Novel Association of the NOTCH Pathway Regulator <i>MIB1</i> Gene With the Development of Bicuspid Aortic Valve

Tessler, Idit; Albuisson, Juliette; Piñeiro-Sabarís, Rebeca; Verstraeten, Aline; Kamber Kaya, Hatem Elif; Siguero-Álvarez, Marcos; Goudot, Guillaume; MacGrogan, Donal; Luyckx, Ilse; Shpitzen, Shoshana; Levin, Galina; Kelman, Guy; Reshef, Noga; Mananet, Hugo; Holdcraft, Jake; Muehlschlegel, Jochen D.; Peloso, Gina M.; Oppenheim, Olya; Cheng, Charles; Mazzella, Jean-Michael; Andelfinger, Gregor; Mital, Seema; Eriksson, Per; Billon, Clarisse; Heydarpour, Mahyar; Dietz, Harry C.; Jeunemaitre, Xavier; Leitersdorf, Eran; Sprinzak, David; Blacklow, Stephen C.; Body, Simon C.; Carmi, Shai; Loeys, Bart; de la Pompa, José Luis; Gilon, Dan; Messas, Emmanuel; Durst, Ronen

doi:10.1001/jamacardio.2023.1469

Cited by 9 publications

(8 citation statements)

References 71 publications

(199 reference statements)

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“…Tangeretin could inhibit EndoMT in hiVECs ( Figure S14L ). These observations were consistent with the results of NOTCH1 deletion studies in vivo, 39 therefore, this protocol can be promising for its use in building heart valve disease models.…”

Section: Resultssupporting

confidence: 88%

“…The scRNA-seq analysis demonstrated that NOTCH1 signaling pathway was important in the differentiation of hiPSCs into heart valve cells, and previous studies have reported that the NOTCH1 signaling pathway is critical for the development of heart valves. [37][38][39] In view of the crucial role of NOTCH1 in heart valve development, we sought to investigate whether inhibition of NOTCH1 might affect the differentiation of hiPSCs into heart valve cells. Tangeretin (an inhibitor of NOTCH1) significantly inhibited the differentiation of hiCLPMs and heart valve cells from hiPSCs (Figure S14C through S14G).…”

Section: Longitudinal Scrna-seq Analysis Reveals the Transcriptional ...mentioning

confidence: 99%

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Directed Differentiation of Human Induced Pluripotent Stem Cells to Heart Valve Cells

Cai,

Zhu,

et al. 2024

Circulation

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BACKGROUND: A main obstacle in current valvular heart disease research is the lack of high-quality homogeneous functional heart valve cells. Human induced pluripotent stem cells (hiPSCs)-derived heart valve cells may help with this dilemma. However, there are no well-established protocols to induce hiPSCs to differentiate into functional heart valve cells, and the networks that mediate the differentiation have not been fully elucidated. METHODS: To generate heart valve cells from hiPSCs, we sequentially activated the Wnt, BMP4, VEGF (vascular endothelial growth factor), and NFATc1 signaling pathways using CHIR-99021, BMP4, VEGF-165, and forskolin, respectively. The transcriptional and functional similarity of hiPSC-derived heart valve cells compared with primary heart valve cells were characterized. Longitudinal single-cell RNA sequencing was used to uncover the trajectory, switch genes, pathways, and transcription factors of the differentiation. RESULTS: An efficient protocol was developed to induce hiPSCs to differentiate into functional hiPSC-derived valve endothelial-like cells and hiPSC-derived valve interstitial-like cells. After 6-day differentiation and CD144 magnetic bead sorting, ≈70% CD144 + cells and 30% CD144 – cells were obtained. On the basis of single-cell RNA sequencing data, the CD144 + cells and CD144 – cells were found to be highly similar to primary heart valve endothelial cells and primary heart valve interstitial cells in gene expression profile. Furthermore, CD144 + cells had the typical function of primary heart valve endothelial cells, including tube formation, uptake of low-density lipoprotein, generation of endothelial nitric oxide synthase, and response to shear stress. Meanwhile, CD144 – cells could secret collagen and matrix metalloproteinases, and differentiate into osteogenic or adipogenic lineages like primary heart valve interstitial cells. Therefore, we identified CD144 + cells and CD144 – cells as hiPSC-derived valve endothelial-like cells and hiPSC-derived valve interstitial-like cells, respectively. Using single-cell RNA sequencing analysis, we demonstrated that the trajectory of heart valve cell differentiation was consistent with embryonic valve development. We identified the main switch genes (NOTCH1, HEY1, and MEF2C), signaling pathways (TGF-β, Wnt, and NOTCH), and transcription factors (MSX1, SP5, and MECOM) that mediated the differentiation. Finally, we found that hiPSC-derived valve interstitial-like cells might derive from hiPSC-derived valve endothelial-like cells undergoing endocardial-mesenchymal transition. CONCLUSIONS: In summary, this is the first study to report an efficient strategy to generate functional hiPSC-derived valve endothelial-like cells and hiPSC-derived valve interstitial-like cells from hiPSCs, as well as to elucidate the differentiation trajectory and transcriptional dynamics of hiPSCs differentiated into heart valve cells.

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Section: Resultssupporting

confidence: 88%

Section: Longitudinal Scrna-seq Analysis Reveals the Transcriptional ...mentioning

confidence: 99%

Directed Differentiation of Human Induced Pluripotent Stem Cells to Heart Valve Cells

Cai,

Zhu,

et al. 2024

Circulation

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“…Her project eventually grew into a multinational collaboration involving 2 dozen investigators that identified a novel genetic cause for bicuspid aortic valve. 1 "We decided we wanted to go deeper and try to understand the wide spectrum of clinical expression of bicuspid aortic valve, " she said. "We realized that genetics may be the real story behind this inherited heart condition.…”

mentioning

confidence: 99%

“…Her project eventually grew into a multinational collaboration involving 2 dozen investigators that identified a novel genetic cause for bicuspid aortic valve. 1…”

mentioning

confidence: 99%

International Collaboration Identifies Gene Linked to Congenital Heart Defect

Kuehn

2024

Circulation

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A n encounter with a family affected by inherited bicuspid aortic valve-the most common congenital heart valve defectduring her medical training left Idit Tessler, MD, MPH, a PhD candidate at Sheba Medical Center in Ramat Gan, Israel, with questions no one could answer: Why did a child in the family die of a complication of the condition, but his grandfather lived his entire life seemingly unaffected?Without clear answers, clinicians like Tessler cannot advise patients about what to expect with their condition because 2 patients with similar presentations might have dramatically different disease courses and outcomes. Tessler decided to focus her doctoral thesis on answering these questions. Her project eventually grew into a multinational collaboration involving 2 dozen investigators that identified a novel genetic cause for bicuspid aortic valve. 1 "We decided we wanted to go deeper and try to understand the wide spectrum of clinical expression of bicuspid aortic valve, " she said. "We realized that genetics may be the real story behind this inherited heart condition. "The opinions expressed in this article are not necessarily those of the editors or of the American Heart Association.

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“…The prevalence of LVNC is generally increased in BAV cohorts, and mutation of KCNJ2, another potassium channel subunit, causes a syndromic presentation of BAV with extracardiac features in addition to arrhythmias (57). BAV and TAD also co-segregate with LVNC in some families with mutations in NKX2-5, TBX20 or MIB1, another Notch pathway regulator that was convincingly linked to BAV in recent studies and is recurrently mutated in the EBAV cohort (52,58,59). Our findings provide further evidence for a genetic link between cardiomyopathies, BAV, conduction abnormalities, and TAD that may contribute to early onset complications of BAV disease.…”

Section: Discussionmentioning

confidence: 97%

Whole Exome Sequencing Uncovers the Genetic Complexity of Bicuspid Aortic Valve in Families with Early Onset Complications

Mansoorshahi,

Yetman,

Bissell

et al. 2024

Preprint

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Bicuspid Aortic Valve (BAV) is the most common adult congenital heart lesion with an estimated population prevalence of 1%. We hypothesize that early onset complications of BAV (EBAV) are driven by specific impactful genetic variants. We analyzed whole exome sequences (WES) to identify rare coding variants that contribute to BAV disease in 215 EBAV families. Predicted pathogenic variants of causal genes were present in 111 EBAV families (51% of total), including genes that cause BAV (8%) or heritable thoracic aortic disease (HTAD, 17%). After appropriate filtration, we also identified 93 variants in 26 novel genes that are associated with autosomal dominant congenital heart phenotypes, including recurrent deleterious variation ofFBN2,MYH6, channelopathy genes, and type 1 and 5 collagen genes. These findings confirm our hypothesis that unique rare genetic variants contribute to early onset complications of BAV disease.

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Novel Association of the NOTCH Pathway Regulator MIB1 Gene With the Development of Bicuspid Aortic Valve

Cited by 9 publications

References 71 publications

Directed Differentiation of Human Induced Pluripotent Stem Cells to Heart Valve Cells

Directed Differentiation of Human Induced Pluripotent Stem Cells to Heart Valve Cells

International Collaboration Identifies Gene Linked to Congenital Heart Defect

Whole Exome Sequencing Uncovers the Genetic Complexity of Bicuspid Aortic Valve in Families with Early Onset Complications

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