Intravenous Multipotent Adult Progenitor Cell Therapy Attenuates Activated Microglial/Macrophage Response and Improves Spatial Learning After Traumatic Brain Injury

Bedi, Supinder S.; Hetz, Robert A.; Thomas, Chelsea; Smith, Philippa; Olsen, Alex; Williams, Stephen; Xue, Hasen; Aroom, Kevin R.; Uray, Karen; Hamilton, Jason A.; Mays, Robert W.; Cox, Charles S.

doi:10.5966/sctm.2013-0100

Cited by 66 publications

(80 citation statements)

References 41 publications

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“…Thirty-eight studies met inclusion criteria and underwent data extraction and quality assessment. Of these studies, some reported more than one pertinent outcome measure so that a total of 10 studies presented data for RR outcomes (16–25), 14 presented data on LV outcomes (23, 26–38), 21 assessed NSS outcomes (17–21, 23–26, 28, 29, 31, 36, 38–53), and 13 presented data on MWM testing (17, 18, 24, 26, 28, 29, 36, 38, 49–53). Specific study characteristics are listed in Table 1.…”

Section: Resultsmentioning

confidence: 99%

Preclinical progenitor cell therapy in traumatic brain injury: a meta-analysis

Jackson

Srivastava

Cox

2017

Journal of Surgical Research

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Background: No treatment is available to reverse injury associated with traumatic brain injury (TBI). Progenitor cell therapies show promise in both pre-clinical and clinical studies. We conducted a meta-analysis of pre-clinical studies using progenitor cells to treat TBI. Methods: EMBASE, MEDLINE, Cochrane Review, Biosis, and Google Scholar were searched for articles using pre-specified search strategies. Studies meeting inclusion criteria underwent data extraction. Analysis was performed using Review Manager 5.3 according to a fixed-effects model, and all studies underwent quality scoring. Results: Of 430 abstracts identified, 38 met inclusion criteria and underwent analysis. Average quality score was 4.32 out of 8 possible points. No study achieved a perfect score. Lesion volume (LV) and Neurologic Severity Score (NSS) outcomes favored cell treatment with standard mean difference (SMD) of 0.86 (95%CI 0.64, 1.09) and 1.36 (95%CI 1.11, 1.60) respectively. Rotarod (RR) and Morris Water Maze (MWM) outcomes also favored treatment with improvements in SMD of 0.34 (95%CI 0.02, 0.65) and 0.46 (95%CI 0.17, 74) respectively. While LV and NSS were robust to publication bias assessments, RR and MWM were not. Heterogeneity (I2) ranged from 74% to 85% among the analyses, indicating a high amount of heterogeneity among studies. Precision as a function of quality score showed a statistically significant increase in the size of the confidence interval as quality improved. Conclusions: Our meta-analysis study reveals an overall positive effect of progenitor cell therapies on LV and NSS with a trend towards improved motor function and spatial learning in different TBI animal models.

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Section: Resultsmentioning

confidence: 99%

Preclinical progenitor cell therapy in traumatic brain injury: a meta-analysis

Jackson

Srivastava

Cox

2017

Journal of Surgical Research

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“…A decrease in body temperature, known to decrease inflammatory responses, resulted in an increase in cellular proliferation frequency of dentate gyrus DCX‐immunoreactive cells 7 days post‐trauma [67]. Given the immunomodulatory potential of MSC in TBI [26, 33], it is conceivable that the anti‐inflammatory effects of MSCs contribute to neurogenesis in our model.…”

Section: Discussionmentioning

confidence: 99%

“…Stimulation of the thalamic region years after TBI improves arousal level, motor control, and behavioral responses [81], supporting preservation of the thalamus as a new and promising target to improve TBI outcome. Lastly, the reduction in neuroinflammatory responses holds promise in other neurodegenerative diseases besides TBI [26, 33, 37], such as Alzheimer's disease [82] and multiple sclerosis [83].…”

Section: Discussionmentioning

confidence: 99%

Propranolol and Mesenchymal Stromal Cells Combine to Treat Traumatic Brain Injury

Kota

Prabhakara

Brummen

et al. 2015

Stem Cells Translational Medicine

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More than 6.5 million patients are burdened by the physical, cognitive, and psychosocial deficits associated with traumatic brain injury (TBI) in the U.S. Despite extensive efforts to develop neuroprotective therapies for this devastating disorder, there have been no successful outcomes in human clinical trials to date. Retrospective studies have shown that b-adrenergic receptor blockers, specifically propranolol, significantly decrease mortality of TBI through mechanisms not yet fully elucidated but are thought to counterbalance a hyperadrenergic state resulting from a TBI. Conversely, cellular therapies have been shown to improve long-term behavior following TBI, likely by reducing inflammation. Given the nonredundancy in their therapeutic mechanisms, we hypothesized that a combination of acute propranolol followed by mesenchymal stem cells (MSCs) isolated from human bone marrow would have additive effects in treating a rodent model of TBI. We have found that the treatments are well-tolerated individually and in combination with no adverse events. MSCs decrease BBB permeability at 96 hours after injury, inhibit a significant accumulation of activated microglia/ macrophage in the thalamic region of the brain both short and long term, and enhance neurogenesis short term. Propranolol decreases edema and reduces the number of fully activated microglia at 7 days and the number of semiactivated microglia at 120 days. Combinatory treatment improved cognitive and memory functions 120 days following TBI. Therefore, the results here suggest a new, efficacious sequential treatment for TBI may be achieved using the b-blocker propranolol followed by MSC treatment. STEM CELLS TRANSLATIONAL MEDICINE 2016;5:33-44 SIGNIFICANCEDespite continuous efforts, traumatic brain injury (TBI) remains the leading cause of death and disability worldwide in patients under the age of 44. In this study, an animal model of moderatesevere TBI was treated with an acute dose of propranolol followed by a delayed dose of human mesenchymal stem cells (MSCs), resulting in improved short-and long-term measurements. These results have direct translational application. They reinforce the inevitable clinical trial of MSCs to treat TBI by demonstrating, among other benefits, a notable decrease in chronic neuroinflammation. More importantly, these results demonstrate that MSCs and propranolol, which is increasingly being used clinically for TBI, are compatible treatments that improve overall outcome.

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“…Pati and colleagues have shown that MSCs prevent Evans blue dye extravasation (preserved BBB) after TBI and that this effect is due to up regulation and organization of the tight junctional proteins, VE‐cadherin and β‐catenin. These data have been replicated using different cell types (MAPC and bone marrow mononuclear cells [BMMNCs]) using similar TBI models and various methods to evaluate permeability . The reproducibility in multiple laboratories with various cell types and injuries support that this is one of the principal beneficial mechanisms of action with these cell types.…”

Section: Edema and Icp: Is It A Valid Endpoint?mentioning

confidence: 84%

Clinical trials in traumatic brain injury: cellular therapy and outcome measures

2019

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Clinical trials for traumatic brain injury (TBI) have not successfully produced a new therapeutic for neuroprotection or neurorestoration, despite multiple attempts. Stem cell–based therapies and/or cellular therapies have been developed over the past 20 years such that clinical trials are now in Phase II and III stages for neurologic diseases such as TBI and stroke. Many of the vexing issues from past clinical failures still exist today, namely, preclinical data that may not translate to clinical trial because of design and injury heterogeneity that poorly stratifies enrolled patients. Recognition of these problems has led us to advocate for outcome measures that are clinically meaningful, but do not represent a global functional “score.” Specifically, we seek to measure those early physiologically relevant outcomes (intracranial pressure, edema, and therapeutic intensity) and later structural outcomes in regions of interest that are linked to putative mechanisms of action of cell based therapies. Early approval of therapeutics that are successful by these metrics would then allow further access to treatments that could be further tested via patient registries and other surveillance for ultimate adoption. Continuing to do the same thing with each iterative trial will assure the same results.

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Intravenous Multipotent Adult Progenitor Cell Therapy Attenuates Activated Microglial/Macrophage Response and Improves Spatial Learning After Traumatic Brain Injury

Cited by 66 publications

References 41 publications

Preclinical progenitor cell therapy in traumatic brain injury: a meta-analysis

Preclinical progenitor cell therapy in traumatic brain injury: a meta-analysis

Propranolol and Mesenchymal Stromal Cells Combine to Treat Traumatic Brain Injury

Clinical trials in traumatic brain injury: cellular therapy and outcome measures

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