2010
DOI: 10.1074/jbc.m109.045187
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Structural Correlates of Antibodies Associated with Acute Reversal of Amyloid β-related Behavioral Deficits in a Mouse Model of Alzheimer Disease

Abstract: Immunotherapy targeting of amyloid ␤ (A␤) peptide in transgenic mouse models of Alzheimer disease (AD) has been widely demonstrated to resolve amyloid deposition as well as associated neuronal, glial, and inflammatory pathologies. These successes have provided the basis for ongoing clinical trials of immunotherapy for treatment of AD in humans. Acute as well as chronic A␤-targeted immunotherapy has also been demonstrated to reverse A␤-related behavioral deficits assessing memory in AD transgenic mouse models. … Show more

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Cited by 38 publications
(64 citation statements)
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References 60 publications
(148 reference statements)
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“…The CDRs of the light chain, on the other hand, displayed a high degree of sequence similarity between all high-affinity antibodies, indicating that A ␤ affinity in general is associated with these regions. This idea is supported by the striking resemblance of the light-chain CDRs of our high-affinity antibodies and the antibodies 10D5 (IgG1), 12A11 (IgG1) and 12B4 (IgG2a), all binding to aa 3-7 of the A ␤ peptide [34,35] as well as the antibodies PFA1 (IgG2a) and PFA2 (IgG2a) [36] , where the CDR sequences differ only by a few amino acids.…”
Section: Discussionsupporting
confidence: 50%
See 1 more Smart Citation
“…The CDRs of the light chain, on the other hand, displayed a high degree of sequence similarity between all high-affinity antibodies, indicating that A ␤ affinity in general is associated with these regions. This idea is supported by the striking resemblance of the light-chain CDRs of our high-affinity antibodies and the antibodies 10D5 (IgG1), 12A11 (IgG1) and 12B4 (IgG2a), all binding to aa 3-7 of the A ␤ peptide [34,35] as well as the antibodies PFA1 (IgG2a) and PFA2 (IgG2a) [36] , where the CDR sequences differ only by a few amino acids.…”
Section: Discussionsupporting
confidence: 50%
“…This is further supported by the similarity between our pan-A ␤ antibody mAb1C3 and the antibody 12A11 (IgG1) [34] . These antibodies bind both monomeric and aggregated A ␤ and share 90% of their CDR sequences in the lightchain CDRs as well as in CDR1 and 2 of the heavy chain [35] . Furthermore, the extreme variability in sequence and length of the heavy-chain CDR3 in all antibodies suggests either that this region is not even in contact with the antigen [33] or that the slight variability in antigen recognition is mainly encoded in this CDR.…”
Section: Discussionmentioning
confidence: 99%
“…1c) and engulf extended polypeptide chains within these cavities. 28,29 These antibodies were also shown to bind their antigens through a combination of positively and negatively charged CDR residues (Fig. 1d).…”
mentioning
confidence: 92%
“…(c) Crystal structure of a fragment antigen binding (Fab) from an antibody that is sequence specific for the Aβ N-terminus (PDB code: 3IFN). 29 Aβ N-terminus is colored green; CDR residues are colored yellow (uncharged), blue (basic), and red (basic). (d) Surface representation of the same Fab fragment using the same color coding as in (c).…”
mentioning
confidence: 99%
“…Please refer to Table 1 for additional crystal and refinement information. The structure was solved using SIR-97 [51] and refined using SHELXL-97 [52]. A direct-methods solution was calculated which provided most non-hydrogen atoms from the E-map.…”
Section: Crystallographic Studiesmentioning
confidence: 99%