46 research outputs found
Magnetoconductivity of quantum wires with elastic and inelastic scattering
We use a Boltzmann equation to determine the magnetoconductivity of quantum
wires. The presence of a confining potential in addition to the magnetic field
removes the degeneracy of the Landau levels and allows one to associate a group
velocity with each single-particle state. The distribution function describing
the occupation of these single-particle states satisfies a Boltzmann equation,
which may be solved exactly in the case of impurity scattering. In the case
where the electrons scatter against both phonons and impurities we solve
numerically - and in certain limits analytically - the integral equation for
the distribution function, and determine the conductivity as a function of
temperature and magnetic field. The magnetoconductivity exhibits a maximum at a
temperature, which depends on the relative strength of the impurity and
electron-phonon scattering, and shows oscillations when the Fermi energy or the
magnetic field is varied.Comment: 21 pages (revtex 3.0), 5 postscript figures available upon request at
[email protected] or [email protected]
A Realistic Radiative Fermion Mass Hierarchy in Non-supersymmetric SO(10)
A non-supersymmetric grand unified theory can exhibit a "radiative fermion
mass hierarchy", in which the heavier quarks and leptons get mass at tree level
and the lighter ones get mass from loop diagrams. Recently the first predictive
model of this type was proposed. Here it is analyzed numerically and it is
shown to give an excellent fit to the quark and lepton masses and mixings,
including the CP phase violating phase . A relation between the
neutrino angle and the atmospheric neutrino angle is obtainedComment: 13 pages, 4 figures, RevTeX
Targeted Therapy Resistance Mediated by Dynamic Regulation of Extrachromosomal Mutant EGFR DNA
Intratumoral heterogeneity contributes to cancer drug resistance, but the underlying mechanisms are not understood. Single-cell analyses of patient-derived models and clinical samples from glioblastoma patients treated with epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) demonstrate that tumor cells reversibly up-regulate or suppress mutant EGFR expression, conferring distinct cellular phenotypes to reach an optimal equilibrium for growth. Resistance to EGFR TKIs is shown to occur by elimination of mutant EGFR from extrachromosomal DNA. After drug withdrawal, reemergence of clonal EGFR mutations on extrachromosomal DNA follows. These results indicate a highly specific, dynamic, and adaptive route by which cancers can evade therapies that target oncogenes maintained on extrachromosomal DNA
Various aspects of quantum Hall effect
SIGLEAvailable from British Library Document Supply Centre- DSC:D60702 / BLDSC - British Library Document Supply CentreGBUnited Kingdo
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Large-scale assessment of the gliomasphere model system.
BackgroundGliomasphere cultures are widely utilized for the study of glioblastoma (GBM). However, this model system is not well characterized, and the utility of current classification methods is not clear.MethodsWe used 71 gliomasphere cultures from 68 individuals. Using gene expression-based classification, we performed unsupervised clustering and associated gene expression with gliomasphere phenotypes and patient survival.ResultsSome aspects of the gene expression-based classification method were robust because the gliomasphere cultures retained their classification over many passages, and IDH1 mutant gliomaspheres were all proneural. While gene expression of a subset of gliomasphere cultures was more like the parent tumor than any other tumor, gliomaspheres did not always harbor the same classification as their parent tumor. Classification was not associated with whether a sphere culture was derived from primary or recurrent GBM or associated with the presence of EGFR amplification or rearrangement. Unsupervised clustering of gliomasphere gene expression distinguished 2 general categories (mesenchymal and nonmesenchymal), while multidimensional scaling distinguished 3 main groups and a fourth minor group. Unbiased approaches revealed that PI3Kinase, protein kinase A, mTOR, ERK, Integrin, and beta-catenin pathways were associated with in vitro measures of proliferation and sphere formation. Associating gene expression with gliomasphere phenotypes and patient outcome, we identified genes not previously associated with GBM: PTGR1, which suppresses proliferation, and EFEMP2 and LGALS8, which promote cell proliferation.ConclusionsThis comprehensive assessment reveals advantages and limitations of using gliomaspheres to model GBM biology, and provides a novel strategy for selecting genes for future study
Large-scale assessment of the gliomasphere model system
BACKGROUND: Gliomasphere cultures are widely utilized for the study of glioblastoma (GBM). However, this model system is not well characterized, and the utility of current classification methods is not clear. METHODS: We used 71 gliomasphere cultures from 68 individuals. Using gene expression-based classification, we performed unsupervised clustering and associated gene expression with gliomasphere phenotypes and patient survival. RESULTS: Some aspects of the gene expression-based classification method were robust because the gliomasphere cultures retained their classification over many passages, and IDH1 mutant gliomaspheres were all proneural. While gene expression of a subset of gliomasphere cultures was more like the parent tumor than any other tumor, gliomaspheres did not always harbor the same classification as their parent tumor. Classification was not associated with whether a sphere culture was derived from primary or recurrent GBM or associated with the presence of EGFR amplification or rearrangement. Unsupervised clustering of gliomasphere gene expression distinguished 2 general categories (mesenchymal and nonmesenchymal), while multidimensional scaling distinguished 3 main groups and a fourth minor group. Unbiased approaches revealed that PI3Kinase, protein kinase A, mTOR, ERK, Integrin, and beta-catenin pathways were associated with in vitro measures of proliferation and sphere formation. Associating gene expression with gliomasphere phenotypes and patient outcome, we identified genes not previously associated with GBM: PTGR1, which suppresses proliferation, and EFEMP2 and LGALS8, which promote cell proliferation. CONCLUSIONS: This comprehensive assessment reveals advantages and limitations of using gliomaspheres to model GBM biology, and provides a novel strategy for selecting genes for future study