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Fan-Tso Chien

Researcher at Academia Sinica

Publications -  12
Citations -  578

Fan-Tso Chien is an academic researcher from Academia Sinica. The author has contributed to research in topics: Chromatin & Force spectroscopy. The author has an hindex of 8, co-authored 12 publications receiving 519 citations. Previous affiliations of Fan-Tso Chien include National Tsing Hua University & Leiden University.

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Single-molecule force spectroscopy reveals a highly compliant helical folding for the 30-nm chromatin fiber

TL;DR: The observed high compliance causes extensive thermal breathing, which forms a physical basis for the balance between DNA condensation and accessibility, and points to a solenoid as the underlying topology of the 30-nm fiber.
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Crystal structure and site-directed mutagenesis studies of N-carbamoyl-D-amino-acid amidohydrolase from Agrobacterium radiobacter reveals a homotetramer and insight into a catalytic cleft.

TL;DR: The homologous active-site framework of these enzymes with distinct structures suggests convergent evolution of a common catalytic mechanism.
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Subpiconewton Dynamic Force Spectroscopy Using Magnetic Tweezers

TL;DR: This method allows application of subpiconewton force and twist control by calibration of the applied force from the height of the magnets, allowing the real-time study of transient structures and reaction intermediates.
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10 years of tension on chromatin: results from single molecule force spectroscopy.

TL;DR: Resolving force induced structural changes of chromatin fibers at the single molecule level will help to provide a physical understanding of processes involving chromatin that occur in vivo and will reveal the mechanical constraints that are relevant for processing and maintenance of DNA in eukaryotes.
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STAT3-coordinated migration facilitates the dissemination of diffuse large B-cell lymphomas.

TL;DR: The authors show that STAT3 controls amoeboid migration in DLBCL via the transcriptional activation of RHOH, which then releases RhoA from RhoGDIγ-mediated suppression, or via regulating microtubule dynamics to activate Rho a.