Your search keyword '"Selroos, Olof"' showing total 39 results

1. Budesonide Attains Its Wide Clinical Profile by Alternative Kinetics.

Author

Brattsand, Ralph and Selroos, Olof

Subjects

ADRENERGIC beta agonists, BUDESONIDE, CLINICAL trials, FLUTICASONE propionate, BECLOMETHASONE dipropionate, BONE marrow, ANTI-inflammatory agents

Abstract

The introduction of inhaled corticosteroids (ICSs) changed over a few decades the treatment focus of mild-to-moderate asthma from bronchodilation to reduction in inflammation. This was achieved by inhaling a suitable corticosteroid (CS), giving a high, protracted airway concentration at a low total dose, thereby better combining efficacy and tolerance than oral therapy. Successful trials with the potent, lipophilic "skin" CS beclomethasone dipropionate (BDP) paved the way, suggesting that ICSs require a very low water solubility, prolonging their intraluminal dissolution within airways. The subsequent ICS development, with resulting clinical landmarks, is exemplified here with budesonide (BUD), showing that a similar efficacy/safety relationship is achievable by partly alternative mechanisms. BUD is much less lipophilic, giving it a 100-fold higher water solubility than BDP and later developed ICSs, leading to its more rapid intraluminal dissolution and faster airway and systemic uptake rates. In airway tissue, a BUD fraction is reversibly esterified to intracellular fatty acids, a lipophilic conjugate, which prolongs airway efficacy. Another mechanism is that the rapidly absorbed bulk fraction, via short plasma peaks, adds anti-inflammatory activity at the blood and bone marrow levels. Importantly, these plasma peaks are too short to provoke systemic adverse actions. Controlled clinical trials with BUD changed the use of ICS from a last resort to first-line treatment. Starting ICS treatment immediately after diagnosis ("early intervention") became a landmark for BUD. An established dose response made BUD suitable for the treatment of patients with all degrees of asthma severity. With the development of the budesonide/formoterol combination inhaler (BUD/FORM), BUD contributed to the widely used BUD/FORM maintenance and reliever therapy (MART). Recent studies demonstrated the value of BUD/FORM as a generally recommended as-needed therapy for asthma ("anti-inflammatory reliever", AIR). These abovementioned qualities have all influenced international asthma management and treatment guidelines. [ABSTRACT FROM AUTHOR]

Published

2024

2. Exome Sequencing Identifies Susceptibility Loci for Sarcoidosis Prognosis.

Author

Lahtela, Elisa, Kankainen, Matti, Sinisalo, Juha, Selroos, Olof, and Lokki, Marja-Liisa

Subjects

SARCOIDOSIS, PROGNOSIS, STATISTICS, CHROMOSOMES

Abstract

Many sarcoidosis-associating immunological genes have been shown to be shared between other immune-mediated diseases. In Finnish sarcoidosis patients, good prognosis subjects more commonly have HLA-DRB1 * 03:01 and/or HLA-DRB1 * 04:01-DPB1 * 04:01 haplotype, but no marker for persistent disease have been found. The objective was to further pinpoint genetic differences between prognosis subgroups in relation to the HLA markers. Whole-exome sequencing was conducted for 72 patients selected based on disease activity (resolved disease, n = 36; persistent disease, n = 36). Both groups were further divided by the HLA markers (one/both markers, n = 18; neither of the markers, n = 18). The Finnish exome data from the Genome Aggregation Database was used as a control population in the WES sample. Statistical analyses included single-variant analysis for common variants and gene level analysis for rare variants. We attempted to replicate associated variants in 181 Finnish sarcoidosis patients and 150 controls. An association was found in chromosome 1p36.21 (AADACL3 and C1orf158), which has recently been associated with sarcoidosis in another WES study. In our study, variations in these genes were associated with resolved disease (AADACL3, p = 0.0001 and p = 0.0003; C1orf158, p = 7.03E-05). Another interesting chromosomal region also peaked, Leucocyte Receptor Complex in 19q13.42, but the association diminished in the replication sample. In conclusion, this WES study supports the previously found association in the region 1p36.21. Furthermore, a novel to sarcoidosis region was found, but additional studies are warranted to verify this association. [ABSTRACT FROM AUTHOR]

Published

2019

3. Budesonide/Formoterol Easyhaler: Performance Under Simulated Real-Life Conditions.

Author

Haikarainen, Jussi, Selroos, Olof, Löytänä, Tero, Metsärinne, Sirpa, Happonen, Anita, and Rytilä, Paula

Subjects

BUDESONIDE, FORMOTEROL, DRUG delivery devices, INHALERS, INHALATION administration

Abstract

Introduction: We compared in vitro drug delivery characteristics of two budesonide/formoterol dry powder inhalers, the Bufomix Easyhaler and the budesonide/formoterol Turbuhaler, at different patient air flow rates, and to test dose delivery from the Easyhaler in stressed conditions exposed to moisture, dropping, vibration and freezing/thawing. Methods: A total of 36 inhalers from two batches of both products (160/4.5 µg strength) were used when comparing the effect of flow rate; six inhalers for each of the three flow rates for uniformity of delivered dose (DD), fine particle dose (FPD), mass median aerodynamic diameter (MMAD) and geometric standard deviation (GSD). Consistency of DD, FPD, MMAD and GSD were determined for each inhaler at three different flow rates: 10th, 50th and 90th percentile air flows. Dosing properties as a function of inhaler life were tested. The effects of moisture, dropping, vibration and freezing/thawing on DD and FPD were tested with two to four inhalers per test using all three strengths of Easyhaler: 80/4.5, 160/4.5 and 320/9 µg. Results: The Easyhaler, 160/4.5 µg, showed statistically significantly better dose consistency (expressed as percentage of labelled dose) at all three inhalation flows compared with the Turbuhaler, 160/4.5 µg, ( p < 0.001 for three flow rates). Exposure to moisture, dropping, vibration and freezing/thawing did not affect DD or FDP. These results were similar to all three tested Easyhaler strengths. Conclusion: In vitro performance of the Easyhaler indicates reliable dosing. Dose consistency was superior compared with the Turbuhaler at all tested flow rates. Environmental moisture, dropping, vibration and freezing/thawing did not affect the performance. Funding: Orion Corporation Orion Pharma. [ABSTRACT FROM AUTHOR]

Published

2017

4. SNP Variants in Major Histocompatibility Complex Are Associated with Sarcoidosis Susceptibility--A Joint Analysis in Four European Populations.

Author

Wolin, Annika, Lahtela, Elisa Laura, Anttila, Verneri, Petrek, Martin, Grunewald, Johan, van Moorsel, Coline H. M., Eklund, Anders, Grutters, Jan C., Kolek, Vitezslav, Mrazek, Frantisek, Kishore, Amit, Padyukov, Leonid, Pietinalho, Anne, Ronninger, Marcus, Seppänen, Mikko, Selroos, Olof, and Lokk, Marja-Liisa

Subjects

MAJOR histocompatibility complex, SARCOIDOSIS, LINKAGE disequilibrium

Abstract

Sarcoidosis is a multiorgan inflammatory disorder with heritability estimates up to 66%. Previous studies have shown the major histocompatibility complex (MHC) region to be associated with sarcoidosis, suggesting a functional role for antigen--presenting molecules and immune mediators in the disease pathogenesis. To detect variants predisposing to sarcoidosis and to identify genetic differences between patient subgroups, we studied four genes in the MHC Class III region (LTA, TNF, AGER, BTNL2) and HLA--DRA with tag--SNPs and their relation to HLA--DRB1 alleles. We present results from a joint analysis of four study populations (Finnish, Swedish, Dutch, and Czech). Patients with sarcoidosis (n = 805) were further subdivided based on the disease activity and the presence of Löfgren's syndrome. In a joint analysis, seven SNPs were associated with non--Löfgren sarcoidosis (NL; the strongest association with rs3177928, P = 1.79E--07, OR = 1.9) and eight with Löfgren's syndrome [Löfgren syndrome (LS); the strongest association with rs3129843, P = 3.44E--12, OR = 3.4] when compared with healthy controls (n = 870). Five SNPs were associated with sarcoidosis disease course (the strongest association with rs3177928, P = 0.003, OR = 1.9). The high linkage disequilibrium (LD) between SNPs and an HLA--DRB1 challenged the result interpretation. When the SNPs and HLA--DRB1 alleles were analyzed together, independent association was observed for four SNPs in the HLA--DRA/BTNL2 region: rs3135365 (NL; P = 0.015), rs3177928 (NL; P < 0.001), rs6937545 (LS; P = 0.012), and rs5007259 (disease activity; P = 0.002). These SNPs act as expression quantitative trait loci (eQTL) for HLA--DRB1 and/or HLA--DRB5. In conclusion, we found novel SNPs in BTNL2 and HLA--DRA regions associating with sarcoidosis. Our finding further establishes that polymorphisms in the HLA--DRA and BTNL2 have a role in sarcoidosis susceptibility. This multi--population study demonstrates that at least a part of these associations are HLA--DRB1 independent (e.g., not due to LD) and shared across ancestral origins. The variants that were independent of HLA--DRB1 associations acted as eQTL for HLA--DRB1 and/or --DRB5, suggesting a role in regulating gene expression. [ABSTRACT FROM AUTHOR]

Published

2017

5. Characteristics of reversible and nonreversible COPD and asthma and COPD overlap syndrome patients: an analysis of salbutamol Easyhaler data.

Author

Müller, Veronika, Gálffy, Gabriella, Orosz, Márta, Kováts, Zsuzsanna, Odler, Balázs, Selroos, Olof, and Tamási, Lilla

Published

2016

6. Inhaler Competence and Patient Satisfaction with Easyhaler: Results of Two Real-Life Multicentre Studies in Asthma and COPD.

Author

Gálffy, Gabriella, Mezei, Györgyi, Németh, Gyula, Tamási, Lilla, Müller, Veronika, Selroos, Olof, and Orosz, Marta

Subjects

ASTHMATICS, INHALERS, OBSTRUCTIVE lung diseases, PATIENT satisfaction, PULMONARY function tests

Abstract

Objective: The aim of this study was to investigate patients' inhaler competence and satisfaction with the Easyhaler dry powder inhaler. Design: Two open, uncontrolled, non-randomised studies. Setting: Real life based on patients attending 56 respiratory clinics in Hungary. Participants: Patients with asthma or chronic obstructive pulmonary disease (COPD) ( n = 1016). Intervention: In a 3-month study, adult patients (age range 18-88 years; n = 797) received twice-daily inhalations of formoterol via Easyhaler, and in a consequential study (from one visit to another, with 3-12 months in-between) children and adolescents (age range 4-17 years; n = 219) received salbutamol via Easyhaler as needed. Main Outcome Measures: Control of six Easyhaler handling steps and patients' satisfaction with Easyhaler based on questionnaires. Results: Correct performances (minimum and maximum of the six steps) were noticed after one demonstration in 92-98 % of the adults, 87-99 % of the elderly, 81-96 % of the children and 83-99 % of the adolescents. These figures had markedly increased at the last visit. Repeat instructions were necessary in 26 % of the cases. Investigators found Easyhaler easy to teach in 87 % of the patients and difficult in only 0.5 %. Patients found Easyhaler easy to learn and use, and the patients' (and parents') satisfaction with the inhaler was very high. Lung function values [forced expiratory volume in 1 s (FEV), forced vital capacity (FVC), peak expiratory flow (PEF)] improved statistically significantly during the studies, indicating good inhaler competence and treatment adherence. Conclusion: Investigators found Easyhaler easy to teach and patients found it easy to use, and their satisfaction with the device was high. [ABSTRACT FROM AUTHOR]

Published

2013

7. Is the patient’s baseline inhaled steroid dose a factor for choosing the budesonide/formoterol maintenance and reliever therapy regimen?

Author

Aubier, Michel, Haughney, John, Selroos, Olof, van Schayck, Onno C. P., Ekström, Tommy, Ostinelli, Juliette, and Buhl, Roland

Abstract

Objective: Baseline inhaled corticosteroid (ICS) dose may be a factor for prescribers to consider when they select a budesonide/formoterol maintenance and reliever therapy regimen for symptomatic asthmatics.Methods: A 6-month randomized study compared two maintenance doses of budesonide/formoterol 160/4.5 µg, 1 × 2 and 2 × 2, plus as needed, in 8424 asthma patients with symptoms when treated with ICS ± an inhaled long-acting β2-agonist (LABA). In the total study population, 1339 (17%) were high-dose ICS (HD) users (≥1600 µg/day budesonide). This HD stratum was compared with the rest of the study population, divided into low-dose (LD; 400 µg/day) and medium-dose strata (MD; 401–1599 µg/day) with regard to severe asthma exacerbations and mean changes in five-item Asthma Control Questionnaire (ACQ5) scores from baseline.Results: In all three strata there were fewer exacerbations in the 2 × 2 treatment groups (yearly rates 0.268, 0.172 and 0.094) than in the 1 × 2 treatment groups (yearly rates 0.232, 0.138 and 0.764). In no stratum was the difference between the treatment groups statistically significant. There was no statistically significant difference in time to the first severe exacerbation between the treatments 2 × 2 and 1 × 2 in the HD group (hazard ratio 0.944, p = 0.75). The adjusted mean changes in ACQ5 scores in the HD, MD and LD strata were −0.89, −0.61 and −0.65, respectively, with 1 × 2 treatment and −0.90, −0.74 and −0.76, respectively, with 2 × 2 treatment. In the MD and LD strata, the difference between doses was significant in favour of 2 × 2 (MD p < 0.0001; LD p = 0.004), but not in the HD stratum (p = 0.870). No difference in serious adverse events was seen.Conclusion: Compared with the LD and MD strata, the HD stratum patients had more exacerbations and a shorter time to first exacerbation. However, there were no differences in response between the 1 × 2 and 2 × 2 groups in any of the strata. This indicates that patients using budesonide/formoterol maintenance and reliever therapy, irrespective of baseline ICS dose, can be switched to 1 × 2 with its lower steroid load. ACQ5 scores improved more in the HD stratum than in the MD and LD strata indicating, among other things, that HD patients were not overtreated at baseline.ClinicalTrials.gov registration: NCT00463866 [ABSTRACT FROM PUBLISHER]

Published

2011

8. Use of dry powder inhalers in acute exacerbations of asthma and COPD.

Author

Selroos, Olof, Borgström, Lars, and Ingelf, Jarl

Abstract

To investigate whether dry powder inhalers (DPIs) function in a constrained situation, a literature analysis was performed to evaluate the use of DPIs compared with established therapies in the treatment of acute asthma and COPD, irrespective of rapid-acting β2-agonist used. The external databases Medline, Embase, Biosis and Current Contents and AstraZeneca's internal literature database Planet were searched up to April 2008. Only publications or congress abstracts describing clinical trials in patients treated at EDs or hospitals were considered, and then only those in which exacerbation severity (measured as FEV1) were included. Fifteen clinical studies met these criteria; twelve in acute asthma and three in acute COPD. For acute asthma, eight studies were double-blind, randomised studies (six in adults and two in children), two were open-label studies (one in adults and one in children), and two were investigational (methacholine challenge) studies. For the acute COPD studies, one was double-blind and randomised, one was single-blind and randomised, and one was open-label. This review found that administration of fast-acting bronchodilators via DPIs, the majority of which were Turbuhaler, is effective during an asthma or COPD worsening. Our literature review finds that DPIs function in patients with acute asthma or COPD equally well as established therapies with other inhaler devices. Patients can therefore rely upon DPIs in the same way that they rely upon other inhaler devices. [ABSTRACT FROM PUBLISHER]

Published

2009

9. Budesonide/formoterol as effective as prednisolone plus formoterol in acute exacerbations of COPD A double-blind, randomised, non-inferiority, parallel-group, multicentre study.

Author

Ställberg, Björn, Selroos, Olof, Vogelmeier, Claus, Andersson, Eva, Ekström, Tommy, and Larsson, Kjell

Subjects

FORMOTEROL, BLIND experiment, ADRENOCORTICAL hormones, ANTIBIOTICS, STEROIDS, OBSTRUCTIVE lung diseases, DYSPNEA

Abstract

Background: Oral corticosteroids and inhaled bronchodilators with or without antibiotics represent standard treatment of COPD exacerbations of moderate severity. Frequent courses of oral steroids may be a safety issue. We wanted to evaluate in an out-patient setting whether a 2-week course of inhaled budesonide/formoterol would be equally effective for treatment of acute COPD exacerbations as standard therapy in patients judged by the investigator not to require hospitalisation. Methods: This was a double-blind, randomised, non-inferiority, parallel-group, multicentre study comparing two treatment strategies; two weeks' treatment with inhaled budesonide/formoterol (320/9 μg, qid) was compared with prednisolone (30 mg once daily) plus inhaled formoterol (9 μg bid) in patients with acute exacerbations of COPD attending a primary health care centre. Inclusion criteria were progressive dyspnoea for less than one week, FEV1 30-60% of predicted normal after acute treatment with a single dose of oral corticosteroid plus nebulised salbutamol/ipratropium bromide and no requirement for subsequent immediate hospitalisation, i.e the clinical status after the acute treatment allowed for sending the patient home. A total of 109 patients (mean age 67 years, 33 pack-years, mean FEV1 45% of predicted) were randomized to two weeks' doubleblind treatment with budesonide/formoterol or prednisolone plus formoterol and subsequent open-label budesonide/formoterol (320/9 μg bid) for another 12 weeks. Change in FEV1 was the primary efficacy variable. Non-inferiority was predefined. Results: Non-inferiority of budesonide/formoterol was proven because the lower limit of FEV1-change (97.5% CI) was above 90% of the efficacy of the alternative treatment. Symptoms, quality of life, treatment failures, need for reliever medication (and exacerbations during follow-up) did not differ between the groups. No safety concerns were identified. Conclusion: High dose budesonide/formoterol was as effective as prednisolone plus formoterol for the ambulatory treatment of acute exacerbations in non-hospitalized COPD patients. An early increase in budesonide/formoterol dose may therefore be tried before oral corticosteroids are used. [ABSTRACT FROM AUTHOR]

Published

2009

10. A smarter way to manage asthma with a combination of a long-acting β2-agonist and inhaled corticosteroid.

Author

Selroos, Olof

Published

2007

11. Once-Daily Inhaled Budesonide for the Treatment of Asthma: Clinical Evidence and Pharmacokinetic Explanation.

Author

Selroos, Olof, Edsbäcker, Staffan, and Hultquist, Christer

Subjects

ASTHMA, LUNG diseases, ADRENOCORTICAL hormones, STEROID hormones, ADRENAL cortex, ESTERIFICATION, RESPIRATORY allergy

Abstract

Background. Budesonide, a widely used inhaled corticosteroid(ICS) with a favorable therapeutic ratio, is available via a dry powder inhaler(Pulmicort Turbuhaler®) and as a suspension for nebulization(Pulmicort Respules®). METHODS: MEDLINE and an AstraZeneca database were searched to identify relevant controlled clinical trials published between 1986 and 2002 using the key words budesonide OR inhaled corticosteroid, AND once daily. RESULTS: Thirty-four controlled clinical studies involving once-daily administration of budesonide to asthmatic patients were identified. Excluding long-term studies, this review presents data from 23 controlled studies for 4466 adults or adolescents and 1532 children with asthma and demonstrates efficacy of budesonide in both corticosteroid-naïve patients and patients previously treated with ICS. Once-daily administration of budesonide achieves clinical efficacy comparable with that of twice-daily regimens in patients with mild-to-moderate asthma and is equally effective when given in the morning or evening. Once-daily administration simplifies treatment regimens and may improve patient compliance. The tolerability profiles of budesonide once-daily via Turbuhaler® or as budesonide inhalation suspension are good and comparable with those for twice-daily dosing. CONCLUSIONS: Once-daily budesonide is effective and well tolerated as initial treatment for adults and children with mild asthma and as maintenance therapy in patients with more severe asthma once asthma control has been achieved. [ABSTRACT FROM AUTHOR]

Published

2004

12. Early Treatment of Stage II Sarcoidosis Improves 5-Year Pulmonary Function.

Author

Pietinalho, Anne, Tukiainen, Pentti, Haahtela, Tari, Persson, Tore, and Selroos, Olof

Subjects

ANGIOTENSIN converting enzyme, SARCOIDOSIS treatment, CHEST X rays, ADRENOCORTICAL hormones

Abstract

Study objective: To evaluate the 5-year prognosis of patients with stage I and stage II newly detected (< 3 months) pulmonary sarcoidosis treated immediately after diagnosis with prednisolone for 3 months followed by inhaled budesonide for 15 months. Design: Randomized, double-blind, placebo-controlled, parallel-group study for 18 months. Thereafter, open follow-up without treatment. Setting: Twenty pulmonary medicine departments in Finland. Patients: One hundred eighty-nine adult patients, most of them with normal lung function, were randomized to treatment. One hundred forty-nine patients were followed up for 5 years: 79 patients with initial stage I disease and 70 patients with stage II disease. Treatment: Oral prednisolone for 3 months followed by inhaled budesonide for 15 months (800 µg bid), or placebo tablets followed by placebo inhaler therapy. Thereafter, treatment only on an individual basis in the ease of clinical deterioration. Measurements: Yearly follow-up visits with chest radiographs, lung function tests (FEV[sub 1], FVC), diffusion capacity of the lung for carbon monoxide (DLCO), serum angiotensin-converting enzyme (SACE), and serum and urinary calcium measurements. Results: No initial differences were observed in chest radiographic findings between the active-treatment and placebo-treatment groups, either in patients with initial stage I or stage II(-III) disease. However, after the 5-year follow-up, 18 steroid-treated patients (26%) and 30 placebo-treated patients (38%) still had remaining chest radiographic changes. Placebo-treated patients more frequently required treatment with corticosteroids during the 5-year follow-up (p < 0.05). Steroid-treated patients with initial stage II(-III) disease improved more in FVC and DLCO (p < 0.05). No differences in reported adverse events or in SACE, serum calcium, or urinary calcium values were seen. Conclusion: Immediate treatment of pulmonary stage II(-III) sarcoidosis—but not stage I... [ABSTRACT FROM AUTHOR]

Published

2002

13. Efficacy of budesonide Turbuhaler ® compared with that of beclomethasone dipropionate pMDI in Japanese patients with moderately persistent asthma.

Author

Miyamoto, Terumasa, Takahashi, Terumi, Nakajima, Shigenori, Makino, Sohei, Yamakido, Michio, Mano, Kenji, Nakashima, Mitsuyoshi, Tollemar, Ulf, and Selroos, Olof

Subjects

METERED-dose inhalers, BECLOMETHASONE dipropionate, ASTHMA treatment

Abstract

Compares the efficacy of budesonide Turbuhaler with that of beclomethasone dipropionate pMDI in Japanese patients with persistent asthma. Basis in comparing the outcomes; Approach for improving the efficacy of budesonide; Importance of a higher dose treatment when comparing two formulations.

Published

2001

14. A double-blind, placebo-controlled dose–response study with budesonide Turbuhaler in Japanese asthma patients.

Author

Selroos, Olof, Miyamoto, Terumasa, Takahashi, Terumi, Nakajima, Shigenori, Makino, Sohei, Yamakido, Michio, Mano, Kenji, and Nakashima, Mitsuyoshi

Subjects

ASTHMATICS, DOSE-response relationship in biochemistry

Abstract

Objective:The aim of this study was to investigate the dose–response for inhaled budesonide via Turbuhaler® in Japanese patients with mild to moderate asthma. Methodology:Inhaled budesonide 100 μg, 200 μg, 400 μg or placebo was administered twice daily via Turbuhaler for 6 weeks, to 267 adult Japanese patients (mean age 51 years) with mild-to-moderate, non-steroid-dependent bronchial asthma, in a double-blind, placebo-controlled, randomized, parallel group study. The patients had to be symptomatic for more than 3 days/week and have an average morning peak expiratory flow (PEF) 50–80% of predicted normal value. Results:The response to budesonide was rapid, all treatments showing a significant improvement in morning PEF after 1 week (P < 0.05). During week 6, mean improvements of 15, 45, 53 and 71 L/min were observed for the placebo, 200 μg, 400 μg and 800 μg budesonide groups, respectively. Compared with placebo all improvements in the budesonide groups were statistically significant and a significant dose–response was demonstrated (P < 0.001). The difference between the 200 μg and 800 μg doses was significant. Also, for several secondary efficacy variables (e.g. evening PEF, symptom score, treatment score, daily activity score and sleep score) significant dose–responses were shown. Other variables included the investigators’ assessments of improvement and usefulness. They also showed statistically significant dose–response relationships and confirmed the rapid onset of action. Budesonide was well tolerated at all tested doses, with a low incidence of adverse events, all of which were minor in severity. Conclusions:Budesonide Turbuhaler in the doses 100 μg to 400 μg twice daily was effective, well tolerated and showed a rapid onset of action in patients with mild-to-moderate asthma. Dose–response was demonstrated for several variables of clinical efficacy. [ABSTRACT FROM AUTHOR]

Published

2000

15. A double-blind, placebo-controlled steroid-sparing study with budesonide Turbuhaler in Japanese oral steroid-dependent asthma patients.

Author

Selroos, Olof, Miyamoto, Terumasa, Takahashi, Terumi, Nakajima, Shigenori, Makino, Sohei, Yamakido, Michio, Mano, Kenji, Nakashima, Mitsuyoshi, and Tollemar, Ulf

Subjects

ASTHMA treatment, STEROID drugs

Abstract

Objective:The aim of this study was to evaluate the oral steroid-sparing capacity of budesonide Turbuhaler®. Methodology:One hundred and thirteen oral steroid-dependent patients were treated for 6 months with placebo or budesonide 800 μg or 1600 μg daily. Every second week the oral steroid dose was reduced if asthma control permitted. Results:The reductions in oral steroid doses were 9, 35 and 60% in the placebo and budesonide 800 μg and 1600 μg groups, respectively. Oral steroid treatment could be discontinued in 4% (placebo), 15% (800 μg) and 23% (1600 μg). Mean peak expiratory flow values increased by 21 and 24 L/min in the budesonide groups but decreased by 6 L/min in the placebo group. Asthma attack, activity and sleep scores remained unchanged showing maintained efficacy. Plasma cortisol levels increased and an adrenocorticotropic hormone test showed improved adrenocortical response in both budesonide groups, indicating improved safety. Adverse drug reactions were infrequent and mild in all study groups. Conclusion:Budesonide Turbuhaler, 800 μg and 1600 μg daily, resulted in a significant reduction in oral steroid usage in steroid-dependent patients. The effect was achieved with maintained asthma control together with improvements in lung and adrenal functions. [ABSTRACT FROM AUTHOR]

Published

2000

16. FINE-NEEDLE ASPIRATION BIOPSY OF THE SPLEEN IN DIAGNOSIS OF SARCOIDOSIS.

Author

Selroos, Olof

Published

1976

17. IMMUNOHISTOCHEMICAL DEMONSTRATION OF LYSOZYME IN THE LYMPH NODES AND KVEIM REACTION PAPULES IN SARCOIDOSIS.

Author

Klockars, Matti and Selroos, Olof

Published

1977

18. Sarcoidosis with thyroid involvement, polymyalgia rheumatica and breast carcinoma. A case report.

Author

von Knorring, Johan, Selroos, Olof, von Knorring, J, and Selroos, O

Published

1976

19. Sarcoidosis of the Spleen.

Author

Selroos, Olof

Published

1976

20. LUPUS-LIKE SYNDROME ASSOCIATED WITH PULMONARY REACTION TO NITROFURANTOIN: Report of Three Cases.

Author

Selroos, Olof and Edgren, Johan

Published

1975

21. SARCOIDOSIS AND MYELOMA OF LAMBDA-TYPE IgG.

Author

Selroos, Olof, Brander, Lennart, and Virolainen, Martti

Published

1974

22. Review : Ozone: Causation and Aggravation of Lung Diseases.

Author

Ström, Jeanette, Alfredsson, Lars, Malmfors, Torbjörn, and Selroos, Olof

Abstract

The presence of ozone is to a large extent due to the emissions of hydrocarbons and nitrogen oxides over large areas. During periodic peak concentrations of ozone in the range of 0.1-0.2 ppm in the polluted air of big cities, people may suffer reactions such as eye discomfort, headache, chest discomfort, shortness of breath, and cough. Bronchoconstriction, with an increased airway resis tance resulting in reductions in lung function parameters, arises at concentra tions of ozone > 0.2 ppm. Asthmatics seem to be more sensitive than healthy individuals, but long-term effects in humans are to a large extent unknown since they are very difficult to evaluate. [ABSTRACT FROM PUBLISHER]

Published

1994

23. Review : Nitrogen Dioxide: Causation and Aggravation of Lung Diseases.

Author

Ström, Jeanette, Alfredsson, Lars, Malmfors, Torbjörn, and Selroos, Olof

Abstract

It is of great importance to investigate the role of air pollutants in causing and aggravating lung diseases. The levels of concentration of some of these com bustion products have shown a decreasing emission curve, but the emissions of nitrogen dioxide (NO2) are still increasing. Most of the NO2 emissions origi nate from road traffic. The installation of catalytic converters may well change this. It is established that low concentrations of NO2 affect the respiratory system; this is especially obvious in asthmatics. Regarding long-term effects, it is believed that high levels of NO2 may cause an increased frequency of respi ratory illness, but it is not possible to confirm this suspicion completely. [ABSTRACT FROM PUBLISHER]

Published

1994

24. High-Dose Inhaled Budesonide May Substitute for Oral Therapy After an Acute Asthma Attack.

Author

Nana, Arth, Youngchaiyud, Praparn, Charoenratanakul, Suchai, Boe, Jacob, Löfdahl, Claes-Göran, Selroos, Olof, and Ståhl, Elisabeth

Published

1998

25. Blood Monocytes and Serum and Bone Marrow Lysozyme in Sarcoidosis.

Author

Koivunen, Elli, Grönhagen-Riska, Carola, Klockars, Matti, and Selroos, Olof

Published

1982

26. Prognostic Significance of Lymphopenia in Sarcoidosis.

Author

Selroos, Olof and Koivunen, Elli

Published

1979

27. Use of Budesonide in the Treatment of Pulmonary Sarcoidosis.

Author

SELROOS, OLOF B.

Published

1986

28. Biochemical Markers in Sarcoidosis.

Author

Selroos, Olof B. N.

Published

1986

29. IMMUNOGLOBULINS IN PERNICIOUS ANAEMIA.

Author

Selroos, Olof and Knorring, Johan

Published

1973

30. THROMBOCYTOSIS.

Author

Selroos, Olof

Published

1973

31. INFECTIOUS MONONUCLEOSIS WITH THROMBOCYTOPENIC PURPURA.

Author

Selroos, Olof

Published

1972

32. PULMONARY REACTION TO NITROFURANTOIN.

Author

Brander, Lennart and Selroos, Olof

Published

1969

33. Platelet values in amyloidosis.

Author

Selroos, Olof, Pettersson, Tor, Selroos, O, and Pettersson, T

Published

1973

34. Thrombocytes in fibrinogen-induced arthritis in rabbits.

Author

Selroos, Olof, Wegelius, Otto, Selroos, O, and Wegelius, O

Published

1973

35. Continuous versus intermittent inhaled corticosteroid (budesonide) for mild persistent asthma in children—not too much, not too little.

Author

Turpeinen, Markku, Pelkonen, Anna S., Selroos, Olof, Nikander, Kurt, and Haahtela, Tari

Subjects

CORTICOSTEROIDS, STEROID drugs, ASTHMA treatment, ASTHMA in children, CHARTS, diagrams, etc.

Abstract

The author discusses a study related to the Helsinki Early Intervention Childhood Asthma Programme which is a program that highlights the benefits and safety aspects of intermittent treatment of asthma with budesonide. Several graphs depicting findings of the study are also presented. The author concludes that intermittent treatment using inhaled corticosteroids is an efficient alternative for treating mild persistent asthma in children.

Published

2012

36. Polymyalgia rheumatica and chronic lymphatic leukaemia.

Author

von Knorring, Johan, Selroos, Olof, von Knorring, J, and Selroos, O

Published

1977

37. Thrombocytosis in experimental amyloidosis in rabbits.

Author

Selroos, Olof, Pettersson, Tor, Wegelius, Otto, Selroos, O, Pettersson, T, and Wegelius, O

Published

1973

38. Budesonide/formoterol as effective as prednisolone plus formoterol in acute exacerbations of COPD. A double-blind, randomised, non-inferiority, parallel-group, multicentre study.

Author

Ställberg B, Selroos O, Vogelmeier C, Andersson E, Ekström T, Larsson K, Ställberg, Björn, Selroos, Olof, Vogelmeier, Claus, Andersson, Eva, Ekström, Tommy, and Larsson, Kjell

Abstract

Background: Oral corticosteroids and inhaled bronchodilators with or without antibiotics represent standard treatment of COPD exacerbations of moderate severity. Frequent courses of oral steroids may be a safety issue. We wanted to evaluate in an out-patient setting whether a 2-week course of inhaled budesonide/formoterol would be equally effective for treatment of acute COPD exacerbations as standard therapy in patients judged by the investigator not to require hospitalisation.Methods: This was a double-blind, randomised, non-inferiority, parallel-group, multicentre study comparing two treatment strategies; two weeks' treatment with inhaled budesonide/formoterol (320/9 microg, qid) was compared with prednisolone (30 mg once daily) plus inhaled formoterol (9 microg bid) in patients with acute exacerbations of COPD attending a primary health care centre. Inclusion criteria were progressive dyspnoea for less than one week, FEV1 30-60% of predicted normal after acute treatment with a single dose of oral corticosteroid plus nebulised salbutamol/ipratropium bromide and no requirement for subsequent immediate hospitalisation, i.e the clinical status after the acute treatment allowed for sending the patient home.A total of 109 patients (mean age 67 years, 33 pack-years, mean FEV1 45% of predicted) were randomized to two weeks' double-blind treatment with budesonide/formoterol or prednisolone plus formoterol and subsequent open-label budesonide/formoterol (320/9 microg bid) for another 12 weeks. Change in FEV1 was the primary efficacy variable. Non-inferiority was predefined.Results: Non-inferiority of budesonide/formoterol was proven because the lower limit of FEV1-change (97.5% CI) was above 90% of the efficacy of the alternative treatment. Symptoms, quality of life, treatment failures, need for reliever medication (and exacerbations during follow-up) did not differ between the groups. No safety concerns were identified.Conclusion: High dose budesonide/formoterol was as effective as prednisolone plus formoterol for the ambulatory treatment of acute exacerbations in non-hospitalized COPD patients. An early increase in budesonide/formoterol dose may therefore be tried before oral corticosteroids are used.Clinical Trial Registration: NCT00259779. [ABSTRACT FROM AUTHOR]

Published

2009

39. LIMITING FACTORS IN LOCAL THERAPY FOR THE AIRWAYS.

Author

Selroos, Olof

Subjects

RESPIRATORY obstructions, DRUG therapy, DRUG delivery devices, INHALERS, RESPIRATORY diseases, RESPIRATORY therapy equipment

Abstract

The article presents information on the limiting factors in local therapy for the airways. Some of the factors discussed are: age, handicap, temperature, local side effects, variety of inhalers and spacers, etc.

Published

1993