1,037 research outputs found
Myeloid derived suppressor cells in multiple myeloma: Preclinical research and translational opportunities
Immunosuppressive cells have been reported to play an important role in tumor progression mainly because of their capability to promote immuneescape, angiogenesis and metastasis. Among them, myeloid derived suppressor cells (MDSCs) have been recently identified as immature myeloid cells, induced by tumor-associated inflammation, able to impair both innate and adaptive immunity. While murine MDSCs are usually identified by the expression of CD11b and Gr-1, human MDSCs represent a more heterogeneous population characterized by the expression of CD33 and CD11b, low or no HLA-DR and variable CD14 and CD15. In particular, the last two may alternatively identify monocyte-like or granulocyte-like MDSC subsets with different immunosuppressive properties. Recently, a substantial increase of MDSCs has been found in peripheral blood and bone marrow (BM) of multiple myeloma (MM) patients with a role in disease progression and/or drug resistance. Preclinical models recapitulating the complexity of the MM-related BM microenvironment (BMM) are major tools for the study of the interactions between MM cells and cells of the BMM (including MDSCs) and for the development of new agents targeting MM-associated immune suppressive cells. This review will focus on current strategies for human MDSCs generation and investigation of their immunosuppressive function in vitro and in vivo, taking into account the relevant relationship occurring within the MM-BMM. We will then provide trends in MDSC-associated research and suggest potential application for the treatment of MM
Mapping thermal inertia, soil moisture and evaporation from aircraft day and night thermal data
There are no author-identified significant results in this report
TELLUS: A combined surface temperature, soil moisture and evaporation mapping approach
There are no author-identified significant results in this report
How well do Car-Parrinello simulations reproduce the Born-Oppenheimer surface ? Theory and Examples
We derive an analytic expression for the average difference between the
forces on the ions in a Car-Parrinello simulation and the forces obtained at
the same ionic positions when the electrons are at their ground state. We show
that for common values of the fictitious electron mass, a systematic bias may
affect the Car-Parrinello forces in systems where the electron-ion coupling is
large. We show that in the limit where the electronic orbitals are rigidly
dragged by the ions the difference between the two dynamics amounts to a
rescaling of the ionic masses, thereby leaving the thermodynamics intact. We
study the examples of crystalline magnesium oxide and crystalline and molten
silicon. We find that for crystalline silicon the errors are very small. For
crystalline MgO the errors are very large but the dynamics can be quite well
corrected within the rigid-ion model. We conclude that it is important to
control the effect of the electron mass parameter on the quantities extracted
from Car-Parrinello simulations.Comment: Submitted to the Journal of Chemical Physic
- …