Your search keyword '"MONOCLONAL antibody probes"' showing total 981 results

101. Antitumour activity of the glycoengineered type II anti- CD20 antibody obinutuzumab ( GA101) in combination with the MDM2-selective antagonist idasanutlin ( RG7388).

Author

Herting, Frank, Herter, Sylvia, Friess, Thomas, Muth, Gunther, Bacac, Marina, Sulcova, Jitka, Umana, Pablo, Dangl, Markus, and Klein, Christian

Subjects

*CD20 antigen, *MONOCLONAL antibody probes, *APOPTOSIS, *CELL death, *XENOGRAFTS

Abstract

Objectives To investigate whether the glycoengineered type II anti- CD20 monoclonal antibody obinutuzumab ( GA101) combined with the selective MDM2 antagonist idasanutlin ( RG7388) offers superior efficacy to monotherapy in treating B-lymphoid malignancies in preclinical models. Methods The combined effect of obinutuzumab or rituximab plus idasanutlin on direct cell death/apoptosis induction and antibody-dependent cellular cytotoxicity ( ADCC) was evaluated using p53 wild-type Z-138 and Do HH-2 lymphoma cells. Furthermore, whole blood B-cell depletion was analysed, and tumour growth inhibition was evaluated in subcutaneous xenograft models. Results Idasanutlin induced concentration-dependent death of Z-138 and Do HH-2 cells. At concentrations >10-100 n m, idasanutlin enhanced obinutuzumab-induced death of Do HH-2 and Z-138 cells without negatively impacting obinutuzumab-mediated ADCC, natural killer cell activation or whole blood B-cell depletion. In the Z-138 xenograft model, a suboptimal dose of obinutuzumab with idasanutlin yielded substantial tumour growth inhibition and prolonged survival in a time-to-event analysis. In the Do HH-2 model, idasanutlin plus obinutuzumab showed superior tumour growth inhibition to idasanutlin plus rituximab. Conclusions Obinutuzumab plus idasanutlin enhanced cell death of p53 wild-type tumour cells vs. rituximab plus idasanutlin without affecting obinutuzumab-mediated ADCC or B-cell depletion and showed robust antitumour efficacy in xenograft models, strongly supporting the investigation of this combination in clinical trials. [ABSTRACT FROM AUTHOR]

Published

2016

102. Electrochemical immunosensor based on gold nanoparticles deposited on a conductive polymer to determine estrone in water samples.

Author

Monerris, Melisa Jimena, D´Eramo, Fabiana, Arévalo, Fernando Javier, Fernández, Héctor, Zon, María Alicia, and Molina, Patricia Gabriela

Subjects

*ESTRONE, *ELECTROCHEMICAL sensors, *GOLD nanoparticles, *CONDUCTING polymers, *MONOCLONAL antibody probes, *WATER sampling, *SQUARE waves, *VOLTAMMETRY

Abstract

This paper describes the development of a simple and sensitive electrochemical immunosensor (EI) to quantify estrone (E) in water samples. This EI does not require the sample pre-treatment, to label neither the antigen nor the antibody, and its detection format is based on the fact that E is co-substrate of the horse radish peroxidase (HRP). Therefore, the EI was constructed by immobilization of the anti-E monoclonal antibody (mAbE) on a glassy carbon electrode (GCE) modified with gold nanoparticles (AuNPs) electro-synthesized on a 1-naphtylamine polymer (pNap) film. This format reduced significantly the time of EI preparation. Water samples were spiked with known E concentrations, and then incubated on mAbE-AuNPs-pNap-GCE disk electrode. The electrochemical response was proportional to the amount of pyrocatechol (H 2 Q), another enzyme co-substrate, and inversely proportional to the amount of E presents in water samples. The immunosensor showed a linear range from 8 × 10 − 2 to 2 × 10 4 pg mL − 1 . The limit of detection (LOD) was 0.061 pg mL − 1 . Recovery percentages obtained were very good, with values of 98.20, 105.50, and 100.85% for 50, 100 and 200 pg mL − 1 , respectively. Tests were also conducted to evaluate the cross-reactive of E with other hormones of similar structure such as 17β-estradiol, progesterone and estriol. The EI showed a high selectivity to determine E in the presence of these hormones. Thus, this EI is an attractive tool to determine E in water samples. [ABSTRACT FROM AUTHOR]

Published

2016

103. Romosozumab Treatment in Postmenopausal Women with Osteoporosis.

Author

Cosman, Felicia, Crittenden, Daria B., Adachi, Jonathan D., Binkley, Neil, Czerwinski, Edward, Ferrari, Serge, Hofbauer, Lorenz C., Lau, Edith, Lewiecki, E. Michael, Miyauchi, Akimitsu, Zerbini, Cristiano A. F., Milmont, Cassandra E., Li Chen, Maddox, Judy, Meisner, Paul D., Libanati, Cesar, Grauer, Andreas, and Chen, Li

Subjects

*SCLEROSTIN, *BONE morphogenetic proteins, *BONE resorption, *MONOCLONAL antibody probes, *PLACEBOS, *THERAPEUTIC use of monoclonal antibodies, *BONE fracture prevention, *BONE remodeling, *SUBCUTANEOUS injections, *COMPARATIVE studies, *BONE fractures, *DIPHOSPHONATES, *RESEARCH methodology, *MEDICAL cooperation, *MONOCLONAL antibodies, *OSTEOPOROSIS, *RESEARCH, *STATISTICAL sampling, *EVALUATION research, *SPINAL injuries, *BONE density, *RANDOMIZED controlled trials, *BLIND experiment, *PREVENTION

Abstract

Background: Romosozumab, a monoclonal antibody that binds sclerostin, increases bone formation and decreases bone resorption.Methods: We enrolled 7180 postmenopausal women who had a T score of -2.5 to -3.5 at the total hip or femoral neck. Patients were randomly assigned to receive subcutaneous injections of romosozumab (at a dose of 210 mg) or placebo monthly for 12 months; thereafter, patients in each group received denosumab for 12 months, at a dose of 60 mg, administered subcutaneously every 6 months. The coprimary end points were the cumulative incidences of new vertebral fractures at 12 months and 24 months. Secondary end points included clinical (a composite of nonvertebral and symptomatic vertebral) and nonvertebral fractures.Results: At 12 months, new vertebral fractures had occurred in 16 of 3321 patients (0.5%) in the romosozumab group, as compared with 59 of 3322 (1.8%) in the placebo group (representing a 73% lower risk with romosozumab; P<0.001). Clinical fractures had occurred in 58 of 3589 patients (1.6%) in the romosozumab group, as compared with 90 of 3591 (2.5%) in the placebo group (a 36% lower risk with romosozumab; P=0.008). Nonvertebral fractures had occurred in 56 of 3589 patients (1.6%) in the romosozumab group and in 75 of 3591 (2.1%) in the placebo group (P=0.10). At 24 months, the rates of vertebral fractures were significantly lower in the romosozumab group than in the placebo group after each group made the transition to denosumab (0.6% [21 of 3325 patients] in the romosozumab group vs. 2.5% [84 of 3327] in the placebo group, a 75% lower risk with romosozumab; P<0.001). Adverse events, including instances of hyperostosis, cardiovascular events, osteoarthritis, and cancer, appeared to be balanced between the groups. One atypical femoral fracture and two cases of osteonecrosis of the jaw were observed in the romosozumab group.Conclusions: In postmenopausal women with osteoporosis, romosozumab was associated with a lower risk of vertebral fracture than placebo at 12 months and, after the transition to denosumab, at 24 months. The lower risk of clinical fracture that was seen with romosozumab was evident at 1 year. (Funded by Amgen and UCB Pharma; FRAME ClinicalTrials.gov number, NCT01575834 .). [ABSTRACT FROM AUTHOR]

Published

2016

104. Combined integrated protocol/basket trial design for a first-in-human trial.

Author

Derhaschnig, Ulla, Gilbert, Jim, Jäger, Ulrich, Böhmig, Georg, Stingl, Georg, and Jilma, Bernd

Subjects

*DRUG development, *TREATMENT of rare diseases, *ONCOLOGIC surgery, *MONOCLONAL antibody probes, *HEMOLYTIC anemia

Abstract

Background: Innovative trial designs are sought to streamline drug development in rare diseases. Basket- and integrated protocol designs are two of these new strategies and have been applied in a handful oncologic trials. We have taken the concept outside the realm of oncology and report about a first-in-human integrated protocol design that facilitates the transition from phase Ia in healthy volunteers to phase Ib in patients with rare complement-mediated disorders driven by the classical pathway. Results: We have been conducting a prospective, double-blind, randomized, placebo-controlled first-in-human study with TNT009, which is a humanized monoclonal antibody directed against the C1s subunit of human complement component C1. The trial consisted of three subparts, including normal healthy volunteers (part one and two) and a single cohort of patients in part three. Patients suffered from various complement-mediated diseases sharing the same pathophysiological mechanism, i.e. bullous pemphigoid, antibody-mediated rejection of organ transplants, cold agglutinin disease and warm autoimmune hemolytic anemia. Primary objective of the trial has been to evaluate the safety and tolerability of TNT009 in humans. Conclusions: This trial provides probably the first example that basket trials may not be limited to single genetic aberrations, which is overly restrictive, but our trial design demonstrates that pathway specificity is a viable paradigm for defining baskets. This will hopefully serve as a role model that could benefit other innovative drug development programs targeting rare diseases. [ABSTRACT FROM AUTHOR]

Published

2016

105. Patterns of practice with third-line anti-EGFR antibody for metastatic colorectal cancer.

Author

Ho, M. Y., Renouf, D. J., Cheung, W. Y., Lim, H. J., Speers, C. H., Zhou, C., and Kennecke, H. F.

Subjects

*EPIDERMAL growth factor receptors, *MONOCLONAL antibody probes, *COLON cancer, *PEPTIDE receptors, *PROTEIN-tyrosine kinases

Abstract

Background Therapy with anti-epidermal growth factor receptor (EGFR) monoclonal antibody improves outcomes for patients with metastatic colorectal cancer (mCRC) in the first-, second-, and third-line trial settings. In British Columbia, the use of EGFR inhibitors (EGFRis) is confined to third-line therapy, which might lower the proportion of patients who receive this therapy. The objective of the present study was to describe EGFRi treatment patterns when those agents are limited to the third-line setting. The results will inform decisions about optimal use of EGFRi agents, including earlier in the course of therapy for metastatic disease. Methods All patients with newly diagnosed mCRC who were referred to BC Cancer Agency clinics in 2009 were included in the study. Prognostic and treatment information was prospectively collected; KRAS test results were determined by chart review. Results The study included 443 patients with a median age of 66 years. For the 321 patients who received systemic therapy, median survival was 22.3 months. Of the 117 patients who were treated with 5-fluorouracil, oxaliplatin, and irinotecan, and who were potentially eligible for EGFRi therapy, 90% (105 patients) were tested for KRAS status. Of the 60 patients with KRAS wild-type tumours, 82% (49 patients) received EGFRi therapy. Conclusions When EGFRi therapy is limited to the third-line setting, only a small proportion of patients receive such therapy, with death and poor performance status preventing its use in the rest. Availability of EGFRi in earlier lines of therapy could increase the proportion of patients treated with all active systemic agents. [ABSTRACT FROM AUTHOR]

Published

2016

106. Refractory IgD Multiple Myeloma Treated with Daratumumab: A Case Report and Literature Review.

Author

Husnain, Muhammad, Kurtin, Sandra, Barkett, Nikki, bin Riaz, Irbaz, and Agarwal, Amit

Subjects

*IMMUNOGLOBULIN D, *MULTIPLE myeloma treatment, *IMMUNOLOGICAL adjuvants, *CANCER chemotherapy, *MONOCLONAL antibody probes

Abstract

Patients with relapsed and refractory multiple myeloma have poor prognosis. A recent analysis of patients with relapsed and refractory multiple myeloma who were refractory to both proteasome inhibitors and immunomodulatory drugs showed the median overall survival of 9 months only. Daratumumab is the first-in-class human monoclonal antibody against CD38 cells which was studied in phase I/II trials for treatment of these patients with relapsed refractory multiple myeloma. It showed an overall response rate of 36% and a median overall survival (OS) of 17 months in these patients. We report a case of 40-year-old man with immunoglobulin D (IgD) multiple myeloma whose disease was refractory to at least 5 different chemotherapy regimens including proteasome inhibitors and immunomodulatory drugs. The clinical studies assessing daratumumab did not include any patients with IgD myeloma which is a rare form of multiple myeloma and to our knowledge is the first study reporting use of daratumumab in IgD myeloma. [ABSTRACT FROM AUTHOR]

Published

2016

107. Self-paired monoclonal antibody lateral flow immunoassay strip for rapid detection of Acidovorax avenae subsp. citrulli.

Author

Zeng, Haijuan, Guo, Wenbo, Liang, Beibei, Li, Jianwu, Zhai, Xuzhao, Song, Chunmei, Zhao, Wenjun, Fan, Enguo, and Liu, Qing

Subjects

*MONOCLONAL antibody probes, *COLLOIDAL gold, *IMMUNOASSAY, *POLYMERASE chain reaction, *GRAM-negative bacteria

Abstract

We screened a highly specific monoclonal antibody (McAb), named 6D, against Acidovorax avenae subsp. citrulli (Aac). Single McAb 6D was used as both nanogold-labeled antibody and test antibody to develop a single self-paired colloidal gold immunochromatographic test strip (Sa-GICS). The detection limit achieved using the Sa-GICS approach was 10 CFU/mL, with a result that can be observed by the naked eye within 10 min. Moreover, Sa-GICS can detect eight strains of Aac and display no cross-reactions with other pathogenic plant microorganisms. Artificial contamination experiments demonstrated that Sa-GICS would not be affected by impurities in the leaves or stems of the plants and were consistent with the PCR results. This is the first report on the development of a colloidal gold immunoassay strip with self-paired single McAb for the rapid detection of Aac. [ABSTRACT FROM AUTHOR]

Published

2016

108. Rapid evaluation of artesunate quality with a specific monoclonal antibody-based lateral flow dipstick.

Author

Guo, Suqin, Zhang, Wei, He, Lishan, Tan, Guiyu, Min, Myo, Kyaw, Myat, Wang, Baomin, and Cui, Liwang

Subjects

*PLASMODIUM falciparum, *MONOCLONAL antibody probes, *CARBOXYL group, *CARRIER proteins, *IMMUNOGENETICS, *HIGH performance liquid chromatography, *THERAPEUTICS

Abstract

Artesunate is a frontline antimalarial drug for treating Plasmodium falciparum malaria. To produce specific antibodies to artesunate, the carboxyl group of artesunate was directly conjugated to carrier protein as the immunogen. A specific monoclonal antibody (mAb) 3D2G against artesunate was obtained by high-throughput screening of positive hybridoma clones. This monoclonal antibody had 4.0, 0.5, and 0.9 % cross reactivities with artemisinin, dihydroartemisinin, and artemether, respectively. A dipstick immunoassay was developed, and the indicator range for artesunate was 1000-2000 ng mL. No interference was observed with artemisinin, dihydroartemisinin, artemether, and other commonly used antimalarial drugs for up to 20,000 ng mL. The dipsticks were used for determination of artesunate contents in commercial drugs, and the results were agreeable with those determined by high-performance liquid chromatography. This dipstick, with its specificity and sensitivity for artesunate and simplicity to use, makes it a potential point-of-care device for rapid quality evaluation of artesunate-containing antimalarial drugs. [ABSTRACT FROM AUTHOR]

Published

2016

109. A sensitive immunochromatographic assay using colloidal gold–antibody probe for rapid detection of fumonisin B 1 in corn.

Author

Wang, Xi-Chun, Fan, Hai-Xin, Fan, Meng-Xue, Li, Fu-Hui, Feng, Shi-Bin, Li, Jin-Chun, Wu, Jin-Jie, Li, Yu, and Wang, Jia-Sheng

Subjects

*COLLOIDAL gold, *COLLOIDS, *IMMUNOGOLD labeling, *MONOCLONAL antibody probes, *FUMONISINS

Abstract

A sensitive immunochromatographic assay (ICA) using a colloidal gold–antibody probe for the rapid detection of fumonisin B1 (FB1) in corn samples was developed. The colour density of the test line correlated with the concentration of FB1 in the range 2–40 ng ml–1 by the assay, and the detection limit for FB1 was 2 ng ml–1. The linear range for FB1 was 50–1000 µg kg–1, and the visual limit detection of the test was 1000 µg kg–1 in corn samples. The ICA to detect FB1 is sensitive, specific and rapid. Specific anti-FB1 monoclonal antibody (mAb) and FB1-ovalbumin (FB1-OVA) conjugate antigen were prepared. FB1 mAb, labelled with colloidal gold, was used as the probe on the immunochromatographic strip. FB1-OVA and goat-anti-mouse IgG were coated onto a nitrocellulose (NC) membrane as test lines and control lines, respectively. FB1 in samples will competitively combines the FB1 mAb with the FB1-OVA in an NC membrane and the results are directly observed by the colour of the detection and quality control lines. The concentrations of FB1 mAb labelled with colloidal gold, detecting antigen and goat anti-mouse IgG, were optimised. The results indicate that the test strip is specific for FB1, with no cross-reactivity to other toxins. The strip assay for FB1 was simple, only needing one step without complicated assay performance and expensive equipment, and the total time for visual evaluation was less than 10 min. A survey of 24 corn samples from Hefei, China, was performed with the test strip and HPLC, and the detection results showed that the developed ICA and the HPLC were in excellent agreement. Hence, the developed ICA can be used as a method for rapid detection of FB1 in corn samples. [ABSTRACT FROM AUTHOR]

Published

2016

110. Depletion of Neutrophils Exacerbates the Early Inflammatory Immune Response in Lungs of Mice Infected with Paracoccidioides brasiliensis.

Author

Pino-Tamayo, Paula Andrea, Puerta-Arias, Juan David, Lopera, Damaris, Urán-Jiménez, Martha Eugenia, and González, Ángel

Subjects

*NEUTROPHILS, *INFLAMMATION, *IMMUNE response, *LUNGS, *PARACOCCIDIOIDES brasiliensis, *MONOCLONAL antibody probes, *PARACOCCIDIOIDOMYCOSIS, *CHEMOKINES

Abstract

Neutrophils predominate during the acute phase of the Paracoccidioides brasiliensis infection. Herein, we determined the role of the neutrophil during the early stages of experimental pulmonary paracoccidioidomycosis using a monoclonal antibody (mAb) specific for neutrophils. Male BALB/c mice were inoculated intranasally with 1.5×106 or 2×106 P. brasiliensis yeast cells. The mAb was administered 24 h before infection, followed by doses every 48 h until mice were sacrificed. Survival time was evaluated and mice were sacrificed at 48 h and 96 h after inoculation to assess cellularity, fungal load, cytokine/chemokine levels, and histopathological analysis. Neutrophils from mAb-treated mice were efficiently depleted (99.04%). Eighty percent of the mice treated with the mAb and infected with 1.5×106 yeast cells died during the first two weeks after infection. When mice were treated and infected with 2×106 yeast cells, 100% of them succumbed by the first week after infection. During the acute inflammatory response significant increases in numbers of eosinophils, fungal load and levels of proinflammatory cytokines/chemokines were observed in the mAb-treated mice. We also confirmed that neutrophils are an important source of IFN-γ and IL-17. These results indicate that neutrophils are essential for protection as well as being important for regulating the early inflammatory immune response in experimental pulmonary paracoccidioidomycosis. [ABSTRACT FROM AUTHOR]

Published

2016

111. Selective capture of most celiac immunogenic peptides from hydrolyzed gluten proteins.

Author

Moreno, María de Lourdes, Muñoz-Suano, Alba, López-Casado, Miguel Ángel, Torres, María Isabel, Sousa, Carolina, and Cebolla, Ángel

Subjects

*GLUTEN, *PEPTIDES, *CELIAC disease, *MONOCLONAL antibody probes, *T cells

Abstract

The available immunomethods for gluten quantitation could underestimate or overestimate the net immunoactivity of foods and beverages if the chosen analytical antibody is not specific to the relevant gluten immunogenic peptides (GIP). Accurate detection of the most active GIP is desirable to assess the potential celiac toxicity of food. We evaluated the capacity of the G12 monoclonal antibody for selectively depleting GIP in samples from two different gluteomes. Samples of hydrolyzed gliadin from wheat and a barley beer were used. The input (starting peptide digest of prolamins), the flow-through (unbound peptides), and the output (captured peptides) were analyzed by G12 and R5 competitive ELISA as well as by stimulation assays of T-cells from celiac patients. Most of the GIP were retained by the G12-agarose and represented the largest part of the immunogenicity of the gluten peptidome. G12 immunodepletion experiments with hydrolyzed gluten showed that this antibody reacted with those with the highest immunoactivity for celiac patients. [ABSTRACT FROM AUTHOR]

Published

2016

112. Cigarette smoke-induced chronic obstructive pulmonary disease is attenuated by CCL20-blocker: a rat model.

Author

Desheng Sun, Yao Ouyang, Yanhui Gu, and Xiansheng Liu

Subjects

*DENDRITIC cells, *OBSTRUCTIVE lung diseases, *MONOCLONAL antibody probes, *BRONCHOALVEOLAR lavage, *IMMUNOHISTOCHEMISTRY

Abstract

Aim To evaluate whether the effect of dendritic cells (DCs) on chronic obstructive pulmonary disease (COPD) can be relieved by blocking CCL20. Methods 30 Wistar rats were randomly divided into three groups: control, COPD, and COPD treated with CCL20 monoclonal antibody. In the latter two groups, COPD was induced by four-week cigarette smoke exposure and trachea injection of lipopolysaccharide solution on two occasions. CCL20 monoclonal antibody was injected intraperitoneally on the first day. All animals were sacrificed on the 29th day. Pathomorphology of the lung and bronchiole was analyzed using hematoxylin and eosin staining. The CCR6 content in the bronchoalveolar lavage fluid was detected using ELISA. DC distribution in the lung was examined by immunohistochemistry for OX62. Results COPD rat models showed pathological alterations similar to those in COPD patients. DCs, CCR6, and the severity of emphysema were significantly increased in the COPD group than in controls (all P values <0.001), and they were significantly reduced after anti-CCL20 treatment compared with the COPD group (all P values <0.05). Conclusion The interaction between CCR6 and its ligand CCL20 promotes the effect of DCs in the COPD pathogenesis, which can be reduced by blocking CCL20. [ABSTRACT FROM AUTHOR]

Published

2016

113. Is an in vitro whole blood cytokine assay useful to detect the potential risk of severe infusion reaction of monoclonal antibody pharmaceuticals?

Author

Yoshika Iwata, Asako Harada, Toshiko Hara, Chiyomi Kubo, Tomoaki Inoue, Mitsuyasu Tabo, Ploix, Corinne, Manigold, Tobias, Hinton, Heather, and Mishima, Masayuki

Subjects

*IN vitro studies, *THERAPEUTIC use of cytokines, *INFUSION therapy, *MONOCLONAL antibody probes, *PHARMACEUTICAL technology, *BLOOD cells

Abstract

After the life-threatening cytokine release syndrome (CRS) occurred in the clinical study of the anti-CD28 monoclonal antibody (mAb) TGN1412, in vitro cytokine release assays using human blood cells have been proposed for non-clinical evaluation of the potential risk of CRS. Two basic assay formats are frequently used: human peripheral blood mononuclear cells (PBMC) with immobilized mAbs, and whole blood with aqueous mAbs. However, the suitability of the whole blood cytokine assay (WBCA) has been questioned, because an unrealistically large sample size would be required to detect the potential risk of CRS induced by TGN1412, which has low sensitivity. We performed a WBCA using peripheral blood obtained from 68 healthy volunteers to compare two high risk mAbs, the TGN1412 analogue anti-CD28 superagonistic mAb (CD28SA) and the FcγR-mediated alemutuzumab, with a low risk mAb, panitumumab. Based on the cytokine measurements in this study, the sample size required to detect a statistically significant increase in cytokines with 90% power and 5% significance was determined to be n = 9 for CD28SA and n = 5 for alemtuzumab. The most sensitive marker was IL-8. The results suggest that WBCA is a practical test design that can warn of the potential risk of FcγR-mediated alemtuzumab and T-cell activating CD28SA but, because there was apparently a lower response to CD28SA, it cannot be used as a risk-ranking tool. WBCA is suggested to be a helpful tool for identifying potential FcγRmediated hazards, but further mechanistic understanding of the response to CD28SA is necessary before applying it to T cell-stimulating mAbs. [ABSTRACT FROM AUTHOR]

Published

2016

114. Characterization of epitopes on the rabies virus glycoprotein by selection and analysis of escape mutants.

Author

Fallahi, Firouzeh, Wandeler, Alexander I., and Nadin-Davis, Susan A.

Subjects

*EPITOPES, *RABIES virus, *GLYCOPROTEINS, *MUTANT proteins, *MONOCLONAL antibody probes

Abstract

The glycoprotein (G) is the only surface protein of the lyssavirus particle and the only viral product known to be capable of eliciting the production of neutralizing antibodies. In this study, the isolation of escape mutants resistant to monoclonal antibody (Mab) neutralization was attempted by a selection strategy employing four distinct rabies virus strains: the extensively passaged Evelyn Rokitnicki Abelseth (ERA) strain and three field isolates representing two bat-associated variants and the Western Canada skunk variant (WSKV). No escape mutants were generated from either of the bat-associated viral variants but two neutralization mutants were derived from the WSKV isolate. Seven independent ERA mutants were recovered using Mabs directed against antigenic sites I (four mutants) and IIIa (three mutants) of the glycoprotein. The cross-neutralization patterns of these viral mutants were used to determine the precise location and nature of the G protein epitopes recognized by these Mabs. Nucleotide sequencing of the G gene indicated that those mutants derived using Mabs directed to antigenic site (AS) III all contained amino acid substitutions in this site. However, of the four mutants selected with AS I Mabs, two bore mutations within AS I as expected while the remaining two carried mutations in AS II. WSKV mutants exhibited mutations at the sites appropriate for the Mabs used in their selection. All ERA mutant preparations were more cytopathogenic than the parental virus when propagated in cell culture; when in vivo pathogenicity in mice was examined, three of these mutants exhibited reduced pathogenicity while the remaining four mutants exhibited comparable pathogenic properties to those of the parent virus. [ABSTRACT FROM AUTHOR]

Published

2016

115. Rapid lateral-flow immunoassay for the quantum dot-based detection of puerarin.

Author

Qu, Huihua, Zhang, Yue, Qu, Baoping, Kong, Hui, Qin, Gaofeng, Liu, Shuchen, Cheng, Jinjun, Wang, Qingguo, and Zhao, Yan

Subjects

*QUANTUM dots, *IMMUNOASSAY, *MONOCLONAL antibody probes, *BIOCONJUGATES, *NITROCELLULOSE, *SERUM albumin

Abstract

In this study, a rapid (within 10 min) quantitative lateral-flow immunoassay using a quantum dots (QDs)-antibody probe was developed for the analysis of puerarin (PUE) in water and biological samples. The competitive immunoassay was based on anti-PUE monoclonal antibody conjugated with QDs (detection reagent). Secondary antibody was immobilized on one end of a nitrocellulose membrane (control line) and PUE-bovine serum albumin conjugate was immobilized on the other end (test line). In the quantitative experiment, the detection results were scanned using a membrane strip reader and a detection curve (regression equation: y=−0.11 ln(x)+0.979, R 2 =0.9816) representing the averages of the scanned data was obtained. This curve was linear from 1 to 10 μg/mL. The IC 50 value was 75.58 ng/mL and the qualitative detection limit of PUE was 5.8 ng/mL. The recovery of PUE added to phosphate-buffered saline and biological samples was in the range of 97.38–116.56%. To our knowledge, this is the first report of the quantitative detection of a natural product by QDs-based immunochromatography, which represents a powerful tool for rapidly screening PUE in plant materials and other biological samples. [ABSTRACT FROM AUTHOR]

Published

2016

116. Determination of Bisphenol A by a Gold Nanoflower Enhanced Enzyme-Linked Immunosorbent Assay.

Author

Peng, Chifang, Pan, Na, Xie, Zhengjun, Liu, Liqiang, Xiang, Jie, and Liu, Chunli

Subjects

*NANOSTRUCTURED materials, *ENZYME-linked immunosorbent assay, *MONOCLONAL antibody probes, *GOLD nanoparticles, *HORSERADISH peroxidase, *BISPHENOL A, *IMMUNOGOLD labeling

Abstract

The use of nanomaterials to improve the sensitivity of enzyme-linked immunosorbent assays (ELISA) for small molecules allows wider application of this method. In this work, gold nanoflowers were synthesized by a seed-mediated procedure and used to prepare a horseradish peroxidase-immunoglobulin G-gold nanoflower complex. The complex was used as the signal amplification probe in a novel ELISA for bisphenol A. The gold nanoflower-enhanced ELISA demonstrated excellent detection sensitivity of 0.05 ng/mL, which was 20 times more sensitive than a standard ELISA procedure. A linear dynamic range from 0.1 to 5.0 ng/mL was obtained by this approach. The gold nanoflower-enhanced ELISA was used to determine bisphenol A in lake water, with recoveries from 92.0 to 102.0% in samples fortified at concentrations of 0.5, 1.0, and 3.0 ng/mL. The gold nanoflower-enhanced ELISA was shown to offer good sensitivity, simplicity, and low cost. [ABSTRACT FROM AUTHOR]

Published

2016

117. Specific localization of nesprin-1-α2, the short isoform of nesprin-1 with a KASH domain, in developing, fetal and regenerating muscle, using a new monoclonal antibody.

Author

Holt, Ian, Nguyen Thuy Duong, Qiuping Zhang, Le Thanh Lam, Sewry, Caroline A., Mamchaoui, Kamel, Shanahan, Catherine M., and Morris, Glenn E.

Subjects

*NUCLEAR membranes, *MONOCLONAL antibody probes, *CARDIOMYOPATHIES, *MUSCULAR dystrophy, *PATHOGENIC bacteria, *CALCIUM-binding proteins

Abstract

Background: Nesprin-1-giant (1008kD) is a protein of the outer nuclear membrane that links nuclei to the actin cytoskeleton via amino-terminal calponin homology domains. The short nesprin-1 isoform, nesprin-1-α2, is present only in skeletal and cardiac muscle and several pathogenic mutations occur within it, but the functions of this short isoform without calponin homology domains are unclear. The aim of this study was to determine mRNA levels and protein localization of nesprin-1-α2 at different stages of muscle development in order to shed light on its functions. Results: mRNA levels of all known nesprin-1 isoforms with a KASH domain were determined by quantitative PCR. The mRNA for the 111 kD muscle-specific short isoform, nesprin-1-α2, was not detected in pre-differentiation human myoblasts but was present at significant levels in multinucleate myotubes. We developed a monoclonal antibody against the unique amino-terminal sequence of nesprin-1-α2, enabling specific immunolocalization for the first time. Nesprin-1-α2 protein was undetectable in pre-differentiation myoblasts but appeared at the nuclear rim in post-mitotic, multinucleate myotubes and reached its highest levels in fetal muscle. In muscle from a Duchenne muscular dystrophy biopsy, nesprin-1-α2 protein was detected mainly in regenerating fibres expressing neonatal myosin. Nesprin-1-giant was present at all developmental stages, but was also highest in fetal and regenerating fibres. In fetal muscle, both isoforms were present in the cytoplasm, as well as at the nuclear rim. A pathogenic early stop codon (E7854X) in nesprin-1 caused reduced mRNA levels and loss of protein levels of both nesprin-1-giant and (unexpectedly) nesprin-1-a2, but did not affect myogenesis in vitro. Conclusions: Nesprin-1-α2 mRNA and protein expression is switched on during myogenesis, alongside other known markers of muscle differentiation. The results show that nesprin-1-α2 is dynamically controlled and may be involved in some process occurring during early myofibre formation, such as re-positioning of nuclei. [ABSTRACT FROM AUTHOR]

Published

2016

118. Molecular Bases for Combinatorial Treatment Strategies in Patients with KRAS Mutant Lung Adenocarcinoma and Squamous Cell Lung Carcinoma.

Author

Lazzari, Chiara, Verlicchi, Alberto, Gkountakos, Anastasios, Pilotto, Sara, Santarpia, Mariacarmela, Chaib, Imane, Ramirez Serrano, Jose, Viteri, Santiago, Morales-Espinosa, Daniela, Dazzi, Claudio, Marinis, Filippo, Cao, Peng, Karachaliou, Niki, and Rosell, Rafael

Subjects

*LUNG cancer, *PATIENTS, *ADENOCARCINOMA, *SQUAMOUS cell carcinoma, *PHENOTYPES, *MONOCLONAL antibody probes

Abstract

Innovative therapeutic agents have significantly improved outcomes, with an acceptable safety profile, in a substantial proportion of non-small cell lung cancer (NSCLC) patients in whom the malignant phenotype of the disease is determined by oncogenic molecular alterations. However, the benefit seen with these treatment models has not translated well to NSCLCs with KRAS mutations or squamous cell histology. Although efforts have been made to develop precision medicine approaches, KRAS mutant NSCLC and lung squamous cell carcinoma (LSCC) continue to display resistance to therapy. Recently, based on the results of the Phase III SQUIRE trial, the EGFR monoclonal antibody necitumumab received FDA authorization in combination with cisplatin and gemcitabine for first line treatment of patients with metastatic LSCC. Among the molecular compounds tested in KRAS mutant NSCLC patients, the MEK inhibitor, selumentinib, combined with docetaxel in second line setting, determined a progression-free survival improvement, but no overall survival advantage. Better understanding is needed in regard to signaling pathways which cooperate to induce oncogene transformation in LSCC and KRAS mutant NSCLC and could determine intrinsic or acquired resistance to necitumumab and selumetinib. Greater understanding of such pathways will provide a molecular base upon which to improve the scant clinical benefit with these compounds. [ABSTRACT FROM AUTHOR]

Published

2016

119. Gold nanoparticles based lateral flow immunoassay with largely amplified sensitivity for rapid melamine screening.

Author

Zhong, Youhao, Chen, Yinji, Yao, Li, Zhao, Diping, Zheng, Lei, Liu, Guodong, Ye, Yingwang, and Chen, Wei

Subjects

*GOLD nanoparticles, *IMMUNOASSAY, *MICROBIAL sensitivity tests, *MELAMINE, *NITROCELLULOSE, *FOOD safety, *MONOCLONAL antibody probes, *MILK analysis

Abstract

The sensitivity of current lateral flow strip (LFS) based assays is a technical bottleneck. The authors describe a method for signal amplification to give a 10- to 25-fold improvement of the detection limit without compromising the assay time and operational mode. The assays includes the following steps: (a) immobilization of melamine antibody on gold nanoparticles (AuNPs); (b) immobilization of BSA antibody on other AuNPs; (c) coating a nitrocellulose (NC) membrane with coating antigen and secondary antibody against the melamine antibody as the test line and control line, respectively; (d) introducing an enhancement pad for signal amplification by immuno-recognition of the blocking protein on the first conjugation pad by the antibody on the enhancement pad. This results in dual labeling of AuNPs on the test line and enhances the optical intensity of test line at the same time of detection. The signal amplification makes the optical intensity change of the test line distinguishable even at low concentrations. The assay has a detection limit of 1.4 ppb (at an S/N ratio of 3). It was applied to the determination of melamine in milk, and the results obtained with this LFS are in good agreement with those obtained with instrumental methods. This demonstrates the practical applicability of the amplified LFS to real food samples. In our perception, this approach has a wide scope because it paves the way to the systematic amplification of the sensitivity of lateral flow strips. [Figure not available: see fulltext.] [ABSTRACT FROM AUTHOR]

Published

2016

120. Evaluating the Role of the Air-Solution Interface on the Mechanism of Subvisible Particle Formation Caused by Mechanical Agitation for an IgG1 mAb.

Author

Ghazvini, Saba, Kalonia, Cavan, Volkin, David B., and Dhar, Prajnaparamita

Subjects

*MONOCLONAL antibody probes, *IMMUNOGLOBULINS, *INTERFACIAL stresses, *ATOMIC force microscopy, *ATMOSPHERIC temperature

Abstract

Mechanical agitation of monoclonal antibody (mAb) solutions often leads to protein particle formation. In this study, various formulations of an immunoglobulin G (IgG) 1 mAb were subjected to different controlled interfacial stresses using a Langmuir trough, and protein particles formed at the interface and measured in bulk solution were characterized using atomic force microscopy and flow digital imaging. Results were compared to mAb solutions agitated in glass vials and unstressed controls. At lower pH, mAb solutions exhibited larger hysteresis in their surface pressure versus area isotherms and increased number of particles in bulk solution, when subjected to interfacial stresses. mAb samples subjected to 750-1000 interfacial compression-expansion cycles in 6 h contained high particle numbers in bulk solution, and displayed similar particulation trends when agitated in vials. At compression rates of 50 cycles in 6 h, however, particle levels in mAb solutions were comparable to unstressed controls, despite protein aggregates being present at the air-solution interface. These results suggest that while the air-solution interface serves as a nucleation site for initiating protein aggregation, the number of protein particles measured in bulk mAb solutions depends on the total number of compression cycles that proteins at the air-solution interface are subjected to within a fixed time. [ABSTRACT FROM AUTHOR]

Published

2016

121. Production and characterization of domain-specific monoclonal antibodies against human ECM1.

Author

Li, Ya, Li, Yanqing, Zhao, Junli, Wang, Dongyang, Mao, Qinwen, and Xia, Haibin

Subjects

*MONOCLONAL antibodies, *EXTRACELLULAR matrix proteins, *IMMUNOGLOBULINS, *LIGANDS (Biochemistry), *MONOCLONAL antibody probes

Abstract

Human extracellular matrix protein-1 (hECM1), a secreted glycoprotein, is widely expressed in different tissues and organs. ECM1 has been implicated in multiple biological functions, which are potentially mediated by the interaction of different ECM1 domains with its ligands. However, the exact biological functions of ECM1 have not been elucidated yet, and the functional study of ECM1 has been partially hampered by the lack of sensitive and specific antibodies, especially those targeting different ECM1 domains. In this study, six strains of monoclonal antibody (MAb) against hECM1 were generated using purified, prokaryotically-expressed hECM1 as an immunogen. The MAbs were shown to be highly sensitive and specific, and suitable for western blot, immunoprecipitation assays and immunohistochemistry. Furthermore, the particular ECM1 domains recognized by different MAbs were identified. Lastly, the MAbs were found to have neutralizing activities, inhibiting the proliferation, migration and metastasis of MDA-MB-231 cells. In conclusion, the domain-specific anti-ECM1 MAbs produced in this study should provide a useful tool for investigating ECM1's biological functions, and cellular pathways in which it is involved. [ABSTRACT FROM AUTHOR]

Published

2016

122. Monoclonal IgA Antibodies for Aflatoxin Immunoassays.

Author

Ertekin, Özlem, Pirinçci, Şerife Şeyda, and Öztürk, Selma

Subjects

*AFLATOXINS, *IMMUNOGLOBULIN A, *ENZYME-linked immunosorbent assay, *IMMUNOAFFINITY chromatography, *MONOCLONAL antibody probes

Abstract

Antibody based techniques are widely used for the detection of aflatoxins which are potent toxins with a high rate of occurrence in many crops. We developed a murine monoclonal antibody of immunoglobulin A (IgA) isotype with a strong binding affinity to aflatoxin B1 (AFB1), aflatoxin B2 (AFB2), aflatoxin G1 (AFG1), aflatoxin G2 (AFG2) and aflatoxin M1 (AFM1). The antibody was effectively used in immunoaffinity column (IAC) and ELISA kit development. The performance of the IACs was compatible with AOAC performance standards for affinity columns (Test Method: AOAC 991.31). The total binding capacity of the IACs containing our antibody was 111 ng, 70 ng, 114 ng and 73 ng for AFB1, AFB2, and AFG1 andAFG2, respectively. Furthermore, the recovery rates of 5 ng of each AF derivative loaded to the IACs were determined as 104.9%, 82.4%, 85.5% and 70.7% for AFB1, AFB2, AFG1 and AFG2, respectively. As for the ELISA kit developed using non-oriented, purified IgA antibody, we observed a detection range of 2–50 µg/L with 40 min total test time. The monoclonal antibody developed in this research is hitherto the first presentation of quadruple antigen binding IgA monoclonal antibodies in mycotoxin analysis and also the first study of their utilization in ELISA and IACs. IgA antibodies are valuable alternatives for immunoassay development, in terms of both sensitivity and ease of preparation, since they do not require any orientation effort. [ABSTRACT FROM AUTHOR]

Published

2016

123. Molecularly targeted therapy for the treatment of head and neck cancer: a review of the erbB family inhibitors.

Author

Sacco, Assuntina G. and Worden, Francis P.

Subjects

*HEAD & neck cancer patients, *EPIDERMAL growth factor receptors, *CANCER chemotherapy, *MONOCLONAL antibody probes, *PROTEIN-tyrosine kinases, *CETUXIMAB, *THERAPEUTICS

Abstract

The majority of patients with head and neck squamous cell carcinoma (HNSCC) present with locally advanced disease, which requires site-specific combinations of surgery, radiation, and chemotherapy. Despite aggressive therapy, survival outcomes remain poor, and treatment-related morbidity is not negligible. For patients with recurrent or metastatic disease, therapeutic options are further limited and prognosis is dismal. With this in mind, molecularly targeted therapy provides a promising approach to optimizing treatment efficacy while minimizing associated toxicity. The ErbB family of receptors (ie, epidermal growth factor receptor [EGFR], ErbB2/human epidermal growth factor receptor [HER]-2, ErbB3/HER3, and ErbB4/HER4) is known to contribute to oncogenic processes, such as cellular proliferation and survival. EGFR, specifically, is upregulated in more than 90% of HNSCC, has been implicated in radiation resistance, and correlates with poorer clinical outcomes. The central role of EGFR in the pathogenesis of HNSCC suggests that inhibition of this pathway represents an attractive treatment strategy. As a result, EGFR inhibition has been extensively studied, with the emergence of two classes of drug therapy: monoclonal antibodies and tyrosine kinase inhibitors. While the monoclonal antibody cetuximab is currently the only US Food and Drug Administration-approved EGFR inhibitor for the treatment of HNSCC, numerous investigational drugs are being evaluated in clinical trials. This paper will review the role of the ErbB family in the pathogenesis of HNSCC, as well as the evidence-based data for the use of ErbB family inhibition in clinical practice. [ABSTRACT FROM AUTHOR]

Published

2016

124. Improving gastric cancer preclinical studies using diverse in vitro and in vivo model systems.

Author

Hae Ryung Chang, Hee Seo Park, Young Zoo Ahn, Seungyoon Nam, Hae Rim Jung, Sungjin Park, Sang Jin Lee, Curt Balch, Garth Powis, Ja-Lok Ku, Yon Hui Kim, Chang, Hae Ryung, Park, Hee Seo, Ahn, Young Zoo, Nam, Seungyoon, Jung, Hae Rim, Park, Sungjin, Lee, Sang Jin, Balch, Curt, and Powis, Garth

Subjects

*MONOCLONAL antibodies, *GASTRIC diseases, *MONOCLONAL antibody probes, *MOLECULAR probes, *BREAST cancer, *CANCER cells, *ANIMAL experimentation, *ANTINEOPLASTIC agents, *BIOLOGICAL models, *CELL lines, *CELL receptors, *CELLULAR signal transduction, *DRUG therapy, *DRUG design, *CLINICAL drug trials, *GENE amplification, *GENES, *MICE, *MOLECULAR structure, *STOMACH tumors, *TUMOR classification, *GENE expression profiling, *PHARMACODYNAMICS

Abstract

Background: "Biomarker-driven targeted therapy," the practice of tailoring patients' treatment to the expression/activity levels of disease-specific genes/proteins, remains challenging. For example, while the anti-ERBB2 monoclonal antibody, trastuzumab, was first developed using well-characterized, diverse in vitro breast cancer models (and is now a standard adjuvant therapy for ERBB2-positive breast cancer patients), trastuzumab approval for ERBB2-positive gastric cancer was largely based on preclinical studies of a single cell line, NCI-N87. Ensuing clinical trials revealed only modest patient efficacy, and many ERBB2-positive gastric cancer (GC) patients failed to respond at all (i.e., were inherently recalcitrant), or succumbed to acquired resistance.Method: To assess mechanisms underlying GC insensitivity to ERBB2 therapies, we established a diverse panel of GC cells, differing in ERBB2 expression levels, for comprehensive in vitro and in vivo characterization. For higher throughput assays of ERBB2 DNA and protein levels, we compared the concordance of various laboratory quantification methods, including those of in vitro and in vivo genetic anomalies (FISH and SISH) and xenograft protein expression (Western blot vs. IHC), of both cell and xenograft (tissue-sectioned) microarrays.Results: The biomarker assessment methods strongly agreed, as did correlation between RNA and protein expression. However, although ERBB2 genomic anomalies showed good in vitro vs. in vivo correlation, we observed striking differences in protein expression between cultured cells and mouse xenografts (even within the same GC cell type). Via our unique pathway analysis, we delineated a signaling network, in addition to specific pathways/biological processes, emanating from the ERBB2 signaling cascade, as a potential useful target of clinical treatment. Integrated analysis of public data from gastric tumors revealed frequent (10 - 20 %) amplification of the genes NFKBIE, PTK2, and PIK3CA, each of which resides in an ERBB2-derived subpathway network.Conclusion: Our comprehensive bioinformatics analyses of highly heterogeneous cancer cells, combined with tumor "omics" profiles, can optimally characterize the expression patterns and activity of specific tumor biomarkers. Subsequent in vitro and in vivo validation, of specific disease biomarkers (using multiple methodologies), can improve prediction of patient stratification according to drug response or nonresponse. [ABSTRACT FROM AUTHOR]

Published

2016

125. High treatment efficacy by dual targeting of Burkitt's lymphoma xenografted mice with a Lu-based CD22-specific radioimmunoconjugate and rituximab.

Author

Weber, Tobias, Bötticher, Benedikt, Mier, Walter, Sauter, Max, Krämer, Susanne, Leotta, Karin, Keller, Armin, Schlegelmilch, Anne, Grosse-Hovest, Ludger, Jäger, Dirk, Haberkorn, Uwe, Arndt, Michaela, and Krauss, Jürgen

Subjects

*LYMPHOMA treatment, *MONOCLONAL antibody probes, *LABORATORY mice, *FLOW cytometry, *IMMUNOGLOBULINS

Abstract

Purpose: Dual-targeted therapy has been shown to be a promising treatment option in recurrent and/or refractory B-cell non-Hodgkin's lymphoma (B-NHL). We generated radioimmunoconjugates (RICs) comprising either a novel humanized anti-CD22 monoclonal antibody, huRFB4, or rituximab, and the low-energy β-emitter Lu. Both RICs were evaluated as single agents in a human Burkitt's lymphoma xenograft mouse model. To increase the therapeutic efficacy of the anti-CD22 RIC, combination therapy with unlabelled anti-CD20 rituximab was explored. Methods: The binding activity of CHX-A″-DTPA-conjugated antibodies to target cells was analysed by flow cytometry. To assess tumour targeting of Lu-labelled antibodies, in vivo biodistribution experiments were performed. For radioimmunotherapy (RIT) studies, non-obese diabetic recombination activating gene-1 (NOD-Rag1) interleukin-2 receptor common gamma chain (IL2rγ ) null mice (NRG mice) were xenografted subcutaneously with Raji Burkitt's lymphoma cells. Lu-conjugated antibodies were administered at a single dose of 9.5 MBq per mouse. For dual-targeted therapy, rituximab was injected at weekly intervals (0.5 - 1.0 mg). Tumour accumulation of RICs was monitored by planar scintigraphy. Results: Conjugation of CHX-A'-DTPA resulted in highly stable RICs with excellent antigen-binding properties. Biodistribution experiments revealed higher tumour uptake of the Lu-labelled anti-CD22 IgG than of Lu-labelled rituximab. Treatment with Lu-conjugated huRFB4 resulted in increased tumour growth inhibition and significantly longer survival than treatment with Lu-conjugated rituximab. The therapeutic efficacy of the anti-CD22 RIC could be markedly enhanced by combination with unlabelled rituximab. Conclusion: These findings suggest that dual targeting with Lu-based CD22-specific RIT in combination with rituximab is a promising new treatment option for refractory B-NHL. [ABSTRACT FROM AUTHOR]

Published

2016

126. High zinc ion supplementation of more than 30 μM can increase monoclonal antibody production in recombinant Chinese hamster ovary DG44 cell culture.

Author

Kim, Bong and Park, Hong

Subjects

*CHO cell, *ANIMAL models in research, *CELL culture, *CELL-mediated cytotoxicity, *MONOCLONAL antibody probes

Abstract

Effects of high ZnSO·7HO supplementation on cell growth and monoclonal antibody (mAb) production in chemically defined suspension cultures of recombinant Chinese hamster ovary (rCHO) DG44 cells were examined. The supplementation of ZnSO·7HO up to 120 μM gradually increased specific mAb production rate of rCHO DG44 cells in the early growth phase (0-4 days of culture). The ZnSO·7HO concentration for enhancing mAb production without any cytotoxic effects on cell growth was 30-60 μM. In addition of 60 μM ZnSO·7HO to in-house protein-free medium and in-house chemically defined medium, mAb production was increased 2.0-fold and 6.5-fold, respectively. Moreover, addition of ZnSO·7HO to three kinds of commercial chemically defined media yielded a greater than 1.2-fold enhancement of mAb production. These data indicate that simple supplementation of a relatively high zinc ion concentration to cell culture media without significant changes of rCHO DG44 cell culture process can be useful for achieving high production of mAb. [ABSTRACT FROM AUTHOR]

Published

2016

127. Profile of farletuzumab and its potential in the treatment of solid tumors.

Author

Seiya Sato and Hiroaki Itamochi

Subjects

*IMMUNOGLOBULIN G, *JUNO protein, *NON-small-cell lung carcinoma, *MONOCLONAL antibody probes, *CANCER treatment, *CLINICAL trials, *TUMOR suppressor genes, *CANCER chemotherapy

Abstract

Folate receptor (FR) α expression in normal tissues is restricted to a subpopulation of epithelial cells. In contrast, FRa is overexpressed in epithelial ovarian cancer (EOC) and non-small-cell lung carcinoma. Therefore, FRα is considered a promising therapeutic target for EOC and non-small-cell lung carcinoma. Farletuzumab (MORAb-003) is a humanized monoclonal antibody of immunoglobulin G subtype 1 kappa, targeting human FRα. To date, Phase I/II clinical trials have clearly demonstrated the feasibility and safety of farletuzumab as a treatment option against solid tumors. However, in Phase III clinical trial that was conducted to verify the combined effect of paclitaxel-carboplatin combination therapy and farletuzumab for patients with recurrent EOC, improvement in progression-free survival was not statistically significant. This result might be owing to the fact that the eligibility criteria for these studies did not include FRα expression. The significance of FRα as a predictive/prognostic biomarker remains unclear. In addition, there is currently no established biomarker to predict the response and toxicities among patients receiving farletuzumab therapy. Furthermore, the primary mechanism of action of farletuzumab has not yet been identified. Therefore, further research to identify the mechanism of farletuzumab in tumor suppression is necessary to clarify the full potential of this chemotherapeutic agent. [ABSTRACT FROM AUTHOR]

Published

2016

128. Monoclonal antibody against macrophage colony-stimulating factor suppresses circulating monocytes and tissue macrophage function but does not alter cell infiltration/activation in cutaneous lesions or clinical outcomes in patients with cutaneous lupus erythematosus

Author

Masek‐Hammerman, K., Peeva, E., Ahmad, A., Menon, S., Afsharvand, M., Peng Qu, R., Cheng, J. B., Syed, J., Zhan, Y., O'Neil, S. P., Pleasic‐Williams, S., Cox, L.A., and Beidler, D.

Subjects

*MONOCLONAL antibody probes, *MACROPHAGE colony-stimulating factor, *IMMUNOGLOBULIN G, *LUPUS erythematosus, *SUPPRESSOR cells, *MONOCYTES, *MACROPHAGES, *SKIN diseases

Abstract

This study's objective was to assess the effects of PD-0360324, a fully human immunoglobulin G2 monoclonal antibody against macrophage colony-stimulating factor in cutaneous lupus erythematosus (CLE). Patients with active subacute CLE or discoid lupus erythematosus were randomized to receive 100 or 150 mg PD-0360324 or placebo via intravenous infusion every 2 weeks for 3 months. Blood and urine samples were obtained pre- and post-treatment to analyse pharmacokinetics and pharmacodynamic changes in CD14+ CD16+ monocytes, urinary N-terminal telopeptide (uNTX), alanine/aspartate aminotransferases (ALT/AST) and creatine kinase (CK); tissue biopsy samples were taken to evaluate macrophage populations and T cells using immunohistochemistry. Clinical efficacy assessments included the Cutaneous Lupus Erythematosus Disease Area and Severity Index (CLASI). Among 28 randomized/analysed patients, peak/trough plasma concentrations increased in a greater-than-dose-proportional manner with dose increases from 100 to 150 mg. Statistically significant differences were observed between active treatment and placebo groups in changes from baseline in CD14+ CD16+ cells, uNTX, ALT, AST and CK levels at most time-points. The numbers, density and activation states of tissue macrophages and T cells did not change from baseline to treatment end. No between-group differences were seen in CLASI. Patients receiving PD-0360324 reported significantly more adverse events than those receiving placebo, but no serious adverse events. In patients with CLE, 100 and 150 mg PD-0360324 every 2 weeks for 3 months suppressed a subset of circulating monocytes and altered activity of some tissue macrophages without affecting cell populations in CLE skin lesions or improving clinical end-points. [ABSTRACT FROM AUTHOR]

Published

2016

129. Neoadjuvant therapy for early-stage breast cancer: the clinical utility of pertuzumab.

Author

Gollamudi, Jahnavi, Parvani, Jenny G., Schiemann, William P., and Vinayak, Shaveta

Subjects

BREAST cancer, TUMORS, BREAST cancer treatment, CANCER patients, MONOCLONAL antibody probes, PROTEIN-tyrosine kinases, CELLULAR signal transduction, TRASTUZUMAB

Abstract

Approximately 20% of breast cancer patients harbor tumors that overexpress human epidermal growth factor receptor 2 (HER2; also known as ErbB2), a receptor tyrosine kinase that belongs to the epidermal growth factor receptor family of receptor tyrosine kinases. HER2 amplification and hyperactivation drive the growth and survival of breast cancers through the aberrant activation of proto-oncogenic signaling systems, particularly the Ras/MAP kinase and PI3K/AKT pathways. Although HER2-positive (HER2+) breast cancer was originally considered to be a highly aggressive form of the disease, the clinical landscape of HER2+ breast cancers has literally been transformed by the approval of anti-HER2 agents for adjuvant and neoadjuvant settings. Indeed, pertuzumab is a novel monoclonal antibody that functions as an anti-HER2 agent by targeting the extracellular dimerization domain of the HER2 receptor; it is also the first drug to receive an accelerated approval by the US Food and Drug Administration for use in neoadjuvant settings in early-stage HER2+ breast cancer. Here, we review the molecular and cellular factors that contribute to the pathophysiology of HER2 in breast cancer, as well as summarize the landmark preclinical and clinical findings underlying the approval and use of pertuzumab in the neoadjuvant setting. Finally, the molecular mechanisms operant in mediating resistance to anti-HER2 agents, and perhaps to pertuzumab as well, will be discussed, as will the anticipated clinical impact and future directions of pertuzumab in breast cancer patients. [ABSTRACT FROM AUTHOR]

Published

2016

130. A universal solution for eliminating false positives in myeloma due to therapeutic monoclonal antibody interference.

Author

Mills, John R., Kohlhagen, Mindy C., Willrich, Maria A. V., Kourelis, Taxiarchis, Dispenzieri, Angela, and Murray, David L.

Subjects

*MONOCLONAL antibody probes, *MULTIPLE myeloma diagnosis, *MASS spectrometry, *MOLECULAR weights, *CLONE cells, *BIOLOGICAL tags

Abstract

The article discusses the elimination of false positives in multiple myeloma (MM) which results in the expansion of the clonal plasma cells for immunoglobulin M-proteins. Topics include the monoclonal antibody interference, detection of protein biomarkers, and the molecular mass measurements through mass spectroscopy.

Published

2018

131. Nocebo/drucebo effect in statin-intolerant patients: an attempt at recommendations.

Author

Penson, Peter E and Banach, Maciej

Subjects

DRUGS, MONOCLONAL antibody probes, SUBTILISINS, STATINS (Cardiovascular agents), PLACEBOS

Abstract

The article presents the discussion on novel lipid lowering drugs including monoclonal antibody inhibitors of proprotein convertase subtilisin/kexin type 9 (PCSK9), and inclisiran. Topics include statins commonly available, cheap, safe and effective drugs reducing the risk of cardiovascular (CV) events; and reporting intensity of symptoms not differing between the periods of statin use and placebo.

Published

2021

132. Clinical edge: Treatment of multiple sclerosis with lemtrada

Author

King, John

Published

2015

133. Combination Therapy Using IL-2/IL-2 Monoclonal Antibody Complexes, Rapamycin, and Islet Autoantigen Peptides Increases Regulatory T Cell Frequency and Protects against Spontaneous and Induced Type 1 Diabetes in Nonobese Diabetic Mice.

Author

Manirarora, Jean N. and Cheng-Hong Wei

Subjects

*MONOCLONAL antibody probes, *RAPAMYCIN, *AUTOANTIGENS, *TH2 cells, *TYPE 1 diabetes

Abstract

Regulatory T cells (Treg) play a crucial role in the maintenance of self-tolerance. In this study, we sought to expand Ag-specific Tregs in vivo and investigate whether the expanded Tregs can prevent or delay the development of type 1 diabetes (T1D) in the NOD mouse model. NOD mice were treated with a combination of IL-2/anti-IL-2 Ab complex, islet Ag peptide, and rapamycin. After the combined treatment, CD4+CD25+Foxp3+ Tregs were significantly expanded in vivo, they expressed classical Treg markers, exerted enhanced suppressive functions in vitro, and protected against spontaneous development of T1D in NOD mice. Moreover, treated mice were almost completely protected from the adoptively transferred, aggressive form of T1D caused by in vitro-activated cytotoxic islet Ag-specific CDS T cells. Protection from T1D was transferrable by Tregs and could be attributed to reduced islet infiltration of immune cells as well as the skewing of the immune response toward a Th2 cytokine profile. This new method of peripheral immune regulation could potentially contribute to development of novel imniunotherapeutic strategies to prevent the development of TID or to promote tolerance to islet transplants without using immunosuppressive drugs for long terms. [ABSTRACT FROM AUTHOR]

Published

2015

134. Identification of a high-affinity monoclonal antibody against ochratoxin A and its application in enzyme-linked immunosorbent assay.

Author

Zhang, Xian, Sun, Mengjiao, Kang, Yue, Xie, Hui, Wang, Xin, Song, Houhui, Li, Xiaoliang, and Fang, Weihuan

Subjects

*MONOCLONAL antibody probes, *MONOCLONAL antibodies, *ENZYME-linked immunosorbent assay, *OCHRATOXINS, *MYCOTOXINS, *ASPERGILLUS

Abstract

Ochratoxin A (OTA) is one of the most commonly occurring mycotoxins produced by some species of Aspergillus and can contaminate cereal and cereal products. A high-affinity anti-OTA monoclonal antibody (mAb) was generated from a hybridoma cell line 2D8 using splenocytes from a BALB/c mouse immunized with synthesized OTA-bovine serum albumin conjugate. The mAb 2D8 is specific with high affinity (3.75 × 10 9 L/M). An indirect competitive ELISA (ic-ELISA) was then developed using this mAb for quantitative determination of OTA in corn and feed samples. Using the optimized conditions, there was good linearity between OTA concentration and competitive inhibition (y = −0.6076x + 0.2441, R 2 = 0.9923) with the working range from 2.4 to 23.6 μg/kg, IC 50 at 7.6 μg/kg and lower limit of detection at 1.4 μg/kg. The recovery rates in spiked samples were 91.2–110.3%. Of the 56 corn and feed samples, this ic-ELISA and a commercial kit both found the same 13 samples positive for OTA with good linear correlation between the two methods in OTA quantification (R 2 = 0.9706). We conclude that this ic-ELISA can be used for rapid and quantitative screening of corn and feed samples for the presence of OTA. [ABSTRACT FROM AUTHOR]

Published

2015

135. Secukinumab (AIN457) for the treatment of psoriasis.

Author

López-Ferrer, Anna, Vilarrasa, Eva, and Puig, Lluís

Subjects

PSORIASIS treatment, INTERLEUKIN-17, IMMUNODEFICIENCY, PHYSIOLOGICAL effects of cytokines, MONOCLONAL antibody probes, ETANERCEPT, NASOPHARYNGITIS

Abstract

Psoriasis is a chronic inflammatory disease with a multifactorial origin that appears in patients with genetic predisposition and is induced by environmental factors, and characterized by alterations in the innate and adaptive immunity. IL-17A is one of the specific cytokines involved in the pathogenesis of psoriasis and its inhibition is highly effective in the treatment of patients with moderate and severe psoriasis. Secukinumab is a monoclonal antibody that specifically binds to IL-17A and inhibits the interaction to its receptor, and it has demonstrated its efficacy and safety in the treatment of psoriasis. Phase II and III clinical trials indicate that > 80% of the patients receiving secukinumab achieve Psoriasis Area Severity Index (PASI) 75 at week 12. In the Phase III efficacy of response and safety of two fixed secukinumab regimens in psoriasis trial, PASI 75 rates were 81.6% with 300 mg secukinumab, 71.6% with 150 mg secukinumab and 4.5% with placebo, and responses were maintained up to 52 weeks in the majority of patients. In the Phase III Full Year Investigative Examination Of Secukinumab versus Etanercept Using Two Dosing Regimens To Determine Efficacy in Psoriasis study, the efficacy of secukinumab was compared to etanercept. The results indicate that both doses of secukinumab (150 and 300 mg) showed superior efficacy compared with etanercept throughout the study; PASI 75 rates at week 12 were 77.1% with 300 mg secukinumab, 67% with 150 mg of secukinumab, 44% with etanercept and 4.9% with placebo. PASI 90 and PASI 100 were 54 and 24% with secukinumab 300 mg and 21 and 4% with etanercept at week 12. At week 52, PASI 90 continued to be higher in the secukinumab group (65%) compared with the etanercept group (33%). Regarding safety, the most common side effects were nasopharyngitis and headache. The rate of infections was higher with secukinumab than placebo. This was especially the case for Candida infections, which were more common in the secukinumab group (4.7% with secukinumab 300 mg and 2.3% with secukinumab 150 mg), but all cases were resolved with conventional treatment. Secukinumab is a well-tolerated treatment that has demonstrated efficacy in treating moderate-to-severe plaque psoriasis. Nevertheless, long-term studies are necessary to confirm Phase II and Phase III data. [ABSTRACT FROM AUTHOR]

Published

2015

136. Molecular insights into the inhibition of HIV-1 infection using a CD4 domain-1-specific monoclonal antibody.

Author

Hou, Wangheng, Fang, Chu, Liu, Jiayan, Yu, Hai, Qi, Jialong, Zhang, Zhiqing, Yuan, Ruixue, Xiong, Dan, Gao, Shuangquan, Adam Yuan, Y., Li, Shaowei, Gu, Ying, and Xia, Ningshao

Subjects

*DIAGNOSIS of HIV infections, *CD4 antigen, *MONOCLONAL antibody probes, *BINDING site assay, *CHEMOKINE receptors, *CELL membranes, *THERAPEUTICS

Abstract

An HIV-1 infection in a host cell occurs through an ordered process that involves HIV-1 attachment to the host’s cellular CD4 receptor, co-receptor binding to CCR5 or CXCR4, and the subsequent fusion with the cellular membrane. The natural viral entry pathway into a host cell provides an opportunity to develop agents for the treatment of HIV-1 infections. Several engineered monoclonal antibodies specifically targeting CD4 have shown antiviral activities in clinical trials. Here, we report on an anti-CD4 mAb (15A7) that displays a unique binding specificity for domain 1 of CD4, whose epitope partially overlaps with the gp120 binding region. Moreover, 15A7 displays a much stronger binding affinity to CD4 + cell lines after HIV infection. 15A7 is able to block and neutralize a broad range of primary HIV-1 isolates and T cell-line passage strains. Notably, the bivalent F(ab′) 2 form of 15A7 is more effective than the Fab form in blocking HIV-1 infection, which is further supported by molecular docking analyses. Together, these results suggest that this novel antibody may exert its antiviral activity by blocking gp120 targeting to the CD4 receptor or competing with gp120 for CD4 receptor binding and might present post-attachment neutralization activity. This antibody could provide a new candidate to efficiently block HIV-1 infection or provide new starting materials for HIV treatment, especially when HIV-1-resistant strains against the current CD4 mAb treatments have already been identified. [ABSTRACT FROM AUTHOR]

Published

2015

137. A phase I trial combining carboplatin/doxorubicin with tocilizumab, an anti-IL-6R monoclonal antibody, and interferon-α2b in patients with recurrent epithelial ovarian cancer.

Author

Dijkgraaf, E. M., Santegoets, S. J. A. M., Reyners, A. K. L., Goedemans, R., Wouters, M. C. A., Kenter, G. G., van Erkel, A. R., van Poelgeest, M. I. E., Nijman, H. W., van der Hoeven, J. J. M., Welters, M. J. P., van der Burg, S. H., and Kroep, J. R.

Subjects

*CARBOPLATIN, *DOXORUBICIN, *MONOCLONAL antibody probes, *OVARIAN epithelial cancer, *INTERLEUKIN-6

Abstract

Background: The immune system is important in epithelial ovarian cancer (EOC). Interleukin-6 is associated with chemoresistance and an immune-suppressive tumor microenvironment. We investigated whether a combination of chemotherapeutics, blockade of interleukin 6 (IL-6) receptor (IL-6R; tocilizumab), and immune enhancer interferon-α (Peg-Intron) is feasible, safe, and able to enhance immunity in patients with recurrent EOC. Patients and methods: In this dose-escalation study, patients received tocilizumab 1, 2, 4, or 8 mg/kg i.v., q4 weeks during the first three cycles of carboplatin (AUC5) plus doxorubicin [pegylated liposomal doxorubicin (PLD) 30 mg/m² or doxorubicin 50 mg/m² i.v., day, q4 weeks, for six cycles]. At the highest tocilizumab dose (8 mg/kg), Peg-Intron (1 μg/kg s.c.) was added. Peripheral blood mononuclear cells were collected for immunomonitoring at baseline, after three and six cycles. Dose-limiting toxicity (DLT), CA-, and radiologic response were evaluated. Results: In the 23 patients enrolled, no DLT was established. The most frequent grade 3/4 adverse events (CTCAE v4.03) were neutropenia (23%), febrile neutropenia (19%), and ileus (19%). No treatment-related deaths occurred. Using CT evaluation, 11 of 21 assessable patients responded, 6 had stable disease and 3 progressive disease. Patients receiving highest dose tocilizumab showed a functional blockade of IL-6R with increased levels of serum IL-6 (P = 0.02) and soluble IL-6R (P = 0.008). Consequently, immune cells displayed decreased levels of pSTAT, myeloid cells produced more IL-12 and IL-1β while T cells were more activated and secreted higher amounts of effector cytokines interferon-γ and tumor necrosis factor-α. An increase in sIL-6R was potentially associated with a survival benefit (P = 0.03). Conclusions: Functional IL-6R blocking is feasible and safe in EOC patients treated with carboplatin/(pegylated liposomal) doxorubicin, using 8 mg/kg tocilizumab. This combination is recommended for phase II evaluation based on immune parameters. Clinical trial register: NCT01637532. [ABSTRACT FROM AUTHOR]

Published

2015

138. Functional and Structural Characterization of Human V3-Specific Monoclonal Antibody 2424 with Neutralizing Activity against HIV-1 JRFL.

Author

Kumar, Rajnish, Pan, Ruimin, Upadhyay, Chitra, Mayr, Luzia, Cohen, Sandra, Xiao-Hong Wang, Balasubramanian, Preetha, Nádas, Arthur, Seaman, Michael S., Zolla-Pazner, Susan, Gorny, Miroslaw K., Xiang-Peng Kong, and Hioe, Catarina E.

Subjects

*MONOCLONAL antibody probes, *HIV infections, *MONOCLONAL antibodies, *RECOMBINANT proteins, *GLYCANS

Abstract

The V3 region of HIV-1 gp120 is important for virus-coreceptor interaction and highly immunogenic. Although most anti-V3 antibodies neutralize only the sensitive tier 1 viruses, anti-V3 antibodies effective against the more resistant viruses exist, and a better understanding of these antibodies and their epitopes would be beneficial for the development of novel vaccine immunogens against HIV. The HIV-1 isolate JRFL with its cryptic V3 is resistant to most V3-specific monoclonal antibodies (MAbs). However, the V3MAb2424 achieves 100% neutralization against JRFL. 2424 is encoded by IGHV3-53 and IGLV2-28 genes, a pairing rarely used by the other V3 MAbs. 2424 also has distinct binding and neutralization profiles. Studies of 2424-mediated neutralization of JRFL produced with a mannosidase inhibitor further revealed that its neutralizing activity is unaffected by the glycan composition of the virus envelope. To understand the distinct activity of 2424, we determined the crystal structure of 2424 Fab in complex with a JRFL V3 peptide and showed that the 2424 epitope is located at the tip of the V3 crown (307IHIGPGRAFYT319), dominated by interactions with HisP308, ProP313, and ArgP315. The binding mode of 2424 is similar to that of the well-characterized MAb447-52D, although 2424 is more side chain dependent. The 2424 epitope is focused on the very apex of V3, away from nearby glycans, facilitating antibody access. This feature distinguishes the 2424 epitope from the other V3 crown epitopes and indicates that the tip of V3 is a potential site to target and incorporate into HIV vaccine immunogens. IMPORTANCE HIV/AIDS vaccines are crucial for controlling the HIV epidemics that continue to afflict millions of people worldwide. However, HIV vaccine development has been hampered by significant scientific challenges, one of which is the inability of HIV vaccine candidates evaluated thus far to elicit production of potent and broadly neutralizing antibodies. The V3 loop is one of the few immunogenic targets on the virus envelope glycoprotein that can induce neutralizing antibodies, but in many viruses, parts of V3 are inaccessible for antibody recognition. This study examined a V3-specific monoclonal antibody that can completely neutralize HIV-1 JRFL, a virus isolate resistant to most V3 antibodies. Our data reveal that this antibody recognizes the most distal tip of V3, which is not as occluded as other parts of V3. Hence, the epitope of 2424 is in one of the vulnerable sites on the virus that may be exploited in designing HIV vaccine immunogens. [ABSTRACT FROM AUTHOR]

Published

2015

139. Cocrystal Structures of Antibody N60-i3 and Antibody JR4 in Complex with gp120 Define More Cluster A Epitopes Involved in Effective Antibody-Dependent Effector Function against HIV-1.

Author

Gohain, Neelakshi, Tolbert, William D., Acharya, Priyamvada, Lei Yu, Tongyun Liu, Pingsen Zhao, Orlandi, Chiara, Visciano, Maria L., Kamin-Lewis, Roberta, Sajadi, Mohammad M., Martin, Loïc, Robinson, James E., Peter D. Kwong, DeVico, Anthony L., Ray, Krishanu, Lewis, George K., and Pazgier, Marzena

Subjects

*ANTIBODY-dependent cell cytotoxicity, *EPITOPES, *HIV infections, *MONOCLONAL antibody probes, *IMMUNOGLOBULINS

Abstract

Accumulating evidence indicates a role for Fc receptor (FcR)-mediated effector functions of antibodies, including antibody-dependent cell-mediated cytotoxicity (ADCC), in prevention of human immunodeficiency virus type 1 (HIV-1) acquisition and in postinfection control of viremia. Consequently, an understanding of the molecular basis for Env epitopes that constitute effective ADCC targets is of fundamental interest for humoral anti-HIV-1 immunity and for HIV-1 vaccine design. A substantial portion of FcR effector function of potentially protective anti-HIV-1 antibodies is directed toward nonneutralizing, transitional, CD4-inducible (CD4i) epitopes associated with the gp41-reactive region of gp120 (cluster A epitopes). Our previous studies defined the A32-like epitope within the cluster A region and mapped it to the highly conserved and mobile layers 1 and 2 of the gp120 inner domain within the C1-C2 regions of gp120. Here, we elucidate additional cluster A epitope structures, including an A32-like epitope, recognized by human monoclonal antibody (MAb) N60-i3, and a hybrid A32-C11-like epitope, recognized by rhesus macaque MAb JR4. These studies define for the first time a hybrid A32-C11-like epitope and map it to elements of both the A32-like subregion and the seven-layered β-sheet of the gp41-interactive region of gp120. These studies provide additional evidence that effective antibody-dependent effector function in the cluster A region depends on precise epitope targeting-a combination of epitope footprint and mode of antibody attachment. All together these findings help further an understanding of how cluster A epitopes are targeted by humoral responses. IMPORTANCE HIV/AIDS has claimed the lives of over 30 million people. Although antiretroviral drugs can control viral replication, no vaccine has yet been developed to prevent the spread of the disease. Studies of natural HIV-1 infection, simian immunodeficiency virus (SIV)- or simian-human immunodeficiency virus (SHIV)-infected nonhuman primates (NHPs), and HIV-1-infected humanized mouse models, passive transfer studies in infants born to HIV-infected mothers, and the RV144 clinical trial have linked FcRmediated effector functions of anti-HIV-1 antibodies with postinfection control of viremia and/or blocking viral acquisition. With this report we provide additional definition of the molecular determinants for Env antigen engagement which lead to effective antibody-dependent effector function directed to the nonneutralizing CD4-dependent epitopes in the gp41-reactive region of gp120. These findings have important implications for the development of an effective HIV-1 vaccine. [ABSTRACT FROM AUTHOR]

Published

2015

140. F4+ enterotoxigenic Escherichia coli (ETEC) adhesion mediated by the major fimbrial subunit FaeG.

Author

Xia, Pengpeng, Song, Yujie, Zou, Yajie, Yang, Ying, and Zhu, Guoqiang

Subjects

PILI (Microbiology), ESCHERICHIA coli, CELL adhesion, GLYCOPROTEINS, EPITHELIAL cells, BACTERIAL cells, MONOCLONAL antibody probes

Abstract

The FaeG subunit is the major constituent of F4+ fimbriae, associated with glycoprotein and/or glycolipid receptor recognition and majorly contributes to the pathogen attachment to the host cells. To investigate the key factor involved in the fimbrial binding of F4+ Escherichia coli, both the recombinant E. coli SE5000 strains carrying the fae operon gene clusters that express the different types of fimbriae in vitro, named as rF4ab, rF4ac, and rF4ad, respectively, corresponding to the fimbrial types F4ab, F4ac, and F4ad, and the three isogenic in-frame faeG gene deletion mutants were constructed. The adhesion assays and adhesion inhibition assays showed that ΔfaeG mutants had a significant reduction in the binding to porcine brush border as well as the intestinal epithelial cell lines, while the complemented strain ΔfaeG/p faeG restored the adhesion function. The recombinant bacterial strains rF4ab, rF4ac, and rF4ad have the same binding property as wild-type F4+ E. coli strains do and improvement in terms of binding to porcine brush border and the intestinal epithelial cells, and the adherence was blocked by the monoclonal antibody anti-F4 fimbriae. These data demonstrate that the fimbrial binding of F4+ E. coli is directly mediated by the major FaeG subunit. [ABSTRACT FROM AUTHOR]

Published

2015

141. Safety, tolerability, and efficacy of idarucizumab for the reversal of the anticoagulant effect of dabigatran in healthy male volunteers: a randomised, placebo-controlled, double-blind phase 1 trial.

Author

Glund, Stephan, Stangier, Joachim, Schmohl, Michael, Gansser, Dietmar, Norris, Stephen, van Ryn, Joanne, Lang, Benjamin, Ramael, Steven, Moschetti, Viktoria, Gruenenfelder, Fredrik, Reilly, Paul, and Kreuzer, Jörg

Subjects

*MONOCLONAL antibody probes, *ANTICOAGULANTS, *PLACEBOS, *BODY mass index, *THROMBIN time

Abstract

Background Idarucizumab is a monoclonal antibody fragment that binds dabigatran with high affinity in a 1:1 molar ratio. We investigated the safety, tolerability, and efficacy of increasing doses of idarucizumab for the reversal of anticoagulant effects of dabigatran in a two-part phase 1 study (rising-dose assessment and dose-finding, proof-of-concept investigation). Here we present the results of the proof-of-concept part of the study. Methods In this randomised, placebo-controlled, double-blind, proof-of-concept phase 1 study, we enrolled healthy volunteers (aged 18–45 years) with a body-mass index of 18·5–29·9 kg/m2 into one of four dose groups at SGS Life Sciences Clinical Research Services, Belgium. Participants were randomly assigned within groups in a 3:1 ratio to idarucizumab or placebo using a pseudorandom number generator and a supplied seed number. Participants and care providers were masked to treatment assignment. All participants received oral dabigatran etexilate 220 mg twice daily for 3 days and a final dose on day 4. Idarucizumab (1 g, 2 g, or 4 g 5-min infusion, or 5 g plus 2·5 g in two 5-min infusions given 1 h apart) was administered about 2 h after the final dabigatran etexilate dose. The primary endpoint was incidence of drug-related adverse events, analysed in all randomly assigned participants who received at least one dose of dabigatran etexilate. Reversal of diluted thrombin time (dTT), ecarin clotting time (ECT), activated partial thromboplastin time (aPTT), and thrombin time (TT) were secondary endpoints assessed by measuring the area under the effect curve from 2 h to 12 h (AUEC2–12) after dabigatran etexilate ingestion on days 3 and 4. This trial is registered with ClinicalTrials.gov, number NCT01688830. Findings Between Feb 23, and Nov 29, 2013, 47 men completed this part of the study. 12 were enrolled into each of the 1 g, 2 g, or 5 g plus 2·5 g idarucizumab groups (nine to idarucizumab and three to placebo in each group), and 11 were enrolled into the 4 g idarucizumab group (eight to idarucizumab and three to placebo). Drug-related adverse events were all of mild intensity and reported in seven participants: one in the 1 g idarucizumab group (infusion site erythema and hot flushes), one in the 5 g plus 2·5 g idarucizumab group (epistaxis); one receiving placebo (infusion site haematoma), and four during dabigatran etexilate pretreatment (three haematuria and one epistaxis). Idarucizumab immediately and completely reversed dabigatran-induced anticoagulation in a dose-dependent manner; the mean ratio of day 4 AUEC2–12 to day 3 AUEC2–12 for dTT was 1·01 with placebo, 0·26 with 1 g idarucizumab (74% reduction), 0·06 with 2 g idarucizumab (94% reduction), 0·02 with 4 g idarucizumab (98% reduction), and 0·01 with 5 g plus 2·5 g idarucizumab (99% reduction). No serious or severe adverse events were reported, no adverse event led to discontinuation of treatment, and no clinically relevant difference in incidence of adverse events was noted between treatment groups. Interpretation These phase 1 results show that idarucizumab was associated with immediate, complete, and sustained reversal of dabigatran-induced anticoagulation in healthy men, and was well tolerated with no unexpected or clinically relevant safety concerns, supporting further testing. Further clinical studies are in progress. INSET: Panel: Research in context.. [ABSTRACT FROM AUTHOR]

Published

2015

142. αB-crystallin reduces ristocetin-induced soluble CD40 ligand release in human platelets: Suppression of thromboxane A2 generation.

Author

MASANORI TSUJIMOTO, TOMOAKI DOI, GEN KUROYANAGI, NAOHIRO YAMAMOTO, RIE MATSUSHIMA-NISHIWAKI, YUKO IIDA, YUKIKO ENOMOTO, HIROKI IIDA, SHINJI OGURA, TAKANOBU OTSUKA, HARUHIKO TOKUDA, OSAMU KOZAWA, and TORU IWAMA

Subjects

*HEAT shock proteins, *PHOSPHORYLATION, *RISTOCETIN, *GLYCOPROTEINS, *MONOCLONAL antibody probes, *PROTEIN kinases

Abstract

Our group has previously shown that αB-crystallin (HSPB5), a small heat shock protein, inhibits human platelet aggregation by ristocetin, an activator of glycoprotein Ib/IX/V. In addition, it was demonstrated that glycoprotein Ib/IX/V activation induces soluble CD40 (sCD40) ligand release via thromboxane (TX) A2. In the present study, the effect of αB-crystallin on the ristocetin-induced sCD40 ligand release in human platelets was investigated. The ristocetin-induced release of sCD40 ligand was suppressed by αB-crystallin. In addition, αB-crystallin reduced the ristocetin-stimulated production of 11-dehydro-TX B2, a stable metabolite of TXA2. αB-crystallin did not suppress the platelet aggregation induced by U46619, a TXA2 receptor agonist. αB-crystallin had little effect on the U46619-induced phosphorylation of p38 mitogen-activated protein kinase or sCD40 ligand release. In addition, αB-crystallin failed to reduce the binding of SZ2, a monoclonal antibody against the sulfated sequence in the α-chain of glycoprotein Ib, to the ristocetin-stimulated platelets. These results strongly suggest that αB-crystallin extracellularly suppresses ristocetin-stimulated release of sCD40 ligand by inhibiting the TXA2 production in human platelets. [ABSTRACT FROM AUTHOR]

Published

2015

143. Serum Immunoglobulin A Cross-Strain Blockade of Human Noroviruses.

Author

Lindesmith, Lisa C., Beltramello, Martina, Swanstrom, Jesica, Jones, Taylor A., Corti, Davide, Lanzavecchia, Antonio, and Baric, Ralph S.

Subjects

*VIRUS-like particles, *IMMUNOGLOBULIN A, *MONOCLONAL antibody probes

Abstract

Background. Human noroviruses are the leading cause of acute viral gastroenteritis, justifying vaccine development despite a limited understanding of strain immunity. After genogroup I (GI).1 norovirus infection and immunization, blockade antibody titers to multiple virus-like particles (VLPs) increase, suggesting that GI cross-protection may occur. Methods. Immunoglobulin (Ig)A was purified from sera collected from GI.1-infected participants, and potential neutralization activity was measured using a surrogate neutralization assay based on antibody blockade of ligand binding. Human and mouse monoclonal antibodies (mAbs) were produced to multiple GI VLPs to characterize GI epitopes. Results. Immunoglobulin A purified from day 14 post-GI.1 challenge sera blocked binding of GI.1, GI.3, and GI.4 to carbohydrate ligands. In some subjects, purified IgA preferentially blocked binding of other GI VLPs compared with GI.1, supporting observations that the immune response to GI.1 infection may be influenced by pre-exposure history. For other subjects, IgA equivalently blocked multiple GI VLPs. Only strain-specific mAbs recognized blockade epitopes, whereas strain cross-reactive mAbs recognized nonblockade epitopes. Conclusions. These studies are the first to describe a functional role for serum IgA in norovirus immunity and the first to characterize human monoclonal antibodies to GI strains, expanding our understanding of norovirus immunobiology. [ABSTRACT FROM AUTHOR]

Published

2015

144. Critical evaluation of ramucirumab in the treatment of advanced gastric and gastroesophageal cancers.

Author

ElHalawani, Hesham and Abdel-Rahman, Omar

Subjects

*ANTINEOPLASTIC agents, *BEVACIZUMAB, *STOMACH cancer treatment, *ESOPHAGOGASTRIC junction cancer, *NEOVASCULARIZATION, *MONOCLONAL antibody probes, *CANCER treatment

Abstract

Gastric (GC) and gastroesophageal junction (GEJ) cancers are two global health problems with a relatively high mortality, particularly in the advanced stage. Inhibition of angiogenesis is now contemplated as a classic treatment preference for myriad tumor types encompassing renal cell carcinoma, non-small cell lung cancer, colorectal cancer, glioblastoma, and ovarian cancer, among others. Bevacizumab and ramucirumab have been widely investigated in GC and GEJ cancer, with some controversy about their therapeutic role. Ramucirumab is a monoclonal antibody for vascular endothelial growth factor receptor-2, with demonstrated activity both as a monotherapy and as a part of combination strategy in the management of advanced GC/GEJ cancer. In this review article, we present a critical evaluation of the preclinical and clinical data underlying the use of this drug in this indication. Moreover, we provide a spotlight on the future perspectives in systemic therapy for advanced GC/GEJ cancer. [ABSTRACT FROM AUTHOR]

Published

2015

145. Regulating against the dysregulation: new treatment options in autoinflammation.

Author

Kallinich, Tilmann

Subjects

*IMMUNOLOGIC diseases, *INFLAMMATION treatment, *CYTOKINES, *STEROID drugs, *IMMUNOSUPPRESSIVE agents, *MONOCLONAL antibody probes, *THERAPEUTICS

Abstract

In autoinflammatory disorders, dysregulation of the innate immune response leads to an excessive cytokine release. The disease course is often characterized by high morbidity and mortality, treatment is mostly difficult and therapeutic options are limited. In most cases, life-long control of ongoing inflammation is necessary in order to improve clinical symptoms and prevent development of damage. Steroids are helpful in many conditions, but the development of serious side effects often limits their long-term use. Other immunosuppressive, steroid-sparing medications are less effective than in the treatment of autoimmune diseases or do not show any effect. So far, anti-IL1α and/or β-blocking agents as well as an IL-6 receptor-blocking monoclonal antibody and, to a lesser extent, TNF-α blocking agents were applied in autoinflammatory disorders and significantly improved the outcome. Although these progresses were made in the last years, there are still numerous challenges in order to improve drug therapy in autoinflammation. This review summarizes the current state of new drug development and discusses advantages and disadvantages of possible targets. [ABSTRACT FROM AUTHOR]

Published

2015

146. Epidermal growth factor receptor immunohistochemistry: new opportunities in metastatic colorectal cancer.

Author

Hutchinson, Ryan A., Adams, Richard A., McArt, Darragh G., Salto-Tellez, Manuel, Jasani, Bharat, and Hamilton, Peter W.

Subjects

*CANCER treatment, *EPIDERMAL growth factor receptors, *IMMUNOHISTOCHEMISTRY, *MONOCLONAL antibody probes, *COLON cancer

Abstract

The treatment of cancer is becoming more precise, targeting specific oncogenic drivers with targeted molecular therapies. The epidermal growth factor receptor has been found to be over-expressed in a multitude of solid tumours. Immunohistochemistry is widely used in the fields of diagnostic and personalised medicine to localise and visualise disease specific proteins. To date the clinical utility of epidermal growth factor receptor immunohistochemistry in determining monoclonal antibody efficacy has remained somewhat inconclusive. The lack of an agreed reproducible scoring criteria for epidermal growth factor receptor immunohistochemistry has, in various clinical trials yielded conflicting results as to the use of epidermal growth factor receptor immunohistochemistry assay as a companion diagnostic. This has resulted in this test being removed from the licence for the drug panitumumab and not performed in clinical practice for cetuximab. In this review we explore the reasons behind this with a particular emphasis on colorectal cancer, and to suggest a way of resolving the situation through improving the precision of epidermal growth factor receptor immunohistochemistry with quantitative image analysis of digitised images complemented with companion molecular morphological techniques such as in situ hybridisation and section based gene mutation analysis. [ABSTRACT FROM AUTHOR]

Published

2015

147. Targeting ADAM-17 with an inhibitory monoclonal antibody has antitumour effects in triple-negative breast cancer cells.

Author

Caiazza, F, McGowan, P M, Mullooly, M, Murray, A, Synnott, N, O'Donovan, N, Flanagan, L, Tape, C J, Murphy, G, Crown, J, and Duffy, M J

Subjects

*TRIPLE-negative breast cancer, *MONOCLONAL antibody probes, *ESTROGEN, *PROGESTERONE receptors, *ANTINEOPLASTIC agents, *EPIDERMAL growth factor receptors

Abstract

Background:Identification and validation of a targeted therapy for triple-negative breast cancer (TNBC), that is, breast cancers negative for oestrogen receptors, progesterone receptors and HER2 amplification, is currently one of the most urgent problems in breast cancer treatment. EGFR is one of the best-validated driver genes for TNBC. EGFR is normally activated following the release of ligands such as TGFα, mediated by the two MMP-like proteases ADAM (a disintegrin and metalloproteinase)-10 and ADAM-17. The aim of this study was to investigate the antitumour effects of a monoclonal antibody against ADAM-17 on an in vitro model of TNBC.Methods:We investigated an inhibitory cross-domain humanised monoclonal antibody targeting both the catalytic domain and the cysteine-rich domain of ADAM17-D1(A12) in the HCC1937 and HCC1143 cell lines.Results:D1(A12) was found to significantly inhibit the release of TGFα, and to decrease downstream EGFR-dependent cell signalling. D1(A12) treatment reduced proliferation in two-dimensional clonogenic assays, as well as growth in three-dimensional culture. Furthermore, D1(A12) reduced invasion of HCC1937 cells and decreased migration of HCC1143 cells. Finally, D1(A12) enhanced cell death in HCC1143 cells.Conclusion:Our in vitro findings suggest that targeting ADAM-17 with D1(A12) may have anticancer activity in TNBC cells. [ABSTRACT FROM AUTHOR]

Published

2015

148. Antibody Structural Integrity of Site-Specific Antibody-Drug Conjugates Investigated by Hydrogen/Deuterium Exchange Mass Spectrometry.

Author

Lucy Yan Pan, Salas-Solano, Oscar, and Valliere-Douglass, John F.

Subjects

*ANTIBODY-drug conjugates, *DEUTERIUM, *CRYSTAL structure, *HYDROGEN bonding, *MONOCLONAL antibody probes

Abstract

We present the results of a hydrogen/deuterium exchange mass spectrometric (HDX-MS) investigation of an antibody–drug conjugate (ADC) comprised of drug-linkers conjugated to cysteine residues that have been engineered into heavy chain (HC) fragment crystallizable (Fc) domain at position 239. A side-by-side comparison of the HC Ser239 wild type (wt) monoclonal antibody (mAb) and the engineered Cys239 mAb indicates that site directed mutagenesis of Ser239 to cysteine has no impact on the HDX kinetics of the mAb. According to the crystal structure of a homologous immunoglobulin G1 (IgG1) antibody (PDB: 1HZH), the backbone amide of Ser239 is hydrogen-bonded to Val264 backbone amide in the wt-mAb studied here. Replacing Ser239 with a Cys residue does not alter the exchange kinetics of the backbone amide of Val264 suggesting that either Ser or Cys at position 239 has similar amide-hydrogen bonding with Val264. However, a small segment in CH2 domain of the ADC (264VDVS) was found to have a slightly increased HDX rate compared to the wt- and C239-mAb constructs. The slightly increased HDX rate of the segment 264VDVS in ADCs indicates that the further modification of Cys239 with drug-linkers only attenuates the local backbone amide hydrogen-bonding network between Cys239 and Val264. All other regions which are proximal to the site of drug conjugation are unaffected. The results demonstrate that the site-specific drug conjugation at the engineered Cys residue at the position 239 of HC does not impact the structural integrity of antibodies. The results also highlight the utility of applying HDX-MS to ADCs to gain a molecular level insight into the impact of site-specific conjugation technologies on the higher-order structure (HOS) of mAbs. The methodology can be applied generally to site-specific ADC modalities to understand the individual contributions of site-mutagenesis and drug-linker conjugation on the HOS of therapeutic candidate ADCs. [ABSTRACT FROM AUTHOR]

Published

2015

149. On the Analytical Superiority of 1D NMR for Fingerprinting the Higher Order Structure of Protein Therapeutics Compared to Multidimensional NMR Methods.

Author

Poppe, Leszek, Jordan, John B., Rogers, Gary, and Schnier, Paul D.

Subjects

*NUCLEAR magnetic resonance, *DNA fingerprinting, *THERAPEUTIC use of proteins, *MONOCLONAL antibody probes, *GLYCOSYLATED hemoglobin

Abstract

An important aspect in the analytical characterization of protein therapeutics is the comprehensive characterization of higher order structure (HOS). Nuclear magnetic resonance (NMR) is arguably the most sensitive method for fingerprinting HOS of a protein in solution. Traditionally, 1H–15N or 1H–13C correlation spectra are used as a "structural fingerprint" of HOS. Here, we demonstrate that protein fingerprint by line shape enhancement (PROFILE), a 1D 1H NMR spectroscopy fingerprinting approach, is superior to traditional two-dimensional methods using monoclonal antibody samples and a heavily glycosylated protein therapeutic (Epoetin Alfa). PROFILE generates a high resolution structural fingerprint of a therapeutic protein in a fraction of the time required for a 2D NMR experiment. The cross-correlation analysis of PROFILE spectra allows one to distinguish contributions from HOS vs protein heterogeneity, which is difficult to accomplish by 2D NMR. We demonstrate that the major analytical limitation of two-dimensional methods is poor selectivity, which renders these approaches problematic for the purpose of fingerprinting large biological macromolecules. [ABSTRACT FROM AUTHOR]

Published

2015

150. Active immunization with Tocilizumab mimotopes induces specific immune responses.

Author

Lin Yang, Rui Xing, Changhong Li, Yuan Liu, Lin Sun, Xiangyuan Liu, and Yongfu Wang

Subjects

*MONOCLONAL antibody probes, *INTERLEUKIN-6, *PEPTIDES, *IMMUNOASSAY, *CARRIER proteins, *CELL lines

Abstract

Background: Tocilizumab is a humanized monoclonal antibody showing high-affinity binding to both soluble interleukin-6 receptor (sIL-6R) and membrane bound IL-6R (mIL-6R), thereby preventing pro-inflammatory effects of IL-6. However, therapeutic antibodies still have practical limitations. To overcome these limitations, we generated Tocilizumab specific epitope mimics by using the phage display technology and tested whether the peptide mimics could induce similar humoral responses in mice immunized with the peptides. Results: Seven phage mimics were obtained by using phage display peptide library. Four phage mimics (YHTTDKLFYMMR, YSAYEFEYILSS, KTMSAEEFDNWL and LTSHTYRSQADT) were shown to mimic Tocilizumab epitope using immunoassays. The mimotopes were conjugated to immunogenic carrier proteins and used to intraperitoneally immunize BALB/c mice. Sera from the mimotopes immunized mice not only showed specific binding to recombinant IL-6R, but can also IL-6R expressed in Hela, U-937, Jurkat cell lines and in fibroblast-like synoviocytes from patients with RA (FLS-RA). Furthermore, sera from mice immunized with mimotopes-KLH conjugate could reduce the level of phosphorylated- signal transducers and activator of transcription (STAT3), STAT3, phosphorylated- extracellular signal-regulated kinase (Erk) 1/2 and Erk1/2 in HeLa and Jurkat cells. Antibody-dependent cellular cytotoxicity (ADCC) assay showed that antibodies induced by mimotopes-KLH conjugate could elicit specific lysis in Hela and U-937 cells. Conclusions: From phage display library, we successfully isolated four Tocilizumab mimotopes which induced specific humoral and cellular reponses in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2015