Active Vitamin D3 (Calcitriol) Increases Adipose Graft Retention in a Xenograft Model

Author:

Loder Shawn1ORCID,Wang Sheri2ORCID,Amurgis Charles3,DeSanto Marisa4,Stavros Alexander G5,Patadji Stell6,Olevian Dane6,Lee Phoebe7,Guerrero David7,Gusenoff Jeffrey A8,Peter Rubin J9,Kokai Lauren E10

Affiliation:

1. Resident, Department of Plastic Surgery, University of Pittsburgh , Pittsburgh, PA , USA

2. Resident, Department of Anesthesiology, University of Pittsburgh , Pittsburgh, PA

3. Research fellow, Department of Plastic Surgery, University of Pittsburgh , Pittsburgh, PA

4. Resident, Pediatrics, University of Rochester , Rochester, NY

5. Resident, Department of Anesthesiology and Critical Care, University of Pennsylvania , Philadelphia, PA , USA

6. Pathologists, Department of Pathology, Anatomy, and Laboratory Medicine, West Virginia University , Morgantown, WV , USA

7. Medical students, Department of Plastic Surgery, University of Pittsburgh , Pittsburgh, PA , USA

8. Professor of plastic surgery, Department of Plastic Surgery, University of Pittsburgh , Pittsburgh, PA , USA and is a Body Contouring section co-editor

9. Department chair, Department of Plastic Surgery, University of Pittsburgh , Pittsburgh, PA , USA

10. Department of Plastic Surgery, University of Pittsburgh , Pittsburgh, PA , USA

Abstract

Abstract Background Autologous fat grafting, although broadly indicated, is limited by unsatisfactory retention and often requires multiple procedures to achieve durable outcomes. Graft survival is strongly influenced by the magnitude and duration of post-engraftment ischemia. Calcitriol is a pleiotropic, safe nutrient with cell-specific influence on viability and metabolic flux. Objectives Evaluate the efficacy of activated vitamin D3 (calcitriol) in improving grafting outcomes and examine its mechanisms. Methods Lipoaspirate was collected for ex vivo culture (7 unique donors), in vitro bioenergetic analysis (6 unique donors), and in vivo transplantation (5 unique donors). Ex vivo samples were incubated for up to 2 weeks before extraction of the stromal vascular fraction (SVF) for viability or flow cytometry. SVF was collected for Seahorse (Agilent; Santa Clara, CA) analysis of metabolic activity. Human endothelial cell lines were utilized for analyses of endothelial function. In vivo, samples were implanted into athymic mice with calcitriol treatment either (1) once locally or (2) 3 times weekly via intraperitoneal injection. Grafts were assessed photographically, volumetrically, and histologically at 1, 4, and 12 weeks. Hematoxylin and eosin (H&E), Sirius red, perilipin, HIF1α, and CD31 tests were performed. Results Calcitriol-treated lipoaspirate demonstrated dose-dependent increases in SVF viability and metabolic reserve during hypoxic stress. Calcitriol treatment enhanced endothelial mobility ex vivo and endothelial function in vitro. In vivo, calcitriol enhanced adipocyte viability, reduced fibrosis, and improved vascularity. Continuous calcitriol was sufficient to improve graft retention at 12 weeks (P < .05). Conclusions Calcitriol increased fat graft retention in a xenograft model. Calcitriol has potential to be a simple, economical means of increasing fat graft retention and long-term outcomes.

Funder

Plastic Surgery Foundation National Endowment for Plastic Surgery

Publisher

Oxford University Press (OUP)

Subject

General Medicine,Surgery

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