29 research outputs found

    Spin, Statistics, and Reflections, II. Lorentz Invariance

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    The analysis of the relation between modular P1_1CT-symmetry -- a consequence of the Unruh effect -- and Pauli's spin-statistics relation is continued. The result in the predecessor to this article is extended to the Lorentz symmetric situation. A model \G_L of the universal covering \widetilde{L_+^\uparrow}\cong SL(2,\complex) of the restricted Lorentz group L+↑L_+^\uparrow is modelled as a reflection group at the classical level. Based on this picture, a representation of \G_L is constructed from pairs of modular P1_1CT-conjugations, and this representation can easily be verified to satisfy the spin-statistics relation

    From spin groups and modular P(1)CT symmetry to covariant representations and the spin-statistics theorem

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    Genetic Heterogeneity of MET-Aberrant NSCLC and Its Impact on the Outcome of Immunotherapy

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    Introduction: Robust data on the outcome of MET-aberrant NSCLC with nontargeted therapies are limited, especially in consideration of the heterogeneity of MET-amplified tumors (METamp). Methods: A total of 337 tumor specimens of patients with MET-altered Union for International Cancer Control stage IIIB/IV NSCLC were analyzed using next-generation sequencing, fluorescence in situ hybridization, and immunohistochemistry. The evaluation focused on the type of MET aberration, co-occurring mutations, programmed death-ligand 1 expression, and overall survival (OS). Results: METamp tumors (n = 278) had a high frequency of co-occurring mutations (>80% for all amplification levels), whereas 57.6% of the 59 patients with MET gene and exon 14 (METex14) tumors had no additional mutations. In the METamp tumors, with increasing gene copy number (GCN), the frequency of inactivating TP53 mutations increased (GCN 10: 76.5%), whereas the frequency of KRAS mutations decreased (GCN 10: 11.8%). A total of 10.1% of all the METamp tumors with a GCN > 10 had a significant worse OS (4.0 mo; 95% CI: 1.9-6.0) compared with the tumors with GCN 10, and METamp GCN 10 subgroup. (c) 2020 Published by Elsevier Inc. on behalf of International Association for the Study of Lung Cancer
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