2012
DOI: 10.4049/jimmunol.1102425
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Strain-Dependent Airway Hyperresponsiveness and a Chromosome 7 Locus of Elevated Lymphocyte Numbers in Cystic Fibrosis Transmembrane Conductance Regulator-Deficient Mice

Abstract: We previously observed the lungs of naive BALB/cJ Cftrtm1UNC mice to have greater numbers of lymphocytes, by immunohistochemical staining, than did BALB wild type littermates or C57BL/6J Cftrtm1UNC mice. In the present study, we initially investigated whether this mutation in Cftr alters the adaptive immunity phenotype by measuring the lymphocyte populations in the lungs and spleens by FACS and by evaluating CD3-stimulated cytokine secretion, proliferation, and apoptosis responses. Next, we assessed a potentia… Show more

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Cited by 6 publications
(11 citation statements)
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“…We assumed that a dysfunction in the transcriptional or posttranscriptional controlling mechanisms could partly explain the discrepancies between the IHC and SISH results; still we wanted to explore other genes located on chromosome 7. Chromosome 7 is known to harbor genes whose alteration my play an important role in multiple diseases as cystic fibrosis[27], but also in tumorigenesis [28]with over than 1150 protein- coding genes, 605 of which have been validated by transcript sequences. [29] Nevertheless, three genes; EGFR , MET , and BRAF emerge as of special interest in NSCLC.…”
Section: Discussionmentioning
confidence: 99%
“…We assumed that a dysfunction in the transcriptional or posttranscriptional controlling mechanisms could partly explain the discrepancies between the IHC and SISH results; still we wanted to explore other genes located on chromosome 7. Chromosome 7 is known to harbor genes whose alteration my play an important role in multiple diseases as cystic fibrosis[27], but also in tumorigenesis [28]with over than 1150 protein- coding genes, 605 of which have been validated by transcript sequences. [29] Nevertheless, three genes; EGFR , MET , and BRAF emerge as of special interest in NSCLC.…”
Section: Discussionmentioning
confidence: 99%
“…These mice were bred together to produce Cftr tm1Eur mice and wild-type Cftr +/+ controls and were genotyped as previously described (Paradis et al 2010), Cftr +/tm1UNC heterozygous mice on either C57BL/6 or BALB/c background were used to generate knockout ( Cftr tm1UNC ) mice as previously described (Bazett et al 2012; Haston et al 2006). All mice were bred and maintained at the Meakins-Christie Laboratories of McGill University.…”
Section: Methodsmentioning
confidence: 99%
“…All mice were bred and maintained at the Meakins-Christie Laboratories of McGill University. To circumvent possible premature death due to intestinal disease, all mice (CF and WT) were fed standard chow and received PEGLYTE ® (17.8 mmol/L polyethylene glycol, Pharma Science, DIN:00777838) in their drinking water as described previously (Bazett et al 2012; Clarke et al 1996; Haston et al 2006; Paradis et al 2010). Mice were weaned at 3 weeks of age and grouped in ventilated cages of 1–3 mice based on their sex.…”
Section: Methodsmentioning
confidence: 99%
“…The CF traits of airway hyperresponsiveness, bone disease and intestinal disease are reflected in mice deficient for Cftr. Specifically, BALB/c Cftr tm1UNC mice, which harbour a null mutation in Cftr , present with an airway hyperresponsive phenotype compared to the lung response of wild-type littermates 17 , as do FVB/N Cftr tm1Eur mice which have the clinically prevalent delF508-Cftr mutation 18 . The airway hyperresponsive phenotype of these CF mouse models occurs in the absence of observable airway remodelling as indicated by a lack of goblet cell hyperplasia or of increased α-smooth muscle actin 17 18 .…”
mentioning
confidence: 99%
“…Specifically, BALB/c Cftr tm1UNC mice, which harbour a null mutation in Cftr , present with an airway hyperresponsive phenotype compared to the lung response of wild-type littermates 17 , as do FVB/N Cftr tm1Eur mice which have the clinically prevalent delF508-Cftr mutation 18 . The airway hyperresponsive phenotype of these CF mouse models occurs in the absence of observable airway remodelling as indicated by a lack of goblet cell hyperplasia or of increased α-smooth muscle actin 17 18 . BALB/c Cftr tm1UNC mice also develop a bone disease that resembles the clinical phenotype in terms of reduced bone mineral density and an altered bone structure 15 19 and intestinal disease has been documented in the majority of CF mouse models 20 , including BALB/c Cftr tm1UNC mice 21 22 23 .…”
mentioning
confidence: 99%