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2011 | 71 | 1 |

Tytuł artykułu

Biomimetic modulation of cord blood derived stem cells for neural fate control

Warianty tytułu

Języki publikacji

EN

Abstrakty

EN
Bioactive surface domains were applied to investigate cellular developmental processes of human cord blood- derived stem cells and to direct their fate into desired neural lineages. Such domains should represent microenvironmental cues resembling those found in vivo. For that purpose we have created miniaturized cell growth platforms with defined arrays of cell attractive biomaterials serving as functional domains. Emerging technologies applied included a nano/micro-fabrication technique like microcontact printing and piezoelectric (noncontact) microspotting of biomolecules on plasma deposited cell repellent surface. Human Umbilical Cord Blood Neural Stem Cell (HUCB-NSC) line was plated on biodomains at different concentrations and serum conditions. HUCB-NSCs were shown to adhere and differentiate on microarray platforms in a protein type, concentration and cell density dependent manner. Receptor-mediated interactions with extracellular proteins promote neuronal differentiation, while non-specific adhesion to polyaminoacid molecules allows maintaining of stem cells immobilized to the surface in non-differentiated stage. “Smart” functional domains were created by immobilizing to the surface small signaling molecules (e.g wnt, shh, notch or jagged) together with ECM proteins. Stimulation of selected intracellular pathways by signaling molecules resulted in differentiation of HUCB-NSC to either neuronal or astroglial lineage. Miniaturization of such bioengineered active domains combined with appropriate stem cell model may allow application of such stem cell growth platforms for the multiparameter bio-tests and can provide important, additional information on the sensitivity of certain neural stem cell molecular pathways to the selected neurotoxins. Since HUCB-NSC can be cultured and harvested at different developmental stages and was shown to be a good model for developmental toxicity testing, homogenous lineage related pluripotent population is required. For that purpose iPs cells from HUCB-NSC are produced. Sponsored by grant from Polish Ministry of Scientific Research and Higher Education No 0141/B/P01/2008/35, No N N302 597838. and European Commission, JRC.

Słowa kluczowe

Wydawca

-

Rocznik

Tom

71

Numer

1

Opis fizyczny

p.168-169

Twórcy

autor
  • Mossakowski Medical Research Centre, NeuroRepair Department, Polish Academy of Sciences, Warsaw, Poland
autor
  • Mossakowski Medical Research Centre, NeuroRepair Department, Polish Academy of Sciences, Warsaw, Poland

Bibliografia

Typ dokumentu

Bibliografia

Identyfikatory

Identyfikator YADDA

bwmeta1.element.agro-98c03142-91ae-4498-bada-71cde684153b
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