Evolutionary Computation

This book presents several recent advances on Evolutionary Computation, specially evolution-based optimization methods and hybrid algorithms for several applications, from optimization and learning to pattern recognition and bioinformatics. This book also presents new algorithms based on several analogies and metafores, where one of them is based on philosophy, specifically on the philosophy of praxis and dialectics. In this book it is also presented interesting applications on bioinformatics, specially the use of particle swarms to discover gene expression patterns in DNA microarrays. Therefore, this book features representative work on the field of evolutionary computation and applied sciences. The intended audience is graduate, undergraduate, researchers, and anyone who wishes to become familiar with the latest research work on this field

Full genome analysis of microglial activation; ramifications of TREM2

Neuroinflammation is a pathological hallmark of Alzheimer's disease (AD) and it is well established that microglia, the brain's resident phagocytes, are pivotal for the immune response observed in AD. In the healthy brain, microglia attack and remove pathogens and cell debris, but have been shown to become reactive in AD. An apparent link between microglia and AD is Amyloid β (Aβ), which accumulates in the plaques observed in the brains of AD patients and has been reported as a microglia activator. Genome Wide Association Studies (GWAS) have allowed the identification of more than 20 genetic risk associations to AD. Many of these associations highlight the importance of immune pathways (and others) in AD. More recently, the identification of mutations in TREM2 (Triggering Receptor Expressed on Myeloid Cells 2), a gene exclusively expressed by microglia in the brain, has brought microglial activation and dysfunction back to the attention of the AD community. The main focus of this study is to understand microglial activation elicited by different stimuli including Aβ1-42 monomers, oligomers and fibrils- with regards to their inflammatory activation status (M1, M2 or other) and whole-genome expression profile. To this end, the mouse-derived BV2 cell line was used to assess gene expression changes during microglial activation. Data shows that M1 and M2 activators alter gene expression of AD-associated genes in a manner that is potentially detrimental for AD progression. A second objective of this thesis was to use the CRISPR/Cas9 gene editing technology for the generation of Trem2-deficient BV2 cell lines. As a result, Trem2 +/- (haploinsufficient) and Trem2 -/- (knockout) BV2 cell lines were generated. Subsequently, these cell lines were characterised in terms of their phagocytic, proliferation, migration, cytokine release capacities and whole genome expression. In consequence, this study provides new and wellcharacterised in vitro models for the study of Trem2 function

2015 GREAT Day Program

SUNY Geneseo’s Ninth Annual GREAT Day.https://knightscholar.geneseo.edu/program-2007/1009/thumbnail.jp

2013 GREAT Day Program

SUNY Geneseo’s Seventh Annual GREAT Day.https://knightscholar.geneseo.edu/program-2007/1007/thumbnail.jp