| Literature DB >> 27346000 |
Cristian Miere1, Heema Hewitson1, Liani Devito1, Victoria Wood1, Neli Kadeva1, Glenda Cornwell1, Stefano Codognotto1, Emma Stephenson1, Dusko Ilic2.
Abstract
The KCL018 human embryonic stem cell line was derived from an embryo donated for research that carried an autosomal dominant mutation affecting one allele of the DMPK gene encoding the dystrophia myotonica protein kinase (2200 trinucleotide repeats; 14 for the normal allele). The ICM was isolated using laser microsurgery and plated on γ-irradiated human foreskin fibroblasts. Both the derivation and cell line propagation were performed in an animal product-free environment. Pluripotent state and differentiation potential were confirmed by in vitro assays.Entities:
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Year: 2016 PMID: 27346000 PMCID: PMC4823665 DOI: 10.1016/j.scr.2016.01.004
Source DB: PubMed Journal: Stem Cell Res ISSN: 1873-5061 Impact factor: 2.020
| Name of stem cell line | KCL018 |
| Institution | King's College London, London UK |
| Derivation team | Neli Kadeva, Victoria Wood, Glenda Cornwell, Stefano Codognotto, Emma Stephenson |
| Contact person and email | Dusko Ilic, email: |
| Type of resource | Biological reagent: cell line |
| Sub-type | Human pluripotent stem cell line |
| Origin | Human embryo |
| Key marker expression | Pluripotent stem cell markers: NANOG, OCT4, TRA-1-60, TRA-1-81, alkaline phosphatase (AP) activity |
| Authentication | Identity and purity of line confirmed |
| Link to related literature (direct URL links and full references) | Ilic, D., Stephenson, E., Wood, V., Jacquet, L., Stevenson, D., Petrova, A., Kadeva, N., Codognotto, S., Patel, H., Semple, M., Cornwell, G., Ogilvie, C., Braude, P., 2012. Derivation and feeder-free propagation of human embryonic stem cells under xeno-free conditions. Cytotherapy. 14 (1), 122–128. Stephenson, E., Jacquet, L., Miere, C., Wood, V., Kadeva, N., Cornwell, G., Codognotto, S., Dajani, Y., Braude, P., Ilic, D., 2012. Derivation and propagation of human embryonic stem cell lines from frozen embryos in an animal product-free environment. Nat. Protoc. 7 (7), 1366–1381. |
| Information in public databases | KCL018 is a National Institutes of Health (NIH) registered hESC line |
| Ethics | The hESC line KCL018 is derived under license from the UK Human Fertilisation and Embryology Authority (research license numbers: R0075 and R0133) and also has local ethical approval (UK National Health Service Research Ethics Committee Reference: 06/Q0702/90). |
| Consent signed | Aug 12, 2009 |
| Embryo thawed | Aug 23, 2009 |
| UK Stem Cell Bank Deposit Approval | Sep 23, 2010 |
| Sex | Female 46, XX |
| Grade | Research |
| Disease status | Mutation affecting one allele of the |
| Karyotype (aCGH) | No copy number changes detected |
| DNA fingerprint | Allele sizes (in bp) of 17 microsatellite markers specific for chromosomes 13, 18 and 21 ( |
| Viability testing | Pass |
| Pluripotent markers | NANOG, OCT4, TRA-1-60, TRA-1-81, AP activity ( |
| Three germ layers differentiation in vitro | Endoderm: AFP (α-fetoprotein); Ectoderm: TUBB3 (tubulin, β3 class III); Mesoderm: ACTA2 (actin, α2, smooth muscle) ( |
| Sibling lines available | No |
| Chr | Marker | Allele 1 | Allele 2 |
|---|---|---|---|
| 13 | D13S252 | 299 | 299 |
| D13S305 | 443 | 458 | |
| D13S325 | 289 | 297 | |
| D13S628 | 429 | 450 | |
| D13S634 | 397 | 417 | |
| 18 | D18S386 | 383 | 386 |
| D18S390 | 372 | 372 | |
| D18S391 | 209 | 217 | |
| D18S535 | 482 | 486 | |
| D18S819 | 408 | 424 | |
| D18S976 | 479 | 479 | |
| D18S978 | 219 | 219 | |
| 21 | D21S11 | 244 | 251 |
| D21S1409 | 216 | 224 | |
| D21S1411 | 308 | 308 | |
| D21S1435 | 184 | 188 | |
| D21S1437 | 331 | 335 |