Specific ablation of CD4<sup>+</sup> T-cells promotes heart regeneration in juvenile mice

Li, Jiatao; Cai, Liang; Yang, Kevin Yi; Huang, Xiuzhen; Han, Mao Ying; Li, Xisheng; Chan, Vicken W.; Chan, Kathleen S; Liu, Di; Huang, Zhan-Peng; Zhou, Bin; Lui, Kathy O.

doi:10.7150/thno.42943

Cited by 47 publications

(43 citation statements)

References 40 publications

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“…It is believed that cardiomyocyte proliferation contributes to mammalian heart growth largely during the embryonic period, and cardiomyocyte enlargement is thought to be responsible for growth after birth. However, accumulating evidence has demonstrated that cardiomyocytes still have proliferative potential even after birth 8 - 12 . Since we found that LPA 1 and LPA 3 significantly peaked during the early postnatal period and decreased rapidly thereafter, which coincides with the loss of the heart's regenerative potential, the role of LPA signaling in cardiomyocyte proliferation and heart regeneration after birth was elucidated in this study.…”

Section: Introductionmentioning

confidence: 99%

LPA₃-mediated lysophosphatidic acid signaling promotes postnatal heart regeneration in mice

Wang¹,

Liu²,

Pei³

et al. 2020

Theranostics

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Background: Lysophosphatidic acid (LPA) is a small glycerophospholipid that acts as a potent extracellular signal in various biological processes and diseases. Our previous work demonstrated that the expression of the LPA receptors LPA 1 and LPA 3 is elevated in the early postnatal heart. However, the role of this stage-specific expression of LPA 1 and LPA 3 in the heart is unknown. Methods and Results: By using LPA 3 and LPA 1 knockout mice, and neonatal SD rats treated with Ki16425 (LPA 1 /LPA 3 inhibitor), we found that the number of proliferating cardiomyocytes, detected by coimmunostaining pH3, Ki67 or BrdU with cardiac troponin T, was significantly decreased in the LPA 3 knockout mice and the Ki16425-treated rats but not in the LPA 1 knockout mice during the first week of postnatal life. Using a myocardial infarction (MI) model, we found that cardiac function and the number of proliferating cardiomyocytes were decreased in the neonatal LPA 3 KO mice and increased in the AAV9-mediated cardiac-specific LPA 3 overexpression mice. By using lineage tracing and AAV9-LPA 3 , we further found that LPA 3 overexpression in adult mice enhances cardiac function and heart regeneration as assessed by pH3-, Ki67-, and Aurora B-positive cardiomyocytes and clonal cardiomyocytes after MI. Genome-wide transcriptional profiling and additional mechanistic studies showed that LPA induces cardiomyocyte proliferation through the PI3K/AKT, BMP-Smad1/5, Hippo/YAP and MAPK/ERK pathways in vitro , whereas only ERK was confirmed to be activated by LPA-LPA 3 signaling in vivo . Conclusion: Our study reports that LPA 3 -mediated LPA signaling is a crucial factor for cardiomyocyte proliferation in the early postnatal heart. Cardiac-specific LPA 3 overexpression improved cardiac function and promoted cardiac regeneration after myocardial injury induced by MI. This finding suggested that activation of LPA 3 potentially through AAV-mediated gene therapy might be a therapeutic strategy to improve the outcome after MI.

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Section: Introductionmentioning

confidence: 99%

LPA₃-mediated lysophosphatidic acid signaling promotes postnatal heart regeneration in mice

Wang¹,

Liu²,

Pei³

et al. 2020

Theranostics

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“…In addition to the immunomodulation of macrophages, Treg can also suppress the pro-inflammatory response of other activated cells such as effector CD4 + and CD8 + T cells. Intriguingly, a recent study shows a developmentally distinct role of CD4 + T cells in heart repair and regeneration 73 . CD4 + T cells inhibit heart regeneration in the juvenile mice but promote heart repair in the adult mice 73 .…”

Section: Treg In Cardiovascular Repair and Regenerationmentioning

confidence: 99%

“…Intriguingly, a recent study shows a developmentally distinct role of CD4 + T cells in heart repair and regeneration 73 . CD4 + T cells inhibit heart regeneration in the juvenile mice but promote heart repair in the adult mice 73 . Unlike the CD4 + T cells, CD8 + T cells are found unresponsive to heart injury in the juvenile mice 73 .…”

Section: Treg In Cardiovascular Repair and Regenerationmentioning

confidence: 99%

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An emerging role of regulatory T-cells in cardiovascular repair and regeneration

Fung¹,

Yang²,

Lui³

2020

Theranostics

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Accumulating evidence has demonstrated that immune cells play an important role in the regulation of tissue repair and regeneration. After injury, danger signals released by the damaged tissue trigger the initial pro-inflammatory phase essential for removing pathogens or cellular debris that is later replaced by the anti-inflammatory phase responsible for tissue healing. On the other hand, impaired immune regulation can lead to excessive scarring and fibrosis that could be detrimental for the restoration of organ function. Regulatory T-cells (Treg) have been revealed as the master regulator of the immune system that have both the immune and regenerative functions. In this review, we will summarize their immune role in the induction and maintenance of self-tolerance; as well as their regenerative role in directing tissue specific response for repair and regeneration. The latter is clearly demonstrated when Treg enhance the differentiation of stem or progenitor cells such as satellite cells to replace the damaged skeletal muscle, as well as the proliferation of parenchymal cells including neonatal cardiomyocytes for functional regeneration. Moreover, we will also discuss the reparative and regenerative role of Treg with a particular focus on blood vessels and cardiac tissues. Last but not least, we will describe the ongoing clinical trials with Treg in the treatment of autoimmune diseases that could give clinically relevant insights into the development of Treg therapy targeting tissue repair and regeneration.

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“…Several studies highlighted the detrimental role of CD4 + and CD8 + lymphocytes in tissue regeneration and revascularization. For instance, CD4 + cell ablation promotes heart regeneration [ 126 ] and both CD4 + [ 127 ] and CD8 + [ 128 ] blockade improves angiogenesis in diabetic mice. Yet, their functional role in skin regeneration is controversial, as indicated by numerous studies reporting conflicting results, and a clear discrimination of the specific role of circulating and resident lymphocytes is often missing.…”

Section: Lymphocytesmentioning

confidence: 99%

Immune Cell Therapies to Improve Regeneration and Revascularization of Non-Healing Wounds

Groppa

Colliva

Vuerich

et al. 2020

IJMS

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With the increased prevalence of chronic diseases, non-healing wounds place a significant burden on the health system and the quality of life of affected patients. Non-healing wounds are full-thickness skin lesions that persist for months or years. While several factors contribute to their pathogenesis, all non-healing wounds consistently demonstrate inadequate vascularization, resulting in the poor supply of oxygen, nutrients, and growth factors at the level of the lesion. Most existing therapies rely on the use of dermal substitutes, which help the re-epithelialization of the lesion by mimicking a pro-regenerative extracellular matrix. However, in most patients, this approach is not efficient, as non-healing wounds principally affect individuals afflicted with vascular disorders, such as peripheral artery disease and/or diabetes. Over the last 25 years, innovative therapies have been proposed with the aim of fostering the regenerative potential of multiple immune cell types. This can be achieved by promoting cell mobilization into the circulation, their recruitment to the wound site, modulation of their local activity, or their direct injection into the wound. In this review, we summarize preclinical and clinical studies that have explored the potential of various populations of immune cells to promote skin regeneration in non-healing wounds and critically discuss the current limitations that prevent the adoption of these therapies in the clinics.

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Specific ablation of CD4⁺ T-cells promotes heart regeneration in juvenile mice

Cited by 47 publications

References 40 publications

LPA₃-mediated lysophosphatidic acid signaling promotes postnatal heart regeneration in mice

LPA₃-mediated lysophosphatidic acid signaling promotes postnatal heart regeneration in mice

An emerging role of regulatory T-cells in cardiovascular repair and regeneration

Immune Cell Therapies to Improve Regeneration and Revascularization of Non-Healing Wounds

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Specific ablation of CD4+ T-cells promotes heart regeneration in juvenile mice

Cited by 47 publications

References 40 publications

LPA3-mediated lysophosphatidic acid signaling promotes postnatal heart regeneration in mice

LPA3-mediated lysophosphatidic acid signaling promotes postnatal heart regeneration in mice

An emerging role of regulatory T-cells in cardiovascular repair and regeneration

Immune Cell Therapies to Improve Regeneration and Revascularization of Non-Healing Wounds

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Specific ablation of CD4⁺ T-cells promotes heart regeneration in juvenile mice

LPA₃-mediated lysophosphatidic acid signaling promotes postnatal heart regeneration in mice

LPA₃-mediated lysophosphatidic acid signaling promotes postnatal heart regeneration in mice