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An example of a Gastruloid formed from Brachyury::GFP mouse ESCs, treated with a pulse of the Wnt/β-Catenin agonist CHIR99021 between 48 and 72h and imaged by wide-field fluorescence microscopy at 120h. Notice the polarised expression of Brachyury::GFP (Bra) at the elongating tip of the Gastruloid. Image from van den Brink et al. (2014), used with CC-BY licence.

Gastruloids are three dimensional aggregates of embryonic stem cells (ESCs) that, when cultured in specific conditions, exhibit an organization resembling that of an embryo. They develop with three orthogonal axes and contain the primordial cells for various tissues derived from the three germ layers, without the presence of extraembryonic tissues. Notably, they do not possess forebrain, midbrain, and hindbrain structures. Gastruloids serve as a valuable model system for studying mammalian development, including human development, as well as diseases associated with it. They are a model system an embryonic organoid for the study of mammalian development (including humans) and disease. [1] [2] [3]

Background

The Gastruloid model system draws its origins from work by Marikawa et al.. [4] In that study, small numbers of mouse P19 embryonal carcinoma (EC) cells, were aggregated as embryoid bodies (EBs) and used to model and investigate the processes involved in anteroposterior polarity and the formation of a primitive streak region. [4] In this work, the EBs were able to organise themselves into structures with polarised gene expression, axial elongation/organisation and up-regulation of posterior mesodermal markers. This was in stark contrast to work using EBs from mouse ESCs, which had shown some polarisation of gene expression in a small number of cases but no further development of the multicellular system. [5] [6]

Following this study, the Martinez Arias laboratory in the Department of Genetics at the University of Cambridge demonstrated how aggregates of mouse embryonic stem cells (ESCs) were able to generate structures that exhibited collective behaviours with striking similarity to those during early development such as symmetry-breaking (in terms of gene expression), axial elongation and germ-layer specification. [1] [2] [3] To quote from the original paper: "Altogether, these observations further emphasize the similarity between the processes that we have uncovered here and the events in the embryo. The movements are related to those of cells in gastrulating embryos and for this reason we term these aggregates ‘gastruloids’". As noted by the authors of this protocol, a crucial difference between this culture method and previous work with mouse EBs was the use of small numbers of cells which may be important for generating the correct length scale for patterning, and the use of culture conditions derived from directed differentiation of ESCs in adherent culture [1] [7] [3] [2] [8]

Brachyury (T/Bra), a gene which marks the primitive streak and the site of gastrulation, is up-regulated in the Gastruloids following a pulse of the Wnt/β-Catenin agonist CHIR99021 [9] (Chi; other factors have also been tested [1]) and becomes regionalised to the elongating tip of the Gastruloid. From or near the region expressing T/Bra, cells expressing the mesodermal marker tbx6 are extruded from the similar to cells in the gastrulating embryo; it is for this reason that these structures are called Gastruloids. [1]

Further studies revealed that the events that specify T/Bra expression in gastruloids mimic those in the embryo. [2] After seven days gastruloids exhibit an organization very similar to a midgestation embryo with spatially organized primordia for all mesodermal (axial, paraxial, intermediate, cardiac, cranial and hematopoietic) and endodermal derivatives as well as the spinal cord. [10] [11] [3] They also implement Hox gene expression with the spatiotemporal coordinates as the embryo. [3] Gastruloids lack brain as well as extraembryonic tissues but characterisation of the cellular complexity of gastruloids at the level of single cell and spatial transcriptomics, reveals that they contain representatives of the three germ layers including neural crest, Primordial Germ cells and placodal primordia. [12] [13]

A feature of gastruloids is a disconnect between the transcriptional programs and outlines and the morphogenesis. However, changes in the culture conditions can elicit morphogenesis, most significantly gastruloids have been shown to form somites [13] [12] and early cardiac structures. [14] In addition, interactions between gastruloids and extraembryonic tissues promote an anterior, brain-like polarised tissue. [15]

Gastruloids have recently been obtained from human ESCs, [16] which gives developmental biologists the ability to study early human development without needing human embryos. Importantly though, the human gastruloid model is not able to form a human embryo, meaning that is a non-intact, non-viable and non-equivalent to in vivo human embryos.

The term Gastruloid has been expanded to include self-organised human embryonic stem cell arrangements on patterned (micro patterns) that mimic early patterning events in development; [17] [18] these arrangements should be referred to as 2D gastruloids.

References

  1. ^ a b c d e Brink, Susanne C. van den; Baillie-Johnson, Peter; Balayo, Tina; Hadjantonakis, Anna-Katerina; Nowotschin, Sonja; Turner, David A.; Arias, Alfonso Martinez (2014-11-15). "Symmetry breaking, germ layer specification and axial organisation in aggregates of mouse embryonic stem cells". Development. 141 (22): 4231–4242. doi: 10.1242/dev.113001. ISSN  0950-1991. PMC  4302915. PMID  25371360.
  2. ^ a b c d Turner, David A.; Girgin, Mehmet; Alonso-Crisostomo, Luz; Trivedi, Vikas; Baillie-Johnson, Peter; Glodowski, Cherise R.; Hayward, Penelope C.; Collignon, Jérôme; Gustavsen, Carsten (2017-11-01). "Anteroposterior polarity and elongation in the absence of extra-embryonic tissues and of spatially localised signalling in gastruloids: mammalian embryonic organoids". Development. 144 (21): 3894–3906. doi: 10.1242/dev.150391. ISSN  0950-1991. PMC  5702072. PMID  28951435.
  3. ^ a b c d e Beccari, Leonardo; Moris, Naomi; Girgin, Mehmet; Turner, David A.; Baillie-Johnson, Peter; Cossy, Anne-Catherine; Lutolf, Matthias P.; Duboule, Denis; Arias, Alfonso Martinez (October 2018). "Multi-axial self-organization properties of mouse embryonic stem cells into gastruloids". Nature. 562 (7726): 272–276. Bibcode: 2018Natur.562..272B. doi: 10.1038/s41586-018-0578-0. ISSN  0028-0836. PMID  30283134. S2CID  52915553.
  4. ^ a b Marikawa, Yusuke; Tamashiro, Dana Ann A.; Fujita, Toko C.; Alarcón, Vernadeth B. (2009-02-01). "Aggregated P19 mouse embryonal carcinoma cells as a simple in vitro model to study the molecular regulations of mesoderm formation and axial elongation morphogenesis". Genesis. 47 (2): 93–106. doi: 10.1002/dvg.20473. ISSN  1526-968X. PMC  3419260. PMID  19115346.
  5. ^ Leahy, Amy; Xiong, Jing-Wei; Kuhnert, Frank; Stuhlmann, Heidi (1999). "Use of developmental marker genes to define temporal and spatial patterns of differentiation during embryoid body formation". Journal of Experimental Zoology. 284 (1): 67–81. Bibcode: 1999JEZ...284...67L. doi: 10.1002/(SICI)1097-010X(19990615)284:1<67::AID-JEZ10>3.0.CO;2-O. ISSN  1097-010X. PMID  10368935.
  6. ^ ten Berge, Derk; Koole, Wouter; Fuerer, Christophe; Fish, Matt; Eroglu, Elif; Nusse, Roel (November 2008). "Wnt Signaling Mediates Self-Organization and Axis Formation in Embryoid Bodies". Cell Stem Cell. 3 (5): 508–518. doi: 10.1016/j.stem.2008.09.013. PMC  2683270. PMID  18983966.
  7. ^ Baillie-Johnson, Peter; Brink, Susanne Carina van den; Balayo, Tina; Turner, David Andrew; Arias, Alfonso Martinez (2015). "Generation of Aggregates of Mouse Embryonic Stem Cells that Show Symmetry Breaking, Polarization and Emergent Collective Behaviour In Vitro". Journal of Visualized Experiments (105): e53252. doi: 10.3791/53252. PMC  4692741. PMID  26650833.
  8. ^ Girgin, Mehmet; Turner, David Andrew; Baillie-Johnson, Peter; Cossy, Anne-Catherine; Beccari, Leonardo; Moris, Naomi; Lutolf, Matthias; Duboule, Denis; Martinez Arias, Alfonso (2018-10-12). "Generating Gastruloids from Mouse Embryonic Stem Cells". Protocol Exchange. doi: 10.1038/protex.2018.094. ISSN  2043-0116.
  9. ^ Ring, David B.; Johnson, Kirk W.; Henriksen, Erik J.; Nuss, John M.; Goff, Dane; Kinnick, Tyson R.; Ma, Sylvia T.; Reeder, John W.; Samuels, Isa (2003-03-01). "Selective glycogen synthase kinase 3 inhibitors potentiate insulin activation of glucose transport and utilization in vitro and in vivo". Diabetes. 52 (3): 588–595. doi: 10.2337/diabetes.52.3.588. ISSN  0012-1797. PMID  12606497.
  10. ^ Hashmi, Ali; Tlili, Sham; Perrin, Pierre; Martinez-Arias, Alfonso; Lenne, Pierre-François (2020-05-24). "Cell-state transitions and collective cell movement generate an endoderm-like region in gastruloids". doi: 10.1101/2020.05.21.105551. hdl: 10230/53528. S2CID  218891815. {{ cite journal}}: Cite journal requires |journal= ( help)
  11. ^ Vianello, Stefano; Lutolf, Matthias P. (2020-06-09). "In vitro endoderm emergence and self-organisation in the absence of extraembryonic tissues and embryonic architecture". doi: 10.1101/2020.06.07.138883. S2CID  219604191. {{ cite journal}}: Cite journal requires |journal= ( help)
  12. ^ a b Veenvliet, Jesse V; Bolondi, Adriano; Kretzmer, Helene; Haut, Leah; Scholze-Wittler, Manuela; Schifferl, Dennis; Koch, Frederic; Pustet, Milena; Heimann, Simon; Buschow, Rene; Wittler, Lars (2020-03-04). "Mouse embryonic stem cells self-organize into trunk-like structures with neural tube and somites". doi: 10.1101/2020.03.04.974949. hdl: 21.11116/0000-0007-AB69-3. {{ cite journal}}: Cite journal requires |journal= ( help)
  13. ^ a b van den Brink, Susanne C.; Alemany, Anna; van Batenburg, Vincent; Moris, Naomi; Blotenburg, Marloes; Vivié, Judith; Baillie-Johnson, Peter; Nichols, Jennifer; Sonnen, Katharina F.; Martinez Arias, Alfonso; van Oudenaarden, Alexander (June 2020). "Single-cell and spatial transcriptomics reveal somitogenesis in gastruloids". Nature. 582 (7812): 405–409. Bibcode: 2020Natur.582..405V. doi: 10.1038/s41586-020-2024-3. hdl: 10230/56609. ISSN  1476-4687. PMID  32076263. S2CID  211194842.
  14. ^ Rossi, Giuliana; Boni, Andrea; Guiet, Romain; Girgin, Mehmet; Kelly, Robert G.; Lutolf, Matthias P. (2019-10-14). "Embryonic organoids recapitulate early heart organogenesis": 802181. doi: 10.1101/802181. S2CID  208588024. {{ cite journal}}: Cite journal requires |journal= ( help)
  15. ^ Bérenger-Currias, Noémie M. L. P.; Mircea, Maria; Adegeest, Esmée; van den Berg, Patrick R.; Feliksik, Marleen; Hochane, Mazène; Idema, Timon; Tans, Sander J.; Semrau, Stefan (2020-02-14). "Early neurulation recapitulated in assemblies of embryonic and extraembryonic cells". doi: 10.1101/2020.02.13.947655. S2CID  238251910. {{ cite journal}}: Cite journal requires |journal= ( help)
  16. ^ Moris, Naomi; Anlas, Kerim; van den Brink, Susanne C.; Alemany, Anna; Schröder, Julia; Ghimire, Sabitri; Balayo, Tina; van Oudenaarden, Alexander; Martinez Arias, Alfonso (June 2020). "An in vitro model of early anteroposterior organization during human development". Nature. 582 (7812): 410–415. Bibcode: 2020Natur.582..410M. doi: 10.1038/s41586-020-2383-9. ISSN  0028-0836. PMID  32528178. S2CID  219567725.
  17. ^ Etoc, Fred; Metzger, Jakob; Ruzo, Albert; Kirst, Christoph; Yoney, Anna; Ozair, M. Zeeshan; Brivanlou, Ali H.; Siggia, Eric D. (2016). "A Balance between Secreted Inhibitors and Edge Sensing Controls Gastruloid Self-Organization". Developmental Cell. 39 (3): 302–315. doi: 10.1016/j.devcel.2016.09.016. PMC  5113147. PMID  27746044.
  18. ^ Warmflash, Aryeh; Sorre, Benoit; Etoc, Fred; Siggia, Eric D; Brivanlou, Ali H (2014). "A method to recapitulate early embryonic spatial patterning in human embryonic stem cells". Nature Methods. 11 (8): 847–854. doi: 10.1038/nmeth.3016. PMC  4341966. PMID  24973948.
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