Copyright
©The Author(s) 2022.
World J Stem Cells. Jul 26, 2022; 14(7): 503-512
Published online Jul 26, 2022. doi: 10.4252/wjsc.v14.i7.503
Published online Jul 26, 2022. doi: 10.4252/wjsc.v14.i7.503
Table 1 The differences between human and mouse pancreatic embryogenesis
| Differences | Mice | Human | Ref. |
| Morphological change | Early separation of foregut from notochord: e8.75 | Delayed separation of foregut from notochord: 4-5 wpc | [58,59] |
| Early formation of tip and trunk of pancreass: e14-e15 | The tip and trunk pancreas form late: 6-8 wpc | [18,60,61] | |
| Late islet formation: Endocrine cells do not aggregate until birth to form islets | Islet formation is early: formation begins at 12 wpc | [62,63] | |
| Expression of transcription factors | PDX1: Early expression, the current intestinal and notochord is still in contact with the expression | PDX1: Late expression, delayed until the foregut and notochord separated from each other | [58,59] |
| NKX2.2: When it was confined to NGN3+ progenitor cells, it was widely expressed in mouse MPPs up to e13 | NKX2.2: This expression does not appear until the cells have differentiated into endocrine lineage in human | [18,64] | |
| SOX17: It was not present in mouse pancreatic epithelial cells | SOX17: Markers specific to the endoderm of the human islet | [65] | |
| Endocrine cell formation | α cells: e8.5 | α cells: 8-9 wpc | [25,62,66] |
| β cells: e10.5-e.12.5 | β cells: 6 wpc | ||
| δ cells: e14.5 | δ cells: 10 wpc | ||
| PP cells: e10.5-e.12.5 | PP cells: 17 wpc |
Table 2 Advantages and disadvantages of different types of stem cell therapy for diabetes
| Cell types | Advantages | Disadvantages | Ref. |
| Embryonic stem cell | High degree of differentiation | ESCs is weak in directional differentiation and difficult to induce | [35,36] |
| There are ethical issues: ESCs are usually allogeneic | |||
| Teratoma, immune rejection and gene mutation may occur after transplantation | |||
| Induced pluripotent stem cell | IPSC technology does not use embryonic or egg cells, so ethical problems are less likely | At present, the differentiation scheme of induced pluripotent stem cells is not mature, and the induction efficiency is low, the stability is poor, and the cost is high | [39] |
| Proprietary stem cells can be made from a patient's own cells, so there is less immune rejection | The use of virus vectors poses security problems | ||
| Adult stem cell | It is easy to achieve targeted differentiation, and some studies have shown that adult stem cells can be used to treat diabetes | The direction of differentiation is limited, not omnipotent | [43,44] |
| After transplantation, the ability of induced differentiated cells to secrete insulin was usually lower than that of normal islet β cells, and the cell survival rate was also lower | |||
| The efficiency of inducing differentiation at different stages is still low based on reprogramming and small molecule screening |
- Citation: Yang L, Hu ZM, Jiang FX, Wang W. Stem cell therapy for insulin-dependent diabetes: Are we still on the road? World J Stem Cells 2022; 14(7): 503-512
- URL: https://www.wjgnet.com/1948-0210/full/v14/i7/503.htm
- DOI: https://dx.doi.org/10.4252/wjsc.v14.i7.503