{"id":4737,"date":"2021-10-08T14:19:18","date_gmt":"2021-10-08T06:19:18","guid":{"rendered":"http:\/\/43.135.177.8\/?p=4737"},"modified":"2021-10-08T14:19:39","modified_gmt":"2021-10-08T06:19:39","slug":"microfluidic-device-with-brain-extracellular-matrix-promotes-structural-and-functional-maturation-of-human-brain-organoids","status":"publish","type":"post","link":"https:\/\/whmicro.com\/?p=4737","title":{"rendered":"Microfluidic device with brain extracellular matrix promotes structural and functional maturation of human brain organoids"},"content":{"rendered":"<p>[vc_row rt_row_background_width=&#8221;default&#8221; rt_row_style=&#8221;default-style&#8221; rt_row_borders=&#8221;&#8221; rt_row_paddings=&#8221;true&#8221; rt_bg_effect=&#8221;classic&#8221; rt_bg_image_repeat=&#8221;repeat&#8221; rt_bg_size=&#8221;cover&#8221; rt_bg_position=&#8221;right top&#8221; rt_bg_attachment=&#8221;scroll&#8221; rt_bg_video_format=&#8221;self-hosted&#8221;][vc_column width=&#8221;4\/5&#8243; rt_wrp_col_paddings=&#8221;false&#8221; rt_border_top=&#8221;&#8221; rt_border_bottom=&#8221;&#8221; rt_border_left=&#8221;&#8221; rt_border_right=&#8221;&#8221; rt_border_top_mobile=&#8221;&#8221; rt_border_bottom_mobile=&#8221;&#8221; rt_border_left_mobile=&#8221;&#8221; rt_border_right_mobile=&#8221;&#8221; rt_bg_image_repeat=&#8221;repeat&#8221; rt_bg_size=&#8221;auto auto&#8221; rt_bg_position=&#8221;right top&#8221; rt_bg_attachment=&#8221;scroll&#8221;][vc_column_text]<\/p>\n<section lang=\"en\" aria-labelledby=\"Abs1\" data-title=\"Abstract\" data-gtm-vis-first-on-screen-10482319_393=\"731\" data-gtm-vis-total-visible-time-10482319_393=\"10000\" data-gtm-vis-first-on-screen-10482319_401=\"731\" data-gtm-vis-total-visible-time-10482319_401=\"10000\" data-gtm-vis-has-fired-10482319_393=\"1\" data-gtm-vis-has-fired-10482319_401=\"1\">\n<div id=\"Abs1-section\" class=\"c-article-section\">\n<h2 id=\"Abs1\" class=\"c-article-section__title js-section-title js-c-reading-companion-sections-item\">Abstract<\/h2>\n<div id=\"Abs1-content\" class=\"c-article-section__content\">\n<p>Brain organoids derived from human pluripotent stem cells provide a highly valuable in vitro model to recapitulate human brain development and neurological diseases. However, the current systems for brain organoid culture require further improvement for the reliable production of high-quality organoids. Here, we demonstrate two engineering elements to improve human brain organoid culture, (1) a human brain extracellular matrix to provide brain-specific cues and (2) a microfluidic device with periodic flow to improve the survival and reduce the variability of organoids. A three-dimensional culture modified with brain extracellular matrix significantly enhanced neurogenesis in developing brain organoids from human induced pluripotent stem cells. Cortical layer development, volumetric augmentation, and electrophysiological function of human brain organoids were further improved in a reproducible manner by dynamic culture in microfluidic chamber devices. Our engineering concept of reconstituting brain-mimetic microenvironments facilitates the development of a reliable culture platform for brain organoids, enabling effective modeling and drug development for human brain diseases.<\/p>\n<\/div>\n<\/div>\n<\/section>\n<section data-title=\"Introduction\" data-gtm-vis-first-on-screen-10482319_401=\"8075\" data-gtm-vis-total-visible-time-10482319_401=\"10000\" data-gtm-vis-first-on-screen-10482319_393=\"8075\" data-gtm-vis-total-visible-time-10482319_393=\"10000\" data-gtm-vis-has-fired-10482319_393=\"1\" data-gtm-vis-has-fired-10482319_401=\"1\">\n<div id=\"Sec1-section\" class=\"c-article-section\">\n<h2 id=\"Sec1\" class=\"c-article-section__title js-section-title js-c-reading-companion-sections-item\">Introduction<\/h2>\n<div id=\"Sec1-content\" class=\"c-article-section__content\">\n<p>Recent breakthroughs in brain organoid technology have enabled the development of a new in vitro model that promotes significant advancements in the study of nervous system development and diseases<sup><a id=\"ref-link-section-d34615217e858\" title=\"Di Lullo, E. &amp; Kriegstein, A. R. The use of brain organoids to investigate neural development and disease. Nat. Rev. Neurosci. 18, 573 (2017).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR1\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 1\">1<\/a><\/sup>. Sasai and co-workers proposed the idea that differentiated pluripotent cells can form multi-layered organized structures that recapitulate embryonic development when grown in three-dimensional (3D) culture<sup><a id=\"ref-link-section-d34615217e862\" title=\"Eiraku, M. et al. Self-organized formation of polarized cortical tissues from ESCs and its active manipulation by extrinsic signals. Cell Stem Cell 3, 519\u2013532 (2008).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR2\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 2\">2<\/a><\/sup>. Lancaster et al. developed a 3D culture model termed \u201ccerebral organoids\u201d that recapitulate many key features of the human brain in vivo and develop various distinct and interdependent brain regions<sup><a id=\"ref-link-section-d34615217e866\" title=\"Lancaster, M. A. et al. Cerebral organoids model human brain development and microcephaly. Nature 501, 373\u2013379 (2013).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR3\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 3\">3<\/a><\/sup>. The generation of cerebral organoids depends on the intrinsic ability of pluripotent stem cells (PSCs) to spontaneously self-organize upon precisely timed manipulation of culture conditions even in the absence of external patterning factors<sup><a id=\"ref-link-section-d34615217e870\" title=\"Lancaster, M. A. et al. Cerebral organoids model human brain development and microcephaly. Nature 501, 373\u2013379 (2013).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR3\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">3<\/a>,<a id=\"ref-link-section-d34615217e870_1\" title=\"Lancaster, M. A. &amp; Knoblich, J. A. Generation of cerebral organoids from human pluripotent stem cells. Nat. Protoc. 9, 2329\u20132340 (2014).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR4\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">4<\/a>,<a id=\"ref-link-section-d34615217e873\" title=\"Camp, J. G. et al. Human cerebral organoids recapitulate gene expression programs of fetal neocortex development. Proc. Natl Acad. Sci. U. S. A. 112, 15672\u201315677 (2015).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR5\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 5\">5<\/a><\/sup>. Cerebral organoids representing the whole brain have significant advantages over brain region-specific<sup><a id=\"ref-link-section-d34615217e877\" title=\"Eiraku, M. et al. Self-organized formation of polarized cortical tissues from ESCs and its active manipulation by extrinsic signals. Cell Stem Cell 3, 519\u2013532 (2008).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR2\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 2\">2<\/a>,<a id=\"ref-link-section-d34615217e880\" title=\"Kadoshima, T. et al. Self-organization of axial polarity, inside-out layer pattern, and species-specific progenitor dynamics in human ES cell-derived neocortex. Proc. Natl Acad. Sci. U. S. A. 110, 20284\u201320289 (2013).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR6\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">6<\/a>,<a id=\"ref-link-section-d34615217e880_1\" title=\"Pasca, A. M. et al. Functional cortical neurons and astrocytes from human pluripotent stem cells in 3D culture. Nat. Methods 12, 671\u2013678 (2015).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR7\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">7<\/a>,<a id=\"ref-link-section-d34615217e880_2\" title=\"Qian, X. Y. et al. Brain-region-specific organoids using mini-bioreactors for modeling zikv exposure. Cell 165, 1238\u20131254 (2016).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR8\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">8<\/a>,<a id=\"ref-link-section-d34615217e880_3\" title=\"Muguruma, K., Nishiyama, A., Kawakami, H., Hashimoto, K. &amp; Sasai, Y. Self-organization of polarized cerebellar tissue in 3D culture of human pluripotent stem cells. Cell Rep. 10, 537\u2013550 (2015).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR9\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">9<\/a>,<a id=\"ref-link-section-d34615217e880_4\" title=\"Jo, J. et al. Midbrain-like organoids from human pluripotent stem cells contain functional dopaminergic and neuromelanin-producing neurons. Cell Stem Cell 19, 248\u2013257 (2016).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR10\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">10<\/a>,<a id=\"ref-link-section-d34615217e880_5\" title=\"Suga, H. et al. Self-formation of functional adenohypophysis in three-dimensional culture. Nature 480, 57\u201362 (2011).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR11\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">11<\/a>,<a id=\"ref-link-section-d34615217e883\" title=\"Sakaguchi, H. et al. Generation of functional hippocampal neurons from self-organizing human embryonic stem cell-derived dorsomedial telencephalic tissue. Nat. Commun. 6, 8896 (2015).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR12\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 12\">12<\/a><\/sup>\u00a0or extensively patterned organoids<sup><a id=\"ref-link-section-d34615217e888\" title=\"Birey, F. et al. Assembly of functionally integrated human forebrain spheroids. Nature 545, 54 (2017).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR13\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">13<\/a>,<a id=\"ref-link-section-d34615217e888_1\" title=\"Xiang, Y. et al. Fusion of regionally specified hPSC-derived organoids models human brain development and interneuron migration. Cell Stem Cell 21, 383\u2013398 e387 (2017).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR14\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">14<\/a>,<a id=\"ref-link-section-d34615217e888_2\" title=\"Bagley, J. A., Reumann, D., Bian, S., Levi-Strauss, J. &amp; Knoblich, J. A. Fused cerebral organoids model interactions between brain regions. Nat. Methods 14, 743\u2013751 (2017).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR15\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">15<\/a>,<a id=\"ref-link-section-d34615217e888_3\" title=\"Xiang, Y. et al. hESC-derived thalamic organoids form reciprocal projections when fused with cortical organoids. Cell Stem Cell 24, 487\u2013497 (2019).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR16\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\">16<\/a>,<a id=\"ref-link-section-d34615217e891\" title=\"Cederquist, G. Y. et al. Specification of positional identity in forebrain organoids. Nat. Biotechnol. 37, 436\u2013444 (2019).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR17\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 17\">17<\/a><\/sup>\u00a0due to their ability to generate a diverse range of brain cells and recapitulate the major events in overall brain development<sup><a id=\"ref-link-section-d34615217e895\" title=\"Kelava, I. &amp; Lancaster, M. A. Stem cell models of human brain development. Cell Stem Cell 18, 736\u2013748 (2016).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR18\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 18\">18<\/a><\/sup>. Despite the potential of cerebral organoid technology, there are several challenges. Due to the lack of instructive signals during the generation of human cerebral organoids, they recapitulate only some of the earliest stages of human embryonic brain development<sup><a id=\"ref-link-section-d34615217e899\" title=\"Camp, J. G. et al. Human cerebral organoids recapitulate gene expression programs of fetal neocortex development. Proc. Natl Acad. Sci. U. S. A. 112, 15672\u201315677 (2015).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR5\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 5\">5<\/a><\/sup>\u00a0and are not able to mimic the later stages of neurogenesis until extended cultivation for 6\u20139 months<sup><a id=\"ref-link-section-d34615217e903\" title=\"Quadrato, G. et al. Cell diversity and network dynamics in photosensitive human brain organoids. Nature 545, 48\u201353 (2017).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR19\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 19\">19<\/a><\/sup>. Another critical limitation is the extensive cell death in the developing organoids at later stages due to diffusional limitations in oxygen and nutrient transfer<sup><a id=\"ref-link-section-d34615217e907\" title=\"Lancaster, M. A. &amp; Knoblich, J. A. Generation of cerebral organoids from human pluripotent stem cells. Nat. Protoc. 9, 2329\u20132340 (2014).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR4\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 4\">4<\/a>,<a id=\"ref-link-section-d34615217e910\" title=\"Qian, X. Y. et al. Brain-region-specific organoids using mini-bioreactors for modeling zikv exposure. Cell 165, 1238\u20131254 (2016).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR8\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 8\">8<\/a><\/sup>.<\/p>\n<p>Several engineering strategies with biomaterials, bioreactors, devices, and genetic modification have been demonstrated to overcome such limitations of current brain organoid culture. For example, synthetic polymer microfilaments enhanced neuroectoderm formation and cortical development by facilitating guided self-organization via neuroepithelium elongation<sup><a id=\"ref-link-section-d34615217e917\" title=\"Lancaster, M. A. et al. Guided self-organization and cortical plate formation in human brain organoids. Nat. Biotechnol. 35, 659\u2013666 (2017).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR20\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 20\">20<\/a><\/sup>. In other study, miniaturized spinning bioreactors were tested for improving the dynamic culture of brain organoids, which generated more robust disease models with Zika virus infection<sup><a id=\"ref-link-section-d34615217e921\" title=\"Qian, X. Y. et al. Brain-region-specific organoids using mini-bioreactors for modeling zikv exposure. Cell 165, 1238\u20131254 (2016).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR8\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 8\">8<\/a><\/sup>. To increase the oxygen supply, air\u2013liquid interface culture was adapted for cerebral organoids, resulting in improved survival and morphology with extensive axonal outgrowths<sup><a id=\"ref-link-section-d34615217e925\" title=\"Giandomenico, S. L. et al. Cerebral organoids at the air\u2013liquid interface generate diverse nerve tracts with functional output. Nat. Neurosci. 22, 669\u2013679 (2019).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR21\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 21\">21<\/a><\/sup>. Organ-on-a-chip systems were also employed to improve the oxygen supply to the brain organoids<sup><a id=\"ref-link-section-d34615217e929\" title=\"Wang, Y., Wang, L., Guo, Y., Zhu, Y. &amp; Qin, J. Engineering stem cell-derived 3D brain organoids in a perfusable organ-on-a-chip system. RSC Adv. 8, 1677\u20131685 (2018).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR22\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 22\">22<\/a>,<a id=\"ref-link-section-d34615217e932\" title=\"Berger, E. et al. Millifluidic culture improves human midbrain organoid vitality and differentiation. Lab Chip 18, 3172\u20133183 (2018).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR23\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 23\">23<\/a><\/sup>. The vascularization of brain organoids by grafting human brain organoids into the mouse brain or gene editing of vascular transcription factor resulted in progressive neurogenesis with improved neuronal survival<sup><a id=\"ref-link-section-d34615217e936\" title=\"Mansour, A. A. et al. An in vivo model of functional and vascularized human brain organoids. Nat. Biotechnol. 36, 432\u2013441 (2018).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR24\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 24\">24<\/a><\/sup>. Despite these recent technical improvements, certain progenitor cells still showed low abundance, and the cytoarchitecture of the basal zones and cortical layers was not complete<sup><a id=\"ref-link-section-d34615217e941\" title=\"Lancaster, M. A. et al. Cerebral organoids model human brain development and microcephaly. Nature 501, 373\u2013379 (2013).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR3\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 3\">3<\/a>,<a id=\"ref-link-section-d34615217e944\" title=\"Lancaster, M. A. &amp; Knoblich, J. A. Generation of cerebral organoids from human pluripotent stem cells. Nat. Protoc. 9, 2329\u20132340 (2014).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR4\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 4\">4<\/a><\/sup>. Moreover, the current protocols based on spontaneous self-organization have exhibited a significant batch-to-batch variation, which in turn results in poor reproducibility. Therefore, cerebral organoids still need to be improved further for neuronal development, structural maturation, and better electrophysiological functionality, as well as for ensuring consistent organoid quality.<\/p>\n<p>Here, we propose a strategy to engineer human PSC-derived cerebral organoids by reconstituting a 3D brain-mimetic microenvironment with a decellularized human brain tissue-derived brain extracellular matrix (BEM) and dynamic microfluidic systems. BEM can recreate brain-mimetic niches necessary to guide neural and glial differentiation for brain organogenesis, which would likely be deficient in the non-neuronal matrix (e.g. Matrigel)<sup><a id=\"ref-link-section-d34615217e951\" title=\"Faissner, A. &amp; Reinhard, J. The extracellular matrix compartment of neural stem and glial progenitor cells. Glia 63, 1330\u20131349 (2015).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR25\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 25\">25<\/a><\/sup>. The application of microfluidic devices capable of achieving a gravity-driven flow that mimics a fluid flow existing in the cerebrospinal and interstitial spaces can facilitate the oxygen supply and nutrient\/waste exchange, leading to a significant reduction of cell death throughout the structure of organoids. Thus, we reason that providing brain-specific extracellular matrix (ECM) cues together with improved nutrient and oxygen exchange will support cell expansion as well as neuronal differentiation and functional maturation, thereby recapitulating prominent features of human embryonic cortical development in a much precise and reproducible manner.<\/p>\n<\/div>\n<\/div>\n<\/section>\n<section data-title=\"Results\" data-gtm-vis-first-on-screen-10482319_393=\"9808\" data-gtm-vis-total-visible-time-10482319_393=\"10000\" data-gtm-vis-first-on-screen-10482319_401=\"9809\" data-gtm-vis-total-visible-time-10482319_401=\"10000\" data-gtm-vis-has-fired-10482319_393=\"1\" data-gtm-vis-has-fired-10482319_401=\"1\">\n<div id=\"Sec2-section\" class=\"c-article-section\">\n<h2 id=\"Sec2\" class=\"c-article-section__title js-section-title js-c-reading-companion-sections-item\">Results<\/h2>\n<div id=\"Sec2-content\" class=\"c-article-section__content\">\n<h3 id=\"Sec3\" class=\"c-article__sub-heading\">Characterization of a human brain-mimicking 3D hydrogel matrix<\/h3>\n<p>A bioengineering platform to improve human brain organoid culture was set up with human brain-mimicking 3D hydrogel and a microfluidic system. Human cerebral organoids were generated from human induced pluripotent stem cells (iPSCs) as described in Lancaster\u2019s protocol (Supplementary Fig.\u00a0<a href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#MOESM1\" data-track=\"click\" data-track-label=\"link\" data-track-action=\"supplementary material anchor\">1<\/a>)<sup><a id=\"ref-link-section-d34615217e970\" title=\"Lancaster, M. A. &amp; Knoblich, J. A. Generation of cerebral organoids from human pluripotent stem cells. Nat. Protoc. 9, 2329\u20132340 (2014).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR4\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 4\">4<\/a><\/sup>. When embryoid bodies (EBs) were induced to develop into a neuroepithelial lineage at day 11, they were embedded in a 3D matrix supplemented with human BEM (0.4\u2009mg\/ml) (Fig.\u00a0<a href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#Fig1\" data-track=\"click\" data-track-label=\"link\" data-track-action=\"figure anchor\">1a<\/a>). Because Matrigel, a common and essential component of the organoid culture, is refractory to the tissue-specific ECM cues that are required by different tissue types<sup><a id=\"ref-link-section-d34615217e977\" title=\"Yin, X. et al. Engineering stem cell organoids. Cell Stem Cell 18, 25\u201338 (2016).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR26\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 26\">26<\/a>,<a id=\"ref-link-section-d34615217e980\" title=\"Kim, S., Cho, A.-N., Min, S., Kim, S. &amp; Cho, S.-W. Organoids for advanced therapeutics and disease models. Adv. Ther. 2, 1800087 (2018).\" href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#ref-CR27\" data-track=\"click\" data-track-action=\"reference anchor\" data-track-label=\"link\" data-test=\"citation-ref\" aria-label=\"Reference 27\">27<\/a><\/sup>, modification of Matrigel-based organoid culture by supplying human BEM would provide enhanced cell growth and more favorable interactions at an early stage of neurogenesis. After four days of culture in BEM-incorporated gel, the organoids were transferred into the microfluidic device under dynamic conditions (Fig.\u00a0<a href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#Fig1\" data-track=\"click\" data-track-label=\"link\" data-track-action=\"figure anchor\">1a, b<\/a>). Our microfluidic platform can allow for independent control of the cerebral organoids in much smaller medium volume and precisely controlled medium flow with low fluid shear stress (Supplementary Fig.\u00a0<a href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5#MOESM1\" data-track=\"click\" data-track-label=\"link\" data-track-action=\"supplementary material anchor\">2<\/a>), compared to typical bulk scale bioreactors (e.g. spinner flasks, orbital shakers) which require larger volumes and evoke cell damage due to the high shear stress. With the precisely controlled fluid flow, the effective exchange of oxygen, nutrients, and bioactive molecules in the medium leads to the robust expansion and reduced cell apoptosis at an early stage of organoid development. Consequently, more complex structures with elongated cortical layers would be evident in cerebral organoids.<\/p>\n<div id=\"figure-1\" class=\"c-article-section__figure js-c-reading-companion-figures-item\" data-test=\"figure\" data-container-section=\"figure\" data-title=\"Characterization of decellularized human brain-derived extracellular matrix (BEM).\" data-gtm-vis-first-on-screen-10482319_399=\"10455\" data-gtm-vis-total-visible-time-10482319_399=\"10000\" data-gtm-vis-recent-on-screen-10482319_399=\"776511\" data-gtm-vis-has-fired-10482319_399=\"1\"><a href=\"http:\/\/43.135.177.8\/wp-content\/uploads\/2021\/10\/Characterization-of-decellularized-human-brain-derived-extracellular-matrix-BEM.webp\"><img loading=\"lazy\" decoding=\"async\" class=\"alignnone size-medium wp-image-4738\" src=\"http:\/\/43.135.177.8\/wp-content\/uploads\/2021\/10\/Characterization-of-decellularized-human-brain-derived-extracellular-matrix-BEM-300x264.webp\" alt=\"Characterization of decellularized human brain-derived extracellular matrix (BEM)\" width=\"300\" height=\"264\" srcset=\"https:\/\/whmicro.com\/wp-content\/uploads\/2021\/10\/Characterization-of-decellularized-human-brain-derived-extracellular-matrix-BEM-300x264.webp 300w, https:\/\/whmicro.com\/wp-content\/uploads\/2021\/10\/Characterization-of-decellularized-human-brain-derived-extracellular-matrix-BEM.webp 685w\" sizes=\"(max-width: 300px) 100vw, 300px\" \/><\/a><\/div>\n<\/div>\n<div data-test=\"figure\" data-container-section=\"figure\" data-title=\"Characterization of decellularized human brain-derived extracellular matrix (BEM).\" data-gtm-vis-first-on-screen-10482319_399=\"10455\" data-gtm-vis-total-visible-time-10482319_399=\"10000\" data-gtm-vis-recent-on-screen-10482319_399=\"776511\" data-gtm-vis-has-fired-10482319_399=\"1\"><a href=\"https:\/\/www.nature.com\/articles\/s41467-021-24775-5\">\u00a0Read the original article:<\/a><\/div>\n<\/div>\n<\/section>\n<p>[\/vc_column_text][\/vc_column][vc_column width=&#8221;1\/5&#8243; rt_wrp_col_paddings=&#8221;false&#8221; rt_border_top=&#8221;&#8221; rt_border_bottom=&#8221;&#8221; rt_border_left=&#8221;&#8221; rt_border_right=&#8221;&#8221; rt_border_top_mobile=&#8221;&#8221; rt_border_bottom_mobile=&#8221;&#8221; rt_border_left_mobile=&#8221;&#8221; rt_border_right_mobile=&#8221;&#8221; rt_bg_image_repeat=&#8221;repeat&#8221; rt_bg_size=&#8221;auto auto&#8221; rt_bg_position=&#8221;right top&#8221; rt_bg_attachment=&#8221;scroll&#8221;][vc_widget_sidebar sidebar_id=&#8221;sidebar-for-portfolio&#8221;][\/vc_column][\/vc_row]<\/p>\n","protected":false},"excerpt":{"rendered":"<p>Brain organoids derived from human pluripotent stem cells provide a highly valuable in vitro model to recapitulate human brain development and neurological diseases. However, the current systems for brain organoid culture require further improvement for the reliable production of high-quality organoids.<\/p>\n","protected":false},"author":1,"featured_media":4738,"comment_status":"closed","ping_status":"open","sticky":false,"template":"","format":"standard","meta":{"footnotes":""},"categories":[1],"tags":[102],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v18.0 - https:\/\/yoast.com\/wordpress\/plugins\/seo\/ -->\n<title>Microfluidic device with brain extracellular matrix<\/title>\n<meta name=\"description\" content=\"Brain organoids derived from human pluripotent stem cells provide a highly valuable in vitro model to recapitulate human brain development and neurological diseases. 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