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Crystal growth inhibitors for the prevention of L-cystine kidney stones through molecular design.


ABSTRACT: Crystallization of L-cystine is a critical step in the pathogenesis of cystine kidney stones. Treatments for this disease are somewhat effective but often lead to adverse side effects. Real-time in situ atomic force microscopy (AFM) reveals that L-cystine dimethylester (L-CDME) and L-cystine methylester (L-CME) dramatically reduce the growth velocity of the six symmetry-equivalent {100} steps because of specific binding at the crystal surface, which frustrates the attachment of L-cystine molecules. L-CDME and L-CME produce l-cystine crystals with different habits that reveal distinct binding modes at the crystal surfaces. The AFM observations are mirrored by reduced crystal yield and crystal size in the presence of L-CDME and L-CME, collectively suggesting a new pathway to the prevention of L-cystine stones by rational design of crystal growth inhibitors.

SUBMITTER: Rimer JD 

PROVIDER: S-EPMC5166609 | biostudies-literature | 2010 Oct

REPOSITORIES: biostudies-literature

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Crystal growth inhibitors for the prevention of L-cystine kidney stones through molecular design.

Rimer Jeffrey D JD   An Zhihua Z   Zhu Zina Z   Lee Michael H MH   Goldfarb David S DS   Wesson Jeffrey A JA   Ward Michael D MD  

Science (New York, N.Y.) 20101001 6002


Crystallization of L-cystine is a critical step in the pathogenesis of cystine kidney stones. Treatments for this disease are somewhat effective but often lead to adverse side effects. Real-time in situ atomic force microscopy (AFM) reveals that L-cystine dimethylester (L-CDME) and L-cystine methylester (L-CME) dramatically reduce the growth velocity of the six symmetry-equivalent {100} steps because of specific binding at the crystal surface, which frustrates the attachment of L-cystine molecul  ...[more]

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