andrea, additional, Wu, Wilson, additional, Chondros, Dimitrios, additional, Jiang, Ping, additional, Khelifa, Sihem, additional, Pu, Jie, additional, Aldrich, Carrie, additional, and Hendifar, Andrew E., additional

Published
2018
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91. Irinotecan-associated dysarthria: A single institution case series with management implications in patients with gastrointestinal malignancies.

Author

Zhen, David B, McDevitt, Rachel L, Zalupski, Mark M, and Sahai, Vaibhav

Subjects
CANCER chemotherapy, DOSE-effect relationship in pharmacology, DYSARTHRIA, CASE studies, NEUROLOGIC manifestations of general diseases, GASTROINTESTINAL tumors, IRINOTECAN
Abstract

Irinotecan (Camptosar©, CPT-11), a topoisomerase I inhibitor, is a commonly used cytotoxic chemotherapeutic in the treatment of multiple malignancies, particularly of gastrointestinal origin. Dysarthria secondary to irinotecan has been described as a rare side effect in a few case reports with limited data to recommend appropriate management. We describe herein a large single institution experience of patients with gastrointestinal malignancies who experienced dysarthria while being treated with irinotecan-based chemotherapy regimens (FOLFIRINOX or FOLFIRI+/−bevacizumab). Eighteen patients developed neurological manifestations during irinotecan infusion with the majority (n = 17) developing dysarthria. Patients also experienced other known side effects including cholinergic effects (abdominal bloating, diarrhea, facial flushing, diaphoresis, and rhinorrhea), nausea, fatigue, perioral paresthesia and musculoskeletal discomfort. The dysarthria occurred as early as with the first infusion of irinotecan (n = 9), but several patients did not develop symptoms until subsequent infusions (range, 1–6). Dose alterations of irinotecan did not obviously impact the reccurrence or severity of dysarthria. Management strategies included close observation, atropine, slower irinotecan infusion rate, and reassurance. Dysarthria resolved without consequence in all patients within hours of completion of the infusion. Oncologists and pharmacists should be aware of irinotecan-associated dysarthria as a rare, self-limited phenomenon with no long-term sequelae, and appropriately counsel patients and infusion nurses to avoid inadvertently withholding potentially beneficial therapy for patients with gastrointestinal malignancies. [ABSTRACT FROM AUTHOR]

Published
2019
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93. A randomised, open-label, phase II study of neo/adjuvant doxorubicin and ifosfamide versus gemcitabine and docetaxel in patients with localised, high-risk, soft tissue sarcoma

Author

Davis, Elizabeth J., primary, Chugh, Rashmi, additional, Zhao, Lili, additional, Lucas, David R., additional, Biermann, J. Sybil, additional, Zalupski, Mark M., additional, Feng, Mary, additional, Wong, Sandra L., additional, Jacobson, Jon, additional, Zyczynski, Laurie, additional, Reinke, Denise, additional, Metko, Gino, additional, Baker, Laurence H., additional, and Schuetze, Scott M., additional

Published
2015
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94. SWOG S0809: A Phase II Intergroup Trial of Adjuvant Capecitabine and Gemcitabine Followed by Radiotherapy and Concurrent Capecitabine in Extrahepatic Cholangiocarcinoma and Gallbladder Carcinoma

Author

Ben-Josef, Edgar, primary, Guthrie, Katherine A., additional, El-Khoueiry, Anthony B., additional, Corless, Christopher L., additional, Zalupski, Mark M., additional, Lowy, Andrew M., additional, Thomas, Charles R., additional, Alberts, Steven R., additional, Dawson, Laura A., additional, Micetich, Kenneth C., additional, Thomas, Melanie B., additional, Siegel, Abby B., additional, and Blanke, Charles D., additional

Published
2015
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95. Caveolin-1 is Associated with Tumor Progression and Confers a Multi-Modality Resistance Phenotype in Pancreatic Cancer

Author

Chatterjee, Moumita, primary, Ben-Josef, Edgar, additional, Thomas, Dafydd G., additional, Morgan, Meredith A., additional, Zalupski, Mark M., additional, Khan, Gazala, additional, Andrew Robinson, Charles, additional, Griffith, Kent A., additional, Chen, Ching-Shih, additional, Ludwig, Thomas, additional, Bekaii-Saab, Tanios, additional, Chakravarti, Arnab, additional, and Williams, Terence M., additional

Published
2015
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97. Original Article A phase I study of imexon plus gemcitabine as first-line therapy for advanced pancreatic cancer

Author

Cohen, Steven J., Zalupski, Mark M., Modiano, Manuel R., Conkling, Paul, Patt, Yehuda Z., Davis, Peg, Dorr, Robert T., Boytim, Michelle L., and Hersh, Evan M.

Subjects
Adult, Aged, 80 and over, Male, Antimetabolites, Antineoplastic, Dose-Response Relationship, Drug, Adenocarcinoma, Middle Aged, Deoxycytidine, Gemcitabine, Article, Cohort Studies, Pancreatic Neoplasms, Hexanones, Area Under Curve, Antineoplastic Combined Chemotherapy Protocols, Cystine, Humans, Female, Sulfhydryl Compounds, Tomography, X-Ray Computed, Aged, Half-Life
Abstract

Imexon is an aziridine-derived iminopyrrolidone which has synergy with gemcitabine in pancreatic cancer cell lines. Gemcitabine is a standard therapy for pancreatic cancer. We performed a phase I trial of imexon and gemcitabine to evaluate safety, dose-limiting toxicity (DLT), and maximum tolerated dose (MTD) in patients with advanced pancreatic cancer.Patients with untreated locally advanced or metastatic pancreatic adenocarcinoma received therapy in sequential cohorts on regimen A (n = 19; imexon 200 or 280 mg/m(2) intravenously (IV) over 30 min days 1-5, 15-19 and gemcitabine 800 or 1,000 mg/m(2) IV over 30 min on days 1,8,15 every 28 days) or regimen B (n = 86; imexon 280-1,300 mg/m(2) IV over 30-60 min days 1, 8, and 15 and gemcitabine 1,000 mg/m(2) IV over 30 min on days 1, 8, and 15 every 28 days).One hundred five patients received 340 treatment cycles (median 2, range 1-16).median age 63, 61% male, ECOG PS 0/1 50%/50%, 93% metastatic. DLT was abdominal cramping and pain, often with transient, acute diarrhea. Best response was confirmed partial response (PR) in 11.4%, 8.9% unconfirmed PR, and 48.1% with stable disease. There was a dose proportional increase in imexon AUC across the doses tested with terminal half life 69 min at the MTD and no alteration of gemcitabine pharmacokinetics.The recommended phase II dose of imexon is 875 mg/m(2) with gemcitabine 1,000 mg/m(2). DLT was acute abdominal pain and cramping. Encouraging antitumor responses support further evaluation of this combination in advanced pancreatic cancer.

Published
2009

100. A Pilot Study of Diffusion-Weighted MRI in Patients Undergoing Neoadjuvant Chemoradiation for Pancreatic Cancer

Author

Cuneo, Kyle C., primary, Chenevert, Thomas L., additional, Ben-Josef, Edgar, additional, Feng, Mary U., additional, Greenson, Joel K., additional, Hussain, Hero K., additional, Simeone, Diane M., additional, Schipper, Matthew J., additional, Anderson, Michelle A., additional, Zalupski, Mark M., additional, Al-Hawary, Mahmoud, additional, Galban, Craig J., additional, Rehemtulla, Alnawaz, additional, Feng, Felix Y., additional, Lawrence, Theodore S., additional, and Ross, Brian D., additional

Published
2014
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