Literature DB >> 31398502

Ex vivo gene therapy using human bone marrow cells overexpressing BMP-2: "Next-day" gene therapy versus standard "two-step" approach.

Sofia Bougioukli1, Ram Alluri1, William Pannell1, Osamu Sugiyama1, Andrew Vega1, Amy Tang1, Tautis Skorka2, Sang Hyun Park3, Daniel Oakes1, Jay R Lieberman4.   

Abstract

Traditionally, ex vivo gene therapy involves a two-step approach, with culture expansion of cells prior to transduction and implantation. We have tried to simplify this strategy and eliminate the time and cost associated with culture expansion, by introducing "next-day" regional gene therapy using human bone marrow cells. The purpose of this study was to determine whether a lentiviral vector (LV) carrying the cDNA for BMP-2 can transduce freshly isolated human BM cells, leading to abundant BMP production and bone formation in vivo, and evaluate the in vivo osteoinductive potential of "next-day" gene therapy and the standard "two-step" tissue culture expansion approach. To this end, human bone marrow cells (HBMC) from patients undergoing total hip arthroplasty were harvested, transduced with a BMP-2-expressing LV either overnight ("next day" gene therapy; ND) or after culture expansion (cultured "two-step" approach; C) and then implanted into a rat critical-sized femoral defect. The animals were randomly assigned to one of the following groups: I; ND-HBMC transduced with LV-TSTA BMP-2, II; ND-HBMC transduced with LV-TSTA GFP, III; non-transduced ND-HBMC; IV; C-HBMC transduced with LV-TSTA BMP-2, V; C-HBMC transduced with LV-TSTA-GFP, VI; non-transduced C-HBMC. Treatment with either "next-day" or cultured HBMC demonstrated a significant increase in new bone formation compared with all negative control groups as seen in plain radiographs, microCT and histologic/histomorphometric analysis. At 12 weeks post-op, complete defect union on plain X-rays occurred in 7/14 animals in the ND-HBMC/BMP-2 group and 12/14 in the C-HBMC/BMP-2 treated rats. The two-step approach was associated with more consistent results, a higher union rate, and superiority with regards to all of the studied bone healing parameters. In this study we demonstrate proof of concept that BMP-2-transduced human bone marrow cells can be used to enhance bone healing in segmental bone defects, and that regional gene therapy using lentiviral transduction has the osteoinductive potential to heal large bone defects in clinical settings.
Copyright © 2019 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  BMP-2; Bone healing; Ex vivo gene therapy; Human bone marrow

Mesh:

Substances:

Year:  2019        PMID: 31398502      PMCID: PMC6813891          DOI: 10.1016/j.bone.2019.08.005

Source DB:  PubMed          Journal:  Bone        ISSN: 1873-2763            Impact factor:   4.398


  43 in total

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3.  Epidemiology of Fracture Nonunion in 18 Human Bones.

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4.  Healing of critically sized femoral defects, using genetically modified mesenchymal stem cells from human adipose tissue.

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5.  The role of transduced bone marrow cells overexpressing BMP-2 in healing critical-sized defects in a mouse femur.

Authors:  M Pensak; S Hong; A Dukas; B Tinsley; H Drissi; A Tang; M Cote; O Sugiyama; A Lichtler; D Rowe; J R Lieberman
Journal:  Gene Ther       Date:  2015-03-26       Impact factor: 5.250

6.  Influence of short-term adenoviral vector and prolonged lentiviral vector mediated bone morphogenetic protein-2 expression on the quality of bone repair in a rat femoral defect model.

Authors:  Mandeep Singh Virk; Augustine Conduah; Sang-Hyun Park; Nancy Liu; Osamu Sugiyama; Anna Cuomo; Christine Kang; Jay R Lieberman
Journal:  Bone       Date:  2008-01-05       Impact factor: 4.398

Review 7.  Clinical effectiveness and cost-effectiveness of bone morphogenetic proteins in the non-healing of fractures and spinal fusion: a systematic review.

Authors:  K R Garrison; S Donell; J Ryder; I Shemilt; M Mugford; I Harvey; F Song
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8.  Biodistribution of LV-TSTA transduced rat bone marrow cells used for "ex-vivo" regional gene therapy for bone repair.

Authors:  Farhang Alaee; Cynthia Bartholomae; Osamu Sugiyama; Mandeep S Virk; Hicham Drissi; Qian Wu; Manfred Schmidt; Jay R Lieberman
Journal:  Curr Gene Ther       Date:  2015       Impact factor: 4.391

9.  Gene Therapy to Enhance Bone and Cartilage Repair in Orthopaedic Surgery.

Authors:  Sofia Bougioukli; Christopher H Evans; Ram K Alluri; Steven C Ghivizzani; Jay R Lieberman
Journal:  Curr Gene Ther       Date:  2018       Impact factor: 4.391

10.  Office-Based Mesenchymal Stem Cell Therapy for the Treatment of Musculoskeletal Disease: A Systematic Review of Recent Human Studies.

Authors:  Luke Law; Christine L Hunt; Andre J van Wijnen; Ahmad Nassr; A Noelle Larson; Jason S Eldrige; William D Mauck; Mathew J Pingree; Juan Yang; Casey W Muir; Patricia J Erwin; Mohamad Bydon; Wenchun Qu
Journal:  Pain Med       Date:  2018-12-29       Impact factor: 3.750

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Authors:  Sofia Bougioukli; Morgan Chateau; Heidy Morales; Venus Vakhshori; Osamu Sugiyama; Daniel Oakes; Donald Longjohn; Paula Cannon; Jay R Lieberman
Journal:  Gene Ther       Date:  2020-08-17       Impact factor: 5.250

3.  Orthopaedic Gene Therapy: Twenty-Five Years On.

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Review 4.  Modifying MSC Phenotype to Facilitate Bone Healing: Biological Approaches.

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5.  Regional Gene Therapy with Transduced Human Cells: The Influence of "Cell Dose" on Bone Repair.

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Journal:  Tissue Eng Part A       Date:  2021-08-25       Impact factor: 3.845

Review 6.  Gene therapy for bone healing: lessons learned and new approaches.

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Journal:  Transl Res       Date:  2021-05-05       Impact factor: 10.171

Review 7.  Clinical Application of Bone Marrow Mesenchymal Stem/Stromal Cells to Repair Skeletal Tissue.

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Review 8.  Gene Therapy in Orthopaedics: Progress and Challenges in Pre-Clinical Development and Translation.

Authors:  Rachael S Watson-Levings; Glyn D Palmer; Padraic P Levings; E Anthony Dacanay; Christopher H Evans; Steven C Ghivizzani
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