Eileen M. Shore, Ph.D.
Cali and Weldon Research Professor in FOP
Department: Orthopaedic Surgery
Graduate Group Affiliations
Contact information
University of Pennsylvania
Department of Orthopaedic Surgery
424 Stemmler Hall
Philadelphia, PA 19104-6081
Department of Orthopaedic Surgery
424 Stemmler Hall
Philadelphia, PA 19104-6081
Office: 215-898-2331
Fax: 215-573-2133
Fax: 215-573-2133
Email:
SHORE@MAIL.MED.UPENN.EDU
SHORE@MAIL.MED.UPENN.EDU
Publications
Education:
B.S. (Biology)
University of Notre Dame, South Bend, Indiana, 1976.
M.A. (Biology)
Indiana University, Bloomington, Indiana, 1978.
Ph.D. (Cell and Molecular Biology)
University of Pennsylvania, Philadelphia, PA, 1987.
Permanent linkB.S. (Biology)
University of Notre Dame, South Bend, Indiana, 1976.
M.A. (Biology)
Indiana University, Bloomington, Indiana, 1978.
Ph.D. (Cell and Molecular Biology)
University of Pennsylvania, Philadelphia, PA, 1987.
Description of Research Expertise
RESEARCH INTERESTS:Genetic Regulation of Bone Formation: Genetic diseases of bone formation and development. Molecular and cell biology of bone formation and osteoblast differentiation. Cell signaling pathways and transcriptional activation and regulation of bone morphogenetic protein (BMP) and GNAS target genes. Developmental biology of BMP signaling.
KEYWORDS:
Bone formation, cell differentiation, human genetics, molecular biology, cell biology, developmental biology, gene expression, inherited diseases, bone, cartilage, bone morphogenetic protein, BMP, ACVR1, G-proteins, GNAS, FOP, POH.
DESCRIPTION OF RESEARCH:
Research in our laboratory is focused on genetic diseases of bone formation, mainly fibrodysplasia ossificans progressiva (FOP) and progressive osseous heteroplasia (POH). Both of these rare disorders are characterized by de novo formation of bone: in FOP, the ectopic bone forms in deep connective tissues such as muscle; and in POH, bone formation initiates within the skin. Our goals are to investigate the genetic causes of these conditions and the cellular pathways that are involved in the induction of bone development and formation, and to use this information to develop treatments for these and other disorders of bone.
With our identification of the mutated genes for POH and FOP, our experimental directions are focused on determining the functions of these genes and the consequences of the identified mutations. Our current work includes:
POH is caused by heterozygous inactivating mutations in the gene encoding the alpha subunit of the stimulatory G protein of adenylyl cyclase (GNAS). Our data suggest that phenotypic expression of a GNAS mutation may be affected by genomic imprinting. GNAS is a complex gene that encodes multiple transcripts regulated by different promoters. Active areas of investigation include: genetics and epigenetics of GNAS and POH; the roles of GNAS expression in bone and fat cell differentiation; and investigation of the signal transduction pathways mediated by GNAS proteins.
Linkage analysis of families with inheritance of FOP identified a common mutation (R206H) in the ACVR1 gene in patients with classic features of the disease. ACVR1 encodes a BMP type I receptor. Areas of investigation include the genetics and variable expressivity of FOP, for example, recent studies examined the ACVR1 gene in patients with very severe or mild forms of FOP and identified novel ACVRl mutations that suggest genotype-phenotype correlations. We are also investigating the effects of FOP ACVR1 mutations on the BMP signaling pathway and roles in cartilage and bone cell differentiation. Mouse and zebrafish models are being used to investigate the developmental biology of ACVR1 signaling in bone and cartilage as well as other tissues during vertebrate development. Recently initiated studies are investigating the cellular and tissue events that occur prior to aberrant cell differentiation to form bone.
In addition, we are using cell lineage-tracing analyses to investigate the source and identity of the cells that are induced to differentiate into cartilage and/or bone in FOP and POH. We are interested in identifying the earliest cellular events that occur during the induction of bone formation.
Translational studies and drug development are an increasing focus within the lab. Animal models for FOP and POH will be used to evaluate gene therapy and other strategies to treat these conditions.
PUBMED: Shore EM
LAB ROTATION PROJECTS FOR 2012-2013:
Rotation projects are available in most of the research areas described in the Research Summary. Specific projects will be discussed individually. Laboratory research is closely tied to clinical observation and patient care, and students are encouraged to have patient contact.
LAB PERSONNEL: (as of Spring 2012)
Collaborators: FrederickS. Kaplan MD, Robert J. Pignolo, MD, PhD
Students: Andria Culbert (CAMB); Michael Convente (CAMB); Will Towler (CAMB); Edwin Theosmy (post-bac)
Post-doc/Research Associates: Salin Chakkalakal PhD; Julia Haupt PhD; Josef Kaplan PhD; Vitali Lounev PhD; Girish Ramaswamy PhD; Haitao Wang PhD
Research Specialists: Bob Caron; Ruth McCarrick-Walmsley; Meiqi Xu; Deyu Zhang
Selected Publications
Hammond P, Suttie M, Hennekam RC, Allanson J, Shore EM, Kaplan FS: The face signature of fibrodysplasia ossificans progressiva. Am J Med Genet A May 11 2012 Notes: doi: 10/1002/ajmg.a.35346 (Epub ahead of print).Chakkalakal SA, Zhang D, Culbert AL, Convente MR, Caron RJ, Wright AC, Maidment AD, Kaplan FS, Shore EM. : An Acvr1 R206H knock-in mouse has fibrodysplasia ossificans progressiva. J Bone Miner Res April 16 2012 Notes: doi: 10.1002/jbmr.1637 (Epub ahead of print).
Liu JJ, Russell E, Zhang D, Kaplan FS, Pignolo RJ, Shore EM. : Paternally-Inherited GsĪ± Mutation Impairs Adipogenesis and Potentiates a Lean Phenotype In vivo. Stem Cells April 17 2012 Notes: doi: 10.1002/stem.1109 (Epub ahead of print).
Zimmer J, Doelken SC, Horn D, Groppe JC, Shore EM, Kaplan FS, Seemann P. : Functional Analysis of Alleged NOGGIN Mutation G92E Disproves Its Pathogenic Relevance. PLoS One 7(4): e35062, April 18 2012 Notes: PMID#22529972.
Shore EM. : Fibrodysplasia ossificans progressiva (FOP): A human genetic disorder of extra-skeletal bone formation, or - How does one tissue become another? Wiley Interdiscip Rev Dev Biol 1(1): 153-165, January 2012 Notes: PMID#22408652.
Muglu, J.A., A. Garg, T. Pandiarajan, E.M. Shore, F.S. Kaplan, D. Uchil, and M.J. Dickson: Pregnancy in fibrodysplasia ossificans progressiva. Obstet. Med. in press (online publ Dec 2011) December 2011.
Pignolo, R.J., M. Xu, E. Russell, A. Richardson, J. Kaplan, P.C. Billings, F.S. Kaplan, E.M. Shore.: Heterozygous inactivation of Gnas in adipose-derived mesenchymal progenitor cells enhances osteoblast differentiation and promotes heterotopic ossification. JBMR 26(11): 2647-2655, November 2011.
Kaplan, J., F.S. Kaplan, and E.M. Shore : Restoration of normal BMP signaling levels and osteogenic differentiation in FOP mesenchymal progenitor cells by mutant allele-specific targeting. Gene Therapy 10, October 2011 Notes: Published Online ahead of print doi 10.1038/gt 2011.152.
Kan, L.,V.Y. Lounev, R.J. Pignolo, L. Duan, Y. Liu, S.R. Stock, T.L. McGuire, B. Lu, N.P. Gerard, E.M. Shore, F.S. Kaplan and J.A. Kessler.: Substance P signaling mediates BMP-dependant heterotopic ossification. J. Cellular Biochemistry 112(10): 2759-2772, October 2011 Notes: Online doi: 10.1002/jcb.23259.
Shore, E.M. and F.S. Kaplan : Role of altered signal transduction in heterotopic ossification and fibrodysplasia ossificans progressiva. Current Osteoporosis Reports 9(2): 83-88 June 2011.