Chronic wounds are a major threat to public health and the economy and present as a comorbid complication with major diseases in humans. Although the proper healing of cutaneous wounds requires collective and coordinated behaviors of multiple cell types, the rate-determining step is the recruitment and function of dermal fibroblasts, which are directed to invade the wound by a gradient in the concentration of platelet-derived growth factor (PDGF). A great deal is known about the signal transduction pathways activated by PDGF receptors and other receptor tyrosine kinases; yet mechanistic insights about how those pathways are spatially organized to bias the dynamics of the actin cytoskeleton and the directionality of cell migration are still emerging. A still larger fundamental gap lies inthe integration of molecular, supramolecular, cellular, and tissue-level dynamics of wound healing, which span disparate time (seconds to weeks) and spatial (nm to cm) scales. To advance this field, novel approaches are needed to fuse experimental and observational scales that are relatively data-rich (signaling, cytoskeletal dynamics) and data-poor (in vivo dynamics). To that end, we propose to develop a predictive, multiscale model of the proliferative phase of wound healing, incorporating 1) receptor-mediated signal transduction (molecular scale), 2) self-assembly of contractile actomyosin structures (supramolecular scale), 3) morphodynamics and statistics of cell migration (cellular scale), and 4) collective cell behavior in vivo (tissue scal). Our partnership combines expertise in experimental cell biology and biophysical modeling, and model development will be guided by new, quantitative measurements at every scale of biological abstraction.

Public Health Relevance

Chronic wounds in people suffering from diseases, such as diabetes and obesity, present a significant threat to public health in the United States. Proper healing of cutaneous wounds requires collective and coordinated cellular behavior that spans multiple length and time scales. To achieve a systems-level understanding of wound healing requires novel approaches to fuse observational scales that are relatively data-rich (signaling, cytoskeletal dynamics) with those that are data-poor (in vivo dynamics). To that end, we propose to develop a predictive, multiscale model of the proliferative phase of wound healing.

Agency
National Institute of Health (NIH)
Institute
National Institute of Biomedical Imaging and Bioengineering (NIBIB)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01EB018816-02
Application #
8925080
Study Section
Special Emphasis Panel (ZEB1)
Program Officer
Peng, Grace
Project Start
2014-09-15
Project End
2018-05-31
Budget Start
2015-06-01
Budget End
2016-05-31
Support Year
2
Fiscal Year
2015
Total Cost
Indirect Cost
Name
North Carolina State University Raleigh
Department
Engineering (All Types)
Type
Biomed Engr/Col Engr/Engr Sta
DUNS #
042092122
City
Raleigh
State
NC
Country
United States
Zip Code
27695
Mohan, Krithika; Nosbisch, Jamie L; Elston, Timothy C et al. (2017) A Reaction-Diffusion Model Explains Amplification of the PLC/PKC Pathway in Fibroblast Chemotaxis. Biophys J 113:185-194
Rotty, Jeremy D; Brighton, Hailey E; Craig, Stephanie L et al. (2017) Arp2/3 Complex Is Required for Macrophage Integrin Functions but Is Dispensable for FcR Phagocytosis and In Vivo Motility. Dev Cell 42:498-513.e6
Johnson, Heath E; Haugh, Jason M (2016) Are Filopodia Privileged Signaling Structures in Migrating Cells? Biophys J 111:1827-1830
King, Samantha J; Asokan, Sreeja B; Haynes, Elizabeth M et al. (2016) Lamellipodia are crucial for haptotactic sensing and response. J Cell Sci 129:2329-42
Johnson, Heath E; King, Samantha J; Asokan, Sreeja B et al. (2015) F-actin bundles direct the initiation and orientation of lamellipodia through adhesion-based signaling. J Cell Biol 208:443-55
Haynes, Elizabeth M; Asokan, Sreeja B; King, Samantha J et al. (2015) GMF? controls branched actin content and lamellipodial retraction in fibroblasts. J Cell Biol 209:803-12
Asokan, Sreeja B; Johnson, Heath E; Rahman, Anisur et al. (2014) Mesenchymal chemotaxis requires selective inactivation of myosin II at the leading edge via a noncanonical PLC?/PKC? pathway. Dev Cell 31:747-60