Differential expression of both extracellular and intracellular proteins is involved in the lethal or nonlethal phenotypic variation of BrtlIV, a murine model for osteogenesis imperfecta

Forlino, Antonella; Tani, Chiara; Rossi, Antonio; Lupi, A.; Campari, Elena; Gualeni, Benedetta; Bianchi, Laura; Armini, Alessandro; Cetta, Giuseppe; Bini, Luca; Marini, Joan C.

doi:10.1002/pmic.200600919

Cited by 51 publications

(60 citation statements)

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“…42 We recently described ER stress in Brtl fibroblast and calvarial bone, as well as in MSCs differentiating toward the osteoblastic lineage. [30][31][32] In the latter case, we showed an increase in HSP47, a specific molecular chaperone known to bind folded type I procollagen molecules in the ER, similar to previous reports in some OI cases. 43 Thus, we evaluated the expression of HSP47 following silencing and found a significant reduction in F-Mut shRNA-transduced Brtl cells, compared with control fibroblasts, as might be expected based on about 40% total collagen suppression.…”

Section: Discussionsupporting

confidence: 90%

“…The expression level of the target gene was normalized to the housekeeping gene Gapdh (Mm99999915_g1, Applied Biosystems) and the relative expression was calculated using the DDCt method. The evaluation of the specific expression of each Col1a1 allele was then performed by means of allele-specific real-time PCR as described in Forlino et al 30 Collagen analysis F-Mut shRNA transduced and parental Brtl fibroblasts were plated (2.5 Â 10 5 /3 cm Petri dishes) and allowed to adhere for 24 h. Collagen synthesis was stimulated by incubating the cells for 24 h before protein recovery with 100 mg/ml sodium ascorbate in DMEM containing 1% FBS. Type I collagen was extracted and purified from media and cell layer as described previously.…”

Section: Rna Isolation and Real-time Allele-specific Pcrmentioning

confidence: 99%

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Allele-specific Col1a1 silencing reduces mutant collagen in fibroblasts from Brtl mouse, a model for classical osteogenesis imperfecta

et al. 2013

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Gene silencing approaches have the potential to become a powerful curative tool for a variety of monogenic diseases caused by gain-of-function mutations. Classical osteogenesis imperfecta (OI), a dominantly inherited bone dysplasia, is characterized in its more severe forms by synthesis of structurally abnormal type I collagen, which exerts a negative effect on extracellular matrix. Specific suppression of the mutant (Mut) allele would convert severe OI forms to the mild type caused by a quantitative defect in normal collagen. Here, we describe the in vitro and ex vivo investigation of a small interfering RNA (siRNA) approach to allele-specific gene silencing using Mut Col1a1 from the Brtl mouse, a well-characterized model for classical human OI. A human embryonic kidney cell line, which expresses the firefly luciferase gene, combined with either wild-type or Mut Brtl Col1a1 exon 23 sequences, was used for the first screening. The siRNAs selected based on their specificity and the corresponding short hairpin RNAs (shRNAs) subcloned in a lentiviral vector were evaluated ex vivo in Brtl fibroblasts for their effect on collagen transcripts and protein. A preferential reduction of the Mut allele of up to 52% was associated with about 40% decrease of the Mut protein, with no alteration of cell proliferation. Interestingly, a downregulation of HSP47, a specific collagen chaperone known to be upregulated in some OI cases, was detected. Our data support further testing of shRNAs and their delivery by lentivirus as a strategy to specifically suppress the Mut allele in mesenchymal stem cells of OI patients for autologous transplantation.

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Section: Discussionsupporting

confidence: 90%

Section: Rna Isolation and Real-time Allele-specific Pcrmentioning

confidence: 99%

Allele-specific Col1a1 silencing reduces mutant collagen in fibroblasts from Brtl mouse, a model for classical osteogenesis imperfecta

et al. 2013

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“…In untreated animals from our colony, BrtlIV pups had a survival rate 2 times lower compared with WT and, at the same age of 2 months, 65.5% were WT and 34.5% were heterozygous BrtlIV, consistent with previous reports. 20,41 The significantly higher (P ϭ .04) proportion of surviving BrtlIV animals in transplanted mice indicated that the treatment rescued the genotype-related lethality in our murine model.…”

Section: Iut Of Total Bone Marrow Cells Into Brtl and Wt Embryosmentioning

confidence: 99%

“…45,46 From the intensities of the ␣1(I)-S-S-␣1(I) and ␣1(I) bands, we estimated the fraction of collagen molecules with 2 mutant chains as 26.7% plus or minus 4.3% in trabecular and 25.7% plus or minus 2.5% in cortical bone from untreated animals, consistent with previous reports. 41,46 In treated animals, this fraction decreased with increasing bone marrow engraftment of donor cells ( Figure 4B). In animals with the highest engraftment (1.9% Ϯ 0.1%), this fraction was 20.4% plus or minus 2.9% in trabecular and 20.9% plus or minus 2.6% in cortical bone (P Ͻ .05; Figure 4 and supplemental Table 2).…”

Section: Collagen Composition In Treated and Untreated Bones From Brtmentioning

confidence: 99%

“…The second dose was added after 3 to 4 days. After 1 week, the reaction was stopped with acetic acid (0.5 M final concentration), and collagen was precipitated by raising the NaCl concentration to approximately 1 M. The precipitated collagen was washed with 70% ethanol, resolubilized in 0.1 M Na-carbonate, 0.5 M NaCl, pH 9.3, fluorescently labeled with Cy5 (Crt Healthcare), 41 and separated on precast, gradient, Tris-acetate minigels (3%-8%; Invitrogen). The gels were scanned on an FLA5000 fluorescence scanner (Fuji Medical Systems) and analyzed with the ScienceLab software supplied by the manufacturer (Fuji Medical Systems).…”

Section: Collagen Analysismentioning

confidence: 99%

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In utero transplantation of adult bone marrow decreases perinatal lethality and rescues the bone phenotype in the knockin murine model for classical, dominant osteogenesis imperfecta

Panaroni

Gioia

Lupi

et al. 2009

Blood

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4-PBA Treatment Improves Bone Phenotypes in the Aga2 Mouse Model of Osteogenesis Imperfecta

Durán

Zieba

Csukasi

et al. 2020

Journal of Bone and Mineral Research

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Osteogenesis imperfecta (OI) is a genetically heterogenous disorder most often due to heterozygosity for mutations in the type I procollagen genes, COL1A1 or COL1A2. The disorder is characterized by bone fragility leading to increased fracture incidence and longbone deformities. Although multiple mechanisms underlie OI, endoplasmic reticulum (ER) stress as a cellular response to defective collagen trafficking is emerging as a contributor to OI pathogenesis. Herein, we used 4-phenylbutiric acid (4-PBA), an established chemical chaperone, to determine if treatment of Aga2 +/À mice, a model for moderately severe OI due to a Col1a1 structural mutation, could attenuate the phenotype. In vitro, Aga2 +/À osteoblasts show increased protein kinase RNA-like endoplasmic reticulum kinase (PERK) activation protein levels, which improved upon treatment with 4-PBA. The in vivo data demonstrate that a postweaning 5-week 4-PBA treatment increased total body length and weight, decreased fracture incidence, increased femoral bone volume fraction (BV/TV), and increased cortical thickness. These findings were associated with in vivo evidence of decreased bone-derived protein levels of the ER stress markers binding immunoglobulin protein (BiP), CCAAT/Àenhancer-binding protein homologous protein (CHOP), and activating transcription factor 4 (ATF4) as well as increased levels of the autophagosome marker light chain 3A/B (LC3A/B). Genetic ablation of CHOP in Aga2 +/À mice resulted in increased severity of the Aga2 +/À phenotype, suggesting that the reduction in CHOP observed in vitro after treatment is a consequence rather than a cause of reduced ER stress. These findings suggest the potential use of chemical chaperones as an adjunct treatment for forms of OI associated with ER stress.

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Differential expression of both extracellular and intracellular proteins is involved in the lethal or nonlethal phenotypic variation of BrtlIV, a murine model for osteogenesis imperfecta

Cited by 51 publications

References 45 publications

Allele-specific Col1a1 silencing reduces mutant collagen in fibroblasts from Brtl mouse, a model for classical osteogenesis imperfecta

Allele-specific Col1a1 silencing reduces mutant collagen in fibroblasts from Brtl mouse, a model for classical osteogenesis imperfecta

In utero transplantation of adult bone marrow decreases perinatal lethality and rescues the bone phenotype in the knockin murine model for classical, dominant osteogenesis imperfecta

4-PBA Treatment Improves Bone Phenotypes in the Aga2 Mouse Model of Osteogenesis Imperfecta

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