Themed collection Stem Cells

Guest editors Laura J. Suggs and Kacey G. Marra introduce this Journal of Materials Chemistry B themed issue on stem cells.

This review discusses the considerations and approaches that have been employed for designing biomaterial based cultures for replicating the hematopoietic stem and progenitor cell niche.

Pluripotent stem cell derived liver cells (hepatocytes) represent a promising alternative to primary tissue for biological and clinical applications.

Disease-specific pluripotent stem cells can be derived through genetic manipulation of embryonic stem cells or by reprogramming somatic cells (induced pluripotent stem cells).

This review explores the role of protein sequestration in the stem cell niche and how it has inspired the design of biomaterials that exploit natural protein sequestration to influence stem cell fate.

Recent advancements in materials science and engineering may hold the key to overcoming reproducibility and scalability limitations currently hindering the clinical translation of stem cell therapies.

Analysis of efforts to engineer 3D small-diameter (<6 mm) vascular grafts, indicating the importance of stem cells, co-culture, and pulsatile flow.

Various technologies have been developed to increase oxygen delivery in vivo and enhance the effectiveness of tissue engineering strategies. The article provides an overview of the underlying mechanisms driving these technologies.

Human neural stem cells cultured on laminin and Matrigel under hypoxia significantly increase both the stem cell density and the percentage of activity proliferating cells.

Four low molecular weight gels (LMWGs) with different moduli were fabricated as scaffolds to investigate the differentiation of mesenchymal stem cells (MSCs).

The surface chemistry of materials has an interactive influence on cell behavior.

Inflammatory cytokines lead to capillary network disorganization and secreted factor modulation within human microvascularized engineered adipose tissues.

Micromolded gelatin can be used to engineer laminar human myocardium on microelectrode array chips for electrophysiological studies and drug testing.

A novel biodegradable, biocompatible alginate-PEG hydrogel microwell system was developed with tailorable microwell physical and biochemical properties to control the uniform formation and behavior of three-dimensional multicellular human adipose tissue-derived stem cell spheroids.

While mesenchymal stem cell (MSC)-based strategies for critically-sized bone defect repair hold promise, poor cell survival in vivo remains a significant barrier to the translation of these therapeutics.

Osteoblast differentiation of mesenchymal stem cells is regulated by both soluble factor (e.g., bone morphogenetic proteins (BMP)) and mechanically transduced signaling, but the mechanisms have only been partially elucidated.

Chitoson nanoparticle augmented encapsulated alginate (CNPEA) induces definitive endoderm (DE) differentiation of human embryonic stem cells without growth factor supplementation.

Alginate microbeads incorporating adipose-derived stem cells (ASCs) have potential for delivering viable cells capable of facilitating tissue regeneration.

Three dimensional hydrogels are a promising vehicle for delivery of adult human bone-marrow derived mesenchymal stem cells (hMSCs) for cartilage tissue engineering.

Core–shell HA–silk composite nanoparticles as BMP-2 carriers show superior drug loading capacity and sustained release. The improved osteo-differentiation of stem cells on the carriers suggested a promising approach to designing bioactive nanocarrier systems with enhanced functions.

We report the development of a nanoclay-rich bioactive hydrogel for bone regeneration therapy applications.