Abstract
To date, selective cell transplantation has involved injecting cell suspensions into tissues or the vascular system. This study describes attaching cell preparations to bioerodable artificial polymers in cell culture and then implanting this polymer-cell scaffold into animals. Using standard techniques of cell harvest, single cells and clusters of fetal and adult rat and mouse hepatocytes, pancreatic islet cells, and small intestinal cells have been seeded onto biogegradable polymers of polyglactin 910, polyanhydrides, and polyorthoester. Sixty-five fetuses and 14 adult animals served as donors. One hundred fifteen polymer scaffolds were implanted into 70 recipient animals: 66 seeded with hepatocytes; 23 with intestinal cells and clusters; and 26 with pancreatic islet preparations. The cells remained viable in culture, and in the case of fetal intestine and fetal hepatocytes, appeared to proliferate while on the polymer. After four days in culture, the cell-polymer scaffolds were implanted into host animals, either in the omentum, the interscapular fat pad, or the mesentery. In three cases of fetal intestinal implantation coupled with partial hepatectomy, successful engraftment. occurred in the omentum, one forming a visible 6.0 mm cyst. Three cases of hepatocyte implantation, one using adult cells and two using fetal cells, have also engrafted, showing viability of hepatocytes, mitotic figures, and vascularization of the cell mass. To date, no pancreatic islets have survived implantation. This method of cell transplantation, which we have termed "chimeric neomorphogenesis," is an alternative to current methods and requires further study.
| Original language | English |
|---|---|
| Pages (from-to) | 3-9 |
| Number of pages | 7 |
| Journal | Journal of Pediatric Surgery |
| Volume | 23 |
| Issue number | 1 |
| DOIs | |
| State | Published - Jan 1988 |
Bibliographical note
Funding Information:From the Departments of Surgery and Pathology, The Children's Hospital and the Harvard Medical School, Boston, and the Department of Applied Biological Sciences, Massachusetts Institute of Technology, Cambridge. Supported by the March of Dimes Grant No. 5-543, Basil O'Connor Starter Research Grant, and NIH Grant No. 6M 26698. Presented at the 18th Annual Meeting of the American Pediatric Surgical Association, Hilton Head Island, South Carolina, May 6-9, 1987. Address reprint requests to Joseph P. Vacanti, MD, The Children's Hospital, 300 Longwood Ave, Fegan Building, Fifth Floor, Boston, MA 02115. © 1988 by Grune & Stratton, Inc. 0022-3468/88/2301-0002503.00/0
Funding
From the Departments of Surgery and Pathology, The Children's Hospital and the Harvard Medical School, Boston, and the Department of Applied Biological Sciences, Massachusetts Institute of Technology, Cambridge. Supported by the March of Dimes Grant No. 5-543, Basil O'Connor Starter Research Grant, and NIH Grant No. 6M 26698. Presented at the 18th Annual Meeting of the American Pediatric Surgical Association, Hilton Head Island, South Carolina, May 6-9, 1987. Address reprint requests to Joseph P. Vacanti, MD, The Children's Hospital, 300 Longwood Ave, Fegan Building, Fifth Floor, Boston, MA 02115. © 1988 by Grune & Stratton, Inc. 0022-3468/88/2301-0002503.00/0
| Funders | Funder number |
|---|---|
| National Institutes of Health | 6M 26698 |
| March of Dimes Foundation | 5-543 |
Keywords
- Transplantation
- cell culture
- fetal cell transplantation