Future collider signatures of the possible 750 GeV state

If the recent indications of a possible state I broken vertical bar with mass similar to 750 GeV decaying into two photons reported by ATLAS and CMS in LHC collisions at 13 TeV were to become confirmed, the prospects for future collider physics at the LHC and beyond would be affected radically, as we explore in this paper. Even minimal scenarios for the I broken vertical bar resonance and its gamma gamma decays require additional particles with masses . We consider here two benchmark scenarios that exemplify the range of possibilities: one in which I broken vertical bar is a singlet scalar or pseudoscalar boson whose production and gamma gamma decays are due to loops of coloured and charged fermions, and another benchmark scenario in which I broken vertical bar is a superposition of (nearly) degenerate CP-even and CP-odd Higgs bosons in a (possibly supersymmetric) two-Higgs doublet model also with additional fermions to account for the gamma gamma decay rate. We explore the implications of these benchmark scenarios for the production of I broken vertical bar and its new partners at colliders in future runs of the LHC and beyond, at higher-energy pp colliders and at e (+) e (-) and gamma gamma colliders, with emphasis on the bosonic partners expected in the doublet scenario and the fermionic partners expected in both scenarios.

Mycobacteria-responsive sonic hedgehog signaling mediates programmed death-ligand 1-and prostaglandin E-2-induced regulatory T cell expansion

CD4(+)CD25(+)FoxP3(+) regulatory T cells (Tregs) are exploited by mycobacteria to subvert the protective host immune responses. The Treg expansion in the periphery requires signaling by professional antigen presenting cells and in particularly dendritic cells (DC). However, precise molecular mechanisms by which mycobacteria instruct Treg expansion via DCs are not established. Here we demonstrate that mycobacteria-responsive sonic hedgehog (SHH) signaling in human DCs leads to programmed death ligand-1 (PD-L1) expression and cyclooxygenase (COX)-2-catalyzed prostaglandin E-2 (PGE(2)) that orchestrate mycobacterial infection-induced expansion of Tregs. While SHH-responsive transcription factor GLI1 directly arbitrated COX-2 transcription, specific microRNAs, miR-324-5p and miR-338-5p, which target PD-L1 were downregulated by SHH signaling. Further, counter-regulatory roles of SHH and NOTCH1 signaling during mycobacterial-infection of human DCs was also evident. Together, our results establish that Mycobacterium directs a fine-balance of host signaling pathways and molecular regulators in human DCs to expand Tregs that favour immune evasion of the pathogen.