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Immunotherapeutic activity of a conjugate of a Toll-like receptor 7 ligand
by
Takabayashi, Kenji
, Wu, Christina C.N
, Cottam, Howard B
, Sabet, Mojgan
, Smee, Donald F
, Hayashi, Tomoko
, Guiney, Donald D
, Carson, Dennis A
in
adverse effects
/ Agonists
/ Aldehydes - chemistry
/ Animals
/ Antagonist drugs
/ Bacillus anthracis
/ benzaldehyde
/ Biological Sciences
/ blood serum
/ Bone marrow
/ Bronchoalveolar Lavage Fluid
/ Chemical synthesis
/ Cytokines
/ disease models
/ Dose-Response Relationship, Drug
/ Drug Delivery Systems
/ Drug Design
/ Drug therapy
/ Female
/ H1N1 subtype influenza A virus
/ humans
/ hydrazine
/ immunotherapy
/ Immunotherapy - instrumentation
/ Immunotherapy - methods
/ Infections
/ Infectious diseases
/ Influenza A virus
/ Ligands
/ Lung - metabolism
/ Lungs
/ macrophages
/ Mice
/ Mice, Inbred BALB C
/ Mice, Inbred C57BL
/ Models, Chemical
/ Molecules
/ mononuclear leukocytes
/ mortality
/ Rodents
/ serum albumin
/ Serum Albumin - metabolism
/ Side effects
/ Sodium
/ Spores
/ Toll-like receptor 7
/ Toll-Like Receptor 7 - metabolism
/ toxicity
/ Viruses
2007
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Immunotherapeutic activity of a conjugate of a Toll-like receptor 7 ligand
by
Takabayashi, Kenji
, Wu, Christina C.N
, Cottam, Howard B
, Sabet, Mojgan
, Smee, Donald F
, Hayashi, Tomoko
, Guiney, Donald D
, Carson, Dennis A
in
adverse effects
/ Agonists
/ Aldehydes - chemistry
/ Animals
/ Antagonist drugs
/ Bacillus anthracis
/ benzaldehyde
/ Biological Sciences
/ blood serum
/ Bone marrow
/ Bronchoalveolar Lavage Fluid
/ Chemical synthesis
/ Cytokines
/ disease models
/ Dose-Response Relationship, Drug
/ Drug Delivery Systems
/ Drug Design
/ Drug therapy
/ Female
/ H1N1 subtype influenza A virus
/ humans
/ hydrazine
/ immunotherapy
/ Immunotherapy - instrumentation
/ Immunotherapy - methods
/ Infections
/ Infectious diseases
/ Influenza A virus
/ Ligands
/ Lung - metabolism
/ Lungs
/ macrophages
/ Mice
/ Mice, Inbred BALB C
/ Mice, Inbred C57BL
/ Models, Chemical
/ Molecules
/ mononuclear leukocytes
/ mortality
/ Rodents
/ serum albumin
/ Serum Albumin - metabolism
/ Side effects
/ Sodium
/ Spores
/ Toll-like receptor 7
/ Toll-Like Receptor 7 - metabolism
/ toxicity
/ Viruses
2007
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Immunotherapeutic activity of a conjugate of a Toll-like receptor 7 ligand
by
Takabayashi, Kenji
, Wu, Christina C.N
, Cottam, Howard B
, Sabet, Mojgan
, Smee, Donald F
, Hayashi, Tomoko
, Guiney, Donald D
, Carson, Dennis A
in
adverse effects
/ Agonists
/ Aldehydes - chemistry
/ Animals
/ Antagonist drugs
/ Bacillus anthracis
/ benzaldehyde
/ Biological Sciences
/ blood serum
/ Bone marrow
/ Bronchoalveolar Lavage Fluid
/ Chemical synthesis
/ Cytokines
/ disease models
/ Dose-Response Relationship, Drug
/ Drug Delivery Systems
/ Drug Design
/ Drug therapy
/ Female
/ H1N1 subtype influenza A virus
/ humans
/ hydrazine
/ immunotherapy
/ Immunotherapy - instrumentation
/ Immunotherapy - methods
/ Infections
/ Infectious diseases
/ Influenza A virus
/ Ligands
/ Lung - metabolism
/ Lungs
/ macrophages
/ Mice
/ Mice, Inbred BALB C
/ Mice, Inbred C57BL
/ Models, Chemical
/ Molecules
/ mononuclear leukocytes
/ mortality
/ Rodents
/ serum albumin
/ Serum Albumin - metabolism
/ Side effects
/ Sodium
/ Spores
/ Toll-like receptor 7
/ Toll-Like Receptor 7 - metabolism
/ toxicity
/ Viruses
2007
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Immunotherapeutic activity of a conjugate of a Toll-like receptor 7 ligand
Journal Article
Immunotherapeutic activity of a conjugate of a Toll-like receptor 7 ligand
2007
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Overview
The immunotherapeutic activity of Toll-like receptor (TLR) activators has been difficult to exploit because of side effects related to the release and systemic dispersion of proinflammatory cytokines. To overcome this barrier, we have synthesized a versatile TLR7 agonist, 4-[6-amino-8-hydroxy-2-(2-methoxyethoxy)purin-9-ylmethyl]benzaldehyde (UC-1V150), bearing a free aldehyde that could be coupled to many different auxiliary chemical entities through a linker molecule with a hydrazine or amino group without any loss of activity. UC-1V150 was covalently coupled to mouse serum albumin (MSA) at a 5:1 molar ratio to yield a stable molecule with a characteristically altered UV spectrum. Compared with the unconjugated TLR7 agonist, the UC-1V150/MSA was a 10- to 100-fold more potent inducer of cytokine productionin vitro by mouse bone marrow-derived macrophage and human peripheral blood mononuclear cells. When administrated to the lung, the conjugate induced a prolonged local release of cytokines at levels 10-fold or more higher than those found in serum. Under the same conditions, the untethered TLR7 ligand induced quick systemic cytokine release with resultant toxicity. In addition, two pulmonary infectious disease models were investigated wherein mice were pretreated with the conjugate and then challenged with either Bacillus anthracis spores or H1N1 influenza A virus. Significant delay in mortality was observed in both disease models with UC-1V150/MSA-pretreated mice, indicating the potential usefulness of the conjugate as a localized and targeted immunotherapeutic agent.
Publisher
National Academy of Sciences,National Acad Sciences
Subject
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