Matthew P. Murphy
Stanford University
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Featured researches published by Matthew P. Murphy.
Wiley Interdisciplinary Reviews-Developmental Biology | 2018
Alessandra L. Moore; Clement D. Marshall; Leandra A. Barnes; Matthew P. Murphy; Ryan C. Ransom; Michael T. Longaker
Since the discovery of scarless fetal skin wound healing, research in the field has expanded significantly with the hopes of advancing the finding to adult human patients. There are several differences between fetal and adult skin that have been exploited to facilitate scarless healing in adults including growth factors, cytokines, and extracellular matrix substitutes. However, no one therapy, pathway, or cell subtype is sufficient to support scarless wound healing in adult skin. More recently, products that contain or mimic fetal and adult uninjured dermis were introduced to the wound healing market with promising clinical outcomes. Through our review of the major experimental targets of fetal wound healing, we hope to encourage research in areas that may have a significant clinical impact. Additionally, we will investigate therapies currently in clinical use and evaluate whether they represent a legitimate advance in regenerative medicine or a vulnerary agent. WIREs Dev Biol 2018, 7:e309. doi: 10.1002/wdev.309
Nature Protocols | 2018
Gunsagar Gulati; Matthew P. Murphy; Owen Marecic; Michael Lopez; Rachel E. Brewer; Lauren S. Koepke; Anoop Manjunath; Ryan C. Ransom; Ankit Salhotra; Irving L. Weissman; Michael T. Longaker; Charles K. Chan
There are limited methods available to study skeletal stem, progenitor, and progeny cell activity in normal and diseased contexts. Most protocols for skeletal stem cell isolation are based on the extent to which cells adhere to plastic or whether they express a limited repertoire of surface markers. Here, we describe a flow cytometry-based approach that does not require in vitro selection and that uses eight surface markers to distinguish and isolate mouse skeletal stem cells (mSSCs); bone, cartilage, and stromal progenitors (mBCSPs); and five downstream differentiated subtypes, including chondroprogenitors, two types of osteoprogenitors, and two types of hematopoiesis-supportive stroma. We provide instructions for the optimal mechanical and chemical digestion of bone and bone marrow, as well as the subsequent flow-cytometry-activated cell sorting (FACS) gating schemes required to maximally yield viable skeletal-lineage cells. We also describe a methodology for renal subcapsular transplantation and in vitro colony-formation assays on the isolated mSSCs. The isolation of mSSCs can be completed in 9 h, with at least 1 h more required for transplantation. Experience with flow cytometry and mouse surgical procedures is recommended before attempting the protocol. Our system has wide applications and has already been used to study skeletal response to fracture, diabetes, and osteoarthritis, as well as hematopoietic stem cell-niche interactions in the bone marrow.
Nature Communications | 2018
Ryan C. Ransom; Deshka S. Foster; Ankit Salhotra; Ruth Ellen Jones; Clement D. Marshall; Tripp Leavitt; Matthew P. Murphy; Alessandra L. Moore; Charles P. Blackshear; Elizabeth A. Brett; Derrick C. Wan; Michael T. Longaker
In the original version of this Article, the authors inadvertently omitted Elizabeth A. Brett, who contributed to the generation of the histology figures, from the author list.This has now been corrected in both the PDF and HTML versions of the Article.
Journal of Craniofacial Surgery | 2017
Matthew P. Murphy; Dre Irizarry; Michael Lopez; Alessandra L. Moore; Ryan C. Ransom; Michael T. Longaker; Derek C. Wan; Charles K. Chan
Abstract Craniofacial surgery, since its inauguration, has been the culmination of collaborative efforts to solve complex congenital, dysplastic, oncological, and traumatic cranial bone defects. Now, 50 years on from the first craniofacial meeting, the collaborative efforts between surgeons, scientists, and bioengineers are further advancing craniofacial surgery with new discoveries in tissue regeneration. Recent advances in regenerative medicine and stem cell biology have transformed the authors’ understanding of bone healing, the role of stem cells governing bone healing, and the effects of the niche environment and extracellular matrix on stem cell fate. This review aims at summarizing the advances within each of these fields.
Nature Communications | 2018
Ryan C. Ransom; Deshka S. Foster; Ankit Salhotra; Ruth Ellen Jones; Clement D. Marshall; Tripp Leavitt; Matthew P. Murphy; Alessandra L. Moore; Charles P. Blackshear; Derrick C. Wan; Michael T. Longaker
Cell | 2018
Charles K. Chan; Gunsagar Gulati; Rahul Sinha; Justin Vincent Tompkins; Michael Lopez; Ava C. Carter; Ryan C. Ransom; Andreas Reinisch; Taylor Wearda; Matthew P. Murphy; Rachel E. Brewer; Lauren S. Koepke; Owen Marecic; Anoop Manjunath; Eun Young Seo; Tripp Leavitt; Wan-Jin Lu; Allison Nguyen; Stephanie Diana Conley; Ankit Salhotra; Thomas H. Ambrosi; Mimi R. Borrelli; Taylor Siebel; Karen Chan; Katharina Schallmoser; Jun Seita; Debashis Sahoo; Henry Goodnough; Julius A. Bishop; Michael J. Gardner
Plastic and Reconstructive Surgery | 2017
Matthew P. Murphy; Charles K. Chan; Michael T. Longaker
Plastic and reconstructive surgery. Global open | 2018
Heather E. desJardins-Park; Alessandra L. Moore; Matthew P. Murphy; Dre Irizarry; Bryan A. Duoto; Deshka S. Foster; Ruth Ellen Jones; Shamik Mascharak; Leandra A. Barnes; Clement D. Marshall; Gerlinde Wernig; Michael T. Longaker
Plastic and reconstructive surgery. Global open | 2018
Matthew P. Murphy; Lauren S. Koepke; Michael Lopez; Ryan C. Ransome; Rachel E. Brewer; Owen Marecic; Charles Fk Chan; Michael T. Longaker
Nature | 2018
Ryan C. Ransom; Ava C. Carter; Ankit Salhotra; Tripp Leavitt; Owen Marecic; Matthew P. Murphy; Michael Lopez; Yuning Wei; Clement D. Marshall; Ethan Z. Shen; Ruth Ellen Jones; Amnon Sharir; Ophir D. Klein; Charles K. Chan; Derrick C. Wan; Howard Y. Chang; Michael T. Longaker