Mouse models for identifying genes modulating fertility parameters

Laissue, Paul; L’Hôte, David; Serres, Catherine; Vaiman, Daniel

doi:10.1017/s1751731108003315

Cited by 7 publications

(5 citation statements)

References 97 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Here, we are concerned with the maximum stress, s, on the stressstrain curve, stiffness (E ), strain (e) at s, strain energy densities up to e (u) and from e until complete rupture (u p ) (Goh et al, 2005). Since the genome of the C57BL6 mouse has been sequenced, it has been regarded as an ideal murine model in the context of integrative biology study; it is widely used for laboratory experiments to illuminate basic mechanisms that could address similar outcomes in other mammals (Laissue et al, 2009). In particular, tissues from the murine model have been used extensively to evaluate biomechanical properties to study systemic changes caused by injury and during healing (Lin et al, 2004), ageing of ECM (Goh et al, 2008) and disruption of the signal pathway for regulating ECM in genetically engineered mice that produced alterations in collagen (Derwin and Soslowsky, 1999) and PGs (Derwin and Soslowsky, 1999).…”

Section: Introductionmentioning

confidence: 99%

Effects of frozen storage temperature on the elasticity of tendons from a small murine model

Goh

Chen²,

Chou³

et al. 2010

Animal

View full text Add to dashboard Cite

The basic mechanism of reinforcement in tendons addresses the transfer of stress, generated by the deforming proteoglycan (PG)-rich matrix, to the collagen fibrils. Regulating this mechanism involves the interactions of PGs on the fibril with those in the surrounding matrix and between PGs on adjacent fibrils. This understanding is key to establishing new insights on the biomechanics of tendon in various research domains. However, the experimental designs in many studies often involved long sample preparation time. To minimise biological degradation the tendons are usually stored by freezing. Here, we have investigated the effects of commonly used frozen storage temperatures on the mechanical properties of tendons from the tail of a murine model (C57BL6 mouse). Fresh (unfrozen) and thawed samples, frozen at temperatures of 2208C and 2808C, respectively, were stretched to rupture. Freezing at 2208C revealed no effect on the maximum stress (s), stiffness ( E), the corresponding strain (e) at s and strain energy densities up to e (u) and from e until complete rupture (u p ). On the other hand, freezing at 2808C led to higher s, E and u; e and u p were unaffected. The results implicate changes in the long-range order of radially packed collagen molecules in fibrils, resulting in fibril rupture at higher stresses, and changes to the composition of extrafibrillar matrix, resulting in an increase in the interaction energy between fibrils via collagen-bound PGs.Keywords: frozen storage temperature, strength, stiffness, strain energy, collagen Implications Ultra-low storage temperature alters (i) the long-range order of collagen packing in fibrils, resulting in fibril rupture at higher stresses, and (ii) the composition of extra-fibrillar matrix, resulting in an increase in the interaction energy between fibrils via collagen-bound proteoglycans. Consequently, the tissue strength, stiffness and fracture toughness increase.

show abstract

Section: Introductionmentioning

confidence: 99%

Effects of frozen storage temperature on the elasticity of tendons from a small murine model

Goh

Chen²,

Chou³

et al. 2010

Animal

View full text Add to dashboard Cite

show abstract

“…Briefly, the IRCS model was created from an initial cross between two evolutionarily distant parental species of mice (Mus musculus and Mus spretus), followed by two backcrosses involving Mus musculus which reduced the percentage donor (M. spretus) genome introgressed into the receptor's genetic background (Mus musculus) [137,139,140]. Consanguineous (brother-sister) crosses were then performed during > 30 generations to establish 53 IRCS strains, each having an average of 98% M. musculus and 2% M. spretus genomes (fixed at homozygous state).…”

Section: Foxd1 In Mammalian Implantation and Recurrent Pregnancy Lossmentioning

confidence: 99%

The multisystemic functions of FOXD1 in development and disease

Quintero-Ronderos

Laissue

2018

J Mol Med

View full text Add to dashboard Cite

Transcription factors (TFs) participate in a wide range of cellular processes due to their inherent function as essential regulatory proteins. Their dysfunction has been linked to numerous human diseases. The forkhead box (FOX) family of TFs belongs to the "winged helix" superfamily, consisting of proteins sharing a related winged helix-turn-helix DNA-binding motif. FOX genes have been extensively present during vertebrates and invertebrates' evolution, participating in numerous molecular cascades and biological functions, such as embryonic development and organogenesis, cell cycle regulation, metabolism control, stem cell niche maintenance, signal transduction, and many others. FOXD1, a forkhead TF, has been related to different key biological processes such as kidney and retina development and embryo implantation. FOXD1 dysfunction has been linked to different pathologies, thereby constituting a diagnostic biomarker and a promising target for future therapies. This paper aims to present, for the first time, a comprehensive review of FOXD1's role in mouse development and human disease. Molecular, structural, and functional aspects of FOXD1 are presented in light of physiological and pathogenic conditions, including its role in human disease aetiology, such as cancer and recurrent pregnancy loss. Taken together, the information given here should enable a better understanding of FOXD1 function for basic science researchers and clinicians.

show abstract

“…It is worth noting that QTL can be defined as chromosomal regions carrying genes (encoding and regulatory regions) which are responsible for complex, measurable phenotypes. The latter assumption was explored by studying particular mouse models allowing QTL mapping (Laissue et al, 2009b). The interspecific recombinant congenic strains (IRCS) model has been especially useful for mapping short QTL responsible for male (testis and prostate weight, sperm nucleus shape, sperm survival) and female phenotypes (embryonic lethality and resorption) (Laissue et al, 2009c;L'Hôte et al, 2007;Vatin et al, 2012).…”

Section: The Polygenic Nature Of Reproduction and Pofmentioning

confidence: 99%

Aetiological coding sequence variants in non-syndromic premature ovarian failure: From genetic linkage analysis to next generation sequencing

Laissue

2015

Molecular and Cellular Endocrinology

View full text Add to dashboard Cite

Premature ovarian failure (POF) is a frequent pathology affecting 1-1.5% of women under 40 years old. Despite advances in diagnosing and treating human infertility, POF is still classified as being idiopathic in 50-80% of cases, strongly suggesting a genetic origin for the disease. Different types of autosomal and X-linked genetic anomalies can originate the phenotype in syndromic and non-syndromic POF cases. Particular interest has been focused on research into non-syndromic POF causative coding variants during the past two decades. This has been based on the assumption that amino acid substitutions might modify the intrinsic physicochemical properties of functional proteins, thereby inducing pathological phenotypes. In this case, a restricted number of mutations might originate the disease. However, like other complex pathologies, POF might result from synergistic/compensatory effects caused by several low-to-mildly drastic mutations which have frequently been classified as non-functional SNPs. Indeed, reproductive phenotypes can be considered as quantitative traits resulting from the subtle interaction of many genes. Although numerous sequencing projects have involved candidate genes, only a few coding mutations explaining a low percentage of cases have been described. Such apparent failure to identify aetiological coding sequence variations might have been due to the inherent molecular complexity of mammalian reproduction and to the difficulty of simultaneously analysing large genomic regions by Sanger sequencing. The purpose of this review is to present the molecular and cellular effects caused by non-synonymous mutations which have been formally associated, by functional tests, with the aetiology of hypergonadotropic non-syndromic POF. Considerations have also been included regarding the polygenic nature of reproduction and POF, as well as future approaches for identifying novel aetiological genes based on next generation sequencing (NGS).

show abstract

Mouse models for identifying genes modulating fertility parameters

Cited by 7 publications

References 97 publications

Effects of frozen storage temperature on the elasticity of tendons from a small murine model

Effects of frozen storage temperature on the elasticity of tendons from a small murine model

The multisystemic functions of FOXD1 in development and disease

Aetiological coding sequence variants in non-syndromic premature ovarian failure: From genetic linkage analysis to next generation sequencing

Contact Info

Product

Resources

About