Probing RNA native conformational ensembles with structural constraints

TY - JOUR

T1 - Probing RNA native conformational ensembles with structural constraints

AU - Fonseca, Rasmus

AU - van den Bedem, Henry

AU - Bernauer, Julie

PY - 2016

Y1 - 2016

N2 - Noncoding ribonucleic acids (RNA) play a critical role in a wide variety of cellular processes, ranging from regulating gene expression to post-translational modification and protein synthesis. Their activity is modulated by highly dynamic exchanges between three-dimensional conformational substates, which are difficult to characterize experimentally and computationally. Here, we present an innovative, entirely kinematic computational procedure to efficiently explore the native ensemble of RNA molecules. Our procedure projects degrees of freedom onto a subspace of conformation space defined by distance constraints in the tertiary structure. The dimensionality reduction enables efficient exploration of conformational space. We show that the conformational distributions obtained with our method broadly sample the conformational landscape observed in NMR experiments. Compared to normal mode analysis-based exploration, our procedure diffuses faster through the experimental ensemble while also accessing conformational substates to greater precision. Our results suggest that conformational sampling with a highly reduced but fully atomistic representation of noncoding RNA expresses key features of their dynamic nature.

AB - Noncoding ribonucleic acids (RNA) play a critical role in a wide variety of cellular processes, ranging from regulating gene expression to post-translational modification and protein synthesis. Their activity is modulated by highly dynamic exchanges between three-dimensional conformational substates, which are difficult to characterize experimentally and computationally. Here, we present an innovative, entirely kinematic computational procedure to efficiently explore the native ensemble of RNA molecules. Our procedure projects degrees of freedom onto a subspace of conformation space defined by distance constraints in the tertiary structure. The dimensionality reduction enables efficient exploration of conformational space. We show that the conformational distributions obtained with our method broadly sample the conformational landscape observed in NMR experiments. Compared to normal mode analysis-based exploration, our procedure diffuses faster through the experimental ensemble while also accessing conformational substates to greater precision. Our results suggest that conformational sampling with a highly reduced but fully atomistic representation of noncoding RNA expresses key features of their dynamic nature.

KW - combinatorial optimization

KW - computational molecular biology

KW - protein folding

UR - http://www.scopus.com/inward/record.url?scp=84969180377&partnerID=8YFLogxK

U2 - 10.1089/cmb.2015.0201

DO - 10.1089/cmb.2015.0201

M3 - Journal article

C2 - 27028235

AN - SCOPUS:84969180377

SN - 1066-5277

VL - 23

SP - 362

EP - 371

JO - Journal of Computational Biology

JF - Journal of Computational Biology

IS - 5

ER -