Judith Singer-Sam, Ph.D.
- Associate Chair and Professor Emeritus, Department of Cancer Biology
Judith Singer-Sam, Ph.D.
- 2012 - present, Professor Emeritus, Department of Cancer Biology, Beckman Research Institute of City of Hope, Duarte, CA
- 2009 - 2012, Professor and Director, Division of Biology, Beckman Research Institute of City of Hope, Duarte, CA
- 2009 - 2012, Associate Chair, Department of Cancer Biology, Beckman Research Institute of City of Hope, Duarte, CA
- 2006 - 2009, Professor, Department of Biology, Beckman Research Institute of City of Hope, Duarte, CA
- 2001 - 2009, Associate Chair, Department of Biology, Beckman Research Institute of City of Hope, Duarte, CA
- 2003 - 2006, Professor, Department of Biology, Beckman Research Institute of City of Hope, Duarte, CA
- 1999, Associate Professor, Beckman Research Institute of City of Hope, Duarte, CA 1985 - 1993, Associate Research Scientist, Beckman Research Institute of City of Hope, Duarte, CA
- 1981, Visiting Scientist, Pasteur Institute, Paris
- 1979 - 1985, Assistant Research Scientist, City of Hope, Duarte, CA 1976 - 1979, Research Associate, City of Hope, Duarte, CA 1972 - 1975, Postdoctoral Fellow, City of Hope, Duarte, CA
- Cancer Biology
- 1967, City College of New York, B.S., Biology
- 1973, University of California, Santa Barbara, Ph.D., Biology (Microbial Genetics & Biochemistry)
Monoallelic Expression in the Central Nervous System
Although most genes in a cell are expressed from both the maternal and paternal chromosome, there are exceptions. For example, in women, most X-linked genes are expressed from only one of the two X chromosomes, a phenomenon called X inactivation. In addition, there is a class of autosomal genes, termed imprinted genes, for which parental origin determines which allele is expressed. Finally, there are autosomal genes that appear at first glance to be bi-allelically expressed but actually show random monoallelic expression (sometimes termed allelic exclusion) at the single-cell level. These exceptions, examples of epigenetics, have proven to be of great interest for researchers because they shed light on gene regulation, chromatin structure, development, and the pattern of inheritance of certain genetic disorders.
My research program is focused on the potential role of allele-specific expression in development and function of the central nervous system (CNS). What is the evidence that genes likely to play a role in CNS function show such expression? Olfactory receptors, which are expressed in specialized cells of the CNS, show allelic exclusion, as does p120 catenin, which is involved in synapse formation. Intriguing recent work has shown that a number of factors involved in the immune response, including the genes for interleukin-2 and interleukin-4, also show allelic exclusion. Some of these genes are expressed in the CNS, and the possibility arises that other inflammation-sensitive genes in the CNS may show a similar pattern of expression. Using gene expression profiling, we discovered that, Cdkn1a, coding for the cell cycle regulator p21Waf1/Cip1, is inflammation-sensitive in the CNS as well as other tissues. While this gene is bi-allelically expressed, we expect to find additional immune response genes that do undergo monoallelic expression.
We have also developed an imprinting screen using expression microarrays. As a model system, we analyzed mice with imprinting defects in proximal chromosome 7; part of this region is analogous to human chromosome 15q11-q13, a locus associated with a number of behavioral and cognitive disorders including the well-studied Prader-Willi/Angelman Syndrome (PW/AS). Our analysis revealed the presence of two novel paternally expressed intergenic transcripts at the mouse PW/AS locus, in a region highly enriched in LINE-1 elements; the function of these transcripts is still unknown. In separate work, we discovered, in collaboration with Dr. Chauncey Bowers (Department of Neurosciences) that the dense LINE-1 elements in this region are organized in a uniquely asymmetric way, perhaps related to imprinting at the locus.
Our current work involves the identification and characterization of genes that are subject to random monoallelic expression in the CNS. We have developed a microarray-based assay for genes that are both silenced and active at the same locus as evidenced by a dual DNA methylation pattern. We further analyze candidate genes using SNP differences in cDNA of clonal neural stem cell lines derived from F1 hybrids of two different strains of mice. We have found a number of “hits” and are currently characterizing those that appear potentially most relevant to disorders of the CNS.
For a growing number of genes, only one of the two chromosomal copies (or alleles) is expressed, a phenomenon termed monoallelic expression. In some cases, there is random selection of the expressed allele; in others parental origin determines which allele is expressed, which is termed imprinting. Disorders with a genetic component in which either random monoallelic expression or imprinting may play a role include schizophrenia, multiple sclerosis, and diabetes.
Our goal is to understand the mechanism and extent of imprinting and monoallelic expression, and their possible relevance to inherited disorders, particularly those of the central nervous system. Towards this goal, we are studying a mouse locus corresponding to a human inherited mental retardation disorder known to involve imprinted genes, the Prader-Willi/Angelman Syndrome. We are also developing an assay that would make use of state-of-the-art microarray technology to probe for imprinting and monoallelic expression in the entire genome.