Site-specific gene modification by oligodeoxynucleotides in mouse bone marrow-derived mesenchymal stem cells

Flagler, K; Alexeev, Vitali; Pierce, Eric A.; Igoucheva, Olga

doi:10.1038/gt.2008.31

Cited by 8 publications

(10 citation statements)

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“…Primary bone marrow-derived MSCs were isolated from newborn C57BL/6 wild-type mice as described previously (17). Immunodepletion was carried out using mouse lineage depletion kit (Miltenyi Biotec, Auburn, CA).…”

Section: Methodsmentioning

confidence: 99%

“…Receptor expression in primary MSC cultures was determined via FACS using fluorescent-labeled antibodies generated against Ccr3, Ccr4, Ccr5, Ccr6, Ccr7, Ccr9, Ccr10, Cxcr2, Cxcr3, Cxcr4, Cxcr7 (BioLegend, San Diego, CA) as described previously (17). Cells labeled with FITC-, PE-, PerCp/Cy5.5- or Alexa Fluor-647-conjugated antibodies were analyzed with BD FACSCalibur flow cytometer (BD Biosciences).…”

Section: Methodsmentioning

confidence: 99%

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Analysis of chemotactic molecules in bone marrow-derived mesenchymal stem cells and the skin: Ccl27-Ccr10 axis as a basis for targeting to cutaneous tissues

et al. 2013

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Background aims The adult stem cells produce a plethora of extracellular matrix (ECM) molecules and have a high potential as cell-based therapeutics for connective tissue disorders of the skin. However, the primary challenge of the stem cell-based approach is associated with the inefficient homing of systemically infused stem cells to the skin. Methods We examined chemotactic mechanisms that govern directional migration of the mesenchymal stem cells (MSCs) into the skin by conducting a comprehensive expression analysis of chemotactic molecules in MSCs and defined cutaneous tissues from normal and hereditary epidermolysis bullosa (EB)-affected skin. Results Analysis of chemokine receptors in short and long-term MSC cultures showed tissue culture-dependent expression of several receptors. Assessment of epidermis- and dermis-derived chemokines showed that majority of skin-originated chemotactic signals preferentially recruit different sets of leukocytes rather than MSCs. Analysis of the chemotactic molecules derived from EB-affected non-blistered skin showed only minor changes in expression of selected chemokines and receptors. Nevertheless, the data allowed us to define Ccl27-Ccr10 chemotactic axis as the most potent for the recruitment of MSCs to the skin. Our in vivo analysis demonstrated that uniform expression of Ccr10 on MSCs and alteration of Ccl27 level in the skin enhance extravasation of stem cells from circulation and facilitate their migration within cutaneous tissue. Conclusions Collectively, our study provides a comprehensive analysis of chemotactic signal in normal and EB-affected skin and proof-of-concept data demonstrating that alteration of the chemotactic pathways can enhance skin homing of the therapeutic stem cells.

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Analysis of chemotactic molecules in bone marrow-derived mesenchymal stem cells and the skin: Ccl27-Ccr10 axis as a basis for targeting to cutaneous tissues

et al. 2013

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“…The homogeneous phenomenon of drug metabolic isoenzymes may play a major role in providing physiological regulation to avoid acute rejection [2], [4], [9]. In a recent bone marrow stem cell study, direct DNA sequencing confirmed that phenotype changes were caused by mutations [11]. In our previous study [4], all recipients underwent sequential graft liver biopsies, and DNA sequencing analysis showed that all of the final liver CYP2C19 genotypes of the recipients depended on those of the donors, but were not related to the original characteristic genotype of the recipients after LDLT.…”

Section: Discussionmentioning

confidence: 99%

Pyrosequencing to Identify Homogeneous Phenomenon When Using Recipients/Donors with Different CYP3A5*3 Genotypes in Living Donor Liver Transplantation

et al. 2013

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This study used pyrosequencing to determine the proportional distribution of CYP3A5*3 genotypes to further confirm the homogeneous phenomenon that is observed when recipients and donors in living donor liver transplantation (LDLT) have a different single nucleotide polymorphism (SNP) genotype. We enrolled 42 recipient/living donor pairs and the SNPs of CYP3A5*3 were identified by polymerase chain reaction-restriction fragment length polymorphism. We performed 120 liver graft biopsies as part of clinical investigations after LDLT. Pyrosequencing of the CYP3A5*3 SNPs revealed that among the 16 recipients with the G/G genotype, 94.68% had the G and 5.32% the A allele. Among the 14 recipients with the A/G genotype, 78.08% had the G and 21.92% the A allele, and among the 12 recipients with the A/A genotype, 18.45% had the G and 81.55% the A allele. Among the 12 donors with the G/G genotype, 93.85% had the G and 6.14% the A allele. Among the 26 donors with the A/G genotype, 75.73% had the G and 24.27% the A allele, and among the 4 donors with the A/A genotype, 11.09% had the G and 88.91% the A allele. There were a total of 120 liver graft biopsy samples; among the 37 recipients with the G/G genotype, 89.74% had the G and 10.26% the A allele, among the 70 recipients with the A/G genotype, 71.57% had the G and 28.43% the A allele, and among the 13 recipients with the A/A genotype, 48.25% had the G and 51.75% the A allele. The proportional distribution of G and A alleles of the CYP3A5*3 SNP between recipients/donors and liver grafts after LDLT was significantly different (p<0.001). Pyrosequencing was useful in identifying detailed proportional changes of the CYP3A5*3 SNP allele distribution, and to confirm the homogeneous phenomenon when recipients and donors in LDLT have a different genotype.

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“…First, delivery of ODNs or nucleases in cells maintained in culture it is easier to accomplish as it can rely on both chemical as well as physical methods of delivery. For instance, the use of chemical-based reagents such as Lipofectamine™ 2000, Fugene® HD and other of transfection reagents currently in the market, as well as electroporation devices such as Amaxa Nucleofector™ and Neon® Electroporation System have proven to be effective in delivering naked DNA, including ssODNs as well as plasmids encoding nucleases into muscle progenitor cells, SCs, and ESCs (Bertoni and Rando, 2002; Bertoni et al, 2003, 2005; Dekker et al, 2003, 2006; Pierce et al, 2003; Aarts et al, 2006; Flagler et al, 2008; Kayali et al, 2010; Corti et al, 2012; Fontes and Lakshmipathy, 2013). Additionally, viral vectors can be used to express nucleases in cases where chemical and electroporation methods pose a challenge.…”

Section: Future Of Gene Editing Strategies In Muscle Stem Cellsmentioning

confidence: 99%

Emerging gene editing strategies for Duchenne muscular dystrophy targeting stem cells

Bertoni¹

2014

Front. Physiol.

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The progressive loss of muscle mass characteristic of many muscular dystrophies impairs the efficacy of most of the gene and molecular therapies currently being pursued for the treatment of those disorders. It is becoming increasingly evident that a therapeutic application, to be effective, needs to target not only mature myofibers, but also muscle progenitors cells or muscle stem cells able to form new muscle tissue and to restore myofibers lost as the result of the diseases or during normal homeostasis so as to guarantee effective and lost lasting effects. Correction of the genetic defect using oligodeoxynucleotides (ODNs) or engineered nucleases holds great potential for the treatment of many of the musculoskeletal disorders. The encouraging results obtained by studying in vitro systems and model organisms have set the groundwork for what is likely to become an emerging field in the area of molecular and regenerative medicine. Furthermore, the ability to isolate and expand from patients various types of muscle progenitor cells capable of committing to the myogenic lineage provides the opportunity to establish cell lines that can be used for transplantation following ex vivo manipulation and expansion. The purpose of this article is to provide a perspective on approaches aimed at correcting the genetic defect using gene editing strategies and currently under development for the treatment of Duchenne muscular dystrophy (DMD), the most sever of the neuromuscular disorders. Emphasis will be placed on describing the potential of using the patient own stem cell as source of transplantation and the challenges that gene editing technologies face in the field of regenerative biology.

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Site-specific gene modification by oligodeoxynucleotides in mouse bone marrow-derived mesenchymal stem cells

Cited by 8 publications

References 58 publications

Analysis of chemotactic molecules in bone marrow-derived mesenchymal stem cells and the skin: Ccl27-Ccr10 axis as a basis for targeting to cutaneous tissues

Analysis of chemotactic molecules in bone marrow-derived mesenchymal stem cells and the skin: Ccl27-Ccr10 axis as a basis for targeting to cutaneous tissues

Pyrosequencing to Identify Homogeneous Phenomenon When Using Recipients/Donors with Different CYP3A5*3 Genotypes in Living Donor Liver Transplantation

Emerging gene editing strategies for Duchenne muscular dystrophy targeting stem cells

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