Large-scale production of living brain cells enables entirely new research
Lund University News Jun 29, 2017
With the help of a new method for cell conversion, researchers at Lund University in Sweden have found a way to produce diseased, aging brain cells on a large scale in a cell culture dish.
After performing a biopsy on the patient, the skin cells are transformed into brain cells that effectively imitate the disease and the age of the patient. The fact that the cells can now be produced in large quantities enables researchers to carry out a series of experiments that were previously not possible.
A few years ago, Malin ParmarÂs research team was one of the first in the world to convert human skin cells directly into brain cells without passing the stem cell state. The discovery shocked the researchers and was perceived as almost impossible. The team is now approaching a point where the discovery is about to bear fruit on a wide scale. By following a new method that involves slightly changing the genetic code that triggers cell conversion, the researchers were able to multiply the production of disease–specific brain cells.
ÂPrimarily, we inhibited a protein, REST, involved in establishing identity in cells that are not nerve cells. After limiting this proteinÂs impact in the cells during the conversion process, weÂve seen completely different results. Since then, weÂve been playing around with changing the dosage of the other components in the previous method, which also proved effective. Overall, the efficiency is remarkable. We can now generate almost unlimited amounts of neurons from one skin biopsyÂ, says Malin Parmar, professor of developmental and regenerative neurobiology at Lund University.
The increase in production will have far–reaching effects. The new volumes enable research projects that were simply not viable before. Among other things, it opens up research areas linked to new drug testing, the establishment of more accurate disease models and the development of diagnostics to detect the diseases at an earlier stage.
The new cells are not only able to imitate the disease but also the patientÂs age. By studying the cell in the culture dish, the researchers can now monitor the mechanisms of the disease in an Âold brain cell over time. Neurodegenerative diseases are commonly referred to as Âaging brain diseases and in order to understand them, we must better appreciate how the age specifically affects the course of the disease. The Lund researchers discovery can hopefully contribute a crucial piece to the puzzle with regard to the connection between the onset of disease and cell aging, something which previous research based on animal experiments and stem cells has failed to provide.
ÂThis takes us one step closer to reality, as we can now look inside the human neurons and see what goes on inside the cell in these diseases. If all goes well, this could fundamentally change the field of research, as it helps us better understand the real mechanisms of the disease. We believe that many laboratories around the world would like to start testing on these cells to get closer to the diseasesÂ, says Johan Jakobsson, leader of the molecular neurogenetics research group at Lund University.
The paper titled, "REST suppression mediates neural conversion of adult human fibroblasts via microRNA–dependent and –independent pathways," was published in the journal EMBO Molecular Medicine.
Go to Original
After performing a biopsy on the patient, the skin cells are transformed into brain cells that effectively imitate the disease and the age of the patient. The fact that the cells can now be produced in large quantities enables researchers to carry out a series of experiments that were previously not possible.
A few years ago, Malin ParmarÂs research team was one of the first in the world to convert human skin cells directly into brain cells without passing the stem cell state. The discovery shocked the researchers and was perceived as almost impossible. The team is now approaching a point where the discovery is about to bear fruit on a wide scale. By following a new method that involves slightly changing the genetic code that triggers cell conversion, the researchers were able to multiply the production of disease–specific brain cells.
ÂPrimarily, we inhibited a protein, REST, involved in establishing identity in cells that are not nerve cells. After limiting this proteinÂs impact in the cells during the conversion process, weÂve seen completely different results. Since then, weÂve been playing around with changing the dosage of the other components in the previous method, which also proved effective. Overall, the efficiency is remarkable. We can now generate almost unlimited amounts of neurons from one skin biopsyÂ, says Malin Parmar, professor of developmental and regenerative neurobiology at Lund University.
The increase in production will have far–reaching effects. The new volumes enable research projects that were simply not viable before. Among other things, it opens up research areas linked to new drug testing, the establishment of more accurate disease models and the development of diagnostics to detect the diseases at an earlier stage.
The new cells are not only able to imitate the disease but also the patientÂs age. By studying the cell in the culture dish, the researchers can now monitor the mechanisms of the disease in an Âold brain cell over time. Neurodegenerative diseases are commonly referred to as Âaging brain diseases and in order to understand them, we must better appreciate how the age specifically affects the course of the disease. The Lund researchers discovery can hopefully contribute a crucial piece to the puzzle with regard to the connection between the onset of disease and cell aging, something which previous research based on animal experiments and stem cells has failed to provide.
ÂThis takes us one step closer to reality, as we can now look inside the human neurons and see what goes on inside the cell in these diseases. If all goes well, this could fundamentally change the field of research, as it helps us better understand the real mechanisms of the disease. We believe that many laboratories around the world would like to start testing on these cells to get closer to the diseasesÂ, says Johan Jakobsson, leader of the molecular neurogenetics research group at Lund University.
The paper titled, "REST suppression mediates neural conversion of adult human fibroblasts via microRNA–dependent and –independent pathways," was published in the journal EMBO Molecular Medicine.
Only Doctors with an M3 India account can read this article. Sign up for free or login with your existing account.
4 reasons why Doctors love M3 India
-
Exclusive Write-ups & Webinars by KOLs
-
Daily Quiz by specialty -
Paid Market Research Surveys -
Case discussions, News & Journals' summaries
