Your search keyword '"Posadas, Edwin M"' showing total 41 results

1. ONECUT2 acts as a lineage plasticity driver in adenocarcinoma as well as neuroendocrine variants of prostate cancer.

Author

Qian, Chen, Yang, Qian, Rotinen, Mirja, Huang, Rongrong, Kim, Hyoyoung, Gallent, Brad, Yan, Yiwu, Cadaneanu, Radu M, Zhang, Baohui, Kaochar, Salma, Freedland, Stephen J, Posadas, Edwin M, Ellis, Leigh, Di Vizio, Dolores, Morrissey, Colm, Nelson, Peter S, Brady, Lauren, Murali, Ramachandran, Campbell, Moray J, and Yang, Wei

Published

2024

2. Interleukin 33 supports squamous cell carcinoma growth via a dual effect on tumour proliferation, migration and invasion, and T cell activation.

Author

Perri, Graziela, Vilas Boas, Vanessa Garcia, Nogueira, Maria Renata Sales, Mello Júnior, Edgard José Franco, Coelho, Ana Lucia, Posadas, Edwin M., Hogaboam, Cory, Cavassani, Karen A, and Campanelli, Ana Paula

Abstract

Interleukin (IL)-33 is an important cytokine in the tumour microenvironment; it is known to promote the growth and metastasis of solid cancers, such as gastric, colorectal, ovarian and breast cancer. Our group demonstrated that the IL-33/ST2 pathway enhances the development of squamous cell carcinoma (SCC). Conversely, other researchers have reported that IL-33 inhibits tumour progression. In addition, the crosstalk between IL-33, cancer cells and immune cells in SCC remains unknown. The aim of this study was to investigate the effect of IL-33 on the biology of head and neck SCC lines and to evaluate the impact of IL-33 neutralisation on the T cell response in a preclinical model of SCC. First, we identified epithelial and peritumoural cells as a major local source of IL-33 in human SCC samples. Next, in vitro experiments demonstrated that the addition of IL-33 significantly increased the proliferative index, motility and invasiveness of SCC-25 cells, and downregulated MYC gene expression in SCC cell lines. Finally, IL-33 blockade significantly delayed SCC growth and led to a marked decrease in the severity of skin lesions. Importantly, anti-IL-33 monoclonal antibody therapy increase the percentage of CD4+IFNγ+ T cells and decreased CD4+ and CD8+ T cells secreting IL-4 in tumour-draining lymph nodes. Together, these data suggest that the IL-33/ST2 pathway may be involved in the crosstalk between the tumour and immune cells by modulating the phenotype of head and neck SCC and T cell activity. IL-33 neutralisation may offer a novel therapeutic strategy for SCC. [ABSTRACT FROM AUTHOR]

Published

2024

3. A practical guide for assessing and managing cardiovascular risk during androgen‐deprivation therapy in patients with prostate cancer.

Author

Solanki, Aum J., Kamrava, Mitchell, Posadas, Edwin M., Freedland, Stephen J., Ballas, Leslie, Sandler, Howard M., Bairey Merz, C. Noel, Atkins, Katelyn M., and Nikolova, Andriana P.

Subjects

PROSTATE cancer patients, PROSTATE cancer, CARDIOVASCULAR diseases risk factors, PRIMARY care

Abstract

Prostate cancer is the most common malignancy among men worldwide, and androgen‐deprivation therapy (ADT) is a mainstay of treatment. There are observational data demonstrating an increased risk of cardiovascular events in patients who receive ADT, particularly those who have an elevated baseline cardiovascular risk. Because, for most patients with prostate cancer, death is predominantly from noncancer‐related causes, cardiovascular disease and its risk factors should be optimized during cancer treatment. This review provides an overview of the landscape of ADT treatment and serves as a guide for appropriate cardiovascular screening and risk‐mitigation strategies. The authors emphasize the importance of shared communication between the multidisciplinary cancer team and primary care to improve baseline cardiovascular screening and treatment of modifiable risk factors within this higher risk population. The management of cardiovascular risk factors is significantly underperformed and under‐emphasized for patients with prostate cancer. By using the latest clinical evidence, the authors provide an easy‐to‐use guide for primary care providers and patients' multidisciplinary cancer treatment teams to appropriately address modifiable cardiovascular disease risk factors in this high‐risk population. [ABSTRACT FROM AUTHOR]

Published

2024

4. A cisplatin conjugate with tumor cell specificity exhibits antitumor effects in renal cancer models.

Author

Mrdenovic, Stefan, Wang, Yanping, Yin, Lijuan, Chu, Gina Chia-Yi, Ou, Yan, Lewis, Michael S., Heffer, Marija, Posadas, Edwin M., Zhau, Haiyen E., Chung, Leland W. K., Edderkaoui, Mouad, Pandol, Stephen J., Wang, Ruoxiang, and Zhang, Yi

Subjects

RENAL cancer, DRUG toxicity, RENAL cell carcinoma, NEPHROTOXICOLOGY, CANCER treatment, CELL death, MTOR inhibitors

Abstract

Background: Clear cell renal cell carcinoma (ccRCC) is the most common type of kidney cancer and is notorious for its resistance to both chemotherapy and small-molecule inhibitor targeted therapies. Subcellular targeted cancer therapy may thwart the resistance to produce a substantial effect. Methods: We tested whether the resistance can be circumvented by subcellular targeted cancer therapy with DZ-CIS, which is a chemical conjugate of the tumor-cell specific heptamethine carbocyanine dye (HMCD) with cisplatin (CIS), a chemotherapeutic drug with limited use in ccRCC treatment because of frequent renal toxicity. Results: DZ-CIS displayed cytocidal effects on Caki-1, 786-O, ACHN, and SN12C human ccRCC cell lines and mouse Renca cells in a dose-dependent manner and inhibited ACHN and Renca tumor formation in experimental mouse models. Noticeably, in tumor-bearing mice, repeated DZ-CIS use did not cause renal toxicity, in contrast to the CIS-treated control animals. In ccRCC tumors, DZ-CIS treatment inhibited proliferation markers but induced cell death marker levels. In addition, DZ-CIS at half maximal inhibitory concentration (IC50) sensitized Caki-1 cells to small-molecule mTOR inhibitors. Mechanistically, DZ-CIS selectively accumulated in ccRCC cells' subcellular organelles, where it damages the structure and function of mitochondria, leading to cytochrome C release, caspase activation, and apoptotic cancer cell death. Conclusions: Results from this study strongly suggest DZ-CIS be tested as a safe and effective subcellular targeted cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2023

5. Circulating Fatty Objects and Their Preferential Presence in Pancreatic Cancer Patient Blood Samples.

Author

Wang, Ruoxiang, Nissen, Nicholas N., Zhang, Yi, Shao, Chen, Chu, Chia-Yi, Huynh, Carissa, Posadas, Edwin M., Tomlinson, James S., Lewis, Michael S., and Pandol, Stephen J.

Subjects

PANCREATIC cancer, BLOOD sampling, CANCER patients, MONONUCLEAR leukocytes, CASTRATION-resistant prostate cancer, LIPID analysis, PANCREATIC surgery

Abstract

Human cancers are often complicated with increased incidences of blood vessel occlusion, which are mostly insensitive to anticoagulation therapy. We searched for causal factors of cancer-associated embolism. A total of 2,017 blood samples was examined for visible abnormalities. Examined were peripheral blood samples from cancer patients who were about to undergo surgical treatment for genitourinary, breast, gastrointestinal or abdominal tumors. Samples from ambulatory patients being treated for recurrent or castration-resistant prostate cancers were included in the study. The lipid-rich nature was studied with lipophilic stains and lipid panel analysis, while surface membrane was assessed with specific staining and antibody detection. We identified a new entity, lipid droplet-like objects or circulating fatty objects (CFOs), visible in the blood samples of many cancer patients, with the potential of causing embolism. CFOs were defined as lipid-rich objects with a membrane, capable of gaining in volume through interaction with peripheral blood mononuclear cells in ex vivo culture. Blood samples from pancreatic cancer patients were found to have the highest CFO incidence and largest CFO numbers. Most noticeably, CFOs from many pancreatic cancer samples presented as large clusters entangled in insoluble fiber networks, suggestive of intravascular clotting. This study identifies CFO as an abnormal entity in cancer patient blood, and a contributory factor to intravascular embolism during cancer development and progression. [ABSTRACT FROM AUTHOR]

Published

2022

6. Receptor-interacting protein kinase 2 (RIPK2) stabilizes c-Myc and is a therapeutic target in prostate cancer metastasis.

Author

Yan, Yiwu, Zhou, Bo, Qian, Chen, Vasquez, Alex, Kamra, Mohini, Chatterjee, Avradip, Lee, Yeon-Joo, Yuan, Xiaopu, Ellis, Leigh, Di Vizio, Dolores, Posadas, Edwin M., Kyprianou, Natasha, Knudsen, Beatrice S., Shah, Kavita, Murali, Ramachandran, Gertych, Arkadiusz, You, Sungyong, Freeman, Michael R., and Yang, Wei

Subjects

RECEPTOR-interacting proteins, PROTEIN kinases, METASTASIS, ANDROGEN receptors, MITOGEN-activated protein kinases, PROSTATE cancer

Abstract

Despite progress in prostate cancer (PC) therapeutics, distant metastasis remains a major cause of morbidity and mortality from PC. Thus, there is growing recognition that preventing or delaying PC metastasis holds great potential for substantially improving patient outcomes. Here we show receptor-interacting protein kinase 2 (RIPK2) is a clinically actionable target for inhibiting PC metastasis. RIPK2 is amplified/gained in ~65% of lethal metastatic castration-resistant PC. Its overexpression is associated with disease progression and poor prognosis, and its genetic knockout substantially reduces PC metastasis. Multi-level proteomics analyses reveal that RIPK2 strongly regulates the stability and activity of c-Myc (a driver of metastasis), largely via binding to and activating mitogen-activated protein kinase kinase 7 (MKK7), which we identify as a direct c-Myc-S62 kinase. RIPK2 inhibition by preclinical and clinical drugs inactivates the noncanonical RIPK2/MKK7/c-Myc pathway and effectively impairs PC metastatic outgrowth. These results support targeting RIPK2 signaling to extend metastasis-free and overall survival. Distant metastasis is a major reason for mortality in patients with prostate cancer (PC). Here, the authors show that receptor-interacting protein kinase 2 (RIPK2) stabilizes c-Myc and its targeting impairs PC metastasis development. [ABSTRACT FROM AUTHOR]

Published

2022

7. Niraparib with androgen receptor-axis-targeted therapy in patients with metastatic castration-resistant prostate cancer: safety and pharmacokinetic results from a phase 1b study (BEDIVERE).

Author

Saad, Fred, Chi, Kim N., Shore, Neal D., Graff, Julie N., Posadas, Edwin M., Lattouf, Jean-Baptiste, Espina, Byron M., Zhu, Eugene, Yu, Alex, Hazra, Anasuya, De Meulder, Marc, Mamidi, Rao N. V. S., Bradic, Branislav, Francis, Peter, Hayreh, Vinny, and Rezazadeh Kalebasty, Arash

Subjects

CASTRATION-resistant prostate cancer, ABIRATERONE acetate, PHARMACOKINETICS, THERAPEUTIC use of antineoplastic agents, STEROID drugs, RESEARCH, CLINICAL trials, HETEROCYCLIC compounds, RESEARCH methodology, CELL receptors, HYDANTOIN, ANTINEOPLASTIC agents, MEDICAL cooperation, EVALUATION research, PIPERIDINE, COMPARATIVE studies, PREDNISONE, PROSTATE tumors

Abstract

Purpose: To assess the safety and pharmacokinetics and determine the recommended phase 2 dose (RP2D) of niraparib with apalutamide or abiraterone acetate plus prednisone (AAP) in patients with metastatic castration-resistant prostate cancer (mCRPC).Methods: BEDIVERE was a multicenter, open-label, phase 1b study of niraparib 200 or 300 mg/day with apalutamide 240 mg or AAP (abiraterone acetate 1000 mg; prednisone 10 mg). Patients with mCRPC were previously treated with ≥ 2 lines of systemic therapy, including ≥ 1 androgen receptor-axis-targeted therapy for prostate cancer.Results: Thirty-three patients were enrolled (niraparib-apalutamide, 6; niraparib-AAP, 27). No dose-limiting toxicities (DLTs) were reported when combinations included niraparib 200 mg; five patients receiving niraparib 300 mg experienced DLTs [niraparib-apalutamide, 2/3 patients (66.7%); niraparib-AAP, 3/8 patients (37.5%)]. Although data are limited, niraparib exposures were lower when given with apalutamide compared with historical niraparib monotherapy exposures in patients with solid tumors. Because of the higher incidence of DLTs, the niraparib-apalutamide combination and niraparib 300 mg combination with AAP were not further evaluated. Niraparib 200 mg was selected as the RP2D with AAP. Of 19 patients receiving niraparib 200 mg with AAP, 12 (63.2%) had grade 3/4 treatment-emergent adverse events, the most common being thrombocytopenia (26.3%) and hypertension (21.1%). Five patients (26.3%) had adverse events leading to treatment discontinuation.Conclusions: These results support the choice of niraparib 200 mg as the RP2D with AAP. The niraparib-AAP combination was tolerable in patients with mCRPC, with no new safety signals. An ongoing phase 3 study is further assessing this combination in patients with mCRPC.Trial Registration No: NCT02924766 (ClinicalTrials.gov). [ABSTRACT FROM AUTHOR]

Published

2021

8. Disparities in Cancer Care and the Asian American Population.

Author

Lee, Richard J., Madan, Ravi A., Kim, Jayoung, Posadas, Edwin M., and Yu, Evan Y.

Subjects

RACISM, CULTURE, THERAPEUTICS, HEALTH services accessibility, ATTITUDE (Psychology), HEALTH status indicators, EARLY detection of cancer, TUMORS, CANCER patient medical care

Abstract

Asian Americans are the only racial/ethnic group in the U.S. for whom cancer is the leading cause of death in men and women, unlike heart disease for all other groups. Asian Americans face a confluence of cancer risks, with high rates of cancers endemic to their countries of origin due to infectious and cultural reasons, as well as increasing rates of "Western" cancers that are due in part to assimilation to the American diet and lifestyle. Despite the clear mortality risk, Asian Americans are screened for cancers at lower rates than the majority of Americans. Solutions to eliminate the disparity in cancer care are complicated by language and cultural concerns of this very heterogeneous group. This review addresses the disparities in cancer screening, the historical causes, the potential contribution of racism, the importance of cultural perceptions of health care, and potential strategies to address a very complicated problem. Noting that the health care disparities faced by Asian Americans may be less conspicuous than the structural racism that has inflicted significant damage to the health of Black Americans over more than four centuries, this review is meant to raise awareness and to compel the medical establishment to recognize the urgent need to eliminate health disparities for all. Implications for Practice: Cancer is the leading cause of death in Asian Americans, who face cancers endemic to their native countries, perhaps because of infectious and cultural factors, as well as those faced by all Americans, perhaps because of "Westernization" in terms of diet and lifestyle. Despite the mortality rates, Asian Americans have less cancer screening than other Americans. This review highlights the need to educate Asian Americans to improve cancer literacy and health care providers to understand the important cancer risks of the fastest‐growing racial/ethnic group in the U.S. Eliminating disparities is critical to achieving an equitable society for all Americans. Solutions are needed to eliminate disparities in cancer care for Asian Americans. This review addresses disparities in cancer screening, historical causes, the potential contribution of racism, the importance of cultural perceptions, and potential strategies to address this complicated problem. [ABSTRACT FROM AUTHOR]

Published

2021

9. Intensification of Androgen Deprivation Therapy in High-Risk, Nonmetastatic Prostate Cancer: Lessons From STAMPEDE.

Author

Gong, Jun and Posadas, Edwin M

Subjects

PROSTATE cancer, CANCER chemotherapy, ANDROGEN deprivation therapy, DOCETAXEL, RADIOTHERAPY

Published

2022

10. Covalent Chemistry‐Mediated Multimarker Purification of Circulating Tumor Cells Enables Noninvasive Detection of Molecular Signatures of Hepatocellular Carcinoma.

Author

Sun, Na, Lee, Yi‐Te, Kim, Minhyung, Wang, Jasmine J., Zhang, Ceng, Teng, Pai‐Chi, Qi, Dongping, Zhang, Ryan Y., Tran, Benjamin V., Lee, Yue Tung, Ye, Jinglei, Palomique, Juvelyn, Nissen, Nicholas N., Han, Steven‐Huy B., Sadeghi, Saeed, Finn, Richard S., Saab, Sammy, Busuttil, Ronald W., Posadas, Edwin M., and Liang, Li

Subjects

HEPATOCELLULAR carcinoma, MESSENGER RNA, CANCER diagnosis, DATA analysis, CLICK chemistry

Abstract

Transcriptomic profiling of tumor tissues introduces a large database, which has led to improvements in the ability of cancer diagnosis, treatment, and prevention. However, performing tumor transcriptomic profiling in the clinical setting is very challenging since the procurement of tumor tissues is inherently limited by invasive sampling procedures. Here, the feasibility of purifying hepatocellular carcinoma (HCC) circulating tumor cells (CTCs) from clinical patient samples is demonstrated with improved molecular integrity using Click Chips in conjunction with a multimarker antibody cocktail. The purified CTCs are then subjected to messenger RNA profiling by NanoString nCounter platform, targeting 64 HCC‐specific genes, which are generated from an integrated data analysis framework with eight tissue‐based prognostic gene signatures from seven publicly available HCC transcriptomic studies. After bioinformatics analysis and comparison, the HCC CTC‐derived gene signatures show high concordance with HCC tissue‐derived gene signatures from the Cancer Genome Atlas database, suggesting that HCC CTCs purified by Click Chips can enable the translation of HCC tissue molecular profiling into a noninvasive setting. [ABSTRACT FROM AUTHOR]

Published

2021

11. Integrating PARP Inhibitors Into Advanced Prostate Cancer Therapeutics.

Author

Jun Gong, Posadas, Edwin M., Bhowmick, Neil, Kim, Hyung L., Daskivich, Timothy J., Gupta, Amit, Sandler, Howard M., Kamrava, Mitchell, Zumsteg, Zachary S., Freedland, Stephen J., and Figlin, Robert A.

Abstract

DNA--damage repair (DDR) pathway mutations can sensitize cancer cells to a class of cancer therapeutics known as PARP inhibitors. Given that DDR alterations can be found in up to one-third of advanced prostate cancers, PARP inhibitors have recently been established in treatment-refractory settings. We provide an updated review of the clinical data supporting the 4 PARP inhibitors that have undergone the most investigation thus far in metastatic castrate-resistant prostate cancer (mCRPC). Two of these agents are currently approved for the treatment of DDR-altered mCRPC. We end with a discussion on integration of approved PARP inhibitors into advanced prostate cancer clinical practice. [ABSTRACT FROM AUTHOR]

Published

2021

12. COVID-19 and androgen-targeted therapy for prostate cancer patients.

Author

Bhowmick, Neil A., Oft, Jillian, Dorff, Tanya, Pal, Sumanta, Agarwal, Neeraj, Figlin, Robert A., Posadas, Edwin M., Freedland, Stephen J., and Jun Gong

Subjects

COVID-19, PROSTATE cancer patients, ANGIOTENSIN converting enzyme, SARS-CoV-2, ANDROGEN receptors

Abstract

The current pandemic (COVID-19) caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is a global health challenge with active development of antiviral drugs and vaccines seeking to reduce its significant disease burden. Early reports have confirmed that transmembrane serine protease 2 (TMPRSS2) and angiotensin converting enzyme 2 (ACE2) are critical targets of SARS-CoV-2 that facilitate viral entry into host cells. TMPRSS2 and ACE2 are expressed in multiple human ti ssues beyond the lung including the testes where predisposition to SARS-CoV-2 infection may exist. TMPRSS2 is an androgen-responsive gene and its fusion represents one of the most frequent alterations in prostate cancer. Androgen suppression by androgen deprivation therapy and androgen receptor signaling inhibitors form the foundation of prostate cancer treatment. In this review, we highlight the growing evidence in support of androgen regulation of TMPRSS2 and ACE2 and the potential clinical implications of using androgen suppression to downregulate TMPRSS2 to target SARS-CoV-2. We also discuss the future directions and controversies that need to be addressed in order to establish the viability of targeting TMPRSS2 and/or ACE2 through androgen signaling regulation for COVID-19 treatment, particularly its relevance in the context of prostate cancer management. [ABSTRACT FROM AUTHOR]

Published

2020

13. Cancer epithelia-derived mitochondrial DNA is a targetable initiator of a paracrine signaling loop that confers taxane resistance.

Author

Haldar, Subhash, Mishra, Rajeev, Billet, Sandrine, Thiruvalluvan, Manish, Placencio-Hickok, Veronica R., Madhav, Anisha, Duong, Frank, Angara, Bryan, Agarwal, Priyanka, Tighiouart, Mourad, Posadas, Edwin M., and Bhowmick, Neil A.

Subjects

MITOCHONDRIAL DNA, PATTERN perception receptors, PARACRINE mechanisms, MEMBRANE proteins, DOCETAXEL

Abstract

Stromal-epithelial interactions dictate cancer progression and therapeutic response. Prostate cancer (PCa) cells were identified to secrete greater concentration of mitochondrial DNA (mtDNA) compared to noncancer epithelia. Based on the recognized coevolution of cancer-associated fibroblasts (CAF) with tumor progression, we tested the role of cancer-derived mtDNA in a mechanism of paracrine signaling. We found that prostatic CAF expressed DEC205, which was not expressed by normal tissue-associated fibroblasts. DEC205 is a transmembrane protein that bound mtDNA and contributed to pattern recognition by Toll-like receptor 9 (TLR9). Complement C3 was the dominant gene targeted by TLR9-induced NF-κB signaling in CAF. The subsequent maturation complement C3 maturation to anaphylatoxin C3a was dependent on PCa epithelial inhibition of catalase in CAF. In a syngeneic tissue recombination model of PCa and associated fibroblast, the antagonism of the C3a receptor and the fibroblastic knockout of TLR9 similarly resulted in immune suppression with a significant reduction in tumor progression, compared to saline-treated tumors associated with wild-type prostatic fibroblasts. Interestingly, docetaxel, a common therapy for advanced PCa, further promoted mtDNA secretion in cultured epithelia, mice, and PCa patients. The antiapoptotic signaling downstream of anaphylatoxin C3a signaling in tumor cells contributed to docetaxel resistance. The inhibition of C3a receptor sensitized PCa epithelia to docetaxel in a synergistic manner. Tumor models of human PCa epithelia with CAF expanded similarly in mice in the presence or absence of docetaxel. The combination therapy of docetaxel and C3 receptor antagonist disrupted the mtDNA/C3a paracrine loop and restored docetaxel sensitivity. [ABSTRACT FROM AUTHOR]

Published

2020

14. Loss of testosterone impairs anti-tumor neutrophil function.

Author

Markman, Janet L., Porritt, Rebecca A., Wakita, Daiko, Lane, Malcolm E., Martinon, Daisy, Noval Rivas, Magali, Luu, Michael, Posadas, Edwin M., Crother, Timothy R., and Arditi, Moshe

Subjects

ANDROGEN drugs, TESTOSTERONE, PROSTATE cancer patients, CELL physiology, CANCER prognosis

Abstract

In men, the incidence of melanoma rises rapidly after age 50, and nearly two thirds of melanoma deaths are male. The immune system is known to play a key role in controlling the growth and spread of malignancies, but whether age- and sex-dependent changes in immune cell function account for this effect remains unknown. Here, we show that in castrated male mice, neutrophil maturation and function are impaired, leading to elevated metastatic burden in two models of melanoma. Replacement of testosterone effectively normalized the tumor burden in castrated male mice. Further, the aberrant neutrophil phenotype was also observed in prostate cancer patients receiving androgen deprivation therapy, highlighting the evolutionary conservation and clinical relevance of the phenotype. Taken together, these results provide a better understanding of the role of androgen signaling in neutrophil function and the impact of this biology on immune control of malignancies. It is known that there are sex differences in the incidence and prognosis of certain cancers, including melanoma. In this study, the authors utilize a melanoma model to reveal that castrated mice have a higher metastatic burden associated with androgen dependent impaired neutrophil function. [ABSTRACT FROM AUTHOR]

Published

2020

15. Developments in the use of tyrosine kinase inhibitors in the treatment of renal cell carcinoma.

Author

Reed, Jarred P., Posadas, Edwin M., and Figlin, Robert A.

Abstract

Introduction: Renal cell carcinoma (RCC) is among the most commonly diagnosed solid malignancies, but until recently there were few systemic treatment options for advanced disease. Since 2005, the treatment landscape has been transformed by the development of several novel systemic therapies. In particular, tyrosine kinase inhibitors (TKIs) targeting the vascular endothelial growth factor (VEGF) pathway have been instrumental in improving outcomes in patients with metastatic disease. Areas covered: The armamentarium of TKIs available for the treatment of RCC has expanded in recent years. The most active area of research at this time is the development of treatment regimens combining newer-generation TKIs and immune checkpoint inhibitors. Emerging data point to a role for combination therapy in the frontline management of advanced RCC. Other ongoing areas of research include the use of TKIs in the adjuvant setting and the role of cytoreductive nephrectomy within a changing treatment landscape. Expert opinion: Although TKIs and immune checkpoint inhibitors have incrementally improved outcomes for patients with advanced RCC, long-term survival remains poor. The development of regimens combining these agents represents the next step in the evolution of the field. For the clinician, this will offer exciting possibilities and novel challenges. [ABSTRACT FROM AUTHOR]

Published

2019

16. An Open Label Phase Ib Dose Escalation Study of TRC105 (Anti‐Endoglin Antibody) with Axitinib in Patients with Metastatic Renal Cell Carcinoma.

Author

Choueiri, Toni K., Michaelson, M. Dror, Posadas, Edwin M., Sonpavde, Guru P., McDermott, David F., Nixon, Andrew B., Liu, Yingmiao, Yuan, Zhenhua, Seon, Ben K., Walsh, Meghara, Jivani, Manoj A., Adams, Bonne J., and Theuer, Charles P.

Subjects

COMBINATION drug therapy, CLINICAL trials, CYTOKINES, DRUG tolerance, DRUG dosage, DRUG toxicity, ENDOGLIN, METASTASIS, RENAL cell carcinoma, SURVIVAL, TRANSFORMING growth factors-beta, PROTEIN-tyrosine kinase inhibitors, TREATMENT effectiveness, DISEASE progression, CHEMICAL inhibitors, PROGNOSIS, THERAPEUTICS

Abstract

Background: TRC105 is an IgG1 endoglin monoclonal antibody that potentiates VEGF inhibitors in preclinical models. We assessed safety, pharmacokinetics, and antitumor activity of TRC105 in combination with axitinib in patients with metastatic renal cell carcinoma (mRCC). Subjects, Materials, and Methods: Heavily pretreated mRCC patients were treated with TRC105 weekly (8 mg/kg and then 10 mg/kg) in combination with axitinib (initially at 5 mg b.i.d. and then escalated per patient tolerance to a maximum of 10 mg b.i.d.) until disease progression or unacceptable toxicity using a standard 3 + 3 phase I design. Results: Eighteen patients (median number of prior therapies = 3) were treated. TRC105 dose escalation proceeded to 10 mg/kg weekly without dose‐limiting toxicity. Adverse event characteristics of each drug were not increased in frequency or severity when the two drugs were administered concurrently. TRC105 and axitinib demonstrated preliminary evidence of activity, including partial responses (PR) by RECIST in 29% of patients, and median progression‐free survival (11.3 months). None of the patients with PR had PR to prior first‐line treatment. Lower baseline levels of osteopontin and higher baseline levels of TGF‐β receptor 3 correlated with overall response rate. Conclusion: TRC105 at 8 and 10 mg/kg weekly was well tolerated in combination with axitinib, with encouraging evidence of activity in patients with mRCC. A multicenter, randomized phase II trial of TRC105 and axitinib has recently completed enrollment (NCT01806064). Implications for Practice: TRC105 is a monoclonal antibody to endoglin (CD105), a receptor densely expressed on proliferating endothelial cells and also on renal cancer stem cells that is implicated as a mediator of resistance to inhibitors of the VEGF pathway. In this Phase I trial, TRC105 combined safely with axitinib at the recommended single agent doses of each drug in patients with renal cell carcinoma. The combination demonstrated durable activity in a VEGF inhibitor‐refractory population and modulated several angiogenic biomarkers. A randomized Phase II trial testing TRC105 in combination with axitinib in clear cell renal cell carcinoma has completed accrual. This article reports the results of an open label phase I clinical study that assessed the safety, tolerability, pharmacokinetics, pharmacodynamics, and antitumor activity of TRC105 when given concurrently with axitinib to adult patients with metastatic renal cell carcinoma who progressed following prior treatment with at least one VEGFR TKI. [ABSTRACT FROM AUTHOR]

Published

2019

17. Safety and Efficacy of BIND-014, a Docetaxel Nanoparticle Targeting Prostate-Specific Membrane Antigen for Patients With Metastatic Castration-Resistant Prostate Cancer: A Phase 2 Clinical Trial.

Author

Autio, Karen A., Dreicer, Robert, Anderson, Justine, Garcia, Jorge A., Alva, Ajjai, Hart, Lowell L., Milowsky, Matthew I., Posadas, Edwin M., Ryan, Charles J., Graf, Ryon P., Dittamore, Ryan, Schreiber, Nicole A., Summa, Jason M., Youssoufian, Hagop, Morris, Michael J., and Scher, Howard I.

Published

2018

18. Circulating monocytes from prostate cancer patients promote invasion and motility of epithelial cells.

Author

Cavassani, Karen A., Meza, Rebecca J., Habiel, David M., Chen, Jie‐Fu, Montes, Alexander, Tripathi, Manisha, Martins, Gislâine A., Crother, Timothy R., You, Sungyong, Hogaboam, Cory M., Bhowmick, Neil, and Posadas, Edwin M.

Subjects

PROSTATE cancer, CANCER immunology, MYELOID leukemia, MONOCYTES, EPITHELIAL cells, CANCER cell motility, DISEASE progression

Abstract

Abstract: Background: Recruited myeloid cells are known to promote cancer initiation, malignant progression, metastasis, and resistance to therapy in the tumor niche. We tested the hypothesis that circulating blood monocytes from advanced prostate cancer (PCa) patients exhibit a protumor phenotype and directly influence the tumor microenvironment in response to tumor‐derived signals. Methods: Blood monocytes from advanced and stable PCa patients were cultured, and the conditioned media (CM) were collected and analyzed using standard invasion and wound closure assays to measure effects on invasion and motility of PCa tumor cells. We then identified the proteome profile of these monocytes using proteome array and ELISA. Results: Conditioned media from circulating monocytes in patients with metastatic prostate cancer (PCa‐M) increased invasion of epithelial PCa cells in vitro. Proteome Profiler Analysis revealed that monocyte‐derived CM from metastatic castration‐resistant (mCRPC) patients presented high levels of chitinase‐3‐like 1 (CHI3L1, YKL‐40) when compared to patients with stable disease (PCa‐N) and healthy control individuals (HC). The only described receptor for CHI3L1, interleukin‐13 receptor α2 (IL‐13Rα2), was significantly up‐regulated in the human metastatic PCa cell line, ARCaPM. Accordingly, we observed that the activation of IL‐13Rα2 from PCa‐M CM increased the invasiveness of ARCaPM cells while siRNA directed against this receptor significantly reduced invasiveness of these cells in the presence of CM from PCa‐M patients. Conclusions: Thus, we show that circulating monocytes from metastatic PCa patients exert a tumor‐promoting role via the secretion of CHI3L1, and CHI3L1 demands further exploration as a possible therapeutic target in advanced PCa. [ABSTRACT FROM AUTHOR]

Published

2018

19. Glycan Stimulation Enables Purification of Prostate Cancer Circulating Tumor Cells on PEDOT NanoVelcro Chips for RNA Biomarker Detection.

Author

Shen, Mo‐Yuan, Chen, Jie‐Fu, Luo, Chun‐Hao, Lee, Sangjun, Li, Cheng‐Hsuan, Yang, Yung‐Ling, Tsai, Yu‐Han, Ho, Bo‐Cheng, Bao, Li‐Rong, Lee, Tien‐Jung, Jan, Yu Jen, Zhu, Ya‐Zhen, Cheng, Shirley, Feng, Felix Y., Chen, Peilin, Hou, Shuang, Agopian, Vatche, Hsiao, Yu‐Sheng, Tseng, Hsian‐Rong, and Posadas, Edwin M.

Published

2018

20. Circulating Tumor Cells in Prostate Cancer: Beyond Enumeration.

Author

Jie-Fu Chen, Yi-Tsung Lu, Cheng, Shirley, Hsian-Rong Tseng, Figlin, Robert A., and Posadas, Edwin M.

Published

2017

21. Saracatinib as a metastasis inhibitor in metastatic castration-resistant prostate cancer: A University of Chicago Phase 2 Consortium and DOD/PCF Prostate Cancer Clinical Trials Consortium Study.

Author

Posadas, Edwin M., Ahmed, Rafi S., Karrison, Theodore, Szmulewitz, Russell Z., O'Donnell, Peter H., Wade, James L., Shen, James, Gururajan, Murali, Sievert, Margarit, and Stadler, Walter M.

Published

2016

22. Is computed tomography a necessary part of a metastatic evaluation for castration-resistant prostate cancer? Results from the Shared Equal Access Regional Cancer Hospital Database.

Author

Hanyok, Brian T., Howard, Lauren E., Amling, Christopher L., Aronson, William J., Cooperberg, Matthew R., Kane, Christopher J., Terris, Martha K., Posadas, Edwin M., and Freedland, Stephen J.

Subjects

PROSTATE cancer, COMPUTED tomography, PROSTATE-specific antigen, SOFT tissue tumors, METASTASIS, UNIVARIATE analysis, LYMPH node cancer, DIAGNOSIS, BONE tumors, CANCER invasiveness, DATABASES, LYMPH nodes, PROGNOSIS, PROSTATE tumors, RESEARCH funding, RISK assessment, SURVIVAL analysis (Biometry), TUMOR classification, LOGISTIC regression analysis, PREDICTIVE tests, RETROSPECTIVE studies

Abstract

Background: Metastatic lesions in prostate cancer beyond the bone have prognostic importance and affect clinical therapeutic decisions. Few data exist regarding the prevalence of soft-tissue metastases at the initial diagnosis of metastatic castration-resistant prostate cancer (mCRPC).Methods: This study analyzed 232 men with nonmetastatic (M0) castration-resistant prostate cancer (CRPC) who developed metastases detected by a bone scan or computed tomography (CT). All bone scans and CT scans within the 30 days before or after the mCRPC diagnosis were reviewed. The rate of soft-tissue metastases among those undergoing CT was determined. Then, predictors of soft-tissue metastases and visceral and lymph node metastases were identified.Results: Compared with men undergoing CT (n = 118), men undergoing only bone scans (n = 114) were more likely to have received primary treatment (P = .048), were older (P = .013), and less recently developed metastases (P = .018). Among those undergoing CT, 52 (44%) had soft-tissue metastases, including 20 visceral metastases (17%) and 41 lymph node metastases (35%), whereas 30% had no bone involvement. In a univariable analysis, only prostate-specific antigen (PSA) predicted soft-tissue metastases (odds ratio [OR], 1.27; P = .047), and no statistically significant predictors of visceral metastases were found. A higher PSA level was associated with an increased risk of lymph node metastases (OR, 1.38; P = .014), whereas receiving primary treatment was associated with decreased risk (OR, 0.36; P = .015).Conclusions: The data suggest that there is a relatively high rate of soft-tissue metastasis (44%) among CRPC patients undergoing CT at the initial diagnosis of metastases, including some men with no bone involvement. Therefore, forgoing CT during a metastatic evaluation may lead to an underdiagnosis of soft-tissue metastases and an underdiagnosis of metastases in general. Cancer 2015. © 2015 American Cancer Society. Cancer 2016;122:222-229. © 2015 American Cancer Society. [ABSTRACT FROM AUTHOR]

Published

2016

23. Subclassification of prostate cancer circulating tumor cells by nuclear size reveals very small nuclear circulating tumor cells in patients with visceral metastases.

Author

Chen, Jie‐Fu, Ho, Hao, Lichterman, Jake, Lu, Yi‐Tsung, Zhang, Yang, Garcia, Mitch A., Chen, Shang‐Fu, Liang, An‐Jou, Hodara, Elisabeth, Zhau, Haiyen E., Hou, Shuang, Ahmed, Rafi S., Luthringer, Daniel J., Huang, Jiaoti, Li, Ker‐Chau, Chung, Leland W. K., Ke, Zunfu, Tseng, Hsian‐Rong, and Posadas, Edwin M.

Subjects

PROSTATE cancer, TUMOR classification, CELL migration, CELL nuclei, METASTASIS, GAUSSIAN mixture models, PATIENTS

Abstract

BACKGROUND Although enumeration of circulating tumor cells (CTCs) has shown some clinical value, the pool of CTCs contains a mixture of cells that contains additional information that can be extracted. The authors subclassified CTCs by shape features focusing on nuclear size and related this with clinical information. METHODS A total of 148 blood samples were obtained from 57 patients with prostate cancer across the spectrum of metastatic states: no metastasis, nonvisceral metastasis, and visceral metastasis. CTCs captured and enumerated on NanoVelcro Chips (CytoLumina, Los Angeles, Calif) were subjected to pathologic review including nuclear size. The distribution of nuclear size was analyzed using a Gaussian mixture model. Correlations were made between CTC subpopulations and metastatic status. RESULTS Statistical modeling of nuclear size distribution revealed 3 distinct subpopulations: large nuclear CTCs, small nuclear CTCs, and very small nuclear CTCs (vsnCTCs). Small nuclear CTCs and vsnCTC identified those patients with metastatic disease. However, vsnCTC counts alone were found to be elevated in patients with visceral metastases when compared with those without (0.36 ± 0.69 vs 1.95 ± 3.77 cells/mL blood; P<.001). Serial enumeration studies suggested the emergence of vsnCTCs occurred before the detection of visceral metastases. CONCLUSIONS There are morphologic subsets of CTCs that can be identified by fundamental pathologic approaches, such as nuclear size measurement. The results of this observational study strongly suggest that CTCs contain relevant information regarding disease status. In particular, the detection of vsnCTCs was found to be correlated with the presence of visceral metastases and should be formally explored as a putative blood-borne biomarker to identify patients at risk of developing this clinical evolution of prostate cancer. Cancer 2015;121:3240-3251. © 2015 American Cancer Society. [ABSTRACT FROM AUTHOR]

Published

2015

24. Presurgical Therapy for Renal Cell Carcinoma and Implications for Window-of-Opportunity Trials.

Author

Kim, Hyung L., Posadas, Edwin M., and Figlin, Robert A.

Published

2012

25. Calcitriol and Vitamin D Analogs.

Author

Jensen, Ana R., Szmulewitz, Russell Z., Beer, Tomasz M., and Posadas, Edwin M.

Abstract

Calcitriol (1,25-dihydroxycholecaliferol) is a synthetic analog of vitamin D that is physiologically active in absorption of calcium from the gastrointestinal tract. Recent clinical and laboratory developments have fueled enthusiasm for studying the role of vitamin D and its relationship to oncogenesis and malignant progression. There are epidemiological data pointing toward a link between vitamin D and prostate cancer as well as preclinical and clinical data linking antineoplastic activity of vitamin D receptor ligands with prostate cancer. As such, efforts have been geared toward the development of vitamin D receptor ligand-based therapy for early and advanced prostate cancer. In this chapter we will discuss the historic and current thoughts on the role that vitamin D may play in prostate cancer risk and treatment. [ABSTRACT FROM AUTHOR]

Published

2010

26. Detection of Live Circulating Tumor Cells by a Class of Near-Infrared Heptamethine Carbocyanine Dyes in Patients with Localized and Metastatic Prostate Cancer.

Author

Shao, Chen, Liao, Chun-Peng, Hu, Peizhen, Chu, Chia-Yi, Zhang, Lei, Bui, Matthew H. T., Ng, Christopher S., Josephson, David Y., Knudsen, Beatrice, Tighiouart, Mourad, Kim, Hyung L., Zhau, Haiyen E., Chung, Leland W. K., Wang, Ruoxiang, and Posadas, Edwin M.

Subjects

CANCER cells, DYES & dyeing, PROSTATE cancer patients, CELL adhesion, APOPTOSIS, FLOW cytometry, LYMPH nodes

Abstract

Tumor cells are inherently heterogeneous and often exhibit diminished adhesion, resulting in the shedding of tumor cells into the circulation to form circulating tumor cells (CTCs). A fraction of these are live CTCs with potential of metastatic colonization whereas others are at various stages of apoptosis making them likely to be less relevant to understanding the disease. Isolation and characterization of live CTCs may augment information yielded by standard enumeration to help physicians to more accurately establish diagnosis, choose therapy, monitor response, and provide prognosis. We previously reported on a group of near-infrared (NIR) heptamethine carbocyanine dyes that are specifically and actively transported into live cancer cells. In this study, this viable tumor cell-specific behavior was utilized to detect live CTCs in prostate cancer patients. Peripheral blood mononuclear cells (PBMCs) from 40 patients with localized prostate cancer together with 5 patients with metastatic disease were stained with IR-783, the prototype heptamethine cyanine dye. Stained cells were subjected to flow cytometric analysis to identify live (NIR+) CTCs from the pool of total CTCs, which were identified by EpCAM staining. In patients with localized tumor, live CTC counts corresponded with total CTC numbers. Higher live CTC counts were seen in patients with larger tumors and those with more aggressive pathologic features including positive margins and/or lymph node invasion. Even higher CTC numbers (live and total) were detected in patients with metastatic disease. Live CTC counts declined when patients were receiving effective treatments, and conversely the counts tended to rise at the time of disease progression. Our study demonstrates the feasibility of applying of this staining technique to identify live CTCs, creating an opportunity for further molecular interrogation of a more biologically relevant CTC population. [ABSTRACT FROM AUTHOR]

Published

2014

27. High-Purity Prostate Circulating Tumor Cell Isolation by a Polymer Nanofiber-Embedded Microchip for Whole Exome Sequencing.

Author

Zhao, Libo, Lu, Yi-Tsung, Li, Fuqiang, Wu, Kui, Hou, Shuang, Yu, Juehua, Shen, Qinglin, Wu, Dongxia, Song, Min, OuYang, Wei-Han, Luo, Zheng, Lee, Tom, Fang, Xiaohong, Shao, Chen, Xu, Xun, Garcia, Mitch A., Chung, Leland W. K., Rettig, Matthew, Tseng, Hsian-Rong, and Posadas, Edwin M.

Published

2013

28. Systemic Therapy in Renal Cell Carcinoma: Advancing Paradigms.

Author

Posadas, Edwin M. and Figlin, Robert A.

Abstract

The article discusses the innovation in the framework of renal cell carcinoma (RCC) therapy in the U.S. It explains the favorable reviews of the Oncologic Drugs Advisory Committee on vascular endothelial growth factor receptor (VEGFR) inhibitor and the development of other molecular targets for RCC treatment. It also cites the opportunities and challenges presented by the availability of active agents for additional clinical maneuvers such as adjuvant therapy and combinatorial therapies.

Published

2012

29. Fyn: a novel molecular target in cancer.

Author

Saito YD, Jensen AR, Salgia R, Posadas EM, Saito, Yoshihito D, Jensen, Ana R, Salgia, Ravi, and Posadas, Edwin M

Abstract

Fyn is 59-kDa member of the Src family of kinases that is historically associated with T-cell and neuronal signaling in development and normal cellular physiology. Whereas Src has been heavily studied in cancer, less attention has been traditionally awarded to the other Src kinases such as Fyn. Our group has shown that Fyn is particularly upregulated in prostate cancer in contrast to the alternative members of the Src family. This suggests that it may mediate several important processes attributed to Src kinases in prostate cancer and other malignancies. These functions include not only cellular growth and proliferation but also morphogenesis and cellular motility. Together, these suggest a role for Fyn in both progression and metastasis. As several agents in clinical development affect Fyn activation, understanding the role that Fyn plays in cancer is of great importance in oncology. Cancer 2010. (c) 2010 American Cancer Society. [ABSTRACT FROM AUTHOR]

Published

2010

30. A Novel Molecular Target in Cancer.

Author

Saito, Yoshihito D., Jensen, Ana R., Salgia, Ravi, and Posadas, Edwin M.

Subjects

PROSTATE cancer treatment, MOLECULAR biology, MORPHOLOGY, BIOTRANSFORMATION (Metabolism), ONCOLOGY

Abstract

The article presents a study which examines the molecular targeting role of Fyn, a member of the Src family kinases (SFKs), in the field of oncology. It states that the structure and pattern of activation of SFK proteins were also evaluated in the study. It also mentions that normal cells' morphologic transformation is driven by the overexpression of Fyn. Moreover, it concludes that inhibiting Fyn plays a vital role in the treatment and diagnosis of prostate cancer.

Published

2010

31. Third-Line Treatment Options for Kidney Cancer.

Author

Posadas, Edwin M., Limvorasak, Suwicha, and Figlin, Robert A.

Published

2016

32. FYN is overexpressed in human prostate cancer.

Author

Posadas, Edwin M., Al-Ahmadie, Hikmat, Robinson, Victoria L., Jagadeeswaran, Ramasamy, Otto, Kristen, Kasza, Kristen E., Tretiakov, Maria, Siddiqui, Javed, Pienta, Kenneth J., Stadler, Walter M., Rinker-Schaeffer, Carrie, and Salgia, Ravi

Subjects

PROSTATE cancer, IMMUNOBLOTTING, IMMUNOASSAY, CANCER cells, CELL lines, DNA polymerases, POLYMERASE chain reaction

Abstract

OBJECTIVE To test the hypothesis that FYN, a member of the SRC family of kinases (SFKs), is up-regulated in prostate cancer, as FYN is functionally distinct from other SFKs, and interacts with FAK and paxillin (PXN), regulators of cell morphology and motility. MATERIALS AND METHODS Through data-mining in Oncomine ( ), cell-line profiling with immunoblotting, quantitative reverse transcription and polymerase chain reaction (RT-PCR) and immunohistochemical analysis, we described FYN expression in prostate cancer. The analysis included 32 cases of prostate cancer, nine of prostatic intraepithelial neoplasia (PIN) and 19 normal prostates. Samples were scored for the percentage of stained glands and intensity of staining (from 0 to 3). Each sample was assigned a composite score generated by multiplying percentage and intensity. RESULTS Data-mining showed an eight times greater FYN expression in prostate cancer than in normal tissue; this was specific to FYN and not present for other SFKs. Expression of FYN in prostate cancer cell lines (LNCaP, 22Rv1, PC3, DuPro) was detected using quantitative RT-PCR and immunoblotting. Expression of FYN and its signalling partners FAK and PXN was detected in human tissue. Comparing normal with cancer samples, there was a 2.1-fold increase in median composite score for FYN ( P < 0.001) 1.7-fold increase in FAK ( P < 0.001), and a doubling in PXN ( P < 0.05). There was a 1.7-fold increase in FYN ( P < 0.05) and a 1.6-fold increase in FAK ( P < 0.01) in cancer compared with PIN. CONCLUSIONS These studies support the hypothesis that FYN and its related signalling partners are up-regulated in prostate cancer, and support further investigation into the role of the FYN as a therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2009

33. A phase II and pharmacodynamic study of gefitinib in patients with refractory or recurrent epithelial ovarian cancer.

Author

Posadas, Edwin M, Liel, Meghan S, Kwitkowski, Virginia, Minasian, Lori, Godwin, Andrew K, Hussain, Mahrukh M, Espina, Virginia, Wood, Bradford J, Steinberg, Seth M, and Kohn, Elise C

Subjects

ANTINEOPLASTIC agents, HETEROCYCLIC compounds, ADENOCARCINOMA, CANCER relapse, CELLULAR signal transduction, CLINICAL trials, COMPARATIVE studies, EPIDERMAL growth factor, EPITHELIAL cell tumors, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, OVARIAN tumors, PHOSPHORYLATION, POLYMERASE chain reaction, PROGNOSIS, RESEARCH, RESEARCH funding, TIME, TRANSFERASES, TUMORS, ENDOMETRIAL tumors, EVALUATION research, TREATMENT effectiveness, PAPILLARY carcinoma, CHEMICAL inhibitors

Abstract

Background: The primary objective of this study was to evaluate the biochemical effects of gefitinib on its target signal-transduction pathways in patients with recurrent epithelial ovarian cancer (EOC). The secondary objectives included assessing clinical activity and toxicity and determining the association between biochemical and clinical outcomes.Methods: Twenty-four heavily pretreated patients with EOC who had good end-organ function and performance status and who had measurable disease received gefitinib 500 mg daily. Prospectively planned core-needle tumor biopsies were obtained before treatment and after 4 weeks. Protein expression of total and phosphorylated (p) epidermal growth factor receptor (EGFR), protein kinase B (AKT), and extracellular regulated kinase (ERK) was quantified in microdissected tumor cells using tissue lysate array proteomics.Results: All tumor samples had detectable levels of EGFR and p-EGFR. A decrease in the quantity of both EGFR and p-EGFR was observed with gefitinib therapy in >50% of patients. This was not associated with clinical benefit, nor were responses observed. However, trends for increased gastrointestinal and skin toxicity were observed with greater phosphorylation or quantities of EGFR, ERK, and AKT in tumor samples (P Conclusions: The results from this study demonstrated that gefitinib inhibited the phosphorylation of EGFR in EOC tumor cells, providing proof of target in a clinical setting. Combinatorial therapy with molecular therapeutics against complementary targets may prove successful. [ABSTRACT FROM AUTHOR]

Published

2007

34. Proteomics and ovarian cancer: implications for diagnosis and treatment: a critical review of the recent literature.

Author

Posadas, Edwin M, Davidson, Ben, and Kohn, Elise C

Published

2004

35. The emerging role of bisphosphonates in prostate cancer.

Author

Posadas EM, Dahut WL, Gulley J, Posadas, Edwin M, Dahut, William L, and Gulley, James

Published

2004

36. Frontiers in prostate cancer. Telomeres and chaos.

Author

Sommerfeld, Hans J., Meeker, Alan K., Posadas, Edwin M., and Coffey, Donald S.

Published

1995

37. Large extracellular vesicles carry most of the tumour DNA circulating in prostate cancer patient plasma.

Author

Vagner, Tatyana, Spinelli, Cristiana, Minciacchi, Valentina R., Balaj, Leonora, Zandian, Mandana, Conley, Andrew, Zijlstra, Andries, Freeman, Michael R., Demichelis, Francesca, De, Subhajyoti, Posadas, Edwin M., Tanaka, Hisashi, and Di Vizio, Dolores

Subjects

PROSTATE cancer, CANCER cells, VESICLES (Cytology)

Abstract

Cancer-derived extracellular vesicles (EVs) are membrane-enclosed structures of highly variable size. EVs contain a myriad of substances (proteins, lipid, RNA, DNA) that provide a reservoir of circulating molecules, thus offering a good source of biomarkers. We demonstrate here that large EVs (L-EV) (large oncosomes) isolated from prostate cancer (PCa) cells and patient plasma are an EV population that is enriched in chromosomal DNA, including large fragments up to 2 million base pair long. While L-EVs and small EVs (S-EV) (exosomes) isolated from the same cells contained similar amounts of protein, the DNA was more abundant in L-EVs, despite S-EVs being more numerous. Consistent with in vitro observations, the abundance of DNA in L-EV obtained from PCa patient plasma was variable but frequently high. Conversely, negligible amounts of DNA were present in the S-EVs from the same patients. Controlled experimental conditions, with spike-ins of L-EVs and S-EVs from cancer cells in human plasma from healthy subjects, showed that circulating DNA is almost exclusively enclosed in L-EVs. Whole genome sequencing revealed that the DNA in L-EVs reflects genetic aberrations of the cell of origin, including copy number variations of genes frequently altered in metastatic PCa (i.e. MYC, AKT1, PTK2, KLF10 and PTEN). These results demonstrate that L-EV-derived DNA reflects the genomic make-up of the tumour of origin. They also support the conclusion that L-EVs are the fraction of plasma EVs with DNA content that should be interrogated for tumour-derived genomic alterations. [ABSTRACT FROM AUTHOR]

Published

2018

38. RNA Biomarkers: Glycan Stimulation Enables Purification of Prostate Cancer Circulating Tumor Cells on PEDOT NanoVelcro Chips for RNA Biomarker Detection (Adv. Healthcare Mater. 3/2018).

Author

Shen, Mo‐Yuan, Chen, Jie‐Fu, Luo, Chun‐Hao, Lee, Sangjun, Li, Cheng‐Hsuan, Yang, Yung‐Ling, Tsai, Yu‐Han, Ho, Bo‐Cheng, Bao, Li‐Rong, Lee, Tien‐Jung, Jan, Yu Jen, Zhu, Ya‐Zhen, Cheng, Shirley, Feng, Felix Y., Chen, Peilin, Hou, Shuang, Agopian, Vatche, Hsiao, Yu‐Sheng, Tseng, Hsian‐Rong, and Posadas, Edwin M.

Published

2018

39. Large extracellular vesicles carry most of the tumour DNA circulating in prostate cancer patient plasma.

Author

Vagner, Tatyana, Spinelli, Cristiana, Minciacchi, Valentina R., Balaj, Leonora, Zandian, Mandana, Conley, Andrew, Zijlstra, Andries, Freeman, Michael R., Demichelis, Francesca, De, Subhajyoti, Posadas, Edwin M., Tanaka, Hisashi, and Di Vizio, Dolores

Subjects

VESICLES (Cytology), CANCER cells, PROSTATE cancer patients, MEMBRANE proteins, DNA replication

Abstract

Cancer-derived extracellular vesicles (EVs) are membrane-enclosed structures of highly variable size. EVs contain a myriad of substances (proteins, lipid, RNA, DNA) that provide a reservoir of circulating molecules, thus offering a good source of biomarkers. We demonstrate here that large EVs (L-EV) (large oncosomes) isolated from prostate cancer (PCa) cells and patient plasma are an EV population that is enriched in chromosomal DNA, including large fragments up to 2 million base pair long. While L-EVs and small EVs (S-EV) (exosomes) isolated from the same cells contained similar amounts of protein, the DNA was more abundant in L-EVs, despite S-EVs being more numerous. Consistent with in vitro observations, the abundance of DNA in L-EV obtained from PCa patient plasma was variable but frequently high. Conversely, negligible amounts of DNA were present in the S-EVs from the same patients. Controlled experimental conditions, with spike-ins of L-EVs and S-EVs from cancer cells in human plasma from healthy subjects, showed that circulating DNA is almost exclusively enclosed in L-EVs. Whole genome sequencing revealed that the DNA in L-EVs reflects genetic aberrations of the cell of origin, including copy number variations of genes frequently altered in metastatic PCa (i.e. MYC, AKT1, PTK2, KLF10 and PTEN). These results demonstrate that L-EV-derived DNA reflects the genomic make-up of the tumour of origin. They also support the conclusion that L-EVs are the fraction of plasma EVs with DNA content that should be interrogated for tumour-derived genomic alterations. [ABSTRACT FROM AUTHOR]

Published

2018

40. MP90-13 CIRCULATING TUMOR CELLS-DERIVED PATIENT XENOGRAFTS: A NOVEL APPROACH TO STUDY PROSTATE CANCER LETHAL PROGRESSION.

Author

Chu, Gina C.Y., Wang, Ruoxiang, Zhau, Haiyen E., Posadas, Edwin M., and Chung, Leland W.K.

Published

2016

41. Tumor Cell Isolation: High-Purity Prostate Circulating Tumor Cell Isolation by a Polymer Nanofiber-Embedded Microchip for Whole Exome Sequencing (Adv. Mater. 21/2013).

Author

Zhao, Libo, Lu, Yi-Tsung, Li, Fuqiang, Wu, Kui, Hou, Shuang, Yu, Juehua, Shen, Qinglin, Wu, Dongxia, Song, Min, OuYang, Wei-Han, Luo, Zheng, Lee, Tom, Fang, Xiaohong, Shao, Chen, Xu, Xun, Garcia, Mitch A., Chung, Leland W. K., Rettig, Matthew, Tseng, Hsian-Rong, and Posadas, Edwin M.

Published

2013