<i>Reactibodies</i>
            generated by kinetic selection couple chemical reactivity with favorable protein dynamics

Смирнов, Иван; Carletti, E.; Kurkova, I. N.; Nachon, Florian; Nicolet, Yvain; Mitkevich, Vladimir A.; Débat, Hélène; Avalle, Bérangère; Belogurov, Alexey A.; Kuznetsov, Nikita А.; Reshetnyak, Andrey V.; Masson, Patrick; Tonevitsky, Alexander G.; Пономаренко, Н. А.; Makarov, Alexander А.; Friboulet, Alain; Tramontano, Alfonso; Gabibov, Alexander

doi:10.1073/pnas.1108460108

Cited by 50 publications

(57 citation statements)

References 40 publications

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“…Recently, a unique catalytic antibody A17 named a “reactibody” was prepared by Smirnov et al (11) by employing an innovative idea and technique. It could cleave paraoxon and possesses an unusual deep cavity at the interface of V L and V H .…”

Section: Introductionmentioning

confidence: 99%

Biochemical Features of a Catalytic Antibody Light Chain, 22F6, Prepared from Human Lymphocytes

Hifumi

Fujimoto

Arakawa

et al. 2013

Journal of Biological Chemistry

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Background: We explored catalytic antibodies applicable to patients.Results: A human light chain (22F6) possessing both amidase and nuclease activities and preventing infection of influenza virus was obtained.Conclusion: The 22F6 light chain holds a huge potential as a new drug for patient therapies in the future.Significance: The procedure developed in this study is highly noteworthy for developing new drugs.

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Section: Introductionmentioning

confidence: 99%

Biochemical Features of a Catalytic Antibody Light Chain, 22F6, Prepared from Human Lymphocytes

Hifumi

Fujimoto

Arakawa

et al. 2013

Journal of Biological Chemistry

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“…Recent advances have demonstrated that CYP3A4 cooperativity involves the binding of multiple (at least 2) substrate molecules to the binding pocket and represents a case of true allostery characterized by effector-induced conformational transitions (Davydov and Halpert, 2008). On the basis of the above theory and our results, the differential effects of PXT on the metabolism of MDZ, similar to the effectors of citral, 6-gingerol, and D-limonene (Zhang and Lim, 2008), can be explained by a two-site model (Korzekwa et al, 1998;Domanski et al, 2001) or a multi-site model (Kenworthy et al, 2001;Manoj et al, 2010;Smirnov et al, 2011) of CYP3A4. It can be hypothesized that PXT can bind to one defined site that is also occupied by MDZ in the position required for 4-hydroxylation (or 19-hydroxylation) and that both substrates can displace each other.…”

Section: Discussionmentioning

confidence: 87%

Identification of the Active Components in Shenmai Injection that Differentially Affect Cyp3a4-Mediated 1′-Hydroxylation and 4-Hydroxylation of Midazolam

Zeng

Xia

et al. 2013

Drug Metab Dispos

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Shenmai injection (SMI) is a popular herbal preparation that is widely used for the treatment of atherosclerotic coronary heart disease and viral myocarditis. In our previous study, SMI was shown to differentially affect CYP3A4-mediated 19-hydroxylation and 4-hydroxylation of midazolam (MDZ). The present study was conducted to identify the active components in SMI responsible for the differential effects on MDZ metabolism, using in vitro incubation systems (rat and human liver microsomes and a recombinant CYP3A4 system) to measure 19-hydroxylation and 4-hydroxylation of MDZ. First, different fractions of SMI were obtained by gradient elution on an solid phase extraction system and individually tested for their effects on MDZ metabolism. The results demonstrated that lipid-soluble constituents were likely to be the predominant active components of SMI. Second, the possible active components were gradually separated on an high-performance liquid chromatography system under different conditions and individually tested in vitro for their effects on MDZ metabolism. Third, the active component obtained in the above experiment was collected and subjected to structural analysis, and identified as panaxytriol (PXT). Finally, it was validated that PXT had significant differential effects on 19-hydroxylation and 4-hydroxylation of MDZ in various in vitro systems that were similar to those of SMI. We conclude that PXT is the constituent of SMI responsible for the differential effects on CYP3A4-mediated 19-hydroxylation and 4-hydroxylation of MDZ.

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“…The oligonucleotides VH.link (5 -ACT CCC GCC ACC TCC TGA AGA GAC GGT ) and VL.link (5 -GGT GGC GGG AGT GAA ATT GTG CG-3 ) that include overlapping segments were used in order to reduce the original linker [(G 4 S) 3 ] to G 4 S. The conditions for the amplifications, overlapping reaction and cloning into the expression vector pSyn1 were the same as previously described [20].…”

Section: Construction Of Diabody 6009fmentioning

confidence: 99%

“…Antibody engineering technologies have evolved rapidly over the last three decades, and it is now possible to produce a set of different antibody fragments for use in a wide range of applications that avoid the process of immunizing an animal [1][2][3]. Due to their versatility, recombinant antibody fragments have become important tools in research, diagnostics and therapy [4].…”

Section: Introductionmentioning

confidence: 99%

Evaluation of three different formats of a neutralizing single chain human antibody against toxin Cn2: Neutralization capacity versus thermodynamic stability

et al. 2012

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Reactibodies generated by kinetic selection couple chemical reactivity with favorable protein dynamics

Cited by 50 publications

References 40 publications

Biochemical Features of a Catalytic Antibody Light Chain, 22F6, Prepared from Human Lymphocytes

Biochemical Features of a Catalytic Antibody Light Chain, 22F6, Prepared from Human Lymphocytes

Identification of the Active Components in Shenmai Injection that Differentially Affect Cyp3a4-Mediated 1′-Hydroxylation and 4-Hydroxylation of Midazolam

Evaluation of three different formats of a neutralizing single chain human antibody against toxin Cn2: Neutralization capacity versus thermodynamic stability

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