Xenotransplant cardiac chimera: immune tolerance of adult stem cells

Saito, Takayuki; Kuang, Jinqiang; Bittira, Bindu; Al-Khaldi, Abdulaziz; Chiu, Ray Chu‐Jeng

doi:10.1016/s0003-4975(02)03591-9

Cited by 244 publications

(145 citation statements)

References 15 publications

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“…Even xenogeneic transplantation of MSCs was well tolerated as demonstrated by the capacity of murine MSCs to colonize and engraft into the injured myocardium of rats after coronary ligation. 19 In these last experiments, it must be emphasized that not only allogeneic MSCs were not rejected but they kept their potential of differentiation. These data thus suggest that an universal donor for MSCs may be used in a therapeutic design.…”

Section: Immunological Characteristics Of Mscsmentioning

confidence: 99%

Engineering mesenchymal stem cells for immunotherapy

et al. 2003

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Section: Immunological Characteristics Of Mscsmentioning

confidence: 99%

Engineering mesenchymal stem cells for immunotherapy

et al. 2003

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“…Such immunological characteristics of BMSCs theoretically can make them impervious to immunorejection following xenogenic transplantation, irrespective of the use of immune suppression. Previous studies have reported conflicting results following xenogenic BMSCS transplantation into non-immunosuppressed hosts, ranging from no survival to differentiation into destination cells [9,19,28,30]. However, in our literature review, we were unable to find any study that had investigated the results of xenogenic BMSCs transplantation in a spine fusion model.…”

Section: Discussionmentioning

confidence: 83%

Transplanted xenogenic bone marrow stem cells survive and generate new bone formation in the posterolateral lumbar spine of non-immunosuppressed rabbits

et al. 2008

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“…12,13,20 Orlic et al showed that BMCs, mobilized by G-CSF and stem cell factor, migrate to the infarcted region, regenerated the de novo myocardium, and improved contractile function and survival in a mouse model of AMI. 20 Kocher et al intravenously injected cytokine-mobilized CD34-positive BMCs, which were purified by flow cytometry using a fluorescence activated cell sorter, in a nude rat model of AMI.…”

Section: Discussionmentioning

confidence: 99%

“…8 Bone marrow is another cell source that has been used clinically, [5][6][7] the advantages of which are that abundant autologous cells can be harvested and, in contrast to SMs, bone marrow cells (BMCs) have the potential to transdifferentiation into cardiomyocytes. [9][10][11] Moreover, they have the unique capacity of migration to the injured site of the heart, 12,13 which may enable noninvasive strategies of BMC transplantation after intravenous (IV) injection. However, it remains unclear whether systemic administration of BMCs is as effective as direct transplantation into the failing heart.…”

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confidence: 99%

Delivery Route in Bone Marrow Cell Transplantation Should be Optimized According to the Etiology of Heart Disease

Nakajima

Sakakibara

Tambara

et al. 2008

Circ J

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Preparation of BMCsBMCs were harvested from 8-week-old syngenic and transgenic male C57Bl/6 mice expressing enhanced green fluorescent protein (GFP), by flushing the femurs and tibias Circ J 2008; 72: 1528 -1535 (Received August 23, 2006 revised manuscript received April 28, 2008; accepted May 9, 2008 Background Recent studies have revealed that bone marrow cell (BMC) transplantation is effective not only for myocardial infarction (MI), but also for dilated cardiomyopathy (DCM). However, the method of administering donor cells remains unknown, and may differ between MI and DCM. In the present study, intramyocardial (IM) injection and intravenous (IV) delivery of BMC were compared in each etiological model. Methods and Results MI was induced in 72 mice and DCM in another 36 mice by doxorubicin. BMCs were administered IV or IM in an acute MI (AMI), old MI (OMI) or DCM model. In the AMI model, left ventricular (LV) remodeling was reduced in both the IM-and IV-groups, but only in the IM-group in the OMI model. In the DCM model, the LV dimension of the IV-group was smaller than that of the IM-group. Histological examination showed that green fluorescent protein (GFP) cells were equally distributed in the infarct area of the IV-and IMgroups in AMI, and in the IM-group in the OMI model. In the DCM model, GFP cells were diffusely scattered throughout the ventricular wall in the IV-group, but were confined to the injection site in the IM-group. Conclusions In OMI, IM delivery of BMCs was more effective than IV; however, IV delivery was superior in DCM. Delivery route should be selected according to the etiology of heart disease to optimize the efficacy of BMC transplantation. (Circ J 2008; 72: 1528 -1535

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Xenotransplant cardiac chimera: immune tolerance of adult stem cells

Cited by 244 publications

References 15 publications

Engineering mesenchymal stem cells for immunotherapy

Engineering mesenchymal stem cells for immunotherapy

Transplanted xenogenic bone marrow stem cells survive and generate new bone formation in the posterolateral lumbar spine of non-immunosuppressed rabbits

Delivery Route in Bone Marrow Cell Transplantation Should be Optimized According to the Etiology of Heart Disease

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