Cartilage link protein 1 (Crtl1), an extracellular matrix component playing an important role in heart development

Wirrig, Elaine E.; Snarr, Brian S.; Chintalapudi, Mastan R.; O'Neal, Jessica; Phelps, Aimee L.; Barth, Jeremy L.; Fresco, Victor M.; Kern, Christine B.; Mjaatvedt, Corey H.; Toole, Bryan P.; Hoffman, Stanley; Trusk, Thomas C.; Argraves, W. Scott; Wessels, Andy

doi:10.1016/j.ydbio.2007.07.041

Cited by 77 publications

(102 citation statements)

References 64 publications

(98 reference statements)

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“…For example, individuals with Down syndrome (Trisomy 21) have remarkably similar types of AVSD that are associated with defects in DMP expansion (Blom et al, 2003). AVSD is also observed in the Ts16 Down syndrome mouse model, in which the DMP is deficient (Webb et al, 1999;Snarr et al, 2007). Here, we demonstrate that AVSD can be the direct result of defective DMP development in mice.…”

Section: Mef2c-ahf-cre; Smosupporting

confidence: 52%

“…However, new findings suggest that AVSDs seen in perinatal humans are more complex in their origins. Previous work has demonstrated that deficient DMP development occurs in mouse (Webb et al, 1999;Snarr et al, 2007b;Wirrig et al, 2007) and human (Blom et al, 2003) fetuses with AVSD. As such individuals exhibit malformations in other septal structures, the specific role of DMP defects in generating these malformations has been unclear.…”

Section: Discussionmentioning

confidence: 99%

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Intracardiac septation requires hedgehog-dependent cellular contributions from outside the heart

et al. 2008

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Septation of the mammalian heart into four chambers requires the orchestration of multiple tissue progenitors. Abnormalities in this process can result in potentially fatal atrioventricular septation defects (AVSD). The contribution of extracardiac cells to atrial septation has recently been recognized. Here, we use a genetic marker and novel magnetic resonance microscopy techniques to demonstrate the origins of the dorsal mesenchymal protrusion in the dorsal mesocardium, and its substantial contribution to atrioventricular septation. We explore the functional significance of this tissue to atrioventricular septation through study of the previously uncharacterized AVSD phenotype of Shh -/-mutant mouse embryos. We demonstrate that Shh signaling is required within the dorsal mesocardium for its contribution to the atria. Failure of this addition results in severe AVSD. These studies demonstrate that AVSD can result from a primary defect in dorsal mesocardium, providing a new paradigm for the understanding of human AVSD.

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Section: Mef2c-ahf-cre; Smosupporting

confidence: 52%

Section: Discussionmentioning

confidence: 99%

Intracardiac septation requires hedgehog-dependent cellular contributions from outside the heart

et al. 2008

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“…11 Thus, as we continued to gain more insight into the matter we opted to use this terminology. 7,12 We acknowledge, however, that "atrial spine", "vestibular spine", and "spina vestibuli" are also commonly, and legitimately, used in other articles to describe this mesenchymal population.…”

Section: Resultsmentioning

confidence: 99%

Isl1 Expression at the Venous Pole Identifies a Novel Role for the Second Heart Field in Cardiac Development

Snarr

O'Neal

Chintalapudi

et al. 2007

Circulation Research

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134

140

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The right ventricle and outflow tract of the developing heart are derived from mesodermal progenitor cells from the second heart field (SHF). SHF cells have been characterized by expression of the transcription factor Islet-1 (Isl1). Although Isl1 expression has also been reported in the venous pole, the specific contribution of the SHF to this part of the heart is unknown. Here we show that Isl1 is strongly expressed in the dorsal mesenchymal protrusion (DMP), a non-endocardially-derived mesenchymal structure involved in atrioventricular septation. We further demonstrate that abnormal development of the SHF-derived DMP is associated with the pathogenesis of atrioventricular septal defects. These results identify a novel role for the SHF. (Circ Res. 2007;101:971-974.)

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“…In addition to tissue colocalization, studies using recombinant proteins have demonstrated the molecular interactions of Crtl1/ Hapln1 in the formation of other proteoglycan aggregates, versican and neurocan (Matsumoto et al, 2003;Shi et al, 2004;Rauch et al, 2004). Although expression of Crtl1/ Hapln1 was reported in several developing tissues (Binette et al, 1994;Deak et al, 1999;Wirrig et al, 2007, Shibata et al, 2003, Colas and Schoenwolf, 2003, a detailed embryonic expression analysis is required for understanding its biological roles. Furthermore, cross-species comparison of Crtl1/Halpn1 would shed light on the evolutionary conservation and/or diversity of the structure and function, though such study has not yet been performed.…”

Section: Introductionmentioning

confidence: 99%

Molecular Cloning and Developmental Expression of a Hyaluronan and Proteoglycan Link Protein Gene,crtl1/hapln1, in Zebrafish

Kang¹,

Kawakami²,

Bekku³

et al. 2008

Zoological Science

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The proteoglycan aggregate of the cartilage is composed of aggrecan, link protein (LP), and hyaluronan, providing resistance to compression in joints and cartilage structures. To further understand the function of LP during the process of chondrogenesis and bone formation in zebrafish, we cloned the zebrafish cDNA for hyaluronan and proteoglycan link protein 1 (crtl1/hapln1) and examined the expression of the gene during embryogenesis using in-situ hybridization. crtl1/hapln1 expression is first observed in the adaxial cells at the bud- stage. Throughout somitogenesis, crtl1/hapln1 is expressed in the sclerotomes, floor plate, and hypochord. In addition, crtl1/hapln1 is expressed in rhombomeres 3 and 5, pharyngeal arches, telecephalon, otic vesicles, and pectral fins. During chondrocranial/skull formation, crtl1/hapln1 expression is highest at around 4 dpf and is colocalized with aggrecan in the cartilaginous arches and with dermacan in the dermal bones.

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Cartilage link protein 1 (Crtl1), an extracellular matrix component playing an important role in heart development

Cited by 77 publications

References 64 publications

Intracardiac septation requires hedgehog-dependent cellular contributions from outside the heart

Intracardiac septation requires hedgehog-dependent cellular contributions from outside the heart

Isl1 Expression at the Venous Pole Identifies a Novel Role for the Second Heart Field in Cardiac Development

Molecular Cloning and Developmental Expression of a Hyaluronan and Proteoglycan Link Protein Gene,crtl1/hapln1, in Zebrafish

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