Role of Wnt5a and Possible Pathway of Action Through Ror2 in Proximodistal Outgrowth of the Limb

Dahl, Tiffanie M.

11 March 2011

Despite over 60 years of study, the molecular pathways and mechanisms governing limb outgrowth and patterning remain poorly understood. Fgfs expressed in the AER are known to be necessary and sufficient for proximodistal limb outgrowth and have been proposed to have a chemoattractive role. Wnt5a is a secreted factor which is expressed in a gradient in the distal limb with the highest concentration next to the AER. The presence of the AER is necessary to establish this gradient. Expression of Wnt5a in a concentration dependant manner can be induced in the limb through the implantation of a bead soaked in recombinant Fgf4 protein. This indicates that Fgfs from the AER may establish the gradient of Wnt5a in the limb mesenchyme. Wnt5a-/- mutants exhibit severe shortening of the face, limbs, and body axis, with limbs being progressively truncated proximally to distally. In normal limb proximodistal outgrowth, cells are seen to grow directionally toward the AER. Previous studies done in the Barrow lab, as well as those done by myself, have shown that if a portion of the AER is removed and the cells proximal to this area are labeled, those which are close enough to intact AER will redirect their growth toward this intact AER. When Wnt5a secreting cells are implanted in the limb mesenchyme of the chick this ectopic source of Wnt5a is sufficient to redirect the growth of the mesenchyme cells toward the Wnt5a source. This indicates that the AER may mediate directed growth of limb mesenchyme cells through the establishment of the Wnt5a gradient which provides positional information to the cells. This Wnt5a gradient results in the recruitment of the mesenchyme cells toward the AER. The Ror2 receptor has been found to be involved in several different pathways involving Wnt5a which are involved in changes in polarity and migration. This makes Ror2 a likely candidate for causing changes in cell polarity and migration during distal outgrowth in the limb. To test whether Ror2 is necessary for the polarizing response of limb mesenchyme cells to the Wnt5a gradient in vivo I co-transfected a dominant-negative Ror2 (Ror2ΔC) and a GFP expression vector in the embryonic chick limb using sonoporation. Limb mesenchyme cells transfected with dominant-negative Ror2 grew as radial clones in contrast to the directional outgrowth of the control limb mesenchyme cells along the proximodistal axis. This indicates that cells expressing the dominant-negative Ror2 could no longer respond to the Wnt5a gradient in the limb mesenchyme. This supports a role for Ror2 as a receptor or co-receptor for Wnt5a in mediating directional growth and movement during proximodistal outgrowth and patterning in the limb.

AER

Fgf

Wnt5a gradient

Ror2

DiI

sonoporation

directional outgrowth

limb mesenchyme

chicken

Cell and Developmental Biology

Physiology

The role of muscle segment homeobox genes in early pregnancy events

Cha, Jeeyeon

25 October 2013

No description available.

Developmental Biology

Msx genes

uterus

embryo implantation

embryonic diapause

delayed implantation

Wnt5a

Applied Molecular Recognition of HECA-452 and Wnt5a in Pathological Inflammation

Kummitha, China Malakondaiah

16 April 2010

No description available.

Pathology

Molecular Recognition

Sialyl Lewis x

HECA-452

Wnt5a

Sanwich ELISA

q-PCR

Molecular Alterations in Bone Development and Bone Tumorigenesis

Mahoney, Emilia

02 September 2009

No description available.

Molecular Biology

bone

limb development

Gremlin

osteoblasts

protein kinase A

PML protein

beta-catenin

Wnt5a

Untersuchungen zur Rolle von Wnt5a beim Basalzellkarzinom / Analysis of the role of Wnt5a in basal cell carcinoma

Carstens, Per-Ole

27 July 2010

No description available.

610 Medizin, Gesundheit

Medicine

Humane und murine Basalzellkarzinome

Hedgehog/Patched-Signalweg

Wnt5a

Wnt-Signalwege.

Human and murine basal cell carcinoma

Hedgehog/Patched-signalling

Wnt5a

Wnt-pathways.

44.81

44.93

MED 283: Molekularbiologie {Medizin}

Localização dos transcritos dos genes WNT5A e HOXB5 em carcinomas epidermóides de boca através da técnica de hibridização “in situ”. / WNT5A e HOXB5 localization study in oral squamous cell carcinoma with in situ hybridization.

Almeida, Fernanda Campos Sousa de

10 December 2004

São freqüentes alterações em vias de sinalização de genes de desenvolvimento, no que diz respeito ao carcinoma epidermóide de boca (CEB). Vinte e nove casos de CEB e tecido não tumoral adjacente à neoplasia foram investigados através da técnica de hibridização “in situ". Os transcritos dos genes WNT5A e HOXB5 foram observados em todos os casos de tumor. A hibridização “in situ" revelou que o WNT5A estava mais expresso em tumores bem diferenciados. Adicionalmente, observou-se transcritos do WNT5A em glândulas salivares menores, estroma glandular, estroma tumoral e alguns vasos sanguíneos Entretanto, com respeito ao HOXB5 não foi possível estabelecer mudança do padrão do transcrito nos diferentes graus histológicos nas amostras de CEB. O HOXB5 também pôde ser identificado em alguns fragmentos de glândulas salivares menores, tecido muscular e em endotélio. Os resultados do presente estudo sugerem que a expressão dos genes WNT5A e HOXB5 podem estar relacionadas com a diferenciação e progressão do câncer de boca. / Disruption in developmental genes pathway are common in oral squamous cell carcinoma (OSCC). This study investigated the pattern of expression of two developmental genes, WNT5A and HOXB5, in 29 cases of OSCC and adjacent non tumoural tissue using in situ hybridization technique. Transcripts for WNT5A and HOXB5 were detected in all tumoral samples. In situ hybridization technique demonstrated that WNT5A transcripts were mainly detected in well differentiated tumors when compared with moderately and undifferentiated OSCC. WNT5A transcripts were also observed in accessory salivary glands, glandular stroma, and vessels. Therefore, for the HOXB5 transcript it was not possible to stability a relationship with the tumoral histological grade. The expression of HOXB5 transcripts in non tumoral samples was detected in salivary glands, glandular stroma, endothelium, and muscle. Results suggest that WNT5A and HOXB5 genes play a possible role in tumor differentiation and cancer progression.

câncer de boca

carcinoma epidermóide

hibridização

homeobox

HOXB5

oral cancer

RT-PCR

Squamous cell carcinoma

WNT5A – RT-PCR- In situ hybridization

Regulation of lymphangiogenesis by WNT siganlling: Focus on WNT5A

Lutze, Grit

08 January 2019

No description available.

610

Wnt5a

Wnt

Wnt siganlling

lymphangiogenesis

Medizin (PPN619874732)

Biologie (PPN619875151)

Localização dos transcritos dos genes WNT5A e HOXB5 em carcinomas epidermóides de boca através da técnica de hibridização “in situ”. / WNT5A e HOXB5 localization study in oral squamous cell carcinoma with in situ hybridization.

Fernanda Campos Sousa de Almeida

10 December 2004

São freqüentes alterações em vias de sinalização de genes de desenvolvimento, no que diz respeito ao carcinoma epidermóide de boca (CEB). Vinte e nove casos de CEB e tecido não tumoral adjacente à neoplasia foram investigados através da técnica de hibridização “in situ”. Os transcritos dos genes WNT5A e HOXB5 foram observados em todos os casos de tumor. A hibridização “in situ” revelou que o WNT5A estava mais expresso em tumores bem diferenciados. Adicionalmente, observou-se transcritos do WNT5A em glândulas salivares menores, estroma glandular, estroma tumoral e alguns vasos sanguíneos Entretanto, com respeito ao HOXB5 não foi possível estabelecer mudança do padrão do transcrito nos diferentes graus histológicos nas amostras de CEB. O HOXB5 também pôde ser identificado em alguns fragmentos de glândulas salivares menores, tecido muscular e em endotélio. Os resultados do presente estudo sugerem que a expressão dos genes WNT5A e HOXB5 podem estar relacionadas com a diferenciação e progressão do câncer de boca. / Disruption in developmental genes pathway are common in oral squamous cell carcinoma (OSCC). This study investigated the pattern of expression of two developmental genes, WNT5A and HOXB5, in 29 cases of OSCC and adjacent non tumoural tissue using in situ hybridization technique. Transcripts for WNT5A and HOXB5 were detected in all tumoral samples. In situ hybridization technique demonstrated that WNT5A transcripts were mainly detected in well differentiated tumors when compared with moderately and undifferentiated OSCC. WNT5A transcripts were also observed in accessory salivary glands, glandular stroma, and vessels. Therefore, for the HOXB5 transcript it was not possible to stability a relationship with the tumoral histological grade. The expression of HOXB5 transcripts in non tumoral samples was detected in salivary glands, glandular stroma, endothelium, and muscle. Results suggest that WNT5A and HOXB5 genes play a possible role in tumor differentiation and cancer progression.

câncer de boca

carcinoma epidermóide

hibridização

RT-PCR

homeobox

HOXB5

oral cancer

Squamous cell carcinoma

WNT5A – RT-PCR- In situ hybridization

Understanding and Exploiting Wnt5a and GSK3 Signaling in Inflammatory Disease

Bhatt, Pooja

07 June 2013

No description available.

Biomedical Research

Cellular Biology

Molecular Biology

Atherosclerosis

Wnt5a

Alzheimer's disease

inflammation

GSK3

cytokines

beta catenin

inflammatory diseases

Molecular and Cellular Mechanisms Whereby the Apical Ectodermal Ridge (AER), Via Wnt5a, Mediates Directional Migration of the Adjacent Mesenchyme During Vertebrate Limb Development

Kmetzsch, Kate E.

07 August 2009

The vertebrate embryonic limb is a key model in elucidating the genetic basis underlying the three dimensional morphogenesis of structures. Despite the wealth of insights that have been generated from this model, many long-standing questions remain. For example, it has been known for over 70 years that the apical ectodermal ridge (AER) of the embryonic limb is essential for distal outgrowth and patterning of the adjacent limb mesenchyme. The mechanisms whereby the AER does accomplish outgrowth and patterning are still poorly understood. We propose that secreted FGFs from the AER activate Wnt5a expression in gradient fashion, which in turn provides an instructional cue to direct outgrowth in the direction of increasing Wnt5a expression (i.e. toward the distal tip of the limb). In vivo and in vitro models were used to test this hypothesis. We placed Wnt5a expressing L-cell implants into stage 23 chick limb buds and demonstrate that labeled mesenchyme cells grow toward the source of Wnt5a. Purified Wnt5a soaked heparin bead implants have only a marginal effect on directed growth of the adjacent mesenchyme, whereas a greater effect was seen with beads soaked in Wnt5a conditioned media. Using an in vitro model where cultured limb mesenchyme cells were subjected to a gradient of conditioned Wnt5a media or purified Wnt5a, we show no specific migratory direction. However, clusters of cells tended to move toward the source of Wnt5a indicating that it might be necessary for the cells to be in complete contact to respond to the Wnt5a signal. Taken together, our results suggest that Wnt5a is sufficient to direct limb mesenchyme. This finding has given support to a new model of limb development proposed by our lab and referred to as the Mesenchyme Recruitment Model.

limb development

apical ectodermal ridge (AER)

Wnt5a

cell migration

Dunn chamber

mesenchyme

chick embryo

Cell and Developmental Biology

Physiology