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Molecular map of brain organoids reveals unprecedented levels of neuronal cell maturation and diversity

Broad Institute News May 03, 2017

Single–cell analysis of human brain organoids cultured for more than nine months reveals novel neuron diversity, maturation, and responsiveness — suggesting potential use for modeling brain development and neuropsychiatric disease.
In a new Nature journal paper, researchers from the Broad Institute of MIT and Harvard and Harvard University developed protocols and culture conditions for human brain organoids that allow the tissues to grow and develop over periods of nine months or longer and enable unprecedented levels of cell maturation. The team saw some striking developments in the organoids, including spontaneously active neural networks and the development of light–sensitive cells. The paper provides the largest–to–date molecular map of the diversity and reproducibility of cell types generated in brain organoids, and suggests that three–dimensional brain organoids have the potential to model higher–order functions such as cellular interactions and neural circuit dysfunctions related to developmental and psychiatric disorders.

“In the past, researchers have used a cocktail of factors to develop pluripotent stem cells into different types of cells from the nervous system — neurons, astrocytes, sometimes even specific classes of neurons,” explains senior author Paola Arlotta, an institute member in the Stanley Center for Psychiatric Research at the Broad Institute, co–director of the nervous system disease program at the Harvard Stem Cell Institute, and professor of stem cell and regenerative biology at Harvard University. “But the brain contains an incredible diversity of cell types that interact and form connections. We took on the challenge of investigating to what extent such complexity and diversity of cell types can be produced in the dish, and how closely the organoid cell types mirror those in the endogenous tissue.”

Giorgia Quadrato, a postdoctoral fellow in Arlotta’s lab and first author on the paper, and colleagues adapted lab protocols to enable the organoids to develop long–term from healthy induced pluripotent stem cell lines. To identify the diverse cell types that organoids generate, the team used single–cell RNA sequencing (a recent invention named Drop–seq) to analyze gene expression in more than 80,000 individual cells isolated from 31 brain organoids, and then compared the results to expression documented in human brain tissue samples.

The team found that the longer the organoids developed, the more cell types they formed. “The cellular diversity that the organoids generated stunned all of us,” says paper co–author Steve McCarroll, an institute member at Broad, director of genetics for the Stanley Center for Psychiatric Research, and associate professor of genetics at Harvard Medical School. “The ability of stem cells within organoids to generate so many of the brain’s cell types – using their own genetic and molecular instruction book – evokes how development works inside the body.”

These cells included subtypes of neurons and progenitors of the cerebral cortex. Surprisingly, they also included many cell types of the visual system. Analysis showed that the organoids had generated a virtually complete array of cell types documented from the human retina – including photoreceptor–like cells. When the researchers shined light on the organoids, the stimulus affected neuronal activity. The team proposes that this model may someday make it possible to study the response of neuronal networks to physiological sensory stimuli. “This is something that could allow detection of even subtle functional abnormalities in the neurons of organoids generated from neuropsychiatric patients,” says Quadrato.
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