Lethal giant larvae 2 regulates development of the ciliated organ Kupffer’s vesicle

Tay, Hwee Goon; Schulze, Sabrina; Compagnon, Julien; Foley, Fiona C.; Heisenberg, Carl‐Philipp; Yost, H. Joseph; Abdelilah‐Seyfried, Salim; Amack, Jeffrey D.

doi:10.1242/dev.087130

Cited by 26 publications

(48 citation statements)

References 67 publications

(90 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These data suggest that KV morphogenesis can be uncoupled from KV ciliogenesis. This is consistent with published reports in which reduced KV lumen can have normal cilia length (Tay et al, 2013). Moreover, KV formation is a multistep process requiring proper migration and adhesion of precursor cells, lumenogenesis and ciliogenesis (Oteiza et al, 2010; Schneider et al, 2008; Tayeh et al, 2008; Yen et al, 2006).…”

Section: Discussionsupporting

confidence: 94%

Functional characterization of Prickle2 and BBS7 identify overlapping phenotypes yet distinct mechanisms

Xue

Westfall

Zhang

et al. 2014

Developmental Biology

View full text Add to dashboard Cite

Ciliopathies are genetic disorders that are caused by dysfunctional cilia and affect multiple organs. One type of ciliopathy, Bardet-Biedl Syndrome, is a rare disorder characterized by obesity, retinitis pigmentosa, polydactyly, mental retardation and susceptibility to cardiovascular diseases. The Wnt/Planar Cell Polarity (PCP) has been associated with cilia function and ciliogenesis in directing the orientation of cilia and basal bodies. Yet the exact relationship between PCP and ciliopathy is not well understood. Here, we examine interactions between a core PCP component, Prickle2 (Pk2), and a central BBS gene, Bbs7, using gene knockdown in the zebrafish. pk2 and bbs7 knockdown both disrupt the formation of a ciliated organ, the Kupffer’s Vesicle (KV), but do not display a synergistic interaction. By measuring cell polarity in the neural tube, we find that bbs7 activity is not required for Pk asymmetric localization. Moreover, BBS protein complex formation is preserved in the Pk2-deficient (Pk2−/−) mouse. Previously we reported an intracellular melanosome transport delay as a cardinal feature of reduced bbs gene activity. We find that pk2 knockdown suppresses bbs7-related retrograde transport delay. Similarly, knockdown of ift22, an anterograde intraflagellar transport component, also suppresses the bbs7-related retrograde delay. Notably, we find that pk2 knockdown larvae show a delay in anterograde transport. These data suggest a novel role for Pk2 in directional intracellular transport and our analyses show that PCP and BBS function independently, yet result in overlapping phenotypes when knocked down in zebrafish.

show abstract

Section: Discussionsupporting

confidence: 94%

Functional characterization of Prickle2 and BBS7 identify overlapping phenotypes yet distinct mechanisms

Xue

Westfall

Zhang

et al. 2014

Developmental Biology

View full text Add to dashboard Cite

show abstract

“…Thus, we found that atp1b1a and lgl2 not only genetically interact during epidermal cell polarity and malignancy but also during edema formation and Na/K-ATPase a-subunit localization ( Figure 7-figure supplement 1), in line with previous reports of pronephric defects and mild edema formation in lgl2 morphants (Tay et al, 2013). However, atp1b1a and lgl2 mutants also display differences.…”

Section: The Cooperation Between Atp1b1a and Lgl2supporting

confidence: 91%

509 Tumor suppression in basal keratinocytes via dual non-cell-autonomous functions of a Na,K-ATPase beta subunit

Hatzold

Beleggia

Herzig

et al. 2016

Journal of Investigative Dermatology

View full text Add to dashboard Cite

The molecular pathways underlying tumor suppression are incompletely understood.Here, we identify cooperative non-cell-autonomous functions of a single gene that together provide a novel mechanism of tumor suppression in basal keratinocytes of zebrafish embryos. A loss-of-function mutation in atp1b1a, encoding the beta subunit of a Na,K-ATPase pump, causes edema and epidermal malignancy. Strikingly, basal cell carcinogenesis only occurs when Atp1b1a function is compromised in both the overlying periderm (resulting in compromised epithelial polarity and adhesiveness) and in kidney and heart (resulting in hypotonic stress). Blockade of the ensuing PI3K-AKT-mTORC1-NFkB-MMP9 pathway activation in basal cells, as well as systemic isotonicity, prevents malignant transformation. Our results identify hypotonic stress as a (previously unrecognized) contributor to tumor development and establish a novel paradigm of tumor suppression.

show abstract

“…In addition to previously described probes ( cmlc2 , foxa3 and spaw ), pitx2c and elovl6 probes were made from corresponding cDNAs amplified from a zebrafish cDNA library (see primer sequences above) and cloned using a TOPO TA cloning Kit (invitrogen). elovl6 expression was analyzed in cftr pd1048 mutants (Navis et al, 2013) or embryos injected with Lgl2 morpholino (5′-gcccatgacgcctgaacctcttcat-3′) (Tay et al, 2013). gh1 (primers: 5′-atggctagagcattggtgc-3′ and 5′-tacagggtacagttggaatc-3′) and pomca (primers: 5′-atggtgaggggagtgaggatg-3′ and tcact-catccttcctcggttg-3′) cDNA fragments were cloned using a TOPO TA cloning kit with a pCRII-TOPO vector (Invitrogen) and used as templates for antisense probes.…”

Section: Methodsmentioning

confidence: 99%

Mutations in zebrafish pitx2 model congenital malformations in Axenfeld-Rieger syndrome but do not disrupt left-right placement of visceral organs

Buel

Amack

2016

Developmental Biology

Self Cite

View full text Add to dashboard Cite

Pitx2 is a conserved homeodomain transcription factor that has multiple functions during embryonic development. Mutations in human PITX2 cause autosomal dominant Axenfeld-Rieger syndrome (ARS), characterized by congenital eye and tooth malformations. Pitx2−/− knockout mouse models recapitulate aspects of ARS, but are embryonic lethal. To date, ARS treatments remain limited to managing individual symptoms due to an incomplete understanding of PITX2 function. In addition to regulating eye and tooth development, Pitx2 is a target of a conserved Nodal (TGFβ) signaling pathway that mediates left-right (LR) asymmetry of visceral organs. Based on its highly conserved asymmetric expression domain, the Nodal-Pitx2 axis has long been considered a common denominator of LR development in vertebrate embryos. However, functions of Pitx2 during asymmetric organ morphogenesis are not well understood. To gain new insight into Pitx2 function we used genome editing to create mutations in the zebrafish pitx2 gene. Mutations in the pitx2 homeodomain caused phenotypes reminiscent of ARS, including aberrant development of the cornea and anterior chamber of the eye and reduced or absent teeth. Intriguingly, LR asymmetric looping of the heart and gut was normal in pitx2 mutants. These results suggest conserved roles for Pitx2 in eye and tooth development and indicate Pitx2 is not required for asymmetric looping of zebrafish visceral organs. This work establishes zebrafish pitx2 mutants as a new animal model for investigating mechanisms underlying congenital malformations in ARS and high-throughput drug screening for ARS therapeutics. Additionally, pitx2 mutants present a unique opportunity to identify new genes involved in vertebrate LR patterning. We show Nodal signaling—independent of Pitx2—controls asymmetric expression of the fatty acid elongase elovl6 in zebrafish, pointing to a potential novel pathway during LR organogenesis.

show abstract

Lethal giant larvae 2 regulates development of the ciliated organ Kupffer’s vesicle

Cited by 26 publications

References 67 publications

Functional characterization of Prickle2 and BBS7 identify overlapping phenotypes yet distinct mechanisms

Functional characterization of Prickle2 and BBS7 identify overlapping phenotypes yet distinct mechanisms

509 Tumor suppression in basal keratinocytes via dual non-cell-autonomous functions of a Na,K-ATPase beta subunit

Mutations in zebrafish pitx2 model congenital malformations in Axenfeld-Rieger syndrome but do not disrupt left-right placement of visceral organs

Contact Info

Product

Resources

About