HNF1B controls proximal-intermediate nephron segment identity in vertebrates by regulating Notch signalling components and <i>Irx1/2</i>

Heliot, Claire; Desgrange, Audrey; Buisson, Isabelle; Prunskaite‐Hyyryläinen, Renata; Shan, Jingdong; Vainio, Seppo; Umbhauer, Muriel; Cereghini, Silvia

doi:10.1242/dev.086538

Cited by 107 publications

(143 citation statements)

References 49 publications

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“…Interestingly, the inactivation of Hnf1b in nephron progenitors using a Wnt4-Cre line and another Hnf1b floxed allele gave rise to the same phenotype. This confirms the crucial role of HNF1b in nephron tubular specification (Heliot et al, 2013). …”

Section: Research Article Hnf1β In Nephron Developmentsupporting

confidence: 76%

Hepatocyte nuclear factor 1β controls nephron tubular development

et al. 2013

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SUMMARYNephron morphogenesis is a complex process that generates blood-filtration units (glomeruli) connected to extremely long and patterned tubular structures. Hepatocyte nuclear factor 1β (HNF1β) is a divergent homeobox transcription factor that is expressed in kidney from the first steps of nephrogenesis. Mutations in HNF1B (OMIM #137920) are frequently found in patients with developmental renal pathologies, the mechanisms of which have not been completely elucidated. Here we show that inactivation of Hnf1b in the murine metanephric mesenchyme leads to a drastic tubular defect characterized by the absence of proximal, distal and Henle's loop segments. Nephrons were eventually characterized by glomeruli, with a dilated urinary space, directly connected to collecting ducts via a primitive and short tubule. In the absence of HNF1β early nephron precursors gave rise to deformed S-shaped bodies characterized by the absence of the typical bulge of epithelial cells at the bend between the mid and lower segments. The lack of this bulge eventually led to the absence of proximal tubules and Henle's loops. The expression of several genes, including Irx1, Osr2 and Pou3f3, was downregulated in the S-shaped bodies. We also observed decreased expression of Dll1 and the consequent defective activation of Notch in the prospective tubular compartment of comma-and S-shaped bodies. Our results reveal a novel hierarchical relationship between HNF1β and key genes involved in renal development. In addition, these studies define a novel structural and functional component of S-shaped bodies at the origin of tubule formation.

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Section: Research Article Hnf1β In Nephron Developmentsupporting

confidence: 76%

Hepatocyte nuclear factor 1β controls nephron tubular development

et al. 2013

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“…A direct regulation of Dll1 by Hnf1b, as recently shown in the kidney (Heliot et al, 2013;Massa et al, 2013), does not seem to occur in the pancreas, as ChIP on E12.5 pancreata showed no Hnf1b recruitment to a conserved region of Dll1 (data not shown). Recent data suggested a role for Dll1, which is activated by Ptf1a, in MPC proliferation (Ahnfelt-Ronne et al, 2012).…”

Section: Mpcs Proliferation and Survivalsupporting

confidence: 52%

“…We performed a conditional deletion of Hnf1b in pancreatic MPCs using a Hnf1b-floxed mouse line (Heliot et al, 2013) crossed with the Pdx1-Cre (Wells et al, 2007) or the tamoxifen (TM)-inducible Sox9-CreER T2 line (Kopp et al, 2011), as Pdx1 and Sox9 share a common expression domain with Hnf1b in the early pancreas Maestro et al, 2003;Seymour et al, 2007). Pdx1-Cre;Hnf1b +/LacZ and Hnf1b Flox/Flox mice were crossed to generate Pdx1-Cre;Hnf1b…”

Section: Resultsmentioning

confidence: 99%

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Hnf1b controls pancreas morphogenesis and the generation of Ngn3+ endocrine progenitors

et al. 2015

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Heterozygous mutations in the human HNF1B gene are associated with maturity-onset diabetes of the young type 5 (MODY5) and pancreas hypoplasia. In mouse, Hnf1b heterozygous mutants do not exhibit any phenotype, whereas the homozygous deletion in the entire epiblast leads to pancreas agenesis associated with abnormal gut regionalization. Here, we examine the specific role of Hnf1b during pancreas development, using constitutive and inducible conditional inactivation approaches at key developmental stages. Hnf1b early deletion leads to a reduced pool of pancreatic multipotent progenitor cells (MPCs) due to decreased proliferation and increased apoptosis. Lack of Hnf1b either during the first or the secondary transitions is associated with cystic ducts. Ductal cells exhibit aberrant polarity and decreased expression of several cystic disease genes, some of which we identified as novel Hnf1b targets. Notably, we show that Glis3, a transcription factor involved in duct morphogenesis and endocrine cell development, is downstream Hnf1b. In addition, a loss and abnormal differentiation of acinar cells are observed. Strikingly, inactivation of Hnf1b at different time points results in the absence of Ngn3 + endocrine precursors throughout embryogenesis. We further show that Hnf1b occupies novel Ngn3 putative regulatory sequences in vivo. Thus, Hnf1b plays a crucial role in the regulatory networks that control pancreatic MPC expansion, acinar cell identity, duct morphogenesis and generation of endocrine precursors. Our results uncover an unappreciated requirement of Hnf1b in endocrine cell specification and suggest a mechanistic explanation of diabetes onset in individuals with MODY5.

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“…There is evidence that certain transcription factors such as Hnf1b are critical for nephron patterning, and Hnf1b-null mice do not develop a differentiated tubule (36,37). Notch signaling is also required for proximal tubule differentiation, and mice with deficiencies in this pathway have abnormal tubule differentiation (38 -44).…”

Section: ϫ/ϫmentioning

confidence: 99%

The Integrin β1 Subunit Regulates Paracellular Permeability of Kidney Proximal Tubule Cells

Elias

Mathew

Srichai

et al. 2014

Journal of Biological Chemistry

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Background: Proximal tubule kidney epithelial cells differentiate into a "loose" epithelium by unknown mechanisms. Results: Deleting integrin ␤1 converts proximal tubule cells from a "loose" to a "tight" epithelium. Conclusion: Integrin ␤1 regulates the composition and function of tight and adherens junctions that define paracellular transport properties of proximal tubule epithelial cells. Significance: Integrins might regulate terminal differentiation of polarized epithelial cells.

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HNF1B controls proximal-intermediate nephron segment identity in vertebrates by regulating Notch signalling components and Irx1/2

Cited by 107 publications

References 49 publications

Hepatocyte nuclear factor 1β controls nephron tubular development

Hepatocyte nuclear factor 1β controls nephron tubular development

Hnf1b controls pancreas morphogenesis and the generation of Ngn3+ endocrine progenitors

The Integrin β1 Subunit Regulates Paracellular Permeability of Kidney Proximal Tubule Cells

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