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Genetic repair of a human induced pluripotent cell line from patient with Dutch-type cerebral amyloid angiopathy
Vascularized hiPSC-derived 3D cardiac microtissue on chip
ETV2 upregulation marks the specification of early cardiomyocytes and endothelial cells during co-differentiation
ETV2 upregulation marks the specification of early cardiomyocytes and endothelial cells during co-differentiation
Multiplexed fluidic circuit board for controlled perfusion of 3D blood vessels-on-a-chip
On-chip analysis of glycolysis and mitochondrial respiration in human induced pluripotent stem cells
Pressure-driven perfusion system to control, multiplex, and recirculate cell culture medium for organs-on-chips
Vascular defects associated with hereditary hemorrhagic telangiectasia revealed in patient-derived isogenic iPSCs in 3D vessels on chip
Microphysiological stem cell models of the human heart
Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia
Perspectives for future use of cardiac microtissues from human pluripotent stem cells
Rapid prototyping of organ-on-a-chip devices using maskless photolithography
Engineered 3D vessel-on-chip using hiPSC-derived endothelial- and vascular smooth muscle cells
Heart defects recapitulated in human cardioids
Generation, functional analysis and applications of isogenic three-dimensional self-aggregating cardiac microtissues from human pluripotent stem cells
Introductions to the Community: Early-Career Researchers in the Time of COVID-19
Vascular tumor recapitulated in endothelial cells from hiPSCs engineered to express the SERPINE1-FOSB translocation
Fibronectin patches as anchoring points for force sensing and transmission in human induced pluripotent stem cell-derived pericytes
Human-iPSC-derived cardiac stromal cells enhance maturation in 3D cardiac microtissues and reveal non-cardiomyocyte contributions to heart disease
Human-iPSC-derived cardiac stromal cells enhance maturation in 3D cardiac microtissues and reveal non-cardiomyocyte contributions to heart disease

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