BMI1 enables interspecies chimerism with human pluripotent stem cells

Huang, Ke; Zhu, Yanling; Ma, Yanlin; Zhao, Bingzi; Fan, Nana; Li, Yuhang; Sui, Hong; Chu, Shilong; Ouyang, Zhen; Zhang, Quanjun; Xing, Qi; Lai, Chengdan; Li, Nan; Zhang, Tian; Gu, Jiaming; Kang, Baoqiang; Shan, Yongli; Lai, Keyu; Huang, Wenhao; Mai, Yuchan; Wang, Qing; Li, Jinbing; Lin, Aiping; Zhang, Yanqi; Zhong, Xiaofen; Liao, Baojian; Lai, Liangxue; Chen, Jiekai; Pei, Duanqing; Pan, Guoshun

doi:10.1038/s41467-018-07098-w

Cited by 42 publications

(50 citation statements)

References 37 publications

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“…hPSCs (3–5 × 10 3 ) (hESCs, primed RH6; pRH6) suspended in 8—5 μL culture medium were engrafted into HH2, HH3, and HH4 PS stages ( Table S1 ). Since anti-apoptotic factors improve interspecies chimera formation of primed pluripotent cells ( Huang et al., 2018 ; Masaki et al., 2016 ; Wang et al., 2018 ), the cell suspension was supplemented with 10 μM Y27632 (ROCK inhibitor). Similar to the results obtained for injection of medium, 40% of chicken embryos injected at HH4 survived, while survival after injection of HH2 and HH3 was poor (6% and 14% survival, respectively) ( Table S1 ).…”

Section: Resultsmentioning

confidence: 99%

“…Previous studies indicated that heterochronic chimera formation is feasible when enhancing survival of primed PSCs ( Huang et al., 2018 ; Kang et al., 2018 ; Masaki et al., 2016 ; Wang et al., 2018 ). To test this hypothesis, we injected primed pRH6 and piPSCs into BLD-stage chicken embryos after treatment with Y27632.…”

Section: Resultsmentioning

confidence: 99%

“…On the other hand, some studies indicated that interspecies chimerism can be achieved with non-stage-matching (NSM) rat EpiSCs or primed hPSCs and mouse pre-implantation embryos when the survival of primed cells was enhanced by overexpression of anti-apoptotic genes. These findings questioned the necessity of an SM approach ( Huang et al., 2018 ; Masaki et al., 2016 ; Wang et al., 2018 ).…”

Section: Introductionmentioning

confidence: 99%

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Chicken Interspecies Chimerism Unveils Human Pluripotency

et al. 2021

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Human pluripotent stem cells (hPSCs) are commonly kept in a primed state but also able to acquire a more immature naive state under specific conditions in vitro. Acquisition of naive state changes several properties of hPSCs and might affect their contribution to embryonic development in vivo. However, the lack of an appropriate animal test system has made it difficult to assess potential differences for chimera formation between naive and primed hPSCs. Here, we report that the developing chicken embryo is a permissive host for hPSCs, allowing analysis of the pluripotency potential of hPSCs. Transplantation of naive-like and primed hPSCs at matched developmental stages resulted in robust chimerism. Importantly, the ability of naive-like but not of primed hPSCs to form chimera was substantially reduced when injected at non-matched developmental stages. We propose that contribution to chick embryogenesis is an informative and versatile test to identify different pluripotent states of hPSCs.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Chicken Interspecies Chimerism Unveils Human Pluripotency

et al. 2021

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“…Previous studies have shown that inhibiting apoptosis either by the addition of the Rock inhibitor Y27632 (Kang et al, 2018), or by overexpression of the anti-apoptotic genes BCL2 (Masaki et al, 2016) or BMI1 (Huang et al, 2018) enables primed PSCs to colonize host embryos. Therefore, in a final series of microinjections, we asked whether inhibition of apoptosis could improve the engraftment of naïve PSCs into the host embryo.…”

Section: Premature Differentiation Of Rhesus Naïve Pscs After Injectimentioning

confidence: 99%

Apoptosis, G1 phase stall and premature differentiation account for low chimeric competence of Human and rhesus monkey naïve pluripotent stem cells

Aksoy

Rognard

Moulin

et al. 2020

Preprint

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After reprogramming to naïve pluripotency, human pluripotent stem cells (PSCs) still exhibit very low ability to make interspecies chimeras in mice and pigs. Whether this is because they are inherently devoid of the attributes of chimeric competency or because naïve PSCs in general cannot colonize embryos from distant species remains to be elucidated. Here, we have used different types of mouse, human and rhesus monkey naïve PSCs and we have analyzed their ability to colonize both distant (rabbit) and close (cynomolgus monkey) embryos. Mouse embryonic stem cells (ESCs) remained mitotically active after injection into rabbit and cynomolgus embryos and contributed to the formation of the neural tube in postimplantation rabbit embryos. In contrast, primate naive PSCs colonized rabbit and cynomolgus embryos with much lower efficiency, regardless of the reprogramming protocols. Unlike mouse ESCs, they slowed DNA replication following colony dissociation and, after injection into host embryos, they stalled in the G1 phase of the cell cycle and differentiated prematurely, regardless of host species, distant or close. These results show that, unlike mouse ESCs, primate naive PSCs do not make chimeras because they are inherently unfit to stay mitotically active during embryo colonization.

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“…Given that human iPSCs fundamentally lack the ability to form chimeras, blastocyst complementation cannot be applied directly to humans. Inducing the expression of anti-apoptotic genes could give some chimera-forming ability to human iPSCs [40,41], but the long-term safety would require clarification because these are also recognized oncogenes. Another issue is that basing this method on systemic chimera formation leads to the serious ethical concern of chimera formation in host gametes or neural tissue other than the target organs.…”

Section: Blastocyst Complementationmentioning

confidence: 99%

A Novel Strategy for Xeno-Regenerative Therapy

Fujimoto¹,

Yokoo²,

Kobayashi³

2020

Xenotransplantation - Comprehensive Study

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The shortage of organs for transplantation is of critical importance worldwide. Xenotransplantation or xeno-embryonic organ transplantation can stably supply organs and is considered to be an established alternative treatment. Regenerative medicine is another option, and recent advances in stem cell research have enabled the reproduction of miniature organs, called organoids, derived in vitro from human induced pluripotent stem cells. However, the in vitro production of large and complex organs that can efficiently function in vivo is not yet accomplished. We proposed a novel strategy for xenotransplantation in which a chimeric kidney is constructed by injecting human nephron progenitor cells into a porcine embryonic kidney, thereby eliminating pig nephron progenitor cells and allowing transplantation into a human and long-term survival. In this chapter, we discussed advantages and pitfalls of xenotransplantation and xeno-embryonic kidney transplantation. Recent attempts of human organoids and blastocyst complementation were reviewed. Finally, we proposed our novel xeno-regenerative therapeutic strategy.

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BMI1 enables interspecies chimerism with human pluripotent stem cells

Cited by 42 publications

References 37 publications

Chicken Interspecies Chimerism Unveils Human Pluripotency

Chicken Interspecies Chimerism Unveils Human Pluripotency

Apoptosis, G1 phase stall and premature differentiation account for low chimeric competence of Human and rhesus monkey naïve pluripotent stem cells

A Novel Strategy for Xeno-Regenerative Therapy

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