Salk Institute
Rusty Gage
Laboratory of Genetics
Vi and John Adler Chair for Research on Age-Related Neurodegenerative Disease
Rusty Gage

Laboratory of Genetics
Vi and John Adler Chair for Research on Age-Related Neurodegenerative Disease


Fred H. "Rusty" Gage, a professor in the Laboratory of Genetics, concentrates on the adult central nervous system and unexpected plasticity and adaptability to environmental stimulation that remains throughout the life of all mammals. Gage's lab showed that, contrary to accepted dogma, human beings are capable of growing new nerve cells throughout life. Small populations of immature nerve cells are found in the adult Human brain, a process called Neurogenesis. Gage is working to understand how these cells can be induced to become mature functioning nerve cells in the adult brain and spinal cord. They showed that environmental enrichment and physical exercise can enhance the growth of new brain cells and they are studying the underlying cellular and molecular mechanisms of neurogenesis.

In addition, the Gage lab focuses on modeling diseases in vitro using human stem cells. Through reprogramming of human somatic cells from patients with neurologic and psychiatric disease, his work seeks to understand the progression and mechanisms that lead to neuronal and glial dysfunction. Finally his lab studies the genomic mosaicism that exists in the brain as a result of mobile elements that are active during neurogenesis. Specifically, Dr. Gage is interested in differences between individuals and how somatic-induced genomic mosaicism may lead to functional diversity.

"Differences arise at every level of the brain's astonishingly intricate architecture, leading to variances in how we think, learn and behave and in our propensity for mental illness. Jumping genes may explain how some of these differences arise, even in identical twins."

Variations in the genes we inherit from our parents ensure that each of our brains is wired differently. But even identical twins, who inherit the same set of genes, can differ markedly in their mental functioning, behavioral traits and risk of mental illness or neurodegenerative disease. From where do these differences arise?

Gage's laboratory has identified a likely suspect in the hunt for an explanation for this mysterious variability in brain function: jumping genes. Such genes (also known as "retrotransposons") can insert copies of themselves into other parts of the genetic code, making one neuron function very differently than its neighbor. Many such insertions may create a mosaic of cells possessing varying genetic operating instructions, which in turn could influence cognitive abilities, personality traits and susceptibility to neurological problems.

To better understand how jumping genes play a role in brain function, Gage and his colleagues have investigated the genetic underpinnings of Rett syndrome, a rare neurodevelopmental disease that affects mostly girls and is considered one of the autism spectrum disorders. Typical features of the disorder include loss of speech, stereotypic movements, mental retardation and social behavioral problems. Although almost all cases are caused by a mutation in the MeCP2 gene, how severely people are affected by the symptoms of Rett syndrome varies widely.

Gage's team found that a mutation in the MeCP2 gene mobilizes the L1 retrotransposons in brain cells of Rett syndrome patients, reshuffling their genomes. Their research showed that the mutation in the brains of mice with Rett syndrome resulted in a significant increase in numbers of L1 insertions in their neurons, suggesting that the jumping genes might account for some of the effects of the MeCP2 mutation. Using stem cell reprogramming techniques, the researchers generated neurons from skin cells of Rett syndrome patients, which they could then study in the laboratory. Similar to the findings in mice, these human neurons possessed high numbers of L1 copies, which might explain the variability in symptoms seen in people with the disorder.

Gage's findings may not only explain how a single mutation can cause the baffling variability of symptoms typical of Rett syndrome but also shed new light on the complexity of molecular events that underlie other psychiatric disorders, such as autism and schizophrenia.

Lab Photo

Top row, left to right: Jenny Erwin, Apua Paquola, Anthony Simone, David Husband, Cedric Bardy, Dane Clemenson, Matthew Ellis, Mark Van Den Hurk, Ruben Hernandez, Krishnan Padmanabhan, Roberto Jappelli, Arianna Mei, Vicki Sciorra, Wei Deng, Yangling Mu

Middle row, left to right: Mohamedi Kagalwala, Tiago Goncalves, Julia Wrin-Piper, Michael McConnell, Benjamin Lacar, Fernando Flores, Eunice Mejia, Christopher Tse, Jinju Han, Jun Yao, Ahmet Denli, Bilal Kerman, Hyung Joon Kim, Yongsung Kim, Iryna Gallina

Front row, left to right: Ngoc Tran, Kristen Brennand, Leah Boyer, Inigo Narvazia, Yanelli Nunez, Elmar Malek, John Jepsen, Fred. H. Gage, Benjamin Campbell, Elisa Nabel, Diana Yu, Lynne Moore, Isabelle Guimont, Carol Marchetto, Ruth Keithley, Star Lee, Tithi Baul, Cheyenne Butcher, Yan Li, Chunmei Zhao

Salk News Releases

Awards and Honors

  • President of the International Society for Stem Cell Research 2011-12
  • Member, American Philosophical Society, 2010
  • Keio Medical Science Prize Award, shared with Shimon Sakaguchi, 2008
  • Fellow of the American Academy of Arts and Sciences, 2005
  • Fellow of the National Academy of Sciences, 2003
  • MetLife Award for Medical Research, 2002
  • National Academy of Medicine, 2001
  • President, Society for Neuroscience, 2001
  • Max Planck Research Prize, 1999
  • Christopher Reeve Research Medal, 1997
  • Achievements in Health and Education, 1993
  • Charles A. Dana Award for Pioneering Achievements in Health and Education, 1993
  • IPSEN Prize in Neuronal Plasticity, 1990

Patients' own cells yield new insights into the biology of schizophrenia

March 17, 2011

After a century of studying the causes of schizophrenia-the most persistent disabling condition among adults-the cause of the disorder remains unknown. Now induced pluripotent stem cells (iPSCs) generated from schizophrenic patients have brought researchers from the Salk Institute for Biological Studies a step closer to a fundamental understanding of the biological underpinnings of the disease. Read more>>

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