Comparative analysis of cell lineage differentiation during hepatogenesis in humans and mice at the single-cell transcriptome level

Wang, Xin; Yang, Li; Wang, Yanchun; Xu, Ziran; Feng, Yang; Zhang, Jing; Wang, Yi; Xu, Cheng‐Ran

doi:10.1038/s41422-020-0378-6

Cited by 85 publications

(81 citation statements)

References 92 publications

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“…However, Wang and co-workers found the opposite results. They found that, in both humans and mice, the proliferation rate of hepatoblasts/hepatocytes decreased throughout development ( Wang et al, 2020 ). These differences between studies may be related to both the selection of embryonic stage and the methods.…”

Section: Discussionmentioning

confidence: 99%

“…The liver consists of greater than 20 cell types, including hepatocytes, liver endothelial cells, biliary ductal cells (cholangiocytes), mesothelial cells, Kupffer cells, and various circulatory immune cells, which are all organized to form the foundation for liver functions, including glycolytic and urea metabolism, immune responses, and drug detoxification ( Wang et al, 2020 ). In the development of human fetus, liver is an essential hemopoietic organ.…”

Section: Introductionmentioning

confidence: 99%

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Integrating Spatial Transcriptomics and Single-Cell RNA-seq Reveals the Gene Expression Profling of the Human Embryonic Liver

Hou

Yang²,

Li³

et al. 2021

Front. Cell Dev. Biol.

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The liver is one of vital organs of the human body, and it plays an important role in the metabolism and detoxification. Moreover, fetal liver is one of the hematopoietic places during ontogeny. Understanding how this complex organ develops during embryogenesis will yield insights into how functional liver replacement tissue can be engineered and how liver regeneration can be promoted. Here, we combine the advantages of single-cell RNA sequencing and Spatial Transcriptomics (ST) technology for unbiased analysis of fetal livers over developmental time from 8 post-conception weeks (PCW) and 17 PCW in humans. We systematically identified nine cell types, and defined the developmental pathways of the major cell types. The results showed that human fetal livers experienced blood rapid growth and immigration during the period studied in our experiments, and identified the differentially expressed genes, and metabolic changes in the developmental process of erythroid cells. In addition, we focus on the expression of liver disease related genes, and found that 17 genes published and linked to liver disease mainly expressed in megakaryocyte and endothelial, hardly expressed in any other cell types. Together, our findings provide a comprehensive and clear understanding of the differentiation processes of all main cell types in the human fetal livers, which may provide reference data and information for liver disease treatment and liver regeneration.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Integrating Spatial Transcriptomics and Single-Cell RNA-seq Reveals the Gene Expression Profling of the Human Embryonic Liver

Hou

Yang²,

Li³

et al. 2021

Front. Cell Dev. Biol.

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“…The specification of hepatoblasts toward hepatocytes has shown to be a default‐directed progressive process in which the transition is characterized by gradual changes in gene expression. However, this is not the case for cholangiocytes which the transition requires regulated signaling and also requires to escape from the default‐directed hepatoblast‐hepatocyte transition (Wang et al, 2020). Differentiation of hepatoblasts into cholangiocytes is promoted by FGF, BMP, and dominantly TGF‐β (through notch signaling) gradients, whereas other signaling molecules such as HGF, OSM, and glucocorticoids induce hepatocyte differentiation (Shin and Monga, 2013; Snykers, De Kock, Rogiers, & Vanhaecke, 2009).…”

Section: Signaling Moleculesmentioning

confidence: 99%

“…Although the main phases of liver regeneration were discussed separately in previous sections, mechanistically, numerous investigations have indicated a complex array of interactive signaling factors between these phases, which shows an orchestrated operation of these phases with highly overlapping functions. During early hepatogenesis where the differentiation of progenitor cells toward specified hepatocytes is pursued, not only the proliferation of progenitor cells along with progressive gene specialization (toward hepatocytes) occurs, but also, simultaneously, the proliferation of highly specified hepatocytes is followed where a mixture of proliferating hepatoblast and hepatocytes is detectable in the developing tissue (Butler, Hoffman, Smibert, Papalexi, & Satija, 2018; Michalopoulos & DeFrances, 1997; Wang et al, 2020). In fact, as the tissue development proceeds, the ratio of hepatoblast/hepatocytes is decreased until the time in which the regeneration is further followed only by hepatocyte proliferation (Butler et al, 2018; Wang et al, 2020).…”

Section: Regeneration Time Framementioning

confidence: 99%

“…During early hepatogenesis where the differentiation of progenitor cells toward specified hepatocytes is pursued, not only the proliferation of progenitor cells along with progressive gene specialization (toward hepatocytes) occurs, but also, simultaneously, the proliferation of highly specified hepatocytes is followed where a mixture of proliferating hepatoblast and hepatocytes is detectable in the developing tissue (Butler, Hoffman, Smibert, Papalexi, & Satija, 2018; Michalopoulos & DeFrances, 1997; Wang et al, 2020). In fact, as the tissue development proceeds, the ratio of hepatoblast/hepatocytes is decreased until the time in which the regeneration is further followed only by hepatocyte proliferation (Butler et al, 2018; Wang et al, 2020). Similarly, in the regeneration process after partial hepatectomy of mice liver, if no delay in hepatocyte proliferation occurs, a rough simultaneous specification of hepatic resident progenitors and cell cycle activity of parenchymal hepatocytes proceeds, whereas if the hepatocytes proliferation impaired or delayed, the hepatoblast specification precedes, and they invade the adjacent tissue as they proliferate (Li et al, 2013).…”

Section: Regeneration Time Framementioning

confidence: 99%

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Signaling molecules orchestrating liver regenerative medicine

Zakeri

Mirdamadi

Kalhori

et al. 2020

J Tissue Eng Regen Med

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The liver is in charge of more than 500 functions in the human body, which any damage and failure to the liver can significantly compromise human life. Numerous studies are being carried out in regenerative medicine, as a potential driving force, toward alleviating the need for liver donors and fabrication of a 3D‐engineered transplantable hepatic tissue. Liver tissue engineering brings three main factors of cells, extracellular matrix (ECM), and signaling molecules together, while each of these three factors tries to mimic the physiological state of the tissue to direct tissue regeneration. Signaling molecules play a crucial role in directing tissue fabrication in liver tissue engineering. When mimicking the natural in vivo process of regeneration, it is tightly associated with three main phases of differentiation, proliferation (progression), and tissue maturation through vascularization while directing each of these phases is highly regulated by the specific signaling molecules. The understanding of how these signaling molecules guide the dynamic behavior of regeneration would be a tool for further tailoring of bioengineered systems to help the liver regeneration with many cellular, molecular, and tissue‐level functions. Hence, the signaling molecules come to aid all these phases for further improvements toward the clinical use of liver tissue engineering as the goal.

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Sexually Dimorphic Response to Hepatic Injury in Newborn Suffering from Intrauterine Growth Restriction

Wei,

Tang,

Mao

et al. 2024

Advanced Science

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Intrauterine growth restriction (IUGR), when a fetus does not grow as expected, is associated with a reduction in hepatic functionality and a higher risk for chronic liver disease in adulthood. Utilizing early developmental plasticity to reverse the outcome of poor fetal programming remains an unexplored area. Focusing on the biochemical profiles of neonates and previous transcriptome findings, piglets from the same fetus are selected as models for studying IUGR. The cellular landscape of the liver is created by scRNA‐seq to reveal sex‐dependent patterns in IUGR‐induced hepatic injury. One week after birth, IUGR piglets experience hypoxic stress. IUGR females exhibit fibroblast‐driven T cell conversion into an immune‐adapted phenotype, which effectively alleviates inflammation and fosters hepatic regeneration. In contrast, males experience even more severe hepatic injury. Prolonged inflammation due to disrupted lipid metabolism hinders intercellular communication among non‐immune cells, which ultimately impairs liver regeneration even into adulthood. Additionally, Apolipoprotein A4 (APOA4) is explored as a novel biomarker by reducing hepatic triglyceride deposition as a protective response against hypoxia in IUGR males. PPARα activation can mitigate hepatic damage and meanwhile restore over‐expressed APOA4 to normal in IUGR males. The pioneering study offers valuable insights into the sexually dimorphic responses to hepatic injury during IUGR.

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Comparative analysis of cell lineage differentiation during hepatogenesis in humans and mice at the single-cell transcriptome level

Cited by 85 publications

References 92 publications

Integrating Spatial Transcriptomics and Single-Cell RNA-seq Reveals the Gene Expression Profling of the Human Embryonic Liver

Integrating Spatial Transcriptomics and Single-Cell RNA-seq Reveals the Gene Expression Profling of the Human Embryonic Liver

Signaling molecules orchestrating liver regenerative medicine

Sexually Dimorphic Response to Hepatic Injury in Newborn Suffering from Intrauterine Growth Restriction

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