Carol L. Beck, PhD
Associate Professor
Associate Dean, Jefferson College of Life Sciences
Contact Information
1020 Locust Street
Room M-46
Philadelphia, PA 19107
215-503-6539
215-503-3433 fax
Associate Professor
Associate Dean, Jefferson College of Life Sciences
Education
PhD, Vanderbilt University (1993)
BS, PharmD, University of Kentucky (1983)
Publications
- Therapeutic drug monitoring in the long-term care facility.
- Human Infection with Herpes Zoster: Etiology, Pathophysiology, Diagnosis, Clinical Course, and Treatment
- Patient tolerance to intravenous potassium chloride with and without lidocaine
- Evaluation of therapeutic drug monitoring in a long-term care facility: a pilot project
- Evaluation of Creatinine Clearance Estimation in an Elderly Male Population
Research & Clinical Interests
Mutations in the skeletal muscle chloride channel gene (CLCN-1) have been implicated in the human diseases myotonia congenita and recessive generalized myotonia and in animal models of myotonia in mouse, goat and dog. Myotonia is characterized by delayed relaxation of muscle secondary to sarcolemmal hyperexcitability and is the result of diminished chloride conductance in the muscle cell membrane. When chloride conductance (GCl) is reduced, either by drugs or dysfunctional channels, the repetitive myotonic contractions characteristic of the disease occur. These hereditary mutations are significant links between the pathology of these diseases and the basic physiology of skeletal muscle. We are using a combination of approaches to further our understanding of structure-function relationships of the affected voltage-gated ion channels and of the skeletal muscle diseases.
We want to understand how the molecular structure of ion channels contributes to their function. The carboxyl terminus of the ClC-1 chloride channel surrounding the mutation identified in myotonic goats contains multiple praline residues. Proline-rich domains have been found to participate in protein-protein interactions with specific binding motifs such as Src homology and WW domains. We hypothesize that the carboxyl terminus of ClC-1 participates in protein-protein interactions and that these interactions are important for proper channel function.
In other research in the laboratory, we have identified two murine members of the CLCA family (calcium-activated chloride channels), mCLCA5 and mCLCA6. We are examining the function of these proteins.