K Lewis scite author profile

K Lewis

5Publications

79Citation Statements Received

31Citation Statements Given

How they've been cited

151

How they cite others

Affiliations

University of Oxford, The Honourable Society of Lincoln's Inn, University of California, Santa Cruz

Publications

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Label-free Imaging of Microtubules with Sub-nm Precision Using Interferometric Scattering Microscopy

Andrecka

Arroyo

Lewis

et al. 2016

Biophysical Journal

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Current in vitro optical studies of microtubule dynamics tend to rely on fluorescent labeling of tubulin, with tracking accuracy thereby limited by the quantum yield of fluorophores and by photobleaching. Here, we demonstrate label-free tracking of microtubules with nanometer precision at kilohertz frame rates using interferometric scattering microscopy (iSCAT). With microtubules tethered to a glass substrate using low-density kinesin, we readily detect sequential 8 nm steps in the microtubule center of mass, characteristic of a single kinesin molecule moving a microtubule. iSCAT also permits dynamic changes in filament length to be measured with <5 nm precision. Using the arbitrarily long observation time enabled by label-free iSCAT imaging, we demonstrate continuous monitoring of microtubule disassembly over a 30 min period. The ability of iSCAT to track microtubules with nm precision together with its potential for label-free single protein detection and simultaneous single molecule fluorescence imaging represent a unique platform for novel approaches to studying microtubule dynamics.

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Studies with monoclonal antibody raised against partially purified oestradiol receptor from human myometrium

King

Coffer

Lewis

1984

Journal of Steroid Biochemistry

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In vivo dimeric association of class I MHC heavy chains. Possible relationship to class I MHC heavy chain-beta 2-microglobulin dissociation.

Capps

Robinson

Lewis

et al. 1993

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Class I MHC molecules have been thought to occur in vivo both as class I MHC heavy chain-beta 2-m heterodimers, which are or are not associated with antigenic peptide, and as free class I MHC heavy chains. Class I MHC molecules are now found also to occur in another type of structure: a heavy chain-heavy chain dimer. Biochemical studies show that heavy chain dimers are disulfide-linked via a conserved cytoplasmic domain cysteine. H-2Ld, H-2Db, and H-2Dd class I dimers fail to react with certain alpha 1 and alpha 2 domain-specific antibodies. Furthermore, although beta 2-m-specific antibodies coprecipitate class I MHC heavy chains, they do not coprecipitate class I MHC heavy chain dimers. Pulse-chase studies show that heavy chain dimer formation occurs at different points in the biosynthesis of class I MHC molecules in beta 2-m+ and beta 2-m- cells: in beta 2-m+ cells, heavy chain dimers form after the class I molecules have traversed the medial Golgi cisternae, whereas in beta 2-m- cells they form immediately. Culturing of beta 2-m+ cells with exogenous beta 2-m prevents the formation of H-2Ld/Db heavy chain dimers. We conclude that dimer formation occurs as a consequence of loss or unavailability of beta 2-m. Class I MHC heavy chain dimerization may provide a mechanism for removal of immunologically dysfunctional molecules.

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Simplified procedure for the detection of antigens by crossed immunoelectrophoresis.

Keyser¹,

Lewis²

1973

J Clin Pathol

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Allergen-specific monoclonal antibodies directed against the major peanut allergens Ara h 1 and Ara h 2

Pomés¹,

Lewis²,

Burks³

et al. 2002

Journal of Allergy and Clinical Immunology

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K Lewis

Label-free Imaging of Microtubules with Sub-nm Precision Using Interferometric Scattering Microscopy

Studies with monoclonal antibody raised against partially purified oestradiol receptor from human myometrium

In vivo dimeric association of class I MHC heavy chains. Possible relationship to class I MHC heavy chain-beta 2-microglobulin dissociation.

Simplified procedure for the detection of antigens by crossed immunoelectrophoresis.

Allergen-specific monoclonal antibodies directed against the major peanut allergens Ara h 1 and Ara h 2

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