Science To learn is to myelinate Patrick Long and Gabriel Corfas Science 346, 298 (2014); DOI: 10.1126/science.1261127 This copy is for your personal, non-commercial use only. If you wish to distribute this article to others, you can order high-quality copies for your colleagues, clients, or customers by clicking here. Permission to republish or repurpose articles or portions of articles can be obtained by following the guidelines here. The following resources related to this article are available online at www.sciencemag.org (this information is current as of October 16, 2014 ): o Updated information and services, including high-resolution figures, can be found in the online reversion of this article at: http://www.sciencemag.org/content/346/6207/298.full.html a5 o A list of selected additional articles on the Science Web sites related to this article can be o found at: O 03 http://www.sciencemag.Org/content/346/6207/298.full.html#related This article cites 12 articles, 5 of which can be accessed free: http://www.sciencemag.Org/content/346/6207/298.full.html#ref-list-1 6> co This article appears in the following subject collections: I Neuroscience ^ http://www.sciencemag.org/cgi/collection/neuroscience ® in T3 CD T3 CD O O Q Science (print ISSN 0036-8075; online ISSN 1095-9203) is published weekly, except the last week in December, by the American Association for the Advancement of Science, 1200 New York Avenue NW, Washington, DC 20005. Copyright 2014 by the American Association for the Advancement of Science; all rights reserved. The title Science is a registered trademark of AAAS. INSIGHTS I PERSPECTIVES tion could, in essence, ban DTC genetic testing as we have known it in Europe. Whether a website providing information regarding a genetic test is advertisement per se, or simply informational, may be debatable. These articles in the proposed regulation are likely to strengthen the trend of DTC companies incorporating physicians into their model of test provision, as well as redirecting their advertising efforts (including continuing medical education) to health care professionals. This may present problems related to impartiality similar to those observed with prescription drugs, especially when clinicians are recruited, trained by, and often remunerated by the companies selling the services (12). Inclusion of a health care professional, even a clinical geneticist, does not necessarily safeguard against all the concerns "If the proposed regulation is approved, it is not obvious that crossing the Atlantic will make it easier for companies." surrounding scientific validity or clinical validity raised by the proposed regulation and the FDA. Given the speeds at which new tests are being developed and at which new technologies allow for genotyping and sequencing, it is unreasonable to expect that simply adding a medical professional will solve all problems raised by DTC genetic testing. Not only are such professionals not currently prepared to interpret all genetic tests offered by DTC companies, but their involvement does not necessarily assure that tests offered will have appropriate quality and/or benefit to the users. Although a decision of the Council of the EU was originally planned before the May 2014 European elections, only a June 2014 meeting providing guidance for future work has taken place (13), with further debates and negotiations to follow. If the proposed IVD regulation is accepted by the Council, it will clearly affect the way genetic testing is being offered beyond the clinic. It will also potentially affect the clinicians who will be sought by consumers for genetic testing prescriptions. The future of European DTC genetic testing companies—and of non-European companies in the EU market-may also be heavily affected by coming policy decisions. For example, companies may want to broaden their sales outside the United States into foreign markets, in 298 IV OCTOBER 2014 • VOL 346 ISSUE 620V order to circumvent FDA demands. This was showcased recently when 23andMe announced it would resume selling its Personal Genome Service in Canada (14). If the proposed regulation is approved, it is not obvious that crossing the Atlantic will make it easier for companies (15). ■ REFERENCES AND NOTES 1. FDA, FDAto23andMe, Inc., 22 November2013(FDA, Silver Spring, MD, 2014); www.fda.gov/iceci/enforcementactions/ warningletters/2013/ucm376296.htm. 2. In June 2014, it was announced that the FDA would review a premarket 510(k) application for Bloom syndrome submitted by the company. Such an application for a single disorder could be considered much simpler than an application (or many applications) for genome-wide testing, from which results are returned for a multitude of phenotypes. 3. European Commission, Proposal for a regulation of the European Parliament and the Council on in vitro diagnostic medical devices (2012); http://ec.europa. eu/health/medical-devices/files/revision_docs/ proposal_2012_541_en.pdf 4. European Union, Regulations, Directives and other Acts: http://europa.eu/eu-law/decision-making/legal-acts/ index_en.htm. 5. Council of the European Union, The decision-making process in the European Union (2014); www.consilium. europa.eu/council/decision-making-process?lang=en. 6. European Parliament, Amendments adopted by the European Parliament on 22 October 2013 on the proposal for a regulation of the European Parliament and of the Council on in vitro diagnostic medical devices [COM(2012)0541 - C7-0317/2012 - 2012/0267(COD)] (2013); www.europarl.europa.eu/sides/getDoc. do?type=TA&reference=P7-TA-2013-0427&language=EN &ring=A7-2013-0327. 7. Global Harmonization Task Force, Principles of In Vitro Diagnostic (IVD) Medical Devices Classification (SGI Final Document GHTF/SG1/N045:2008, GHTF, 2008). 8. The main taskof Notified Bodies is to analyze claims made by manufacturers. Notified Bodies do not assess whether a test has sufficient clinical utility to be offered to patients or individuals. The proposed regulation includes rules that aim to promote transparency and similar standards to be met by Notified Bodies during assessment. 9. P. Brice, EU legal amendments threaten genomic medicine and research (PHG Foundation, Cambridge, 2013): www.phgfoundation.org/news/14842/. 10. Council of Europe, Additional Protocol to the Convention on Human Rights and Biomedicine, concerning Genetic Testing for Health Purposes (2008); http://conventions. coe.int/Treaty/en/Treaties/Html/203.htm. 11. European Society of Human Genetics, New legal opinion finds EU does not have the power to enact radical genetic counselling laws (2014); https:// www.eshg.org/fileadmin/eshg/documents/IVD/ IVDLegalOpinionExecutiveSummaryApril2014.pdf 12. H. C. Howard, P. Börry, J. Community Genet. 3,105 (2012). 13. Council of the European Union, 3323 Council Meeting, Employment, Social Policy, Health, and Consumers Affairs [press release] (2014); www.consilium.europa.eu/ uedocs/cms_data/docs/pressdata/en/lsa/143271.pdf 14. Canada News Wire, 23andMe announces new service for Canada [press release] (2014); www.bizjournals. com/sacramento/prnewswire/press_releases/ California/2014/10/01/C2766. 15. S. Locke, The FDA won't let 23andMe test your genes—so it may go to Europe (2014); www.vox. com/2014/5/12/5709766/the-fda-wont-let-23andme-test-your-genes-so-it-may-go-to-europe. ACKNOWLEDGMENTS Part of this work was supported by a doctoral fellowship from the Research Foundation Flanders (FW0), the Swedish Foundation for Humanities and Social Sciences, the Biobanking and Molecular Resource Infrastructure of Sweden (BBMRI.se), and the CHIP ME COST Action IS1303. 10.1126/science.l256396 NEUROSCIENCE To learn is to myelinate The adult mammalian brain requires the production of new glial cells and myelin for learning By Patrick Long and Gabriel Corfas Learning triggers neuronal changes in the brain that contribute to information acquisition and memory formation, including the activity and strength of existing synapses, the formation of new synapses, and possibly the birth of new neurons (1). Therefore, it is not surprising that neurons have been seen as the sole components of the nervous system, capable of responding to experience and responsible for learning and long-term behavioral plasticity. However, this notion is being challenged by recent findings on glial biology. On page 318 of this issue, McKenzie et al. (2) add to this argument by revealing that the generation of new oligodendrocytes—one of the brain's non-neu-ronal cell types—is required for learning a complex motor skill. The finding advances our understanding of brain plasticity and points to roles for glia and myelin in cognitive function. Oligodendrocytes generate myelin, the insulating membrane that covers many neuronal axons and facilitates the propagation of electrical signals along neuronal circuits. Although oligodendrocytes and the myelin they create were assumed to be static, recent studies indicate that myelin is much more malleable than once thought. Imaging studies have shown that various forms of learning correlate with structural changes in the human brain's white matter, and animal studies have demonstrated oligodendrocyte and myelin changes in response to social and environmental conditions (3). These observations raise the possibility that myelin is highly dynamic and that changes in myelination are important components of brain plasticity. Oligodendrocytes send out multiple cellular processes that attach and ensheath axons with concentric layers of compacted cellular membrane to form myelin (see the figure). Myelination increases the speed by which electrical impulses travel along neuronal processes, and differences in the de- sciencemag.org SCIENCE Published by AAAS gree to which axons are myelinated affect the timing of the flow of information between neurons. The composition of myelinated axons in the brain is heterogeneous; axons may be highly myelinated, not myelinated, or incompletely myelinated, and the pattern of myelination may vary along a single axon (4). Most myelination in the mammalian brain occurs during early life. At that stage, oligodendrocyte progenitor cells (OPCs) give rise to oligodendrocytes, which go on to myelinate axons as they mature. Remarkably, a high density of OPCs remains in the adult brain long after the developmental period of myelination is complete. Adult OPCs retain the capacity to differentiate into myelinating oligodendrocytes in response to injury or demyelinating diseases, such as multiple sclerosis (5). These precursor cells may also give rise to newly generated oligodendrocytes to remodel myelin along previously myelinated axons in the adult brain (6). Yet, the potential functional importance of this apparent reservoir of undifferentiated cells for plasticity in the normal brain has been a mystery. McKenzie et al. sought to determine whether adult-born oligodendrocytes are necessary for learning to occur. They observed that young adult mice that learn to run on a "complex running wheel" with irregularly spaced rungs have a transient elevation in OPC proliferation and production of adult-born oligodendrocytes in the corpus callosum, an axon-dense area of the brain connecting the two cerebral hemispheres. To analyze the contribution of new oligodendrocyte formation to motor learning, the authors used genetically modified mice in which they had eliminated the ability of OPCs to make new oligodendrocytes without affecting preexisting oligodendrocytes or myelin. They achieved this by inactivating the myelin regulatory factor (Myrf) gene in adult OPCs. Myrf encodes a protein required for OPCs to differentiate into mature myelinating oligodendrocytes. McKenzie et al. discovered that mice lacking the capacity to form new oligodendrocytes also failed to develop an effective running strategy in the complex running wheel. By contrast, when mice were allowed to train on the complex running wheel before Myrf Kresge Hearing Research Institute, The University of Michigan, 1150 West Medical Center Drive, Ann Arbor, Ml 48109-5616, USA. E-mail: cor1as@med.umich.edu inactivation, they performed comparably to normal control mice. This indicates that although the production of new oligodendrocytes is not required for information retrieval, it is critical for learning new motor behavior. How is learning linked to changes in myelination? OPCs express numerous receptors that make them responsive to neurotransmitters. OPCs can also respond to neuron-derived mitogens and trophic factors such as neuregulin-1 (NRG1) and brain-derived neurotrophic factor (BDNF), whose release is modulated by neuronal activity. Interestingly, cell-culture experiments have shown that NRG1 and BDNF influence whether neuronal activity stimulates myelination (7). In vivo optogenetics studies have also shown that elevated neuronal activity increases OPC proliferation elin. Several psychiatric illnesses, such as schizophrenia and bipolar disorder, are associated with defects in myelin (