Your search keyword '"McMahon, Andrew P."' showing total 1,325 results

601. Cloning, Expression, and Chromosomal Location of SHHand IHH: Two Human Homologues of the DrosophilaSegment Polarity Gene Hedgehog

Author

Marigo, Valeria, Roberts, Drucilla J., Lee, Scott M.K., Tsukurov, Olga, Levi, Tatjana, Gastier, Julie M., Epstein, Douglas J., Gilbert, Debra J., Copeland, Neal G., Seidman, Christine E., Jenkins, Nancy A., Seidman, J.G., Mcmahon, Andrew P., and Tabin, Cliff

Abstract

The hedgehog genes encode signaling molecules that play a role in regulating embryonic morphogenesis. We have cloned and sequenced human cDNA copies of two of these genes, SHHand IHH. The SHHclone includes the full coding sequence and encodes a protein 92.4% identical to its murine homologue. The IHHclone is 89% complete and encodes a protein 94.6% identical to its murine homologue. IHHis expressed in adult kidney and liver. SHHexpression was not detected in adult tissues examined; however, it is expressed in fetal intestine, liver, lung, and kidney. SHHmapped to chromosome 7q and IHHto chromosome 2 by PCR with DNA from a panel of rodent-human somatic cell hybrids. To identify the cbromosomal location of SHHmore precisely, a P1 genomic clone of SHHwas isolated. This phage contained a CA repeat sequence tagged site that was used to map SHHrelative to a polysyndactyly disease locus, using DNA prepared from affected and unaffected members of a large pedigree. SHH is closely linked, but distinct from the polysyndactyly disease locus at 7q36 (maximum lad score = 4.82, θ = 0.05) tightly linked to the EN2locus. The murine homologues Shh, Ihh, and Dhhwere mapped using (C57BL/6J × Mus sprectus)F1× C57BL/6J interspecific backcross. Shhmapped to a position 0.6 cM distal to En2and 1.9 cM proximal to H6on mouse chromosome 5. This location is closely linked but distinct from the murine limb mutation Hxanti syntenie to human chromosome 7q136.

Published

1995

602. Evidence that FGF8 signalling from the midbrain-hindbrain junction regulates growth and polarity in the developing midbrain

Author

Lee, Scott M. K., Danielian, Paul S., Fritzsch, Bernd, and McMahon, Andrew P.

Abstract

The developing vertebrate mesencephalon shows a rostrocaudal gradient in the expression of a number of molecular markers and in the cytoarchitectonic differentiation of the tectum, where cells cease proliferating and differentiate in a rostral to caudal progression. Tissue grafting experiments have implicated cell signalling by the mesencephalicmetencephalic (mid-hindbrain) junction (or isthmus) in orchestrating these events. We have explored the role of Wnt-1 and FGF8 signalling in the regulation of mesencephalic polarity. Wnt-1 is expressed in the caudal mesencephalon and Fgf8 in the most rostral metencephalon. Wnt-1 regulates Fgf8 expression in the adjacent metencephalon, most likely via a secondary mesencephalic signal. Ectopic expression of Fgf8 in the mesencephalon is sufficient to activate expression of Engrailed-2 (En-2) and ELF-1, two genes normally expressed in a decreasing caudal to rostral gradient in the posterior mesencephalon. Ectopic expression of Engrailed-1 (En-1), a functionally equivalent homologue of En-2 is sufficient to activate ELF-1 expression by itself. These results indicate the existence of a molecular hierarchy in which FGF8 signalling establishes the graded expression of En-2 within the tectum. This in turn may act to specify other aspects of A-P polarity such as graded ELF-1 expression. Our studies also reveal that FGF8 is a potent mitogen within the mesencephalon: when ectopically expressed, neural precursors continue to proliferate and neurogenesis is prevented. Taken together our results suggest that FGF8 signalling from the isthmus has a key role in coordinately regulating growth and polarity in the developing mesencephalon.

Published

1997

603. Novel regulatory interactions revealed by studies of murine limb pattern in Wnt-7a and En-1 mutants

Author

Cygan, Jennifer A., Johnson, Randy L., and McMahon, Andrew P.

Abstract

Classical embryological experiments have demonstrated that dorsal-ventral patterning of the vertebrate limb is dependent upon ectodermal signals. One such factor is Wnt-7a, a member of the Wnt family of secreted proteins, which is expressed in the dorsal ectoderm. Loss of Wnt-7a results in the appearance of ventral characteristics in the dorsal half of the distal limb. Conversely, En-1, a homeo-domain transcription factor, is expressed exclusively in the ventral ectoderm, where it represses Wnt-7a. En-1 mutants have dorsal characteristics in the ventral half of the distal limb. Experiments in the chick suggest that the dorsalizing activity of Wnt-7a in the mesenchyme is mediated through the regulation of the LIM-homeodomain transcription factor Lmx-1. Here we have examined the relationship between Wnt-7a, En-1 and Lmx-1b, a mouse homolog of chick Lmx-1, in patterning the mammalian limb. We find that Wnt-7a is required for Lmx-1b expression in distal limb mesenchyme, and that Lmx-1b activation in the ventral mesenchyme of En-1 mutants requires Wnt-7a. Consistent with Lmx-1b playing a primary role in dorsal-ization of the limb, we find a direct correlation between regions of the anterior distal limb in which Lmx-1b is misregulated during limb development and the localization of dorsal-ventral patterning defects in Wnt-7a and En-1 mutant adults. Thus, ectopic Wnt-7a expression and Lmx-1b activation underlie the dorsalized En-1 phenotype, although our analysis also reveals a Wnt-7a-independent activity for En-1 in the repression of pigmentation in the ventral epidermis. Finally, we demonstrate that ectopic expression of Wnt-7a in the ventral limb ectoderm of En-1 mutants results in the formation of a second, ventral apical ectodermal ridge (AER) at the junction between Wnt-7a-expressing and nonexpressing ectoderm. Unlike the normal AER, ectopic AER formation is dependent upon Wnt-7a activity, indicating that distinct genetic mechanisms may be involved in primary and secondary AER formation.

Published

1997

604. Antagonizing cAMP-dependent protein kinase A in the dorsal CNS activates a conserved Sonic hedgehog signaling pathway

Author

Epstein, Douglas J., Martí, Elisa, Scott, Matthew P., and McMahon, Andrew P.

Abstract

Hedgehog (Hh) signaling plays a significant role in defining the polarity of a variety of tissue types along the anterior/posterior and dorsal/ventral axes in both vertebrate and invertebrate organisms. The pathway through which Hh transduces its signal is still obscure, however, recent data have implicated the cyclic AMP-dependent protein kinase A as a negative regulator of the Hh signal transduction pathway. One of the vertebrate Hh family members, Sonic hedgehog (Shh), can induce ventral neural cell types both in vivo and in vitro; high concentrations induce floor plate and lower concentrations motor neurons. To investigate whether PKA plays an active role in the suppression of ventral neural differentiation, we generated transgenic embryos expressing a dominant negative form of PKA (dnPKA) in primarily dorsal aspects of the mouse CNS. Similar to our earlier results with Shh, we observed the induction of floor plate and motor neuron markers in embryos expressing the dominant negative PKA transgene and the loss of dorsal gene expression at rostral levels. Thus suppression of PKA activity is sufficient to activate targets of the Shh signaling pathway in the vertebrate CNS suggesting that induction of ventral cell types occurs via the antagonistic action of Shh on PKA activity. Two mammalian target genes that are strongly expressed in ectopic dorsal locations in response to dnPKA are Ptc and Gli. As both of these are targets of Drosophila Hh signaling, our data point to an evolutionary conservation in both the mechanisms of signaling and the effectors of the signaling pathway.

Published

1996

605. Cadherin adhesion complexes direct cell aggregation in the epithelial transition of Wnt-induced nephron progenitor cells.

Author

Der, Balint, Bugacov, Helena, Briantseva, Bohdana-Myroslava, and McMahon, Andrew P.

Subjects

*EPITHELIAL-mesenchymal transition, *CELL aggregation, *KIDNEY tubules, *PROGENITOR cells, *CADHERINS

Abstract

In the developing mammalian kidney, nephron formation is initiated by a subset of nephron progenitor cells (NPCs). Wnt input activates a ß-catenin (Ctnnb1)-driven, transcriptional nephrogenic program and the mesenchymal to epithelial transition (MET) of NPCs. Using an in vitro mouse NPC culturemodel, we observed that activation of the Wnt pathway results in the aggregation of induced NPCs, which is an initiating step in the MET program. Genetic removal showed aggregation was dependent on ß-catenin. Modulating extracellular Ca2+ levels showed cell-cell contacts were Ca2+ dependent, suggesting a role for cadherin (Cdh)-directed cell adhesion. Molecular analysis identified Cdh2, Cdh4 and Cdh11 in NPCs, and the ß-catenin directed upregulation of Cdh3 and Cdh4 accompanying the MET of induced NPCs. Mutational analysis of ß-catenin supported a role for a Lef/Tcf-ß-cateninmediated transcriptional response in the cell aggregation process. Genetic removal of all four cadherins, and independent removal of a-catenin or of ß-catenin-a-catenin interactions, abolished aggregation, but not the inductive response to Wnt pathway activation. These findings, and data in an accompanying article highlight the role of ß-catenin in linking transcriptional programs to the morphogenesis of NPCs in mammalian nephrogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

606. Dose-dependent responses to canonical Wnt transcriptional complexes in the regulation of mammalian nephron progenitors.

Author

Bugacov, Helena, Der, Balint, Briantseva, Bohdana-Myroslava, Qiuyu Guo, Sunghyun Kim, Lindström, Nils O., and McMahon, Andrew P.

Subjects

*GENE expression, *PROGENITOR cells, *KIDNEY tubules, *GENETIC transcription regulation, *CELL proliferation, *WNT signal transduction

Abstract

In vivo and in vitro studies argue that concentration-dependent Wnt signaling regulates mammalian nephron progenitor cell (NPC) programs. Canonical Wnt signaling is regulated through the stabilization of ß-catenin, a transcriptional co-activator when complexed with Lef/Tcf DNA-binding partners. Using the GSK3ß inhibitor CHIR99021 (CHIR) to block GSK3ß-dependent destruction of ß-catenin, we examined dose-dependent responses to ß-catenin in mouse NPCs, using mRNA transduction to modify gene expression. Low CHIR-dependent proliferation of NPCs was blocked on ß-catenin removal, with evidence of NPCs arresting at the G2-M transition. While NPC identity was maintained following ß-catenin removal, mRNA-seq identified low CHIR and ß-catenin dependent genes. High CHIR activated nephrogenesis. Nephrogenic programming was dependent on Lef/Tcf factors and ß-catenin transcriptional activity. Molecular and cellular features of early nephrogenesis were driven in the absence of CHIR by a mutated stabilized form of ß-catenin. Chromatin association studies indicate low and high CHIR response genes are likely direct targets of canonical Wnt transcriptional complexes. Together, these studies provide evidence for concentration-dependent Wnt signaling in the regulation of NPCs and provide new insight into Wnt targets initiating mammalian nephrogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

607. A tale of two morphogen gradients: Identifying Gli targets of Hedgehog Signaling

Author

Vokes, Steven A., Ji, Hongkai, Wong, Wing H., and McMahon, Andrew P.

Published

2006

608. Amplification-Free Detection of Viruses in Minutes using Single-Particle Imaging and Machine Learning

Author

Shiaelis, Nicolas, Peto, Leon, McMahon, Andrew, Hepp, Chritof, Bickerton, Erica, Favard, Cyril, Muriaux, Delphine, Andersson, Monique, Vaughan, Alison, Matthews, Philippa, Stoesser, Nicole, Crook, Derrick, Kapanidis, Achillefs N., and Robb, Nicole C.

Published

2021

609. High-Throughput Super-Resolution Microscopy of Viral Particles Reveals Insights into their Morphology and Organisation

Author

McMahon, Andrew, Hepp, Christof, and Robb, Nicole C.

Published

2021

610. Engrailed-1 as a target of the Wnt-1 signalling pathway in vertebrate midbrain development.

Author

Danielian, Paul S. and McMahon, Andrew P.

Subjects

*GENETICS, *MESENCEPHALON

Abstract

Describes the results of the expression of the engrailed gene En-1 in the developing midbrain of Wnt-1 gene-null embryos. The rescue of early midbrain and anterior hindbrain development; The role of Wnt-1 signalling; The maintenance of En expression; The role in the genetics of both mice and fruit flies.

Published

1996

611. Inducible expression of a cloned heat shock fusion gene in sea urchin embryos

Author

McMahon, Andrew P., Novak, Thomas J., Britten, Roy J., Davidson, Eric H., McMahon, Andrew P., Novak, Thomas J., Britten, Roy J., and Davidson, Eric H.

Abstract

A fusion gene construct, in which the coding sequence for bacterial chloramphenicol acetyltransferase (CAT; acetyl-CoA: chloramphenicol 3-O-acetyltransferase, EC 2.3.1.28) was placed under the control of the regulatory region of the Drosophila gene encoding the 70-kilodalton heat shock protein [Di Nocera, P. P. & Dawid, I. B. (1983) Proc. Natl. Acad. Sci. USA 80, 7095-7098], was microinjected into the cytoplasm of unfertilized sea urchin eggs. Pluteus-stage embryos developing from the injected eggs were exposed to high temperature conditions that we found would elicit an endogenous sea urchin heat shock response. These embryos express the gene for CAT and, after heat treatment, display 8-10 times more CAT enzyme activity than do extracts from control embryos cultured at normal temperatures. The injected DNA is present in high molecular weight concatenates and, during development, is amplified about 100-fold. Amplified sequences are responsible for all or most of the induced CAT enzyme activity.

Published

1984

612. Multi-omic approaches to acute kidney injury and repair

Author

Gerhardt, Louisa M.S. and McMahon, Andrew P.

Abstract

The kidney has a remarkable regenerative capacity. In response to ischemic or toxic injury, proximal tubule cells can proliferate to rebuild damaged tubules and restore kidney function. However, severe acute kidney injury (AKI) or recurrent AKI events can lead to maladaptive repair and disease progression from AKI to chronic kidney disease (CKD). The application of single-cell technologies has identified injured proximal tubule cell states weeks after AKI, distinguished by a proinflammatory senescent molecular signature. Epigenetic studies have highlighted dynamic changes in the chromatin landscape of the kidney following AKI and have described key transcription factors linked to the AKI response. The integration of multi-omic technologies opens new possibilities to improve our understanding of AKI and the driving forces behind the AKI-to-CKD transition, with the ultimate goal of designing tailored diagnostic and therapeutic strategies to improve AKI outcomes and prevent kidney disease progression.

Published

2021

613. Multi-omics integration in the age of million single-cell data.

Author

Miao, Zhen, Humphreys, Benjamin D., McMahon, Andrew P., and Kim, Junhyong

Subjects

*DATA integration, *DATA visualization, *BIOLOGICAL networks, *BIOLOGICAL models, *TRANSCRIPTOMES, *BIOLOGICAL classification

Abstract

An explosion in single-cell technologies has revealed a previously underappreciated heterogeneity of cell types and novel cell-state associations with sex, disease, development and other processes. Starting with transcriptome analyses, single-cell techniques have extended to multi-omics approaches and now enable the simultaneous measurement of data modalities and spatial cellular context. Data are now available for millions of cells, for whole-genome measurements and for multiple modalities. Although analyses of such multimodal datasets have the potential to provide new insights into biological processes that cannot be inferred with a single mode of assay, the integration of very large, complex, multimodal data into biological models and mechanisms represents a considerable challenge. An understanding of the principles of data integration and visualization methods is required to determine what methods are best applied to a particular single-cell dataset. Each class of method has advantages and pitfalls in terms of its ability to achieve various biological goals, including cell-type classification, regulatory network modelling and biological process inference. In choosing a data integration strategy, consideration must be given to whether the multi-omics data are matched (that is, measured on the same cell) or unmatched (that is, measured on different cells) and, more importantly, the overall modelling and visualization goals of the integrated analysis. [ABSTRACT FROM AUTHOR]

Published

2021

614. A late B lymphocyte action in dysfunctional tissue repair following kidney injury and transplantation.

Author

Cippà, Pietro E., Liu, Jing, Sun, Bo, Kumar, Sanjeev, Naesens, Maarten, and McMahon, Andrew P.

Abstract

The mechanisms initiating late immune responses to an allograft are poorly understood. Here we show, via transcriptome analysis of serial protocol biopsies from kidney transplants, that the initial responses to kidney injury correlate with a late B lymphocyte signature relating to renal dysfunction and fibrosis. With a potential link between dysfunctional repair and immunoreactivity, we investigate the immunological consequences of dysfunctional repair examining chronic disease in mouse kidneys 18 months after a bilateral ischemia/reperfusion injury event. In the absence of foreign antigens, a sustained immune response involving both innate and adaptive immune systems accompanies a transition to chronic kidney damage. At late stages, B lymphocytes exhibite an antigen-driven proliferation, selection and maturation into broadly-reacting antibody-secreting cells. These findings reveal a previously unappreciated role for dysfunctional tissue repair in local immunomodulation that may have particular relevance to transplant-associated immunobiology. Allograft can induces local chronic inflammation, but how this feeds back to regulating late immunity is still not clear. Here the authors show, by charactering B cell transcriptome landscape dynamic in human allografts and in mouse kidneys transitioning from acute to chronic injury, that late B cell activation is associated with renal dysfunction and inflammation. [ABSTRACT FROM AUTHOR]

Published

2019

615. A high-resolution anatomical ontology of the developing murine genitourinary tract

Author

Little, Melissa H., Jane Brennan, Kylie Georgas, Davies, Jamie A., Davidson, Duncan R., Baldock, Richard A., Annemiek Beverdam, John Bertram, Blanche Capel, Han Sheng Chiu, Dave Clements, Luise Anne Cullen-McEwen, Fleming, Jean S., Thierry Gilbert, Derek Houghton, Kaufman, Matt H., Elena Kleymenova, Peter Anthony Koopman, Lewis, Alfor G., Mcmahon, Andrew P., Mendelsohn, Cathy L., Eleanor Katherine Mitchell, Rumballe, Bree A., Sweeney, Derina E., Todd Valerius, M., Gen Yamada, Yiya Yang, and Jing Yu

616. Sonic Hedgehog Is Required for Progenitor Cell Maintenance in Telencephalic Stem Cell Niches

Author

Machold, Robert, Hayashi, Shigemi, Rutlin, Michael, Muzumdar, Mandar D, Nery, Susana, Corbin, Joshua G, Gritli-Linde, Amel, Dellovade, Tammy, Porter, Jeffery A, Rubin, Lee L, Dudek, Henryk, McMahon, Andrew P, and Fishell, Gord

Published

2003

617. Expression of the proto-oncogene int-1 is restricted to specific neural cells in the developing mouse embryo

Author

Wilkinson, David G., primary, Bailes, Juliet A., additional, and McMahon, Andrew P., additional

Published

1987

618. Ectopic expression of the proto-oncogene int-1 in Xenopus embryos leads to duplication of the embryonic axis

Author

McMahon, Andrew P., primary and Moon, Randall T., additional

Published

1989

619. cDNA cloning, sequencing and chromosome mapping of a non-erythroid spectrin, human α-fodrin

Author

McMahon, Andrew P., primary, Giebelhaus, Dawn H., additional, Champion, Janet E., additional, Bailes, Juliet A., additional, Lacey, Simon, additional, Carritt, Ben, additional, Henchman, Susan K., additional, and Moon, Randall T., additional

Published

1987

620. Introduction of cloned DNA into sea urchin egg cytoplasm: Replication and persistence during embryogenesis

Author

McMahon, Andrew P., primary, Flytzanis, Constantin N., additional, Hough-Evans, Barbara R., additional, Katula, Karen S., additional, Britten, Roy J., additional, and Davidson, Eric H., additional

Published

1985

621. Persistence and integration of cloned DNA in postembryonic sea urchins

Author

Flytzanis, Constantin N., primary, McMahon, Andrew P., additional, Hough-Evans, Barbara R., additional, Katula, Karen S., additional, Britten, Roy J., additional, and Davidson, Eric H., additional

Published

1985

622. Image-based modeling of kidney branching morphogenesis reveals GDNF-RET based Turing-type mechanism and pattern-modulating WNT11 feedback.

Author

Menshykau, Denis, Michos, Odyssé, Lang, Christine, Conrad, Lisa, McMahon, Andrew P., and Iber, Dagmar

Abstract

Branching patterns and regulatory networks differ between branched organs. It has remained unclear whether a common regulatory mechanism exists and how organ-specific patterns can emerge. Of all previously proposed signalling-based mechanisms, only a ligand-receptor-based Turing mechanism based on FGF10 and SHH quantitatively recapitulates the lung branching patterns. We now show that a GDNF-dependent ligand-receptor-based Turing mechanism quantitatively recapitulates branching of cultured wildtype and mutant ureteric buds, and achieves similar branching patterns when directing domain outgrowth in silico. We further predict and confirm experimentally that the kidney-specific positive feedback between WNT11 and GDNF permits the dense packing of ureteric tips. We conclude that the ligand-receptor based Turing mechanism presents a common regulatory mechanism for lungs and kidneys, despite the differences in the molecular implementation. Given its flexibility and robustness, we expect that the ligand-receptor-based Turing mechanism constitutes a likely general mechanism to guide branching morphogenesis and other symmetry breaks during organogenesis. Many organs develop through branching morphogenesis, but whether the underlying mechanisms are shared is unknown. Here, the authors show that a ligand-receptor based Turing mechanisms, similar to that observed in lung development, likely underlies branching morphogenesis of the kidney. [ABSTRACT FROM AUTHOR]

Published

2019

623. The activity of Gli transcription factors is essential for Kras-induced pancreatic tumorigenesis.

Author

Rajurkar, Mihir, De Jesus-Monge, Wilfredo E., Driscoll, David R., Appleman, Victoria A., He Huang, Cotton, Jennifer L., Klimstra, David S., Zhu, Lihua J., Simin, Karl, Lan Xu, McMahon, Andrew P., Lewis, Brian C., and Junhao Mao

Subjects

TRANSCRIPTION factors, PANCREATIC tumors

Abstract

An abstract of the article "The activity of Gli transcription factors is essential for Kras-induced pancreatic tumorigenesis," by Mihir Rajurkar and colleagues is presented.

Published

2012

624. Correction: Foxf Genes Integrate Tbx5 and Hedgehog Pathways in the Second Heart Field for Cardiac Septation.

Author

Hoffmann, Andrew D., Yang, Xinan Holly, Burnicka-Turek, Ozanna, Bosman, Joshua D., Ren, Xiaomeng, Xie, Linglin, Steimle, Jeffrey D., Vokes, Steven A., McMahon, Andrew P., Kalinichenko, Vladimir V., and Moskowitz, Ivan P.

Subjects

HEDGEHOG signaling proteins, CYSTS (Pathology), FORKHEAD transcription factors, THERAPEUTICS

Abstract

A correction to the article "Foxf Genes Integrate Tbx5 and Hedgehog Pathways in the Second Heart Field for Cardiac Septation" that was published in the December 29, 2016 issue is presented.

Published

2016

625. Corrigendum: The dynamics of methylammonium ions in hybrid organic-inorganic perovskite solar cells.

Author

Leguy, Aurelien M.A., Frost, Jarvist Moore, McMahon, Andrew P., Sakai, Victoria Garcia, Kockelmann, W., Law, ChunHung, Li, Xiaoe, Foglia, Fabrizia, Walsh, Aron, O'Regan, Brian C., Nelson, Jenny, Cabral, João T., and Barnes, Piers R.F.

Published

2015

626. The dynamics of methylammonium ions in hybrid organic-inorganic perovskite solar cells.

Author

Leguy, Aurelien M. A., Frost, Jarvist Moore, McMahon, Andrew P., Sakai, Victoria Garcia, Kochelmann, W., Law, ChunHung, Li, Xiaoe, Foglia, Fabrizia, Walsh, Aron, O'Regan, Brian C., Nelson, Jenny, Cabral, João T., and Barnes, Piers R. F.

Published

2015

627. Temporal Differences in Granulosa Cell Specification in the Ovary Reflect Distinct Follicle Fates in Mice1

Author

Mork, Lindsey, Maatouk, Danielle M., McMahon, Jill A., Guo, Jin Jin, Zhang, Pumin, McMahon, Andrew P., and Capel, Blanche

Published

2011

628. Monitoring and robust induction of nephrogenic intermediate mesoderm from human pluripotent stem cells.

Author

Mae, Shin-Ichi, Shono, Akemi, Shiota, Fumihiko, Yasuno, Tetsuhiko, Kajiwara, Masatoshi, Gotoda-Nishimura, Nanaka, Arai, Sayaka, Sato-Otubo, Aiko, Toyoda, Taro, Takahashi, Kazutoshi, Nakayama, Naoki, Cowan, Chad A., Aoi, Takashi, Ogawa, Seishi, McMahon, Andrew P., Yamanaka, Shinya, and Osafune, Kenji

Abstract

A method for stimulating the differentiation of human pluripotent stem cells into kidney lineages remains to be developed. Most cells in kidney are derived from an embryonic germ layer known as intermediate mesoderm. Here we show the establishment of an efficient system of homologous recombination in human pluripotent stem cells by means of bacterial artificial chromosome-based vectors and single-nucleotide polymorphism array-based detection. This system allowed us to generate human-induced pluripotent stem cell lines containing green fluorescence protein knocked into OSR1, a specific intermediate mesoderm marker. We have also established a robust induction protocol for intermediate mesoderm, which produces up to 90% OSR1+ cells. These human intermediate mesoderm cells can differentiate into multiple cell types of intermediate mesoderm-derived organs in vitro and in vivo, thereby supplying a useful system to elucidate the mechanisms of intermediate mesoderm development and potentially providing a cell source for regenerative therapies of the kidney. [ABSTRACT FROM AUTHOR]

Published

2013

629. Hedgehog Signalling: Kif7 Is Not That Fishy After All

Author

Ingham, Philip W. and McMahon, Andrew P.

Subjects

*CELLULAR signal transduction, *DROSOPHILA, *KINESIN, *MICROTUBULES, *TUBULINS, *BIOCHEMICAL mechanism of action

Abstract

Summary: Recent reports examining the mammalian kinesin relative Kif7 highlight the conserved role for microtubule motor proteins in Drosophila and vertebrate Hedgehog signalling. Mammalian Kif7 action centres at the primary cilium, an organelle absent from Drosophila. These studies raise interesting questions about the coupling of microtubule trafficking to the Hedgehog pathway. [Copyright &y& Elsevier]

Published

2009

630. Independent functions and mechanisms for homeobox gene Barx1 in patterning mouse stomach and spleen.

Author

Byeong-Moo Kim, Miletich, Isabelle, Junhao Mao, McMahon, Andrew P., Sharpe, Paul A., and Shivdasani, Ramesh A.

Subjects

HOMEOBOX genes, MORPHOGENESIS, EMBRYOS, MESENCHYME, SPLEEN

Abstract

Homeobox genes convey positional information in embryos and their role in patterning the mammalian gut is a topic of considerable interest. Barx1 is expressed selectively in fetal stomach mesenchyme and directs differentiation of overlying endoderm. Recombinant tissue cultures and study of young mouse embryos previously suggested that Barx1 controls expression of secreted Wnt antagonists, which suppress endodermal Wnt signaling, to enable stomach epithelial differentiation. We overcame mid-gestational lethality of Barx1-/- mouse embryos and report here the spectrum of anomalies in a distinctive and unprecedented model of gastrointestinal homeotic transformation. Using various mouse models, we confirm the importance of attenuated Wnt signaling in stomach development and the role of Barx1 in suppressing endodermal Wnt activity. Absence of Barx1 also results in fully penetrant defects in positioning and expansion of the spleen, an organ that originates within the mesothelial lining of the stomach. Barx1 is absent from the spleen primordium but highly expressed in the mesogastrium, indicating an indirect effect on spleen development. However, our results argue against a role for Wnt antagonism in genesis of the spleen. Mouse spleen development relies on several homeodomain transcriptional regulators that are expressed in the spleen primordium. Loss of Barx1 does not affect expression of any of these genes but notably reduces expression of Wt1, a transcription factor implicated in spleen morphogenesis and expressed in the mesothelium. These observations place Barx1 proximally within a Wt1 pathway of spleen development and reveal how a homeotic regulator employs different molecular mechanisms to mold neighboring organs. [ABSTRACT FROM AUTHOR]

Published

2007

631. Wnt/ß-catenin signaling regulates nephron induction during mouse kidney development.

Author

Joo-Seop Park, Valerius, M. Todd, and McMahon, Andrew P.

Subjects

KIDNEY tubules, WNT proteins, KIDNEYS, MORPHOGENESIS, EPITHELIAL cells, MESENCHYME, LABORATORY mice

Abstract

Mammalian nephrons form as a result of a complex morphogenesis and patterning of a simple epithelial precursor, the renal vesicle. Renal vesicles are established from a mesenchymal progenitor population in response to inductive signals. Several lines of evidence support the sequential roles of two Wnt family members, Wnt9b and Wnt4, in renal vesicle induction. Using genetic approaches to specifically manipulate the activity of β-catenin within the mesenchymal progenitor pool in mice, we investigated the potential role of the canonical Wnt pathway in these inductive events. Progenitor-cell-specific removal of β-catenin activity completely blocked both the formation of renal vesicles and the expected molecular signature of an earlier inductive response. By contrast, activation of stabilized β-catenin in the same cell population causes ectopic expression of mesenchymal induction markers in vitro and functionally replaces the requirement for Wnt9b and Wnt4 in their inductive roles in vivo. Thus, canonical Wnt signaling is both necessary and sufficient for initiating and maintaining inductive pathways mediated by Wnt9b and Wnt4. However, the failure of induced mesenchyme with high levels of β-catenin activity to form epithelial structures suggests that modulating canonical signaling may be crucial for the cellular transition to the renal vesicle. [ABSTRACT FROM AUTHOR]

Published

2007

632. Notch2, but not Notch1, is required for proximal fate acquisition in the mammalian nephron.

Author

Hui-Teng Cheng, Mijin Kim, Valerius, M. Todd, Surendran, Kameswaran, Schuster-Gossler, Karin, Gossler, Achim, McMahon, Andrew P., and Kopan, Raphael

Subjects

NOTCH genes, CELL determination, KIDNEY tubules, NOTCH proteins, DROSOPHILA genetics

Abstract

The Notch pathway regulates cell fate determination in numerous developmental processes. Here we report that Notch2 acts non-redundantly to control the processes of nephron segmentation through an Rbp-J-dependent process. Notch1 and Notch2 are detected in the early renal vesicle. Genetic analysis reveals that only Notch2 is required for the differentiation of proximal nephron structures (podocytes and proximal convoluted tubules) despite the presence of activated Notch1 in the nuclei of putative proximal progenitors. The inability of endogenous Notch1 to compensate for Notch2 deficiency may reflect sub-threshold Notch1 levels in the nucleus. In line with this view, forced expression of a γ-secretase-independent form of Notch1 intracellular domain drives the specification of proximal fates where all endogenous, ligand-dependent Notch signaling is blocked by a γ-secretase inhibitor. These results establish distinct (non-redundant), instructive roles for Notch receptors in nephron segmentation. [ABSTRACT FROM AUTHOR]

Published

2007

633. Distinct roles for Hedgehog and canonical Wnt signaling in specification, differentiation and maintenance of osteoblast progenitors.

Author

Rodda, Stephen J. and McMahon, Andrew P.

Subjects

*CELL differentiation, *CELL determination, *WNT genes, *GENES, *BONES

Abstract

Hedgehog and canonical Wnt/β-catenin signaling are implicated in development of the osteoblast, the bone matrix-secreting cell of the vertebrate skeleton. We have used genetic approaches to dissect the roles of these pathways in specification of the osteoblast lineage. Previous studies indicate that Ihh signaling in the long bones is essential for initial specification of an osteoblast progenitor to a Runx2+ osteoblast precursor. We show here that this is a transient requirement, as removal of Hh responsiveness in later Runx2+, Osx1+ osteoblast precursors does not disrupt the formation of mature osteoblasts. By contrast, the removal of canonical Wnt signaling by conditional removal of the β-catenin gene in early osteoblast progenitors or in Runx2+, Osx1+ osteoblast precursors results in a similar phenotype: osteoblasts fail to progress to a terminal osteocalcin+ fate and instead convert to a chondrocyte fate. By contrast, stabilization of β-catenin signaling in Runx2+, Osx1+ osteoblast precursors leads to the premature differentiation of bone matrix secreting osteoblasts. These data demonstrate that commitment within the osteoblast lineage requires sequential, stage-specific, Ihh and canonical Wnt/β-catenin signaling to promote osteogenic, and block chondrogenic, programs of cell fate specification. [ABSTRACT FROM AUTHOR]

Published

2006

634. Hedgehog Signaling: Iguana Debuts as a Nuclear Gatekeeper

Author

Vokes, Steven A. and McMahon, Andrew P.

Subjects

*IGUANA (Genus), *CELL nuclei, *TRANSCRIPTION factors, *GENETICS

Abstract

The intracellular pathway that controls the cytoplasmic versus nuclear distribution of Gli transcriptional regulators in response to Hedgehog signaling remains poorly understood. Iguana appears to play a role in regulating this process independently of Hedgehog signaling. [Copyright &y& Elsevier]

Published

2004

635. Molecular genetic analysis of Wnt signals in mouse development

Author

Lee, Scott M.K., Dickinson, Mary E., Parr, Brian A., Vainio, Seppo, and McMahon, Andrew P.

Published

1995

636. Isolation of cDNAs partially encoding four Xenopus[formula omitted] proteins and characterization of their transient expression during embryonic development

Author

Christian, Jan L., Gavin, Brian J., McMahon, Andrew P., and Moon, Randall T.

Published

1991

637. A Super Family of Putative Developmental Signaling Molecules Related to the Proto-Oncogene Wnt-1/int-1

Author

McMahon, Andrew P.

Published

1992

638. [46] Factors influencing frequency production of transgenic mice

Author

Mann, Jeffrey R. and McMahon, Andrew P.

Published

1993

639. [39] Cloning developmentally regulated gene families

Author

Gavin, Brian J. and McMahon, Andrew P.

Published

1993

640. Temporal Differences in Granulosa Cell Specification in the Ovary Reflect Distinct Follicle Fates.

Author

Mork, Lindsey, Maatouk, Danielle, McMahon, Jill A., Guo, Jin Jin, Zhang, Pumin, McMahon, Andrew P., McMahon, Jill A., and Capel, Blanche

Abstract

Sex determination results from a fate commitment decision in a population of gonadal cells called the “supporting cell precursors.” These progenitors arise from the proliferative surface epithelium of the gonad. When the sex-determining gene, Sry, is present (eg. in XY gonads), it is expressed in these cells and controls their committment to the Sertoli fate. In XY gonads, supporting cells enclose germ cells inside testis cords and give rise to the entire adult population of Sertoli cells. In the absence of Sryexpression (when Sryis deleted in an XY background, or in wild type XX gonads), these cells up-regulate Foxl2, a gene characteristic of granulosa cell differentiation. Although some experiments suggested that these cells could give rise to a few granulosa cells in the ovary soon after birth, their contribution to the definitive population of adult granulosa cells has not been documented. We used tamoxifen-induced lineage tracing of fetal cells expressing Foxl2to show that descendants of the bipotential supporting cell precursors are limited to the population of medullary follicles that begin to grow immediately after birth and undergo atresia prior to puberty. Using a vital dye to trace coelomic epithelial cells from fetal to perinatal stages, we show that granulosa cells that populate the definitive cortical primordial follicles derive from the surface epithelium perinatally and enter mitotic arrest until they are activated in adult reproductive cycles. Ingression of adult granulosa precursors from the surface epithelium continues until postnatal day 7, when surviving oocytes are individually surrounded by a layer of follicle cells. Thus, those primordial follicles that grow during adult life are comprised of granulosa cells specified long after sex determination, just prior to and throughout the postnatal follicle assembly period, adding complexity to current models.Work in BC's laboratory was supported by a grant from the NIH (HD39963). Work in APM's laboratory was supported by a grant from the NIH (DK070181).

Published

2012

641. DANDY-WALKER MALFORMATION IN TRANSGENIC MICE THAT ECTOPICALLY EXPRESSENGRAILED-1, A HOMEODOMAIN TRANSCRIPTION FACTOR, IN THE EMBRYONIC BRAIN • 302

Author

Rowitch, David H, Danielian, Paul S, McMahon, Andrew P, and Zec, Natasha

Published

1998

642. 729-3 Left Ventricular Hypertrophy in Essential Hypertension Depends on ACE Genotype

Author

O’Kane, Kevin P.J., Prasad, Neeraj, Johnstone, Heather A., Macleod, Catherine, McMahon, Andrew D., MacDonald, Thomas M., and Webb, David J.

Abstract

A deletion/insertion polymorphism in the ACE gene accounts for approximately 50% of the variance in plasma angiotensin converting enzyme (ACE) concentration, and may be linked to tissue ACE activity. The deletion allele (D) occurs with increased frequency in patients with hypertrophic and dilated cardiomyopathy. Left ventricular hypertrophy (LVH) is a recognised complication of essential hypertension, and is associated with increased morbidity and mortality. Angiotensin II, which is produced by ACE, promotes myocyte growth and collagen deposition, and has been causally linked with the development of LVH.

Published

1995

643. Transcriptional and functional motifs defining renal function revealed by single-nucleus RNA sequencing.

Author

Jun Xu, Yifang Liu, Hongjie Li, Tarashansky, Alexander J., Kalicki, Colin H., Ruei-Jiun Hung, Yanhui Hu, Comjean, Aram, Kolluru, Sai Saroja, Bo Wang, Quake, Stephen R., Liqun Luo, McMahon, Andrew P., Dow, Julian A. T., and Perrimon, Norbert

Subjects

*GUANINE nucleotide exchange factors, *HEPATOCYTE nuclear factors, *RNA sequencing, *KIDNEY physiology, *EXCHANGE, *CELL morphology

Abstract

Recent advances in single-cell sequencing provide a unique opportunity to gain novel insights into the diversity, lineage, and functions of cell types constituting a tissue/organ. Here, we performed a single-nucleus study of the adult Drosophila renal system, consisting of Malpighian tubules and nephrocytes, which shares similarities with the mammalian kidney. We identified 11 distinct clusters representing renal stem cells, stellate cells, regionally specific principal cells, garland nephrocyte cells, and pericardial nephrocytes. Characterization of the transcription factors specific to each cluster identified fruitless (fru) as playing a role in stem cell regeneration and Hepatocyte nuclear factor 4 (Hnf4) in regulating glycogen and triglyceride metabolism. In addition, we identified a number of genes, including Rho guanine nucleotide exchange factor at 64C (RhoGEF64c), Frequenin 2 (Frq2), Prip, and CG1093 that are involved in regulating the unusual star shape of stellate cells. Importantly, the single-nucleus dataset allows visualization of the expression at the organ level of genes involved in ion transport and junctional permeability, providing a systems-level view of the organization and physiological roles of the tubules. Finally, a cross-species analysis allowed us to match the fly kidney cell types to mouse kidney cell types and planarian protonephridia, knowledge that will help the generation of kidney disease models. Altogether, our study provides a comprehensive resource for studying the fly kidney. [ABSTRACT FROM AUTHOR]

Published

2022

644. Feedback control of mammalian Hedgehog signaling by the Hedgehog-binding protein, Hip1, modulates Fgf signaling during branching morphogenesis of the lung.

Author

Pao-Tien Chuang, T'Nay Kawcak, and McMahon, Andrew P.

Subjects

*HEDGEHOG signaling proteins, *MORPHOGENESIS, *EMBRYONIC stem cells, *PATTERN formation (Biology), *RESPIRATORY insufficiency

Abstract

Presents a study that examined the role of hedgehog signaling in multiple aspects of embryonic development. Targeted disruption of Hip1 results in neonatal lethality with respiratory failure; Cause of the defective secondary branching in Hip1 mutant lungs; Model for Hip1's role in lung branching morphogenesis.

Published

2003

645. Smoothened Mutants Reveal Redundant Roles for Shh and Ihh Signaling Including Regulation of L/R...

Author

Zhang, Xiaoyan M., Ramalho-Santos, Miguel, and McMahon, Andrew P.

Subjects

*MICE, *MUTAGENESIS, *EMBRYOS

Abstract

Shows that smoothened (Smo) mutants acts epistatic to patched to mediate Sonic and Indian compound mutants in the early mouse embryo development. Genetic analysis of Smo function in mice; Role of hedgehog signaling in mouse left/right (L/R) axis development; Examination of pathways controlling left/right situs.

Published

2001

646. Single-nuclear transcriptomics reveals diversity of proximal tubule cell states in a dynamic response to acute kidney injury.

Author

Gerhardt, Louisa M. S., Jing Liu, Koppitch, Kari, Cippà, Pietro E., and McMahon, Andrew P.

Subjects

*ACUTE kidney failure, *ORGAN donors, *CHRONIC kidney failure, *RNA sequencing, *KIDNEY surgery, *KIDNEY injuries, *COMMERCIAL products, *CURCUMIN

Abstract

Acute kidney injury (AKI), commonly caused by ischemia, sepsis, or nephrotoxic insult, is associated with increased mortality and a heightened risk of chronic kidney disease (CKD). AKI results in the dysfunction or death of proximal tubule cells (PTCs), triggering a poorly understood autologous cellular repair program. Defective repair associates with a long-term transition to CKD. We performed a mild-to-moderate ischemia-reperfusion injury (IRI) to model injury responses reflective of kidney injury in a variety of clinical settings, including kidney transplant surgery. Single-nucleus RNA sequencing of genetically labeled injured PTCs at 7-d ("early") and 28-d ("late") time points post-IRI identified specific gene and pathway activity in the injury-repair transition. In particular, we identified Vcam1+/Ccl2+ PTCs at a late injury stage distinguished by marked activation of NF-κB-, TNF-, and AP-1-signaling pathways. This population of PTCs showed features of a senescence-associated secretory phenotype but did not exhibit G2/M cell cycle arrest, distinct from other reports of maladaptive PTCs following kidney injury. Fate-mapping experiments identified spatially and temporally distinct origins for these cells. At the cortico-medullary boundary (CMB), where injury initiates, the majority of Vcam1+/Ccl2+ PTCs arose from early replicating PTCs. In contrast, in cortical regions, only a subset of Vcam1+/Ccl2+ PTCs could be traced to early repairing cells, suggesting latearising sites of secondary PTC injury. Together, these data indicate even moderate IRI is associated with a lasting injury, which spreads from the CMB to cortical regions. Remaining failed-repair PTCs are likely triggers for chronic disease progression. [ABSTRACT FROM AUTHOR]

Published

2021

647. A β-catenin-driven switch in TCF/LEF transcription factor binding to DNA target sites promotes commitment of mammalian nephron progenitor cells.

Author

Qiuyu Guo, Kim, Albert, Bin Li, Ransick, Andrew, Bugacov, Helena, Xi Chen, Lindström, Nils, Brown, Aaron, Oxburgh, Leif, Ren, Bing, and McMahon, Andrew P.

Subjects

*PROGENITOR cells, *KIDNEY tubules, *TRANSCRIPTION factors, *CATENINS, *DNA, *GENE targeting, *CHROMOSOMES

Abstract

The canonical Wnt pathway transcriptional co-activator β-catenin regulates self-renewal and differentiation of mammalian nephron progenitor cells (NPCs). We modulated b-catenin levels in NPC cultures using the GSK3 inhibitor CHIR99021 (CHIR) to examine opposing developmental actions of β-catenin. Low CHIR-mediated maintenance and expansion of NPCs are independent of direct engagement of TCF/LEF/b-catenin transcriptional complexes at low CHIR-dependent cell-cycle targets. In contrast, in high CHIR, TCF7/LEF1/β-catenin complexes replaced TCF7L1/TCF7L2 binding on enhancers of differentiation-promoting target genes. Chromosome confirmation studies showed pre-established promoter-enhancer connections to these target genes in NPCs. High CHIR-associated de novo looping was observed in positive transcriptional feedback regulation to the canonical Wnt pathway. Thus, β-catenin's direct transcriptional role is restricted to the induction of NPCs, where rising b-catenin levels switch inhibitory TCF7L1/TCF7L2 complexes to activating LEF1/TCF7 complexes at primed gene targets poised for rapid initiation of a nephrogenic program. [ABSTRACT FROM AUTHOR]

Published

2021

648. A novel distal convoluted tubule-specific Cre-recombinase driven by the NaCl cotransporter gene.

Author

Cornelius, Ryan J., Sharma, Avika, Xiao-Tong Su, Jin-Jin Guo, McMahon, Jill A., Ellison, David H., McMahon, Andrew P., and McCormick, James A.

Subjects

*GENETIC recombination, *WESTERN immunoblotting, *GENE targeting, *FLUORESCENT proteins, *CRISPRS

Abstract

Cre-lox technology has revolutionized research in renal physiology by allowing site-specific genetic recombination in individual nephron segments. The distal convoluted tubule (DCT), consisting of distinct early (DCT1) and late (DCT2) segments, plays a central role in Na+ and K+ homeostasis. The only established Cre line targeting the DCT is Pvalb-Cre, which is limited by noninducibility, activity along DCT1 only, and activity in neurons. Here, we report the characterization of the first Cre line specific to the entire DCT. CRISPR/Cas9 targeting was used to introduce a tamoxifen-inducible IRES-Cre- ERT2 cassette downstream of the coding region of the Slc12a3 gene encoding the NaCl cotransporter (NCC). The resulting Slc12a3-Cre- ERT2 mice were crossed with R26R-YFP reporter mice, which revealed minimal leakiness with 6.3% of NCC-positive cells expressing yellow fluorescent protein (YFP) in the absence of tamoxifen. After tamoxifen injection, YFP expression was observed in 91.2% of NCC-positive cells and only in NCC-positive cells, revealing high recombination efficiency and DCT specificity. Crossing to R26RTdTomato mice revealed higher leakiness (64.5%), suggesting differential sensitivity of the floxed site. Western blot analysis revealed no differences in abundances of total NCC or the active phosphorylated form of NCC in Slc12a3-Cre-ERT2 mice of either sex compared with controls. Plasma K+ and Mg2+ concentrations and thiazide-sensitive Na+ and K+ excretion did not differ in Slc12a3-Cre-ERT2 mice compared with controls when sex matched. These data suggest genetic modification had no obvious effect on NCC function. Slc12a3-Cre- ERT2 mice are the first line generated demonstrating inducible Cre recombinase activity along the entire DCT and will be a useful tool to study DCT function. [ABSTRACT FROM AUTHOR]

Published

2020

649. Genetic manipulation of ureteric bud tip progenitors in the mammalian kidney through an Adamts18 enhancer driven tet-on inducible system.

Author

Rutledge, Elisabeth A., Lindström, Nils O., Michos, Odysse, and McMahon, Andrew P.

Subjects

*DIPHTHERIA toxin, *KIDNEYS, *TRANSGENIC mice, *KIDNEY development, *BUDS, *PROXIMAL kidney tubules, *CIS-regulatory elements (Genetics)

Abstract

The ureteric epithelial progenitor (UEP) population within the embryonic kidney generates the arborized epithelial network of the kidney's collecting system and plays a critical role in the expansion and induction of the surrounding nephron progenitor pool. Adamts18 shows UEP- restricted expression in the kidney and progenitor tip-restricted expression in several other organs undergoing branching epithelial growth. Adamts18 is encoded by 23 exons. Genetic removal of genomic sequence spanning exons 1 to 3 led to a specific loss of Adamts18 expression in UEPs, suggesting this region may encode a UEP-specific enhancer. Intron 2 (3 ​kb) was shown to have enhancer activity driving expression of the doxycycline inducible tet-on transcriptional regulator (rtTA) in an Adamts18en-rtTA transgenic mouse strain. Crossing Adamts18en-rtTA mice to a doxycycline dependent GFP reporter mouse enabled the live imaging of embryonic kidney explants. This facilitated the analysis of ureteric epithelial branching events at the cellular level. Ablation of UEPs at the initiation of ureteric bud outgrowth through the doxycycline-mediated induction of Diphtheria Toxin A (DTA) generated a range of phenotypes from complete kidneys agenesis, to duplex kidneys with double ureters. The latter outcome points to the potential of regulative processes to restore UEPs. In contrast, overexpression of YAP prior to ureteric bud outgrowth led to a complete failure of kidney development. Elevating YAP levels at later stages retarded branching growth. A similar phenotype was observed with the overexpression of MYC within the branch-tip localized UEP population. These experiments showcase the utility of the Adamts18en-rtTA transgenic model to the investigation of cellular and molecular events specific to branch tip progenitors within the mammalian kidney complementing existing CRE-dependent genetic tools. Further, the illustrative examples point to areas where new insight may be gained into the regulation of UEP programs. • Adamts18 expression demarcates epithelial branch tip progenitors for several organs. • Genetic analysis identified an Adamts18 enhancer specific to ureteric progenitors. • A tet-on inducible transgenic mouse line enabled genetic modulation in these cells. • The novel line facilitates dynamic high-resolution imaging of ureteric branching. • Tip ablation and YAP/MYC overexpression studies give insights into tip cell actions. [ABSTRACT FROM AUTHOR]

Published

2020

650. Morphogenesis of the kidney and lung requires branch-tip directed activity of the Adamts18 metalloprotease.

Author

Rutledge, Elisabeth A., Parvez, Riana K., Short, Kieran M., Smyth, Ian M., and McMahon, Andrew P.

Subjects

*MORPHOGENESIS, *KIDNEYS, *LUNGS, *ENDOWMENTS, *METALLOPROTEINASES, *PHENOTYPES

Abstract

Adamts18 encodes a secreted metalloprotease restricted to branch-tip progenitor pools directing the morphogenesis of multiple mammalian organs. Adamts18 was targeted to explore a potential role in branching morphogenesis. In the kidney, an arborized collecting system develops through extensive branching morphogenesis of an initial epithelial outgrowth of the mesonephric duct, the ureteric bud. Adamts18 mutants displayed a weakly penetrant phenotype: duplicated ureteric outgrowths forming enlarged, bi-lobed kidneys with an increased nephron endowment. In contrast, Adamts18 mutants showed a fully penetrant lung phenotype: epithelial growth was markedly reduced and early secondary branching scaled to the reduced length of the primary airways. Furthermore, there was a pronounced delay in the appearance of differentiated cell types in both proximal and distally positions of the developing airways. Adamts18 is closely related to Adamts16. In the kidney but not the lung, broad epithelial Adamts16 expression overlaps Adamts18 in branch tips. However, compound Adamts16/18 mutants displayed a comparable low penetrance duplicated ureteric phenotype, ruling out a possible role for Adamts16 as a functional modifier of the Adamts18 kidney phenotype. Given the predicted action of secreted Adamts18 metalloprotease, and broad expression of Adamts18 in branching organ systems, these findings suggest distinct requirements for matrix modelling in the morphogenesis of epithelial networks. • Metalloprotease Adamts18 highlights lung and kidney branch-tip progenitors. • Loss of Adamts18 results in ectopic branches to kidney collecting system. • In lung, Adamts18 regulates growth and patterning of the epithelial airways. [ABSTRACT FROM AUTHOR]

Published

2019