Search

Your search keyword '"Lacaze-Masmonteil T"' showing total 211 results
Start Over Author "Lacaze-Masmonteil T"
211 results on '"Lacaze-Masmonteil T"'

1. Doxapram versus placebo in preterm newborns: a study protocol for an international double blinded multicentre randomized controlled trial (DOXA-trial).

Author

Poppe, J.A., Flint, R.B., Smits, A., Willemsen, S.P., Storm, K.K., Nuytemans, D.H., Onland, W., Poley, M.J., Boode, W.P. de, Carkeek, K., Cassart, V., Cornette, L., Dijk, P.H., Hemels, M.A.C., Hermans, I., Hütten, M.C., Kelen, D., Kort, E.H.M. de, Kroon, A.A., Lefevere, J., Plaskie, K., Stewart, B., Voeten, M., Weissenbruch, M.M. van, Williams, O., Zonnenberg, I.A., Lacaze-Masmonteil, T., Pas, A.B.T., Reiss, I.K.M., Kaam, A.H. van, Allegaert, K., Hutten, G.J., Simons, S.H., Poppe, J.A., Flint, R.B., Smits, A., Willemsen, S.P., Storm, K.K., Nuytemans, D.H., Onland, W., Poley, M.J., Boode, W.P. de, Carkeek, K., Cassart, V., Cornette, L., Dijk, P.H., Hemels, M.A.C., Hermans, I., Hütten, M.C., Kelen, D., Kort, E.H.M. de, Kroon, A.A., Lefevere, J., Plaskie, K., Stewart, B., Voeten, M., Weissenbruch, M.M. van, Williams, O., Zonnenberg, I.A., Lacaze-Masmonteil, T., Pas, A.B.T., Reiss, I.K.M., Kaam, A.H. van, Allegaert, K., Hutten, G.J., and Simons, S.H.

Abstract

Item does not contain fulltext, BACKGROUND: Apnoea of prematurity (AOP) is one of the most common diagnoses among preterm infants. AOP often leads to hypoxemia and bradycardia which are associated with an increased risk of death or disability. In addition to caffeine therapy and non-invasive respiratory support, doxapram might be used to reduce hypoxemic episodes and the need for invasive mechanical ventilation in preterm infants, thereby possibly improving their long-term outcome. However, high-quality trials on doxapram are lacking. The DOXA-trial therefore aims to investigate the safety and efficacy of doxapram compared to placebo in reducing the composite outcome of death or severe disability at 18 to 24 months corrected age. METHODS: The DOXA-trial is a double blinded, multicentre, randomized, placebo-controlled trial conducted in the Netherlands, Belgium and Canada. A total of 396 preterm infants with a gestational age below 29 weeks, suffering from AOP unresponsive to non-invasive respiratory support and caffeine will be randomized to receive doxapram therapy or placebo. The primary outcome is death or severe disability, defined as cognitive delay, cerebral palsy, severe hearing loss, or bilateral blindness, at 18-24 months corrected age. Secondary outcomes are short-term neonatal morbidity, including duration of mechanical ventilation, bronchopulmonary dysplasia and necrotising enterocolitis, hospital mortality, adverse effects, pharmacokinetics and cost-effectiveness. Analysis will be on an intention-to-treat principle. DISCUSSION: Doxapram has the potential to improve neonatal outcomes by improving respiration, but the safety concerns need to be weighed against the potential risks of invasive mechanical ventilation. It is unknown if the use of doxapram improves the long-term outcome. This forms the clinical equipoise of the current trial. This international, multicentre trial will provide the needed high-quality evidence on the efficacy and safety of doxapram in the treatment of AOP in p

Published
2023

2. Doxapram versus placebo in preterm newborns: a study protocol for an international double blinded multicentre randomized controlled trial (DOXA-trial)

Author

MS Neonatologie, Poppe, Jarinda, Flint, Robert, Smits, Anne, Willemsen, Sten, Storm, Kelly, Nuytemans, Debbie, Onland, Wes, Poley, Marten J, de Boode, Willem P, Carkeek, Katherine, Cassart, Vincent, Cornette, Luc, Dijk, Peter, Hemels, Marieke A C, Hermans, Isabelle, Hütten, Matthias C, Kelen, Dorottya, de Kort, Ellen, Kroon, Andre, Lefevere, Julie, Plaskie, Katleen, Steward, Breanne, Voeten, Michiel, Van Weissenbruch, Mirjam, Williams, Olivia, Zonnenberg, Inge, Lacaze-Masmonteil, T, Pas te, Arjan, Reiss, Irwin K M, van Kaam, Anton H., Allegaert, Karel, Hutten, Jeroen, Simons, Sinno H P, MS Neonatologie, Poppe, Jarinda, Flint, Robert, Smits, Anne, Willemsen, Sten, Storm, Kelly, Nuytemans, Debbie, Onland, Wes, Poley, Marten J, de Boode, Willem P, Carkeek, Katherine, Cassart, Vincent, Cornette, Luc, Dijk, Peter, Hemels, Marieke A C, Hermans, Isabelle, Hütten, Matthias C, Kelen, Dorottya, de Kort, Ellen, Kroon, Andre, Lefevere, Julie, Plaskie, Katleen, Steward, Breanne, Voeten, Michiel, Van Weissenbruch, Mirjam, Williams, Olivia, Zonnenberg, Inge, Lacaze-Masmonteil, T, Pas te, Arjan, Reiss, Irwin K M, van Kaam, Anton H., Allegaert, Karel, Hutten, Jeroen, and Simons, Sinno H P

Published
2023

3. Topical nitroglycerin ointment as salvage therapy for peripheral tissue ischemia in newborns: a systematic review

Author

Lacaze-Masmonteil T, Samiee-Zafarghandy S, Sushko K, Ferruccio L, Andrea Gilpin, van den Anker J, Catherine Litalien, Maryann Mazer-Amirshahi, and Anthony K.C. Chan

Subjects
Salvage Therapy, business.industry, Vasodilator Agents, Research, Infant, Newborn, Salvage therapy, General Medicine, Methemoglobinemia, medicine.disease, Administration, Cutaneous, Peripheral, Discontinuation, Ointments, Nitroglycerin, Tissue ischemia, Ischemia, Intensive care, Anesthesia, Intensive Care Units, Neonatal, Catheterization, Peripheral, Medicine, Humans, Adverse effect, Methodological quality, business
Abstract

Background: Topical nitroglycerin (TNG) ointment has been used for almost 3 decades to treat neonatal peripheral tissue ischemia, but this product is now no longer being produced by its Canadian manufacturer. Our aim was to investigate the efficacy and safety of TNG products in newborns in neonatal intensive care units. Methods: In this systematic review we searched Embase, CINAHL, MEDLINE, PubMed and Web of Science from inception to April 2020 for studies on the use of TNG products (TNG ointment, TNG spray, glyceryl trinitrate [GTN] patch) for the treatment of neonatal tissue ischemia. We did not apply language or study design limitations. Animal studies and duplicate records were excluded. Two reviewers screened and extracted data. The Tool for Evaluating the Methodological Quality of Case Reports and Case Series was used to assess the risk of bias of individual studies. Results: We included 23 articles (20 case reports, 2 case series and 1 retrospective audit) describing the use of TNG ointment, TNG spray or GTN patch in the treatment of 39 tissue ischemia events in 37 newborns. Twenty-three (62.2%), 12 (32.4%), 1 (2.7%) and 1 (2.7%) infants received TNG ointment, GTN patch, both TNG ointment and GTN patch, and TNG spray, respectively. Nineteen (76.0%) and 7 (53.8%) injuries treated with TNG ointment and GTN patch showed complete recovery, respectively. Two (16.7%) infants treated with GTN patch experienced adverse events (i.e., methemoglobinemia) requiring treatment discontinuation. Interpretation: TNG ointment presents a safe therapeutic modality for salvage therapy of neonatal tissue ischemia. Engagement of stakeholders is essential to address its recent commercial inaccessibility in Canada.

Published
2021

4. Lower respiratory tract illness and RSV prophylaxis in very premature infants

Author

Lacaze-Masmonteil, T., Truffert, P., Pinquier, D., Daoud, P., Goldfarb, G., Vicaut, E., and Fauroux, B.

Subjects
Respiratory tract infections -- Prevention, Respiratory tract infections -- Drug therapy, Respiratory syncytial virus infection -- Prevention, Respiratory syncytial virus infection -- Drug therapy, Infants (Premature) -- Health aspects, Risk factors (Health), Hospital care, Cohort analysis
Published
2004

11. Genome-wide association study of bronchopulmonary dysplasia:a potential role for variants near the CRP gene

Author

Mahlman, M. (Mari), Karjalainen, M. K. (Minna K.), Huusko, J. M. (Johanna M.), Andersson, S. (Sture), Kari, M. A. (M. Anneli), Tammela, O. K. (Outi K. T.), Sankilampi, U. (Ulla), Lehtonen, L. (Liisa), Marttila, R. H. (Riitta H.), Bassler, D. (Dirk), Poets, C. F. (Christian F.), Lacaze-Masmonteil, T. (Thierry), Danan, C. (Claude), Delacourt, C. (Christophe), Palotie, A. (Aarno), Muglia, L. J. (Louis J.), Lavoie, P. M. (Pascal M.), Hadchouel, A. (Alice), Rämet, M. (Mika), Hallman, M. (Mikko), Mahlman, M. (Mari), Karjalainen, M. K. (Minna K.), Huusko, J. M. (Johanna M.), Andersson, S. (Sture), Kari, M. A. (M. Anneli), Tammela, O. K. (Outi K. T.), Sankilampi, U. (Ulla), Lehtonen, L. (Liisa), Marttila, R. H. (Riitta H.), Bassler, D. (Dirk), Poets, C. F. (Christian F.), Lacaze-Masmonteil, T. (Thierry), Danan, C. (Claude), Delacourt, C. (Christophe), Palotie, A. (Aarno), Muglia, L. J. (Louis J.), Lavoie, P. M. (Pascal M.), Hadchouel, A. (Alice), Rämet, M. (Mika), and Hallman, M. (Mikko)

Abstract

Bronchopulmonary dysplasia (BPD), the main consequence of prematurity, has a significant heritability, but little is known about predisposing genes. The aim of this study was to identify gene loci predisposing infants to BPD. The initial genome-wide association study (GWAS) included 174 Finnish preterm infants of gestational age 24–30 weeks. Thereafter, the most promising single-nucleotide polymorphisms (SNPs) associated with BPD were genotyped in both Finnish (n = 555) and non-Finnish (n = 388) replication cohorts. Finally, plasma CRP levels from the first week of life and the risk of BPD were assessed. SNP rs11265269, flanking the CRP gene, showed the strongest signal in GWAS (odds ratio [OR] 3.2, p = 3.4 × 10⁻⁶). This association was nominally replicated in Finnish and French African populations. A number of other SNPs in the CRP region, including rs3093059, had nominal associations with BPD. During the first week of life the elevated plasma levels of CRP predicted the risk of BPD (OR 3.4, p = 2.9 × 10⁻⁴) and the SNP rs3093059 associated nominally with plasma CRP levels. Finally, SNP rs11265269 was identified as a risk factor of BPD (OR 1.8, p = 5.3 × 10⁻⁵), independently of the robust antenatal risk factors. As such, in BPD, a potential role for variants near CRP gene is proposed.

Published
2017

18. Randomised controlled trial of a new surfactant, surfaxin® (lucinactant) v curosurf® (poractant alfa) for the prevention of rds in very preterm babies

Author

Sinha, S., Soler, A.V.I., Lacaze-Masmonteil, T., Gadzinowski, J., Segal, R., D'Agostino, R., Wiswell, T., and Massaro, J.

Subjects
Curosurf (Medication) -- Evaluation, Respiratory distress syndrome -- Prevention, Surface active agents -- Evaluation -- Health aspects, Infants (Premature) -- Health aspects, Family and marriage, Health, Evaluation, Prevention, Health aspects
Abstract

Objective: To compare the safety and efficacy of the novel surfactant Surfaxin®, which contains KL4-peptide, against the predominately used animal derived (porcine) surfactant, Curosurf®, in the prevention of RDS. Methods: [...]

Published
2004

42. A multicenter, randomized, controlled trial of lucinactant versus poractant alfa among very premature infants at high risk for respiratory distress syndrome.

Author

Sinha SK, Lacaze-Masmonteil T, Soler AV, Wiswell TE, Gadzinowski J, Hajdu J, Bernstein G, Sanchez-Luna M, Segal R, Schaber CJ, Massaro J, d'Agostino R, and Surfaxin Therapy Against Respiratory Distress Syndrome Collaborative Group

Abstract

BACKGROUND: Available therapeutic surfactants are either animal-derived or non-protein-containing synthetic products. Animal-derived surfactants contain variable amounts of surfactant apoproteins, whereas the older-generation synthetic products contain only phospholipids and lack surfactant proteins (SPs). Both decrease morbidity and mortality rates associated with respiratory distress syndrome (RDS) among preterm infants, compared with placebo. However, excess mortality rates have been observed with non-protein-containing synthetic surfactants, compared with the animal-derived products. Evidence suggests that synthetic surfactants consisting solely of phospholipids can be improved with the addition of peptides that are functional analogs of SPs. Lucinactant is a new synthetic peptide-containing surfactant that contains sinapultide, a novel, 21-amino acid peptide (leucine and lysine repeating units, KL4 peptide) designed to mimic human SP-B. It is completely devoid of animal-derived components. OBJECTIVE: We hypothesized that the outcomes for premature infants treated with lucinactant and poractant alfa would be similar. Therefore, we compared lucinactant (Surfaxin; Discovery Laboratories, Doylestown, PA) with porcine-derived, poractant alfa (Curosurf; Chiesi Farmaceutici, Parma, Italy) in a trial to test for noninferiority. METHODS: A total of 252 infants born between 24 and 28 weeks of completed gestation, with birth weights between 600 and 1250 g, were assigned randomly in a multicenter, multinational, noninferiority, randomized, controlled study to receive either lucinactant (n = 124) or poractant alfa (n = 128) within 30 minutes of life. The primary outcome was the incidence of being alive without bronchopulmonary dysplasia (BPD) through 28 days of age. Key secondary outcomes included death at day 28 and 36 weeks postmenstrual age (PMA), air leaks, neuroimaging abnormalities, and other complications related to either prematurity or RDS. An independent, international, data and safety monitoring committee monitored the trial. RESULTS: The treatment difference between lucinactant and poractant alfa for survival without BPD through 28 days was 4.75% (95% confidence interval [CI]: -7.3% to 16.8%) in favor of lucinactant, with the lower boundary of the 95% CI for the difference, ie, -7.3%, being greater than the prespecified noninferiority margin of -14.5%. At 28 days, 45 of 119 infants given lucinactant were alive without BPD (37.8%; 95% CI: 29.1-46.5%), compared with 41 of 124 given poractant alfa (33.1%; 95% CI: 24.8-41.3%); at 36 weeks PMA, the rates were 64.7% and 66.9%, respectively. The corresponding mortality rate through day 28 for the lucinactant group was lower than that for the poractant alfa group (11.8% [95% CI: 6.0-17.6%] vs 16.1% [95% CI: 9.7-22.6%]), as was the rate at 36 weeks PMA (16% and 18.5%, respectively). There were no differences in major dosing complications. In addition, no significant differences were observed in the incidences of common complications of prematurity, including intraventricular hemorrhage (grades 3 and 4) and cystic periventricular leukomalacia (lucinactant: 14.3%; poractant alfa: 16.9%). CONCLUSIONS: Lucinactant and poractant alfa were similar in terms of efficacy and safety when used for the prevention and treatment of RDS among preterm infants. The ability to enhance the performance of a synthetic surfactant with the addition of a peptide that mimics the action of SP-B, such as sinapultide, brings potential advantages to exogenous surfactant therapy. [ABSTRACT FROM AUTHOR]

Published
2005
Full Text
View/download PDF

44. Periventricular leukomalacia: risk factors revisited.

Author

Zupan, Véronique, Gonzalez, Patricia, Lacaze-Masmonteil, Thierry, Boithias, Claire, D'Allest, Anne-Marie, Dehan, Michel, Gabilan, Jean-Claude, Zupan, V, Gonzalez, P, Lacaze-Masmonteil, T, Boithias, C, d'Allest, A M, Dehan, M, and Gabilan, J C

Published
1996
Full Text
View/download PDF

45. A model of pulmonary adenocarcinoma in transgenic mice expressing the simian virus 40 T antigen driven by the rat Calbindin-D9K (CaBP9K) promoter

Author

Chailley-Heu, B., Rambaud, C., Barlier-Mur, A-M., Galateau-Salle, F., Perret, C., Capron, F., and Lacaze-Masmonteil, T.

Abstract

Lung cancer is the most frequent cause of cancer deaths. Its origin and development remain poorly understood, partly because of the lack of pertinent animal models. This study produced transgenic mice expressing the simian virus (SV) 40 T antigen (Tag) driven by a 1011 base-pair DNA fragment of the rat Calbindin-D9K (CaBP9K) promoter. All transgenic animals developed multifocal pulmonary tumours with pathological and ultrastructural features consistent with adenocarcinomas. Using immunohistochemistry, northern blot or western blot, tumours were found to express the transcription factor TTF-1, as well as specific markers of the peripheral airway Clara cells (CC10) and alveolar type II cells (surfactant proteins A, B, C, and D). This model, with its similarities to human adenocarcinoma, should be useful not only for addressing the mechanisms underlying the development and progression of lung cancer, but also for testing new therapeutic approaches. Copyright © 2001 John Wiley & Sons, Ltd.

Published
2001

47. Characterization of proopiomelanocortin transcripts in human nonpituitary tissues.

Author

Lacaze-Masmonteil, T, de Keyzer, Y, Luton, J P, Kahn, A, and Bertagna, X

Abstract

Proopiomelanocortin (POMC), the precursor to adrenocorticotropic hormone and other related peptides, was originally identified in the corticotropic cell. Recent evidence shows that POMC products are also normally present in a variety of nonpituitary tissues. To investigate this phenomenon in humans we looked for the presence and characteristics of POMC transcripts in various adult tissues. Blot hybridization analysis of normal adrenal, thymus, and testis RNAs revealed a small RNA species approximately 400 nucleotides shorter than the 1200-nucleotide pituitary species. Primer extension and S1 nuclease mapping studies showed that this small RNA lacked exon 1 and exon 2 of the gene, and it corresponded to a set of at least six molecules starting 41 to 162 nucleotides downstream from the 5' end of exon 3. These RNAs appear to result from heterogeneous transcription initiation sites presumably under the control of "GC box" promoter sequences located in the 3' end of intron 2. They cannot encode a complete POMC molecule, and the only truncated POMC molecules that could be translated would lack a signal peptide necessary for membrane translocation and precursor processing. The use of highly sensitive S1 nuclease mapping techniques with uniformly labeled single-stranded DNA probes allowed the detection of a small but definite amount of the "normal," 1200-nucleotide, mRNA species. It is suggested that it is this POMC mRNA that is responsible for the local production of all the POMC peptides.

Published
1987
Full Text
View/download PDF

48. Pulmonary surfactant protein A (SP-A) is expressed by epithelial cells of small and large intestine.

Author

Rubio, S, Lacaze-Masmonteil, T, Chailley-Heu, B, Kahn, A, Bourbon, J R, and Ducroc, R

Abstract

Surfactant protein A (SP-A) is the most abundant protein associated with phospholipids in pulmonary surfactant. There are several lines of evidence that pulmonary and gastrointestinal epithelium produce closely related surface-active materials, although the presence of SP-A in gastrointestinal tract has so far not been reported. Indirect immunofluorescence experiments using different antibodies raised against rat pulmonary SP-A showed that some jejunal and colonic but not gastric epithelial cells positively stained for SP-A. Analysis of the proteins in cell lysates from rat small intestine and colon studied by Western blot revealed several immuno-reactive bands, including the characteristic triplet of 26-, 32-, and 38-kDa monomeric proteins, less strongly labeled than in lung cells, and higher molecular mass forms of 66 and 120 kDa also present in lung cells. The 66- and 120-kDa bands displayed the expected isoelectric pH of SP-A after two-dimensional electrophoresis. Alkylation induced conversion of the 120-kDa form (almost completely) and the 66-kDa form (partly) into the 26-38-kDa monomeric species. The presence of SP-A mRNA in rat stomach, small intestine, and colon was then searched for by conventional cDNA/reverse transcriptase-polymerase chain reaction. Products of appropriate size (372 base pairs) identical to that of pulmonary tissue were amplified in small intestine and colon but not in stomach or in other tissues used as controls. Cloning and sequencing of rat colon SP-A cDNA revealed the same sequence as the one reported for rat lung SP-A. Furthermore, analysis of the transcriptional initiation site of SP-A gene in colon by anchored-polymerase chain reaction showed that transcription was initiated at the same site in both colon and lung. These data, which demonstrate that small intestine and colon express SP-A constitutively and that this protein is present in some epithelial cells, extend the concept of intestinal surfactant and underline its close relationships to pulmonary surfactant.

Published
1995

Catalog

Books, media, physical & digital resources
See catalog results