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Principles of scaffold generation for bioengineering of the ovary and uterus: a study focusing on decellularization

Abstract
Introduction: Cancer therapy often result in fertility problems due to inflicted injury to the reproductive organs. Since most women survive cancer, fertility preservation has become an important consideration during cancer therapy. However, options for young women with blood-related cancers are missing. Papers I-II describe the development and characterization of mouse ovarian scaffolds derived from ovarian extracellular ma-trix (ECM). Such scaffolds may be used for future ovarian bioengineering applications as a supporting matrix for the expansion of immature follicles isolated from young can-cer patients to preserve their fertility. Paper III-IV use the rat model to analyse similar scaffolds for uterus bioengineering applications and evaluate if these scaffolds are im-munologically inert after engraftment. Methods: Three decellularisation protocols based on sodium dodecyl sulfate (SDS) and sodium deoxycholate (SDC) were developed for mouse ovary scaffold production (Pa-per I). Scaffolds were then characterised using histology and quantitative analysis for ECM components. Recellularisation was tested using mesenchymal stem cells (Paper II). Previously established uterus scaffolds were grafted to syngeneic (Paper III) or al-logeneic rats (Paper IV) to investigate if the decellularisation process generated any detrimental damaged associated molecular products (DAMPs; Paper III) and if the al-logeneic recipient’s immune system remained stable after scaffold engraftment (Paper IV). Immunohistochemistry and gene expression analysis with digital droplet PCR was used quantify infiltrating immune cells and expression of proinflammatory signals. Results and conclusions: Paper I developed three novel mouse ovarian scaffolds. The SDS and the SDC protocols were found promising, whereas a protocol based on both detergents were found too aggressive on the ECM. Paper III showed that a mild, yet effective decellularisation protocol generated less amounts of DAMPs, and that this scaffold type also remained the most inert to the recipient’s immune system in an al-logeneic setting (Paper IV).
Parts of work
I. AB Alshaikh, AM Padma, M Dehlin, R Akouri, MJ Song, M Brännström, M Hellström. Decellularization of the mouse ovary: comparison of different scaffold generation protocols for future ovarian bioengineering. J. Ovarian Res. 2019; 12:58.::doi::10.1186/s13048-019-0531-3
 
II. AB Alshaikh, AM Padma, M Dehlin, R Akouri, MJ Song, M Brännström, M Hellström. Decellularisation and recellularisation of the ovary for bioengineering applications: Studies in the mouse. Reprod Biol Endocrinol. 2020 Jul 23;18(1):75. ::doi::10.1186/s12958-020-00630-y
 
III. Padma AM, Alshaikh AB, Song MJ, Akouri R, Oltean M, Brännström M, Hellström M. Decellularisation protocol-dependent DAMPs in rat uterus scaffolds differentially activate the immune response after transplantation. Manuscript under revision for Journal of Tissue Engineering and Regenerative Medicine.
 
IV. Padma AM, Alshaikh AB, Song MJ, Akouri R, Akyürek L, Oltean M, Brännström M, Hellström M. Immune response after allogeneic transplantation of decellularized uterine scaffolds in the rat. Biomed Mater. Under 2nd revision
 
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Clinical Sciences. Department of Obstetrics and Gynecology
Disputation
Fredagen den 18 juni 2021, kl.13.00, Carl Kylberg, Medicinaregatan 9, Göteborg
Date of defence
2021-06-18
E-mail
ahmed.alshaikh@gu.se
URI
http://hdl.handle.net/2077/68068
Collections
  • Doctoral Theses / Doktorsavhandlingar Institutionen för kliniska vetenskaper
  • Doctoral Theses from Sahlgrenska Academy
  • Doctoral Theses from University of Gothenburg / Doktorsavhandlingar från Göteborgs universitet
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Cover (2.403Mb)
Thesis frame (949.3Kb)
Abstract (110.4Kb)
Errata (55.74Kb)
Date
2021-05-27
Author
Alshaikh, Ahmed Baker
Keywords
uterus
ovary
decellularization
recellularization
infertility
tissue engineering
Publication type
Doctoral thesis
ISBN
978-91-8009-356-9 (PRINT)
978-91-8009-357-6 (PDF)
Language
eng
Metadata
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