Search

Zhen Yan

Yan, Zhen

Primary Appointment

Professor, Medicine: Cardiovascular Medicine

Education

  • PhD, Vascular Biology, University of Texas Health Sciences Center, Houston

Contact Information

PO Box 801394
MR-4 Room 6041A
Charlottesville, VA 22908
Telephone: 434-982-4477
Email: zy3m@virginia.edu

Research Disciplines

Cardiovascular Biology, Metabolism, Molecular Pharmacology, Physiology

Research Interests

Molecular and Signaling Mechanisms of Skeletal Muscle Plasticity

Research Description

Skeletal muscle is remarkably plastic such that alteration in contractile load, hormonal shifts, or systemic diseases can induce profound phenotypic changes. Research in this laboratory focuses on skeletal muscle adaptations induced by endurance exercise and maladaptation under chronic heart failure and type 2 diabetes mellitus conditions. We employ the state-of-the-art technologies, such as in vivo bioluminescence imaging, in a variety of experimental models ranging from cultured cells to genetically engineered mice. Our goal is to improve the understanding of the molecular and signaling mechanisms underlying physiological adaptation and pathological maladaptation in skeletal muscle.

1. Exercise-induced skeletal muscle adaptation

Accumulating evidence suggests that increased peroxisome proliferator-activated receptor γ co-activator-1a (Pgc-1a) expression plays a pivotal role in exercise-induced adaptation in skeletal muscle; however, the molecular mechanisms remain elusive. Our studies defined an essential role of p38γ mitogen-activated protein kinase (MAPK) in promoting Pgc-1a transcription and metabolic adaptation (mitochondrial biogenesis and angiogenesis). We have also confirmed that p38a and p38β and their downstream E3 ubiquitin ligases and autophagy-related genes in the proteolytic processes in muscle wasting. We are currently investigating the isoform-specific function of p38 MAPK in physiological adaptation induced by endurance exercise training and in pathological maladaptations in catabolic wasting and metabolic disorders.

2. Mitophagy in type 2 diabetes mellitus

Impaired mitochondria play a critical role in the pathogenesis of type 2 diabetes mellitus; however, the precise mechanism remains poorly understood. We have obtained substantial evidence that lipid overload induces accumulation of damaged mitochondria in skeletal muscle. We are taking advantage of various experimental models ranging from cultured muscle cells to genetically engineered mice to address the importance of mitochondrial maintenance in insulin resistance. Specifically, we are interested in the critical steps involved in mitochondrial degeneration and clearance (mitochondrial autophagy or mitophagy).

3. NO-dependent protection against muscle wasting

Cachexia is a severe medical condition characterized by loss of muscle mass (catabolic wasting) and is associated with many chronic diseases. The direct causes are skeletal muscle abnormalities as consequences of accumulation of reactive oxygen species (ROS) and associated cellular damages. It is well known that muscles of oxidative phenotype are resistant to catabolic wasting; however, the underlying mechanism remains to be defined. We have shown that in a mouse genetic model of CHF [cardiac-specific calsequestrin (CSQ) transgenic mice] this muscle protection is due to a nitric oxide (NO)-dependent antioxidant defense through activation of the Keap1/Nrf2 scaffold protein-transcription factor complex. We are focusing on the regulation and function of extracellular superoxide dismutase (EcSOD or SOD3) in NO-dependent protection against cachexia in skeletal muscle using both transgenic and somatic gene transfer approaches.

Selected Publications