Hepatocyte growth factor is involved in the morphogenesis of tooth germ in murine molars

Tabata, M.; Kim, Kenji; Liu, Ji Guang; Yamashita, Kazuo; Matsumura, Tatsushi; Kato, Jun; Iwamoto, Masahiro; Wakisaka, Satoshi; Matsumoto, Kunio; Nakamura, Toshikazu; Kumegawa, Masayoshi; Kurisu, Kojiro

doi:10.1242/dev.122.4.1243

Cited by 77 publications

(2 citation statements)

References 52 publications

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“…Enamel defects have also been reported in others syndromes and the question remains to qualify them as amelogenesis imperfecta. For instance, genes associated with -skin, nails and hair defects among other symptoms are ATR (Tanaka et al, 2012), CLDN1 (Feldmeyer et al, 2006), COG6 (Shaheen et al, 2013), FGF10, FGFR3, FGFR2 (Hollister et al, 1973), HRAS (Goodwin et al, 2014), KRAS, NRAS, KRT14 (Tabata et al, 1996), MBTPS2 (Martino et al, 1992); -with eye defects NAA10; -with skeletal anomalies AKT1, B3GAT3, CYP27B1, CTSK, EVC1, EVC2, ERCC4, ERCC8, GJA1, GNAS, IDUA, IRX5, NDN, PTDSS1, SNORD116, RUNX2, TBCE, VDR; -genito-urinary anomalies HNF1B, VPS33B, VIPAR; -intellectual disability PSPA, GALC; Usher syndrome MYO7A, USH2A, PD2D7, ADGRV1, CLRN1.…”

Section: Discussionmentioning

confidence: 99%

Amelogenesis imperfecta: Next-generation sequencing sheds light on Witkop’s classification

Bloch-Zupan,

Rey,

Jimenez-Armijo

et al. 2023

Front. Physiol.

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Amelogenesis imperfecta (AI) is a heterogeneous group of genetic rare diseases disrupting enamel development (Smith et al., Front Physiol, 2017a, 8, 333). The clinical enamel phenotypes can be described as hypoplastic, hypomineralized or hypomature and serve as a basis, together with the mode of inheritance, to Witkop’s classification (Witkop, J Oral Pathol, 1988, 17, 547–553). AI can be described in isolation or associated with others symptoms in syndromes. Its occurrence was estimated to range from 1/700 to 1/14,000. More than 70 genes have currently been identified as causative.Objectives: We analyzed using next-generation sequencing (NGS) a heterogeneous cohort of AI patients in order to determine the molecular etiology of AI and to improve diagnosis and disease management.Methods: Individuals presenting with so called “isolated” or syndromic AI were enrolled and examined at the Reference Centre for Rare Oral and Dental Diseases (O-Rares) using D4/phenodent protocol (www.phenodent.org). Families gave written informed consents for both phenotyping and molecular analysis and diagnosis using a dedicated NGS panel named GenoDENT. This panel explores currently simultaneously 567 genes. The study is registered under NCT01746121 and NCT02397824 (https://clinicaltrials.gov/).Results: GenoDENT obtained a 60% diagnostic rate. We reported genetics results for 221 persons divided between 115 AI index cases and their 106 associated relatives from a total of 111 families. From this index cohort, 73% were diagnosed with non-syndromic amelogenesis imperfecta and 27% with syndromic amelogenesis imperfecta. Each individual was classified according to the AI phenotype. Type I hypoplastic AI represented 61 individuals (53%), Type II hypomature AI affected 31 individuals (27%), Type III hypomineralized AI was diagnosed in 18 individuals (16%) and Type IV hypoplastic-hypomature AI with taurodontism concerned 5 individuals (4%). We validated the genetic diagnosis, with class 4 (likely pathogenic) or class 5 (pathogenic) variants, for 81% of the cohort, and identified candidate variants (variant of uncertain significance or VUS) for 19% of index cases. Among the 151 sequenced variants, 47 are newly reported and classified as class 4 or 5. The most frequently discovered genotypes were associated with MMP20 and FAM83H for isolated AI. FAM20A and LTBP3 genes were the most frequent genes identified for syndromic AI. Patients negative to the panel were resolved with exome sequencing elucidating for example the gene involved ie ACP4 or digenic inheritance.Conclusion: NGS GenoDENT panel is a validated and cost-efficient technique offering new perspectives to understand underlying molecular mechanisms of AI. Discovering variants in genes involved in syndromic AI (CNNM4, WDR72, FAM20A … ) transformed patient overall care. Unravelling the genetic basis of AI sheds light on Witkop’s AI classification.

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Section: Discussionmentioning

confidence: 99%

Amelogenesis imperfecta: Next-generation sequencing sheds light on Witkop’s classification

Bloch-Zupan,

Rey,

Jimenez-Armijo

et al. 2023

Front. Physiol.

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“…In contrast to WNT, BMP/TGFβ, FGF, and HH, HGF/MET expression emerges later and covers less stages of tooth development. Temporospatial expression pattern of HGF and its receptor MET in tooth germ ranges from the early cap stage through the late bell stage [Tabata et al, 1996]. During the bell stage, HGF mRNA expression has been detected in the mesenchyme and dental papilla but not in the epithelium.…”

Section: Discussionmentioning

confidence: 99%

Hepatocyte Growth Factor Promotes Differentiation Potential and Stress Response of Human Stem Cells from Apical Papilla

Liu¹,

Yan²,

Chen³

et al. 2022

Cells Tissues Organs

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Harsh local microenvironment, such as hypoxia and lack of instructive clues for transplanted stem cells, presents the serious obstacle for stem cell therapies’ efficacy. Therefore, continued efforts have been taken to improve stem cells’ viability and plasticity. Hepatocyte growth factor (HGF) have previously been reported to mitigate complications of various human diseases in animal model studies and in some clinical trials. Besides, human stem cells from root apical papilla (SCAP) are deemed a better resource of mesenchymal stem cells due to derived stem cells holding greater amplification ability in vitro compared with those from other dental resources. To move forward, evaluating effects and understanding underlying molecular mechanisms of HGF on SCAP for periodontal regeneration are needed. In this study, HGF was transgenic expressed in SCAP, and it was found that HGF enhanced osteo/dentinogenic differentiation capacity of SCAP compared with those non-treated control in an ectopic mineralization model. Moreover, HGF reduced apoptosis of SCAP under both normoxia and hypoxia condition, whereas combination of HGF and hypoxia exposure had inhibitory effects on cell proliferation during an eight-day in vitro culture period. Transcriptome analysis further revealed that suppressed cell cycle progression and activated BMP/ TGFβ, Hedgehog, WNT, FGF, HOX and other morphogen family members upon HGF overexpression, which may render SCAP recapitulate part of neural crest stem cells characteristics. Moreover, strengthened stress-response modulation such as unfolded protein response, macroautophagy and anti-apoptotic molecules might explain increased viability of SCAP. In all, our results imply that these potential mechanisms underlying HGF promoting SCAP differentiation could be further elucidated and harnessed to improve dental tissue regeneration.

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Hepatocyte growth factor expression in the developing myocardium: Evidence for a role in the regulation of the mesenchymal cell phenotype and urokinase expression

Song¹,

Majka²,

McGuire³

1999

Dev. Dyn.

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Hepatocyte growth factor is involved in the morphogenesis of tooth germ in murine molars

Cited by 77 publications

References 52 publications

Amelogenesis imperfecta: Next-generation sequencing sheds light on Witkop’s classification

Amelogenesis imperfecta: Next-generation sequencing sheds light on Witkop’s classification

Hepatocyte Growth Factor Promotes Differentiation Potential and Stress Response of Human Stem Cells from Apical Papilla

Hepatocyte growth factor expression in the developing myocardium: Evidence for a role in the regulation of the mesenchymal cell phenotype and urokinase expression

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