𝔖 Bobbio Scriptorium
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Effect of crosslinking on mitochondrial structure and function

✍ Scribed by Tinberg, Harold M. ;Lee, Calvin ;Packer, Lester


Publisher
Wiley (John Wiley & Sons)
Year
1975
Tongue
English
Weight
432 KB
Volume
3
Category
Article
ISSN
0091-7419

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✦ Synopsis


Abstract

Rat liver mitochondria were treated with ethylacetimidateAbbreviations: SDS, sodium dodecylsulfate; DMS, dimethylsuberimidate; EA, ethylacetimidate; MBI, methylbutyrimidate; TMPD, N, N′, N′‐tetramethyl‐p‐phenylenediamine.

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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