Stem cell-based therapy for human diseases

Hoang, Duc M.; Pham, Phuong T.; Bach, Trung Q.; Ngo, Anh Toan; Nguyen, Quyen T.; Phan, Trang T. K.; Nguyen, Giang; Le, Phuong Thi-Bich; Hoang, Van T.; Forsyth, Nicholas R.; Heke, Michael; Nguyen, Liem Thanh

doi:10.1038/s41392-022-01134-4

Cited by 404 publications

(237 citation statements)

References 501 publications

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“…[17] Numerous cell types comprise UCB including HSCs, MSCs, Tregs, monocytes and EPCs. [81] In our review, all four outcomes which demonstrated statistically significant differences between UCB cell types were associated with a favoured modification of treatment effect in MSCs over MNCs. Our review provides further neuropathological support for UCB-MSCs as a potential therapeutic option for infants with perinatal brain injury.…”

Section: Discussionmentioning

confidence: 80%

Umbilical cord blood-derived cell therapy for perinatal brain injury: A systematic review & meta-analysis of preclinical studies - Part B

Purcell

Nguyen

Smith

et al. 2022

Preprint

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IntroductionWe previously described preclinical literature, which supports umbilical cord blood-derived cell (UCBC) therapy use for perinatal brain injury. However, efficacy of UCBCs may be influenced by different patient populations and intervention characteristics.ObjectivesTo systematically review effects of UCBCs on brain outcomes in animal models of perinatal brain injury across subgroups to better understand contribution of model type (preterm versus term), brain injury type, UCB cell type, route of administration, timing of intervention, cell dosage and number of doses.MethodsA systematic search of MEDLINE and Embase databases was performed to identify studies using UCBC therapy in animal models of perinatal brain injury. Subgroup differences were measured by chi2test where possible.ResultsDifferential benefits of UCBCs were seen in a number of subgroup analyses including intraventricular haemorrhage (IVH) vs. hypoxia ischaemia (HI) model (apoptosis white matter (WM): chi2=4.07; P=0.04, neuroinflammation-TNF-α: chi2=5.99; P=0.01), UCB-derived mesenchymal stromal cells (MSCs) vs. UCB-derived mononuclear cells (MNCs) (oligodendrocyte WM: chi2=5.01; P=0.03, neuroinflammation-TNF-α: chi2=3.93; P=0.05, apoptosis grey matter (GM), astrogliosis WM) and intraventricular/intrathecal vs. systemic routes of administration (microglial activation GM: chi2=7.51; P=0.02, astrogliosis WM: chi2=12.44; P=0.002). We identified a serious risk of bias and overall low certainty of evidence.ConclusionsPreclinical evidence suggests greater efficacy for UCBCs in IVH compared to HI injury model, use of UCB-MSCs compared to UCB-MNCs, and use of local administrative routes compared to systemic routes in animal models of perinatal brain injury. Further research is needed to improve certainty of evidence found and address knowledge gaps.SIGNIFICANCE STATEMENTIn neonatal medicine there is a clear need for the development of new therapies that can provide neuroregenerative benefits for infants with brain injuries. This review offers a unique and comprehensive resource to inform the development of future preclinical and clinical studies. In part A of this review, we systematically reviewed the preclinical literature surrounding UCBCs as a therapy for perinatal brain injury. In part B of this review, we investigated the effect variables, such as UCB cell type, timing of administration and dosage, have on the efficacy of UCB-derived cell therapy in animal models of perinatal brain injury. We identified UCBCs to show greater efficacy in the brain injury model of IVH compared to HI, the use of UCB-derived MSCs compared to MNCs and the use of local administrative routes compared to systemic routes. In addition to this, we identified knowledge gaps such as the limited preclinical literature surrounding the effect of dose number and sex.

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Section: Discussionmentioning

confidence: 80%

Umbilical cord blood-derived cell therapy for perinatal brain injury: A systematic review & meta-analysis of preclinical studies - Part B

Purcell

Nguyen

Smith

et al. 2022

Preprint

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“…Therefore, the safety and efficacy of several possible dose levels should be tested in phase I and II clinical trials. Furthermore, the relationship between dose and therapeutic effects needs to be elucidated in pre-clinical settings, by which the minimum effective and saturation levels of the therapeutic agent could be derived [ 56 , 57 ]. In this study, only one dose of ahNSCs was tested for the treatment of ischemic stroke.…”

Section: Discussionmentioning

confidence: 99%

JAK2/STAT3 pathway mediates neuroprotective and pro-angiogenic treatment effects of adult human neural stem cells in middle cerebral artery occlusion stroke animal models

Ha¹,

Kim²,

Park

et al. 2022

Aging

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Mismatches between pre-clinical and clinical results of stem cell therapeutics for ischemic stroke limit their clinical applicability. To overcome these discrepancies, precise planning of pre-clinical experiments that can be translated to clinical trials and the scientific elucidation of treatment mechanisms is important. In this study, adult human neural stem cells (ahNSCs) derived from temporal lobe surgical samples were used (to avoid ethical and safety issues), and their therapeutic effects on ischemic stroke were examined using middle cerebral artery occlusion animal models. 5 × 10⁵ ahNSCs was directly injected into the lateral ventricle of contralateral brain hemispheres of immune suppressed rat stroke models at the subacute phase of stroke. Compared with the mock-treated group, ahNSCs reduced brain tissue atrophy and neurological sensorimotor and memory functional loss. Tissue analysis demonstrated that the significant therapeutic effects were mediated by the neuroprotective and pro-angiogenic activities of ahNSCs, which preserved neurons in ischemic brain areas and decreased reactive astrogliosis and microglial activation. The neuroprotective and proangiogenic effects of ahNSCs were validated in in vitro stroke models and were induced by paracrine factors excreted by ahNSCs. When the JAK2/STAT3 signaling pathway was inhibited by a specific inhibitor, AG490, the paracrine neuroprotective and pro-angiogenic effects of ahNSCs were reversed. This pre-clinical study that closely simulated clinical settings and provided treatment mechanisms of ahNSCs for ischemic stroke may aid the development of protocols for subsequent clinical trials of ahNSCs and the realization of clinically available stem cell therapeutics for ischemic stroke.

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“…The fate of the cells after drug administration, especially the long-term survival of allogeneic cells during treatment, affects their efficacy. At the same time, there are always some dead cells in cell products, which themselves and their secretions have a worrying impact on the health of patients [ 180 ]. Although many methods have been designed to pretreat MSCs before transplantation to solve these problems, including inflammatory cytokines, hypoxia, drugs, biomaterials and different culture conditions [ 181 ], it is difficult to provide quality assurance for clinical MSC [ 182 ].…”

Section: 'Prohibitor'——evs As a Treatment Of Oamentioning

confidence: 99%

Breakthrough of extracellular vesicles in pathogenesis, diagnosis and treatment of osteoarthritis

Liu

Fang

et al. 2023

Bioactive Materials

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Stem cell-based therapy for human diseases

Cited by 404 publications

References 501 publications

Umbilical cord blood-derived cell therapy for perinatal brain injury: A systematic review & meta-analysis of preclinical studies - Part B

Umbilical cord blood-derived cell therapy for perinatal brain injury: A systematic review & meta-analysis of preclinical studies - Part B

JAK2/STAT3 pathway mediates neuroprotective and pro-angiogenic treatment effects of adult human neural stem cells in middle cerebral artery occlusion stroke animal models

Breakthrough of extracellular vesicles in pathogenesis, diagnosis and treatment of osteoarthritis

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