Immunopet Fluorescence Imaging And Radioimmunotherapy Of Psca Positive Prostate Cancer PDF Download
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| Author | : Wen-Ting Tsai |
| Publisher | : |
| Total Pages | : 133 |
| Release | : 2018 |
| Genre | : |
| ISBN | : |
Download ImmunoPET/fluorescence Imaging and Radioimmunotherapy of PSCA-positive Prostate Cancer Book in PDF, ePub and Kindle
Prostate cancer diagnosis and treatment options need to be improved as over- and under-treatment, as well as disease recurrence and resistance to current therapies, continue to be challenges. Prostate stem cell antigen (PSCA) is overexpressed in the majority of prostate cancers and correlates with grade, stage, and metastatic potential. Antibodies, which are highly specific for their target, can be labeled with radionuclides and fluorophores for molecular imaging and therapy. This dissertation describes the use of humanized anti-PSCA antibody fragments for dual-modality immuno-positron emission tomography (immunoPET)/fluorescence imaging and for radioimmunotherapy of prostate cancer in preclinical models. Prostate cancer visualization could be improved by using immunoPET for preoperative non-invasive disease detection, and fluorescence imaging for intraoperative guidance of tumor resection; the power of both imaging modalities can be combined on a single agent. In this work, the dual-labeled humanized anti-PSCA A11 cys-minibody (A11 cMb) was evaluated for successive immunoPET/fluorescence imaging in subcutaneous and orthotopic prostate cancer models. A11 cMb was site-specifically conjugated with the near-infrared fluorophore Cy5.5 and radiolabeled with 124I or 89Zr. 124I- and 89Zr-A11 cMb-Cy5.5 were used to detect subcutaneous and intraprostatic PSCA-positive tumors. High contrast immunoPET/fluorescence imaging with 124I-A11 cMb-Cy5.5 identified both high PSCA-expression and moderate PSCA-expression subcutaneous tumors. 89Zr-A11 cMb-Cy5.5 immunoPET showed uptake in the prostate without interfering signal in the bladder, and ex vivo fluorescence imaging clearly showed signal in the tumor and not the surrounding seminal vesicles. These studies support the potential for dual-modality A11 cMb to be translated for preoperative whole-body disease detection and real-time surgical guidance in prostate cancer patients. Prostate cancer that metastasizes often becomes resistant to current therapies and eventually progresses, and alternative therapy options include radioimmunotherapy which delivers a high radiation dose to the tumor with the aim of minimizing dose to normal organs. Anti-PSCA antibody fragments radiolabeled with a cytotoxic radionuclide, such as the beta-emitter 131I or 177Lu, may be effective for radioimmunotherapy with lower toxicity compared to intact antibodies. 124I- and 89Zr-A11 minibody (A11 Mb) immunoPET was used to guide dosimetry studies, and 131I- and 177Lu-A11 Mb was administered to 22Rv1-PSCA s.c. tumor-bearing nude mice to complete dosimetry estimation. 131I-A11 Mb had a higher projected therapeutic index, or tumor-to-radiosensitive tissue dose, and was used in subsequent therapy studies. 131I-A11 Mb inhibited PSCA-positive tumor growth in a dose-dependent manner and extended survival with minimal off-target toxicity. Additionally, preliminary biodistribution studies in knock-in transgenic mice that express human-PSCA were similar to that of nude mice. Therefore, radioimmunotherapy will likely not be toxic to organs with normal PSCA expression (stomach, bladder), and A11 Mb may be suitable for human translation. The results of this work demonstrate the potential of anti-PSCA minibodies as theranostic agents for disease diagnosis, surgical guidance, and treatment. Additionally, the success of anti-PSCA dual-modality imaging and radioimmunotherapy in preclinical models support further evaluation in the clinic.
| Author | : |
| Publisher | : |
| Total Pages | : 12 |
| Release | : 2014 |
| Genre | : |
| ISBN | : |
Download Applications of ImmunoPET Book in PDF, ePub and Kindle
Here, prostate stem cell antigen (PSCA) is highly expressed in local prostate cancers and prostate cancer bone metastases and its expression correlates with androgen receptor activation and a poor prognosis. Here in this study, we investigate the potential clinical applications of immunoPET with the anti-PSCA A11 minibody, an antibody fragment optimized for use as an imaging agent. We compare A11 minibody immunoPET to 18F-Fluoride PET bone scans for detecting prostate cancer bone tumors and evaluate the ability of the A11 minibody to image tumor response to androgen deprivation. Osteoblastic, PSCA expressing, LAPC-9 intratibial xenografts were imaged with serial 124I-anti-PSCA A11 minibody immunoPET and 18F-Fluoride bone scans. Mice bearing LAPC-9 subcutaneous xenografts were treated with either vehicle or MDV-3100 and imaged with A11 minibody immunoPET/CT scans pre- and post-treatment. Ex vivo flow cytometry measured the change in PSCA expression in response to androgen deprivation. A11 minibody demonstrated improved sensitivity and specificity over 18F-Fluoride bone scans for detecting LAPC-9 intratibial xenografts at all time points. Finally, LAPC-9 subcutaneous xenografts showed downregulation of PSCA when treated with MDV-3100 which A11 minibody immunoPET was able to detect in vivo.
| Author | : Scott Matthew Knowles |
| Publisher | : |
| Total Pages | : 171 |
| Release | : 2013 |
| Genre | : |
| ISBN | : |
Download Anti-PSCA Minibody for ImmunoPET Imaging of Prostate Cancer in Preclinical Models Book in PDF, ePub and Kindle
Prostate stem cell antigen (PSCA) is a cell surface glycoprotein that has low levels of expression in normal prostate, bladder, and stomach, but is expressed in 83-100%, and overexpressed in 40-100%, of prostate cancers. PSCA expression has been shown to correlate with the Gleason score, seminal vesicle and capsular invasion, advanced clinical stage, androgen independence, MYC gene-amplification, and a poor prognosis. PSCA is also highly overexpressed in the majority of prostate cancer bone metastases (87- 100%) and many metastases to other sites (67% liver, 67-95% lymph node). ImmunoPET is a highly flexible imaging technique that can be utilized to image virtually any cell surface protein using radiolabeled antibodies or antibody fragments. This dissertation describes the use of a radiolabeled anti-PSCA A11 minibody (scFv-CH3 dimer, 80 kDa) for immunoPET imaging of PSCA expression in mouse models of prostate cancer and demonstrates the potential of the A11 minibody for highly specific imaging of local prostate cancer and metastases in the clinic. In this work, 124I and 89Zr-DFO radiolabeling of the anti-PSCA minibody are compared. Imaging with both radionuclides showed specific tumor targeting in 22rv1×PSCA and LAPC-9 tumors and achieved high contrast imaging in both tumor models. However, 124I-labeled A11 minibody achieved superior tumor:soft tissue contrast and was determined to have higher clinical potential. A quantitative method of & mu;PET imaging of both 124I and 89Zr radionuclides using recovery coefficient based partial volume correction was also established and validated. The PSCA promoter contains an androgen response element and expression of PSCA has been shown to be regulated by androgens in the mouse prostate and in human prostate cancer biopsy tissue. In the present work, treatment with the second generation anti-androgen MDV-3100 was demonstrated to cause downregulation of PSCA in LAPC-9 xenografts. In addition, 124I-labeled A11 minibody showed decreased uptake in LAPC-9 xenografts treated with MDV-3100 compared to vehicle controls suggesting a potential use for the A11 minibody in imaging response to androgen deprivation therapy. The highest percentage of prostate cancer metastases are osteoblastic bone metastases and most clinical staging of prostate cancer metastases utilizes 99mTc-MDP or 18F- Fluoride bone scans to image increases in bone turnover in response to these metastases. In this work we demonstrate that 124I-labeled A11 minibody has higher sensitivity and specificity for detecting LAPC-9 intratibial xenografts than 18F-Fluoride bone scans. The A11 minibody binds only to human PSCA (hPSCA) and does not cross-react with the murine homologue mPSCA. In order to address the background uptake caused by endoge- nous hPSCA expression, the creation of an hPSCA knock-in mouse and imaging using the A11 minibody in this model is described. We found a pattern of hPSCA expression in these mice similar to the pattern of normal expression in humans. Uptake of 124I-labeled A11 minibody correlated strongly with the expression of hPSCA, but demonstrated that the overall increase in background uptake of the A11 minibody due to endogenous expression of human PSCA is minimal. The results presented in this work demonstrate robust targeting of PSCA expression by the A11 minibody and clinical investigation of the A11 minibody for imaging local prostate cancer and prostate cancer metastases is warranted.
| Author | : Roland E. Kontermann |
| Publisher | : Springer Science & Business Media |
| Total Pages | : 381 |
| Release | : 2011-07-21 |
| Genre | : Medical |
| ISBN | : 3642209106 |
Download Bispecific Antibodies Book in PDF, ePub and Kindle
The concept of using bispecific antibodies for cancer therapy by retargeting immune effector cells was developed several years ago. Initial clinical studies were rather disappointing mainly due to low efficacy, severe side effects and the immunogenicity of the bispecific antibodies. The progress in antibody engineering finally led to the generation of new classes of bispecific antibodies lacking these obstacles. In addition, new applications were established, such as pre-targeting strategies in radioimmunotherapy and dual targeting approaches in order to improve binding, selectivity and efficacy. In this book, the different ways of generating bispecific antibodies are described, with emphasis on recombinant formats. The various applications of bispecific antibodies, e.g. in cellular cancer immunotherapy, radioimmunotherapy and pretargeting strategies are covered, and emerging applications such as dual targeting strategies, which involve the simultaneous inhibition of two targets, are addressed.
| Author | : Scott W. Burchiel |
| Publisher | : Elsevier Publishing Company |
| Total Pages | : 484 |
| Release | : 1983 |
| Genre | : Medical |
| ISBN | : |
Download Radioimmunoimaging and Radioimmunotherapy Book in PDF, ePub and Kindle
| Author | : Françoise Kraeber-Bodéré |
| Publisher | : |
| Total Pages | : 0 |
| Release | : 2020 |
| Genre | : |
| ISBN | : |
Download Nuclear Medicine in the Context of Personalized Medicine Book in PDF, ePub and Kindle
This eBook is a collection of articles from a Frontiers Research Topic. Frontiers Research Topics are very popular trademarks of the Frontiers Journals Series: they are collections of at least ten articles, all centered on a particular subject. With their unique mix of varied contributions from Original Research to Review Articles, Frontiers Research Topics unify the most influential researchers, the latest key findings and historical advances in a hot research area! Find out more on how to host your own Frontiers Research Topic or contribute to one as an author by contacting the Frontiers Editorial Office: frontiersin.org/about/contact.
| Author | : Tod W. Speer |
| Publisher | : Lippincott Williams & Wilkins |
| Total Pages | : 564 |
| Release | : 2012-03-28 |
| Genre | : Medical |
| ISBN | : 1451153260 |
Download Targeted Radionuclide Therapy Book in PDF, ePub and Kindle
Radioimmunotherapy, also known as systemic targeted radiation therapy, uses antibodies, antibody fragments, or compounds as carriers to guide radiation to the targets. It is a topic rapidly increasing in importance and success in treatment of cancer patients. This book represents a comprehensive amalgamation of the radiation physics, chemistry, radiobiology, tumor models, and clinical data for targeted radionuclide therapy. It outlines the current challenges and provides a glimpse at future directions. With significant advances in cell biology and molecular engineering, many targeting constructs are now available that will safely deliver these highly cytotoxic radionuclides in a targeted fashion. A companion website includes the full text and an image bank.
| Author | : Naveen Anand |
| Publisher | : Springer Nature |
| Total Pages | : 170 |
| Release | : 2021-04-15 |
| Genre | : Medical |
| ISBN | : 3030699404 |
Download Imaging Diagnostics in Pancreatic Cancer Book in PDF, ePub and Kindle
This book provides a comprehensive, state-of-the-art overview of imaging modalities used in the diagnosis, staging, and management of pancreatic cancer. In addition to profiling the most commonly-used imaging modalities for pancreatic cancer, the text reviews recent advances in endoscopic ultrasound, staging characteristics utilized in determining appropriate treatment options, and reviews the role of imaging in pancreatic cancer screening in specialized patient populations. The book also spotlights the use of radiation therapy for pancreatic cancer in patients who cannot have surgery, as well as when fiducial marker placement should be considered in targeting a malignancy. Written by experts in the field, Imaging Diagnostics in Pancreatic Cancer: A Clinical Guide is a valuable resource for gastroenterologists, surgeons, oncologists, radiologists, and other practitioners who manage patients with pancreatic cancer.
| Author | : Krishan Kumar |
| Publisher | : Mdpi AG |
| Total Pages | : 262 |
| Release | : 2021-12-06 |
| Genre | : |
| ISBN | : 9783036524276 |
Download Radiolabeled Compounds for Diagnosis and Treatment of Cancer Book in PDF, ePub and Kindle
Radiopharmaceuticals are used in the diagnosis and treatment of various diseases, especially cancer. In general, radiopharmaceuticals are either salts of radionuclides or radionuclides bound to biologically active molecules, drugs, or cells. Tremendous progress has been made in discovering, developing, and commercializing numerous radiopharmaceuticals for the imaging and therapy of cancer. Significant research is ongoing in academia and the pharmaceutical industry to develop more novel radiolabeled compounds as potential radiopharmaceuticals for unmet needs. This Special Issue aims to focus on all aspects of the design, characterization, evaluation, and development of novel radiolabeled compounds for the diagnosis and treatment of cancer and the application of new radiochemistry and methodologies for the development of novel radiolabeled compounds. Outstanding contributions presented in this Special Issue will significantly add to the field of radiopharmaceuticals.
| Author | : Mariana Spetea |
| Publisher | : MDPI |
| Total Pages | : 358 |
| Release | : 2020-12-18 |
| Genre | : Medical |
| ISBN | : 3036500464 |
Download Opioids and Their Receptors Book in PDF, ePub and Kindle
The interest in opioids such as morphine, the prototypical opioid ligand, has been maintained through the years. The identification of endogenous opioids and their receptors (mu, delta, kappa, and nociceptin), molecular cloning, and the elucidation of the crystal structures of opioid receptors represent key milestones in opioid research. The opioid system modulates numerous pharmacological responses, with therapeutic (i.e., analgesia) and detrimental side effects (i.e., addiction). The medical use and misuse of opioids have dramatically increased, leading to the 21st century opioid crisis. This book presents recent developments in opioid drug discovery, specifically in the medicinal chemistry and pharmacology of new ligands targeting the opioid receptors as effective and safe therapeutics for human diseases. Furthermore, it draws a special attention to advancing concepts and strategies in opioid drug discovery to mitigate opioid liabilities. The diversity among the discussed topics is a testimony to the complexity of the opioid system, which results from the expression, regulation, and functional role of ligands and receptors. The array of multidisciplinary research areas illustrates the rapidly developing basic research and translational activities in opioid drug discovery. This book will serve as a useful reference while also stimulating continued research in the chemistry and pharmacology of opioids and their receptors, with the prospect of developing improved therapies for human diseases, but also improving health and quality of life in general.
