Dimethyl adipimidate: a new antisickling agent.

Lubin, Bertram H.; Peña, Vı́ctor Alonso de la; Mentzer, William C.; Bymun, Edwin N.; Bradley, Thomas B.; Packer, Lester

doi:10.1073/pnas.72.1.43

Cited by 49 publications

(27 citation statements)

References 14 publications

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“…wt. components were observed as a function of DMA concentration [6]. Contrary to previous results on proteins treated with monofunctional imidoesters at low protein concentrations [2,4,13] high mol.…”

Section: Discussioncontrasting

confidence: 55%

“…Imidoesters would appear to be appropriate reagents for this purpose since they have been shown to react selectively with protein amino groups [2,3]. MAI* was employed for the initial in vitro studies because: (1) modification of protein amino groups reportedly does not alter the charge of the protein at physiological pH [4] ; (2) reaction of hemoglobin A with MAI does not appreciably affect co-operativity or the Bohr effect [5] ; (3) DMA, a bifunctional imidoester, has been shown to inhibit sickling [6] ; (4) MAI is the smallest imidoester and therefore should introduce less steric obstruction than any other imidoester.…”

Section: Introductionmentioning

confidence: 99%

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Inhibition of sickling by methyl acetimidate

1976

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Section: Discussioncontrasting

confidence: 55%

Section: Introductionmentioning

confidence: 99%

Inhibition of sickling by methyl acetimidate

1976

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“…One particularly interesting application utilizing the mild nature of amidination involves the use of another bifunctional imidate, dimethyl adipimidate, to modify human sickle erythrocytes. Although these treated cells do not display hypoxiainduced sickling, they show little alteration of both rheological and metabolic properties (18).…”

Section: Discussionmentioning

confidence: 99%

Effect of crosslinking on mitochondrial structure and function

Tinberg¹,

Lee²,

Packer

1975

J Supramol Struct

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Rat liver mitochondria were treated with ethylacetimidate and methylbutyrimidate, monofunctional imidates, and with dimethylsuberimidate, a bifunctional imidate, and the effects on structure and function studied. Mitochondria treated with 5 mM dimethylsuberimidate or greater did not respond osmotically when placed in deionized water. Sodium dodecylsulfate‐polyacrylamide gel electrophoresis revealed that at concentrations > 5 mM dimethylsuberimidate nearly all mitochondrial polypeptides failed to enter 6% gels, indicating crosslinking of both membrane and soluble proteins. Extensive amidination by ethylacetimidate and methylbutyrimidate had little effect on ascorbate‐tetramethylphenylenediamine oxidase while extensive inhibition resulted from dimethylsuberimidate treatment. The possible involvement of molecular motion in electron transport is discussed.

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“…It has occurred to a number of investigators that the aggregation of deoxy Hb S might be inhibited by chemical modification of the protein (6)(7)(8)(9)(10)(11). Of the different functional groups in the side chains of this protein, the amino group seems particularly attractive because it can be modified with relatively mild reagents that might be pharmacologically acceptable.…”

mentioning

confidence: 99%

Alternative aspirins as antisickling agents: acetyl-3,5-dibromosalicylic acid.

Walder¹,

Zaugg²,

Iwaoka³

et al. 1977

Proc. Natl. Acad. Sci. U.S.A.

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Acetyl-3,5-dibromosalicylic acid (dibromoas irin) is shown to be a potent acylating agent of intracellular hemoglobin in vitro. Transfer of the actyl group of dibromoaspirin to amino groups of hemoglobins A and S seems to occur predominantly at just two or three sites on these proteins. This acetylation produces moderate increases in the oxygen affinities of normal and sickle erythrocytes. Furthermore, treatment of intracellular hemoglobin S with dibromoaspirin directly inhibits erythrocyte sickling. This antisickling effect is paralleled by an increase in the minimum gelling concentration of deoxy hemoglobin S extracted from sickle erthrocytes that had been exposed to low concentrations of dibromoaspirin. These observations suggest that dibromoaspirin might be an effective antisickling agent in vivo.

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Dimethyl adipimidate: a new antisickling agent.

Cited by 49 publications

References 14 publications

Inhibition of sickling by methyl acetimidate

Inhibition of sickling by methyl acetimidate

Effect of crosslinking on mitochondrial structure and function

Alternative aspirins as antisickling agents: acetyl-3,5-dibromosalicylic acid.

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