2016
DOI: 10.1074/jbc.m116.732180
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Insulin Mimetic Peptide Disrupts the Primary Binding Site of the Insulin Receptor

Abstract: Sets of synthetic peptides that interact with the insulin receptor ectodomain have been discovered by phage display and reported in the literature. These peptides were grouped into three classes termed Site 1, Site 2, and Site 3 based on their mutual competition of binding to the receptor. Further refinement has yielded, in particular, a 36-residue Site 2-Site 1 fusion peptide, S519, that binds the insulin receptor with subnanomolar affinity and exhibits agonist activity in both lipogenesis and glucose uptake … Show more

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Cited by 33 publications
(38 citation statements)
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“…In terms of the buried surface area and shape complementarity of the TAR-TBP6.7 interface, a total of 718 Å 2 of TAR is sequestered, wherein 384 Å 2 is attributable to the ␤2-␤3 loop. Recognition of TAR by TBP6.7 gives an S c value of 0.79 (77), which is comparable with S c values of peptides selected by phage display to bind the insulin receptor ectodomain (136). Overall, these properties closely resemble comparable metrics for the BIV and HIV TAR-Tat complexes (Fig.…”
Section: Lab-evolved Proteins For Hiv-1 Tar Recognitionsupporting
confidence: 61%
“…In terms of the buried surface area and shape complementarity of the TAR-TBP6.7 interface, a total of 718 Å 2 of TAR is sequestered, wherein 384 Å 2 is attributable to the ␤2-␤3 loop. Recognition of TAR by TBP6.7 gives an S c value of 0.79 (77), which is comparable with S c values of peptides selected by phage display to bind the insulin receptor ectodomain (136). Overall, these properties closely resemble comparable metrics for the BIV and HIV TAR-Tat complexes (Fig.…”
Section: Lab-evolved Proteins For Hiv-1 Tar Recognitionsupporting
confidence: 61%
“…Given steric constraints on α CT and its displacement on insulin binding, our models outlined above collectively suggest that in the IR ectodomain S371 binds to L1 in a conformation similar to that of α CT in its apo or displaced positions. These conclusions are consistent with a recently reported crystallographic structure of the mimetic peptide S519C16 (the C‐terminal 16‐residue Site 1 component of S519 that is identical to S371) in complex with a fragment of the IR ectodomain that contains the L1 domain . We show a snapshot of the S519C16/L1 complex in Fig.…”
Section: Discussionsupporting
confidence: 92%
“…As S371 is added to the C‐terminus of the affinity‐optimized agonist S519, we speculate that the Site 2 part of S519 likely folds into short helical motifs similar to the A‐chain of insulin, particularly given that the Site 2 sequence also contains a disulfide bond . Some tentative modeling of the Site 2 sequence in a recent study supports this suggestion . Conversely, S371 is added at the N‐terminus of antagonist S661 and in case it occupies the position of the insulin B‐chain (as shown in Fig.…”
Section: Discussionmentioning
confidence: 72%
“…IRΔβ-zip (Supplementary Table 1 ) was purified by insulin elution from an insulin-affinity column, then complexed with the variable domain module (Fv) of the anti-IR antibody 83-7 12 , and finally subjected to mild endoglycosidase H treatment—the latter two steps initially intended to aid crystallographic study of the complex 13 . Insulin remained bound to IRΔβ-zip throughout these steps (see Methods and Supplementary Fig.…”
Section: Resultsmentioning
confidence: 99%
“…Fv 83-7 was prepared using a Brevibacillus expression system using protocols identical to those described previously 13 . Briefly, codon- and expression-optimised DNA corresponding to murine monoclonal antibody 83-7 variable heavy (VH) chain residues 1-118 5 , 6 , 12 followed by the sequence SLVPRGSSSEQKLISEEDLN (thrombin cleavage site + c-myc tag) was synthesized and then cloned into the vector pCDNA3.1 by DNA2.0 (USA).…”
Section: Methodsmentioning
confidence: 99%