Release of Notch activity coordinated by IL-1β signalling confers differentiation plasticity of airway progenitors via Fosl2 during alveolar regeneration

Choi, Jinwook; Jang, Yu Jin; Dabrowska, Catherine; Iich, Elhadi; Evans, Kelly V.; Hall, Helen; Janes, Sam M.; Simons, Benjamin D.; Koo, Bon–Kyoung; Kim, Jonghwan; Lee, Joo Hyeon

doi:10.1038/s41556-021-00742-6

Cited by 61 publications

(63 citation statements)

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“…Therefore, we aimed to evaluate the functional role of EAAs in directing the fate conversion of secretory cells into DATP‐AT1 cells using an ex vivo three‐dimensional (3D) organoid culture system. We recently identified KDR/FLK1 as the surface marker of airway secretory cells (Choi et al , 2021 ; Jiang et al , 2021 ). Using this marker, we isolated secretory cells (KDR + EpCAM + ) from Lats1/2 dKO lungs, followed by organoid coculture with stromal cells (Fig 3B ).…”

Section: Resultsmentioning

confidence: 99%

Airway secretory cell fate conversion via YAP‐mTORC1‐dependent essential amino acid metabolism

et al. 2022

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Tissue homeostasis requires lineage fidelity of stem cells. Dysregulation of cell fate specification and differentiation leads to various diseases, yet the cellular and molecular mechanisms governing these processes remain elusive. We demonstrate that YAP/TAZ activation reprograms airway secretory cells, which subsequently lose their cellular identity and acquire squamous alveolar type 1 (AT1) fate in the lung. This cell fate conversion is mediated via distinctive transitional cell states of damage-associated transient progenitors (DATPs), recently shown to emerge during injury repair in mouse and human lungs. We further describe a YAP/TAZ signaling cascade to be integral for the fate conversion of secretory cells into AT1 fate, by modulating mTORC1/ATF4-mediated amino acid metabolism in vivo. Importantly, we observed aberrant activation of the YAP/TAZ-mTORC1-ATF4 axis in the altered airway epithelium of bronchiolitis obliterans syndrome, including substantial emergence of DATPs and AT1 cells with severe pulmonary fibrosis. Genetic and pharmacologic inhibition of mTORC1 activity suppresses lineage alteration and subepithelial fibrosis driven by YAP/TAZ activation, proposing a potential therapeutic target for human fibrotic lung diseases.

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Section: Resultsmentioning

confidence: 99%

Airway secretory cell fate conversion via YAP‐mTORC1‐dependent essential amino acid metabolism

et al. 2022

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“…Using a Sftpc + ATII depletion mouse model, it was concluded that there are more Sftpc + ATII cells derived from alveolar ATII cells than from BASCs [ 15 ]. However, a recent study found that mouse Scgb1a1 derived Sftpc + BASCs (also termed secretory ATII cells, sAT2 cells) are capable of long-term self-renewal, more so than residual AT2 cells in in vitro organoids [ 16 ]. It remains unknown in lung fibrosis if ATII cell depletion occurs within fibrotic area or if BASCs or the remaining ATII cells are the major source for regeneration of ATII cells in the alveoli.…”

Section: Introductionmentioning

confidence: 99%

“…Besides BASCs, studies have shown that club cells [ 3 ], BCs, integrin α6β4 positive cells, H2-K1 high, and Uroplakin3a ( Upk3a ) expressing airway epithelial progenitors can migrate to the alveoli and give rise to ATII cells under conditions of severe injury that involve broad epithelial denudation [ 17 – 21 ]. An abnormal cluster of Fstl1 + secretory cells were found during defective club cells (or secretory cells) transition to ATII cells [ 16 ]. These cells were marked by Id3, Porcn , and Cdkn1c and blocked the fate conversion from secretory to ATII cells when lacking sustained Notch activity.…”

Section: Introductionmentioning

confidence: 99%

“…Further, Wnt activity antagonized Notch signaling to favor LNEPs differentiation into ATII cells for recovery [ 19 , 29 ]. In addition, Notch inhibition skews the differentiation of human secretory cells ( CC10 + KDR + HTII280 − ) into ATII cells instead of ciliated cells and BCs in culture conditions [ 16 ]. Recent scRNA-seq mapping of epithelial cell types for normal and IPF human airways suggested that BC subpopulations constitute a hierarchy regulated by Notch signaling.…”

Section: Introductionmentioning

confidence: 99%

“…It is reported that macrophage derived IL1β activated a subpopulation of primed ATII cells expressing IL1R1 for differentiation into DATPs, while chronic IL1β halted DATPs transition into functional ATI cells, which results in impaired alveolar regeneration in fibrotic lung [ 10 ]. The same group did follow-up research and found that IL1β signaling through IL1R1 on ciliated cells via paracrine Notch ligands, JAG1 and JAG2, is essential for secretory cell differentiation of ATII cells [ 16 ]. These studies suggest that inflammatory signals are required for ATII cell mediated alveolar regeneration but sustained inflammatory response can cause defects for generating functional alveolar niche following injury.…”

Section: Introductionmentioning

confidence: 99%

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Abnormal respiratory progenitors in fibrotic lung injury

et al. 2022

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Recent advances in single-cell RNA sequencing (scRNA-seq) and epithelium lineage labeling have yielded identification of multiple abnormal epithelial progenitor populations during alveolar type 2 (ATII) cell differentiation into alveolar type 1 (ATI) cells during regenerative lung post-fibrotic injury. These abnormal cells include basaloid/basal-like cells, ATII transition cells, and persistent epithelial progenitors (PEPs). These cells occurred and accumulated during the regeneration of distal airway and alveoli in response to both chronic and acute pulmonary injury. Among the alveolar epithelial progenitors, PEPs express a distinct Krt8+ phenotype that is rarely found in intact alveoli. However, post-injury, the Krt8+ phenotype is seen in dysplastic epithelial cells. Fully understanding the characteristics and functions of these newly found, injury-induced abnormal behavioral epithelial progenitors and the signaling pathways regulating their phenotype could potentially point the way to unique therapeutic targets for fibrosing lung diseases. This review summarizes recent advances in understanding these epithelial progenitors as they relate to uncovering regenerative mechanisms.

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m⁶A‐Dependent Modulation via IGF2BP3/MCM5/Notch Axis Promotes Partial EMT and LUAD Metastasis

et al. 2023

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The importance of mRNA N6‐methyladenosine (m6A) modification during tumor metastasis is controversial as it plays distinct roles in different biological contexts. Moreover, how cancer cell plasticity is shaped by m6A modification is interesting but remains uncharacterized. Here, this work shows that m6A reader insulin like growth factor 2 mRNA binding protein 3 (IGF2BP3) is remarkably upregulated in metastatic lung adenocarcinoma (LUAD) and indicates worse prognosis of patients. Interestingly, IGF2BP3 induces partial epithelial‐mesenchymal‐transition (EMT) and confers LUAD cells plasticity to metastasize through m6A‐dependent overactivation of Notch signaling. Mechanistically, IGF2BP3 recognized m6A‐modified minichromosome maintenance complex component (MCM5) mRNAs to prolong stability of them, subsequently upregulating MCM5 protein, which competitively inhibits SIRT1‐mediated deacetylation of Notch1 intracellular domain (NICD1), stabilizes NICD1 protein and contributes to m6A‐dependent IGF2BP3‐mediated cellular plasticity. Notably, a tight correlation of the IGF2BP3/MCM5/Notch axis is evidenced in clinical LUAD specimens. Therefore, this study elucidates a critical role of m6A modification on LUAD cell plasticity in fostering tumor metastasis via the above axis, providing potential targets for metastatic LUAD.

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Release of Notch activity coordinated by IL-1β signalling confers differentiation plasticity of airway progenitors via Fosl2 during alveolar regeneration

Cited by 61 publications

References 64 publications

Airway secretory cell fate conversion via YAP‐mTORC1‐dependent essential amino acid metabolism

Airway secretory cell fate conversion via YAP‐mTORC1‐dependent essential amino acid metabolism

Abnormal respiratory progenitors in fibrotic lung injury

m⁶A‐Dependent Modulation via IGF2BP3/MCM5/Notch Axis Promotes Partial EMT and LUAD Metastasis

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Release of Notch activity coordinated by IL-1β signalling confers differentiation plasticity of airway progenitors via Fosl2 during alveolar regeneration

Cited by 61 publications

References 64 publications

Airway secretory cell fate conversion via YAP‐mTORC1‐dependent essential amino acid metabolism

Airway secretory cell fate conversion via YAP‐mTORC1‐dependent essential amino acid metabolism

Abnormal respiratory progenitors in fibrotic lung injury

m6A‐Dependent Modulation via IGF2BP3/MCM5/Notch Axis Promotes Partial EMT and LUAD Metastasis

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m⁶A‐Dependent Modulation via IGF2BP3/MCM5/Notch Axis Promotes Partial EMT and LUAD Metastasis