Absence of Basement Membranes after Targeting the <i>LAMC1</i> Gene Results in Embryonic Lethality Due to Failure of Endoderm Differentiation

Smyth, Neil; Vatansever, Hafize Seda; Murray, Patricia; Meyer, Michaël; Frie, Christian; Paulsson, Mats; Edgar, David

doi:10.1083/jcb.144.1.151

Cited by 482 publications

(417 citation statements)

References 53 publications

Supporting

Mentioning

390

Contrasting

Unclassified

Order By: Relevance

“…Dab2 is a PTB domain containing adaptor protein that modulates cellular adhesiveness during megakaryocytic differentiation of the human chronic myeloid leukemic cell line K562 (Tseng et al, 2003) and transiently interacts with Integrin ␤1 to regulate its activation during induced epithelial to mesenchymal transition in normal murine mammary gland cells (Prunier and Howe, 2005). Moreover, mutation of LamC1 and Integrin␤1, genes known to modulate cell adhesiveness, causes similar phenotypes (Stephens et al, 1995;Smyth et al, 1999). These genes thus represent excellent candidates for regulating cell sorting since PE lineage progenitors form but do not segregate to the surface of the ICM in these mutants.…”

Section: Molecular Regulation Of Epi/ Pe Lineage Formationmentioning

confidence: 99%

Cell and molecular regulation of the mouse blastocyst

Yamanaka

Ralston

Stephenson

et al. 2006

Developmental Dynamics

264

221

View full text Add to dashboard Cite

Animals use diverse strategies to specify tissue lineages during development. A common strategy is to partition maternally supplied and localized lineage determinants into progenitor cells. The mouse embryo appears to use a different, more regulative strategy to specify the first three lineages: the epiblast (EPI: future embryo), the trophectoderm (TE: future placenta), and the primitive endoderm (PE: future yolk sac). These lineages are specified during two successive differentiation steps leading to formation of the blastocyst. Here, we review classic and contemporary models of early lineage specification in the mouse, and describe recent efforts to understand the molecular regulation of these events. We describe evidence that trophectoderm differentiation bears resemblance to the process of epithelialization and describe the importance of apical/basal protein complexes in regulating this process. Next, we present a revised model of PE specification, and describe evidence that PE cells in the inner cell mass sort out to occupy their ultimate position on the surface of the EPI. Finally, we describe factors that reinforce these lineages and three distinct stem cell types that can be isolated from them. Together, these mechanisms guide the differentiation of the first lineages of the mouse and thereby set up tissues that will be important for the first steps of embryonic body patterning. Developmental Dynamics 235:2301-2314, 2006.

show abstract

Section: Molecular Regulation Of Epi/ Pe Lineage Formationmentioning

confidence: 99%

Cell and molecular regulation of the mouse blastocyst

Yamanaka

Ralston

Stephenson

et al. 2006

Developmental Dynamics

264

221

View full text Add to dashboard Cite

show abstract

“…(Costell et al, 1999) Tenascin C Extracellular matrix Total NC cells fail to disperse laterally (Tucker, 2001) Laminin γ1 Extracellular matrix Total Death at E5.5, lack of basement membranes (Smyth et al, 1999) Laminin β2 Extracellular matrix Total Postnatal death between P15-30, neuromuscular junctions and glomerular defects (Noakes et al, 1995a;Noakes et al, 1995b;Patton et al, 1997) Laminin α2 Extracellular matrix Total Death by 5 weeks postnatal, severe muscular dystrophy and peripheral neurophathy (Miyagoe et al, 1997) Laminin α2 (dy/dy) Extracellular matrix Spontaneous Adult lethality, severe muscular dystrophy and peripheral nerve dysmyelination (Patton et al, 1999;Patton et al, 1997) Laminin α3 Extracellular matrix Total Death at P2-3, epithelial adhesion defect (Ryan et al, 1999) Laminin α4 Extracellular matrix Total Transient microvascular defect with hemorrhages and misalignment of neuromuscular junctions (Patton et al, 2001;Thyboll et al, 2002) Laminin α5 Extracellular matrix Total Death at E14-E17, with placental vessel, neural (Miner et al, 1998;Miner and Li, 2000) Protein Function Type Phenotype Reference tube, limb, and kidney defects Fibronectin Extracellular matrix Total Death before E14.5, shortened anterior-posterior axes, deformed neural tubes, and defects in mesodermally derived tissues. (George et al, 1993) Collagen XVIII Extracellular matrix Total Eye abnormalities modeling Knoblock syndrome (Fukai et al, 2002) Extracellular matrix Total Basement membrane defects (Utriainen et al, 2004) Collagen XV Extracellular matrix Total Skeletal myopathy and cardiovascular defects (Eklund et al, 2001) betaglycan Extracellular matrix Total Embryonic lethality of heart and liver defects (Stenvers et al, 2003) Connexin 43 Cell-cell adhesion In vitro studies of cells from knockout mice…”

Section: Note On Nomenclaturementioning

confidence: 99%

Cell biology of embryonic migration

Kurosaka¹,

Kashina²

2008

Birth Defects Research Pt C

113

View full text Add to dashboard Cite

Cell migration is an evolutionarily conserved mechanism that underlies the development and functioning of uni-and multicellular organisms and takes place in normal and pathogenic processes, including various events of embryogenesis, wound healing, immune response, cancer metastases, and angiogenesis. Despite the differences in the cell types that take part in different migratory events, it is believed that all of these migrations occur by similar molecular mechanisms, whose major components have been functionally conserved in evolution and whose perturbation leads to severe developmental defects. These mechanisms involve intricate cytoskeleton-based molecular machines that can sense the environment, respond to signals, and modulate the entire cell behavior. A big question that has concerned the researchers for decades relates to the coordination of cell migration in situ and its relation to the intracellular aspects of the cell migratory mechanisms. Traditionally, this question has been addressed by researchers that considered the intra-and extracellular mechanisms driving migration in separate sets of studies. As more data accumulate researchers are now able to integrate all of the available information and consider the intracellular mechanisms of cell migration in the context of the developing organisms that contain additional levels of complexity provided by extracellular regulation. This review provides a broad summary of the existing and emerging data in the cell and developmental biology fields regarding cell migration during development.

show abstract

“…They are formed by the combination of three chains, a, b, and g (Durbeej, 2010). Several laminins are essential for embryogenesis and their assembly is the first step of basement membrane formation and also a prerequisite for the incorporation of the other basement membrane components (Smyth et al, 1999;Miner and Yurchenco, 2004;Yurchenco and Patton, 2009;Durbeej, 2010). Laminin 111 and 511 are part of the basement membrane of the epithelial somites, dermomyotome, and myotome (Bajanca et al, 2006;Anderson et al, 2009;Thorsteinsdóttir et al, 2011).…”

Section: Introductionmentioning

confidence: 99%

Extracellular matrix remodeling accompanies axial muscle development and morphogenesis in the mouse

Deries

Gonçalves

Vaz

et al. 2011

Developmental Dynamics

View full text Add to dashboard Cite

Background: Skeletal myogenesis is extensively influenced by the surrounding environment. However, how the extracellular matrix (ECM) affects morphogenesis of muscles is not well understood. Results: We mapped the three-dimensional (3D) organization of fibronectin, tenascin, and laminin by immunofluorescence during early epaxial myogenesis in mouse embryos. We define four stages of dermomyotome/myotome development and reveal the 3D organization of myogenic cells within their ECM during those stages. Fibronectin is abundant in all interstitial tissues, while tenascin is restricted to intersegmental borders. Bundles of fibronectin and tenascin also penetrate into the myotome, possibly promoting myocyte alignment. A laminin matrix delineates the dermomyotome and myotome and undergoes dynamic changes, correlating with key developmental events. Conclusion: Our observations cast new light on how myotomal cells interact with their environment and suggest that, as the segmented myotomes transform into the epaxial muscle masses, the laminin matrix disassembles and myocytes use the abundant fibronectin matrix to reach their final organization. Developmental Dynamics 241:350-364,

show abstract

Absence of Basement Membranes after Targeting the LAMC1 Gene Results in Embryonic Lethality Due to Failure of Endoderm Differentiation

Cited by 482 publications

References 53 publications

Cell and molecular regulation of the mouse blastocyst

Cell and molecular regulation of the mouse blastocyst

Cell biology of embryonic migration

Extracellular matrix remodeling accompanies axial muscle development and morphogenesis in the mouse

Contact Info

Product

Resources

About