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51. Levels of murine, but not human, CXCL13 are greatly elevated in NOD-SCID mice bearing the AIDS-associated Burkitt lymphoma cell line, 2F7.

Author

Widney, Daniel P, Olafsen, Tove, Wu, Anna M, Kitchen, Christina MR, Said, Jonathan W, Smith, Jeffrey B, Peña, Guadalupe, Magpantay, Larry I, Penichet, Manuel L, and Martinez-Maza, Otoniel

Subjects
Tumor Cells, Cultured, Animals, Mice, Inbred NOD, Humans, Mice, Mice, SCID, HIV-1, Burkitt Lymphoma, Lymphoma, AIDS-Related, Ascites, Immunoenzyme Techniques, Flow Cytometry, Female, Chemokine CXCL13, Tumor Cells, Cultured, Inbred NOD, SCID, Lymphoma, AIDS-Related, General Science & Technology
Abstract

Currently, few rodent models of AIDS-associated non-Hodgkin's lymphoma (AIDS-NHL) exist. In these studies, a novel mouse/human xenograft model of AIDS-associated Burkitt lymphoma (AIDS-BL) was created by injecting cells of the human AIDS-BL cell line, 2F7, intraperitoneally into NOD-SCID mice. Mice developed tumors in the peritoneal cavity, with metastases to the spleen, thymus, and mesenteric lymph nodes. Expression of the chemokine receptor, CXCR5, was greatly elevated in vivo on BL tumor cells in this model, as shown by flow cytometry. CXCL13 is the ligand for CXCR5, and serum and ascites levels of murine, but not human, CXCL13 showed a striking elevation in tumor-bearing mice, with levels as high as 200,000 pg/ml in ascites, as measured by ELISA. As shown by immunohistochemistry, murine CXCL13 was associated with macrophage-like tumor-infiltrating cells that appeared to be histiocytes. Blocking CXCR5 on 2F7 cells with neutralizing antibodies prior to injection into the mice substantially delayed tumor formation. The marked elevations in tumor cell CXCR5 expression and in murine CXCL13 levels seen in the model may potentially identify an important link between tumor-interacting histiocytes and tumor cells in AIDS-BL. These results also identify CXCL13 as a potential biomarker for this disease, which is consistent with previous studies showing that serum levels of CXCL13 were elevated in human subjects who developed AIDS-lymphoma. This mouse model may be useful for future studies on the interactions of the innate immune system and AIDS-BL tumor cells, as well as for the assessment of potential tumor biomarkers for this disease.

Published
2013

52. Enhanced Growth Inhibition of Osteosarcoma by Cytotoxic Polymerized Liposomal Nanoparticles Targeting the Alcam Cell Surface Receptor

Author

Federman, Noah, Chan, Jason, Nagy, Jon O, Landaw, Elliot M, McCabe, Katelyn, Wu, Anna M, Triche, Timothy, Kang, HyungGyoo, Liu, Bin, Marks, James D, and Denny, Christopher T

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Rare Diseases, Pediatric Cancer, Orphan Drug, Bioengineering, Cancer, Nanotechnology, Pediatric, 5.1 Pharmaceuticals, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Dentistry, Oncology and carcinogenesis
Abstract

Osteosarcoma is the most common primary malignancy of bone in children, adolescents, and adults. Despite extensive surgery and adjuvant aggressive high-dose systemic chemotherapy with potentially severe bystander side effects, cure is attainable in about 70% of patients with localized disease and only 20%-30% of those patients with metastatic disease. Targeted therapies clearly are warranted in improving our treatment of this adolescent killer. However, a lack of osteosarcoma-associated/specific markers has hindered development of targeted therapeutics. We describe a novel osteosarcoma-associated cell surface antigen, ALCAM. We, then, create an engineered anti-ALCAM-hybrid polymerized liposomal nanoparticle immunoconjugate (α-AL-HPLN) to specifically target osteosarcoma cells and deliver a cytotoxic chemotherapeutic agent, doxorubicin. We have demonstrated that α-AL-HPLNs have significantly enhanced cytotoxicity over untargeted HPLNs and over a conventional liposomal doxorubicin formulation. In this way, α-AL-HPLNs are a promising new strategy to specifically deliver cytotoxic agents in osteosarcoma.

Published
2012

53. Targeting CEA in Pancreas Cancer Xenografts with a Mutated scFv-Fc Antibody Fragment

Author

Girgis, Mark D, Olafsen, Tove, Kenanova, Vania, McCabe, Katelyn E, Wu, Anna M, and Tomlinson, James S

Subjects
Biomedical Imaging, Cancer, Pancreatic Cancer, Biotechnology, Rare Diseases, Digestive Diseases, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, imaging, pancreas cancer, CEA, antibody, Medical Biochemistry and Metabolomics, Clinical Sciences, Oncology and Carcinogenesis
Abstract

BackgroundSensitive antibody-based tumor targeting has the potential not only to image metastatic and micrometastatic disease, but also to be the basis of targeted therapy. The vast majority of pancreas cancers express carcinoembryonic antigen (CEA). Thus, we sought to evaluate the potential of CEA as a pancreatic cancer target utilizing a rapidly clearing engineered anti-CEA scFv-Fc antibody fragment with a mutation in the Fc region [anti-CEA scFv-Fc H310A].MethodsImmunohistochemistry (IHC) with the antibody fragment was used to confirm expression of CEA on human pancreas cancer specimens. In vivo tumor targeting was evaluated by tail vein injection of I124-labeled anti-CEA scFv-Fc(H310A) into mice harboring CEA-positive and -negative xenografts. MicroPET/CT imaging was performed at successive time intervals. Radioactivity in blood and tumor was measured after the last time point. Additionally, unlabeled anti-CEA scFv-Fc(H310A) was injected into CEA-positive tumor bearing mice and ex vivo IHC was performed to identify the presence of the antibody to define the microscopic intratumoral pattern of targeting.ResultsModerate to strong staining by IHC was noted on 84% of our human pancreatic cancer specimens and was comparable to staining of our xenografts. Pancreas xenograft imaging with the radiolabeled anti-CEA scFv-Fc(H310A) antibody demonstrated average tumor/blood ratios of 4.0. Immunolocalization demonstrated peripheral antibody fragment penetration of one to five cell diameters (0.75 to 1.5 μm).ConclusionsWe characterized a preclinical xenograft model with respect to CEA expression that was comparable to human cases. We demonstrated that the anti-CEA scFv-Fc(H310A) antibody exhibited antigen-specific tumor targeting and shows promise as an imaging and potentially therapeutic agent.

Published
2011

54. CA19‐9 as a Potential Target for Radiolabeled Antibody‐Based Positron Emission Tomography of Pancreas Cancer

Author

Girgis, Mark D, Olafsen, Tove, Kenanova, Vania, McCabe, Katelyn E, Wu, Anna M, and Tomlinson, James S

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Biomedical Imaging, Rare Diseases, Digestive Diseases, Biotechnology, Cancer
Abstract

Introduction. Sensitive and specific imaging of pancreas cancer are necessary for accurate diagnosis, staging, and treatment. The vast majority of pancreas cancers express the carbohydrate tumor antigen CA19-9. The goal of this study was to determine the potential to target CA19-9 with a radiolabeled anti-CA19-9 antibody for imaging pancreas cancer. Methods. CA19-9 was quantified using flow cytometry on human pancreas cancer cell lines. An intact murine anti-CA19-9 monoclonal antibody was labeled with a positron emitting radionuclide (Iodine-124) and injected into mice harboring antigen positive and negative xenografts. MicroPET/CT were performed at successive time intervals (72 hours, 96 hours, 120 hours) after injection. Radioactivity was measured in blood and tumor to provide objective confirmation of the images. Results. Antigen expression by flow cytometry revealed approximately 1.3 × 10(6) CA19-9 antigens for the positive cell line and no expression in the negative cell line. Pancreas xenograft imaging with Iodine-124-labeled anti-CA19-9 mAb demonstrated an average tumor to blood ratio of 5 and positive to negative tumor ratio of 20. Conclusion. We show in vivo targeting of our antigen positive xenograft with a radiolabeled anti-CA19-9 antibody. These data demonstrate the potential to achieve anti-CA19-9 antibody based positron emission tomography of pancreas cancer.

Published
2011

55. Evaluation of Two Internalizing Carcinoembryonic Antigen Reporter Genes for Molecular Imaging

Author

Barat, Bhaswati, Kenanova, Vania E, Olafsen, Tove, and Wu, Anna M

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biotechnology, Cancer, Genetics, Biomedical Imaging, Animals, Carcinoembryonic Antigen, Endocytosis, Female, Flow Cytometry, Genes, Reporter, Humans, Immunoglobulin Fragments, Immunohistochemistry, Jurkat Cells, Mice, Mice, Nude, Molecular Imaging, Positron-Emission Tomography, Recombinant Proteins, Transfection, Xenograft Model Antitumor Assays, Antibody fragment, CEA reporter gene, Internalization, Jurkat, PET, Physiology, Clinical Sciences, Nuclear Medicine & Medical Imaging, Clinical sciences
Abstract

PurposeThe objective of this article is to develop internalizing positron emission tomography (PET) reporter genes for tracking genetically modified T cells in vivo.ProceduresThe transmembrane and cytoplasmic domains of the human transferrin receptor (TfR) and CD5 were each fused to the carcinoembryonic (CEA) minigene N-A3 and expressed in Jurkat T cells. Internalization was evaluated by confocal microscopy or by intracellular uptake of ¹²⁵I-labeled anti-CEA scFv-Fc. Reporter gene-transfected Jurkat xenografts in mice were analyzed by immunohistochemistry (IHC) and imaged by PET using ¹²⁴I- or ⁶⁴Cu-scFv-Fc as tracers.ResultsSurface expression of TR(1-99)-NA3 was lower than that of NA3-CD5. Both reporter genes were internalized following binding of the anti-CEA antibody fragment. IHC of tumors showed strong staining of NA3-CD5, whereas TR(1-99)-NA3 stained weakly. Specific targeting of TR(1-99)-NA3 or NA3-CD5 was shown by PET in xenografted mice.ConclusionsThe in vivo imaging studies suggest a potential application of the internalizing form of CEA (N-A3) as a PET reporter gene.

Published
2011

56. An affinity matured minibody for PET imaging of prostate stem cell antigen (PSCA)-expressing tumors

Author

Lepin, Eric J, Leyton, Jeffrey V, Zhou, Yu, Olafsen, Tove, Salazar, Felix B, McCabe, Katelyn E, Hahm, Scott, Marks, James D, Reiter, Robert E, and Wu, Anna M

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Urologic Diseases, Biomedical Imaging, Prostate Cancer, Biotechnology, Amino Acid Sequence, Animals, Antibody Affinity, Antigens, Neoplasm, Cell Line, Tumor, GPI-Linked Proteins, Gene Expression Regulation, Neoplastic, Humans, Immunoglobulin Fragments, Male, Mice, Molecular Sequence Data, Mutation, Neoplasm Proteins, Positron-Emission Tomography, Prostatic Neoplasms, Radioactive Tracers, Imaging, Prostate, PSCA, Antibody, PET, Other Physical Sciences, Clinical Sciences, Nuclear Medicine & Medical Imaging, Clinical sciences
Abstract

PurposeProstate stem cell antigen (PSCA), a cell surface glycoprotein expressed in normal human prostate and bladder, is over-expressed in the majority of localized prostate cancer and most bone metastases. We have previously shown that the hu1G8 minibody, a humanized anti-PSCA antibody fragment (single-chain Fv-C(H)3 dimer, 80 kDa), can localize specifically and image PSCA-expressing xenografts at 21 h post-injection. However, the humanization and antibody fragment reformatting decreased its apparent affinity. Here, we sought to evaluate PET imaging contrast with affinity matured minibodies.MethodsYeast scFv display, involving four rounds of selection, was used to generate the three affinity matured antibody fragments (A2, A11, and C5) that were reformatted into minibodies. These three affinity matured anti-PSCA minibodies were characterized in vitro, and following radiolabeling with (124)I were evaluated in vivo for microPET imaging of PSCA-expressing tumors.ResultsThe A2, A11, and C5 minibody variants all demonstrated improved affinity compared to the parental (P) minibody and were ranked as follows: A2 > A11 > C5 > P. The (124)I-labeled A11 minibody demonstrated higher immunoreactivity than the parental minibody and also achieved the best microPET imaging contrast in two xenograft models, LAPC-9 (prostate cancer) and Capan-1 (pancreatic cancer), when evaluated in vivo.ConclusionOf the affinity variant minibodies tested, the A11 minibody that ranked second in affinity was selected as the best immunoPET tracer to image PSCA-expressing xenografts. This candidate is currently under development for evaluation in a pilot clinical imaging study.

Published
2010

57. Characterization of an engineered human purine nucleoside phosphorylase fused to an anti-her2/neu single chain Fv for use in ADEPT

Author

Afshar, Sepideh, Olafsen, Tove, Wu, Anna M, and Morrison, Sherie L

Abstract

Abstract Background Antibody Directed Enzyme Prodrug Therapy (ADEPT) can be used to generate cytotoxic agents at the tumor site. To date non-human enzymes have mainly been utilized in ADEPT. However, these non-human enzymes are immunogenic limiting the number of times that ADEPT can be administered. To overcome the problem of immunogenicity, a fully human enzyme, capable of converting a non-toxic prodrug to cytotoxic drug was developed and joined to a human tumor specific scFv yielding a fully human targeting agent. Methods A double mutant of human purine nucleoside phosphorylase (hDM) was developed which unlike the human enzyme can cleave adenosine-based prodrugs. For tumor-specific targeting, hDM was fused to the human anti-HER2/neu single chain Fv (scFv), C6 MH3B1. Enzymatic activity of hDM with its natural substrates and prodrugs was determined using spectrophotomeric approaches. A cell proliferation assay was used to assess the cytotoxicity generated following conversion of prodrug to drug as a result of enzymatic activity of hDM. Affinity of the targeting scFv, C6 MH3B1 fused to hDM to Her2/neu was confirmed using affinity chromatography, surface plasmon resonance, and flow-cytometry. Results In vitro hDM-C6 MH3B1 binds specifically to HER2/neu expressing tumor cells and localizes hDM to tumor cells, where the enzymatic activity of hDM-C6 MH3B1, but not the wild type enzyme, results in phosphorolysis of the prodrug, 2-fluoro-2'-deoxyadenosine to the cytotoxic drug 2-fluoroadenine (F-Ade) causing inhibition of tumor cell proliferation. Significantly, the toxic small drug diffuses through the cell membrane of HER2/neu expressing cells as well as cells that lack the expression of HER2/neu, causing a bystander effect. F-Ade is toxic to cells irrespective of their growth rate; therefore, both the slowly dividing tumor cells and the non-dividing neighboring stromal cells that support tumor growth should be killed. Analysis of potential novel MHCII binding peptides resulting from fusion of hDM to C6 MH3B1 and the two mutations in hDM, and of the structure of hDM compared to the wild-type enzyme suggests that hDM-C6 MH3B1 should exhibit minimal immunogenicity in humans. Conclusion hDM-C6 MH3B1 constitutes a novel human based protein that addresses some of the limitations of ADEPT that currently preclude its successful use in the clinic.

Published
2009

60. Covalent disulfide‐linked anti‐CEA diabody allows site‐specific conjugation and radiolabeling for tumor targeting applications

Author

Olafsen, Tove, Cheung, Chia‐wei, Yazaki, Paul J., Li, Lin, Sundaresan, Gobalakrishnan, Gambhir, Sanjiv S., Sherman, Mark A., Williams, Lawrence E., Shively, John E., Raubitschek, Andrew A., and Wu, Anna M.

Abstract

An engineered anti-carcinoembryonic antigen (CEA) diabody (scFv dimer, 55 kDa) was previously constructed from the murine anti-CEA T84.66 antibody. Tumor targeting, imaging and biodistribution studies in nude mice bearing LS174T xenografts with radiolabeled anti-CEA diabody demonstrated rapid tumor uptake and fast blood clearance, which are favorable properties for an imaging agent. Current radiolabeling approaches result in random modification of the protein surface, which may impair immunoreactivity especially for smaller antibody fragments. Site-specific conjugation approaches can direct modifications to reactive groups located away from the binding site. Here, cysteine residues were introduced into the anti-CEA diabody at three different locations, to provide specific thiol groups for chemical modification. One version (with a C-terminal Gly-Gly-Cys) existed exclusively as a disulfide-bonded dimer. This cysteine-modified diabody (Cys-diabody) retained high binding to CEA and demonstrated tumor targeting and biodistribution properties identical to the non-covalent diabody. Furthermore, following reduction of the disulfide bond, the Cys-diabody could be chemically modified using a thiol-specific bifunctional chelating agent, for radiometal labeling. Thus, the Cys-diabody provides a covalently linked alternative to conventional diabodies, which can be reduced and modified site-specifically. This format will provide a versatile platform for targeting a variety of agents to CEA-positive tumors.

Published
2004

66. Development of 18F-Labeled hydrophilic trans-cyclooctene as a bioorthogonal tool for PET probe construction.

Author

Xu, Muyun, Ma, Xinrui, Pigga, Jessica E., Zhang, He, Wang, Shuli, Zhao, Weiling, Deng, Huaifu, Wu, Anna M., Liu, Rihe, Wu, Zhanhong, Fox, Joseph M., and Li, Zibo

Abstract

We report the development of a hydrophilic 18F-labeled a-TCO derivative [18F]3 (log P = 0.28) through a readily available precursor and a single-step radiofluorination reaction (RCY up to 52%). We demonstrated that [18F]3 can be used to construct not only multiple small molecule/peptide-based PET agents, but protein/diabody-based imaging probes in parallel. [ABSTRACT FROM AUTHOR]

Published
2023
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73. Supplementary Figures from Near-Infrared Dye-Labeled Anti-Prostate Stem Cell Antigen Minibody Enables Real-Time Fluorescence Imaging and Targeted Surgery in Translational Mouse Models

Author

Zhang, Mo, primary, Kobayashi, Naoko, primary, Zettlitz, Kirstin A., primary, Kono, Evelyn A., primary, Yamashiro, Joyce M., primary, Tsai, Wen-Ting K., primary, Jiang, Ziyue K., primary, Tran, Chau P., primary, Wang, Chung, primary, Guan, Johnny, primary, Wu, Anna M., primary, and Reiter, Robert E., primary

Published
2023
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74. Supplemental Figures from Fluorescent Image–Guided Surgery with an Anti-Prostate Stem Cell Antigen (PSCA) Diabody Enables Targeted Resection of Mouse Prostate Cancer Xenografts in Real Time

Author

Sonn, Geoffrey A., primary, Behesnilian, Andrew S., primary, Jiang, Ziyue Karen, primary, Zettlitz, Kirstin A., primary, Lepin, Eric J., primary, Bentolila, Laurent A., primary, Knowles, Scott M., primary, Lawrence, Daniel, primary, Wu, Anna M., primary, and Reiter, Robert E., primary

Published
2023
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75. Supplementary Video S2 from Near-Infrared Dye-Labeled Anti-Prostate Stem Cell Antigen Minibody Enables Real-Time Fluorescence Imaging and Targeted Surgery in Translational Mouse Models

Author

Zhang, Mo, primary, Kobayashi, Naoko, primary, Zettlitz, Kirstin A., primary, Kono, Evelyn A., primary, Yamashiro, Joyce M., primary, Tsai, Wen-Ting K., primary, Jiang, Ziyue K., primary, Tran, Chau P., primary, Wang, Chung, primary, Guan, Johnny, primary, Wu, Anna M., primary, and Reiter, Robert E., primary

Published
2023
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77. Supporting Information from Optimizing Radiolabeled Engineered Anti-p185HER2 Antibody Fragments for In vivo Imaging

Author

Olafsen, Tove, primary, Kenanova, Vania E., primary, Sundaresan, Gobalakrishnan, primary, Anderson, Anne-Line, primary, Crow, Desiree, primary, Yazaki, Paul J., primary, Li, Lin, primary, Press, Michael F., primary, Gambhir, Sanjiv S., primary, Williams, Lawrence E., primary, Wong, Jeffrey Y.C., primary, Raubitschek, Andrew A., primary, Shively, John E., primary, and Wu, Anna M., primary

Published
2023
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81. Harnessing imaging tools to guide immunotherapy trials: summary from the National Cancer Institute Cancer Imaging Steering Committee workshop

Author

Shankar, Lalitha K, primary, Schöder, Heiko, additional, Sharon, Elad, additional, Wolchok, Jedd, additional, Knopp, Michael V, additional, Wahl, Richard L, additional, Ellingson, Benjamin M, additional, Hall, Nathan C, additional, Yaffe, Martin J, additional, Towbin, Alexander J, additional, Farwell, Michael D, additional, Pryma, Daniel, additional, Poussaint, Tina Young, additional, Wright, Chadwick L, additional, Schwartz, Lawrence, additional, Harisinghani, Mukesh, additional, Mahmood, Umar, additional, Wu, Anna M, additional, Leung, David, additional, de Vries, Elisabeth G E, additional, Tang, Ying, additional, Beach, Gillian, additional, and Reeves, Steven A, additional

Published
2023
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82. First-In-Human Pilot PET Immunoimaging Study of 64Cu-Anti-Carcinoembryonic Antigen Monoclonal Antibody (hT84.66-M5A) in Patients with Carcinoembryonic Antigen-Producing Cancers

Author

Wong, Jeffrey Y.C., primary, Yamauchi, David M., additional, Adhikarla, Vikram, additional, Simpson, Jennifer, additional, Frankel, Paul H., additional, Fong, Yuman, additional, Melstrom, Kurt A., additional, Chen, Yi-jen, additional, Salehian, Behrooz D., additional, Woo, Yanghee, additional, Dandapani, Savita V., additional, Colcher, David M., additional, Poku, Erasmus K., additional, Yazaki, Paul J., additional, Wu, Anna M., additional, and Shively, John E., additional

Published
2023
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96. Abstract 5372: CD3 and CD8 targeting of ionizable lipid nanoparticles for in vivo mRNA delivery to T cells

Author

Robinson, Elise R., primary, Kare, Aris J., additional, Kheirolomoom, Azadeh, additional, Inayathullah, Mohammed, additional, Tumbale, Spencer K., additional, Wu, Bo, additional, Raie, Marina N., additional, Seo, Jai W., additional, Salazar, Felix B., additional, Paulmurugan, Ramasamy, additional, Wu, Anna M., additional, and Ferrara, Katherine W., additional

Published
2022
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97. Biodistribution of Intra-Arterial and Intravenous Delivery of Human Umbilical Cord Mesenchymal Stem Cell-Derived Extracellular Vesicles in a Rat Model to Guide Delivery Strategies for Diabetes Therapies

Author

Li, Junfeng, primary, Komatsu, Hirotake, additional, Poku, Erasmus K., additional, Olafsen, Tove, additional, Huang, Kelly X., additional, Huang, Lina A., additional, Chea, Junie, additional, Bowles, Nicole, additional, Chang, Betty, additional, Rawson, Jeffrey, additional, Peng, Jiangling, additional, Wu, Anna M., additional, Shively, John E., additional, and Kandeel, Fouad R., additional

Published
2022
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