Your search keyword '"Maitland-van der Zee, A. H."' showing total 96 results

1. Dried Blood Spot Method Development and Clinical Validation for the Analysis of Elexacaftor, Elexacaftor-M23, Tezacaftor, Tezacaftor-M1, Ivacaftor, Ivacaftor Carboxylate, and Hydroxymethyl Ivacaftor Using LC-MS/MS.

Author

Vonk, Steffie E. M., van der Meer-Vos, Marloes, Kos, Renate, Neerincx, Anne H., Terheggen-Lagro, Suzanne W. J., Altenburg, Josje, Maitland-van der Zee, Anke H., Mathôt, Ron A. A., and Kemper, E. Marleen

Published

2024

2. Are single‐nucleotide polymorphisms previously linked to inhaled corticosteroid response associated with obese‐asthma in children?

Author

Longo, Cristina, Chiv, Richard, Xu, Zhongli, Forno, Erick, Chen, Wei, Boeck, Andreas, Granell, Raquel, Salvermoser, Michael, Schaub, Bianca, Celedón, Juan C., Turner, Stephen, Vijverberg, Susanne, and Maitland‐van der Zee, Anke H.

Subjects

ASTHMA in children, OVERWEIGHT children, SINGLE nucleotide polymorphisms, REGULATOR genes, RANDOM effects model, ASTHMATICS

Abstract

The article explores the association between single-nucleotide polymorphisms (SNPs) previously linked to inhaled corticosteroid response and obese-asthma in children. Childhood obesity is a significant risk factor for asthma development and may reduce response to conventional treatment. The study suggests that the SNP rs517762 in the NEGR1 gene, implicated in poor ICS response, is also associated with obesity in children with asthma. The findings highlight potential underlying mechanisms of the pediatric obese-asthma phenotype and call for further validation through prospective and functional studies. [Extracted from the article]

Published

2024

3. The Progression of Symptoms in Post COVID-19 Patients: A Multicentre, Prospective, Observational Cohort Study.

Author

Cornelissen, Merel E. B., Haarman, Myrthe M., Twisk, Jos W. R., Houweling, Laura, Baalbaki, Nadia, Sondermeijer, Brigitte, Beijers, Rosanne J. H. C. G., Gach, Debbie, Bloemsma, Lizan D., and Maitland-van der Zee, Anke H.

Subjects

COVID-19, FATIGUE (Physiology), PULMONARY function tests, SYMPTOMS, LOGISTIC regression analysis

Abstract

Background: Although the coronavirus disease 2019 (COVID-19) pandemic is no longer a public health emergency of international concern, 30% of COVID-19 patients still have long-term complaints. A better understanding of the progression of symptoms after COVID-19 is needed to reduce the burden of the post COVID-19 condition. Objective: This study aims to investigate the progression of symptoms, identify patterns of symptom progression, and assess their associations with patient characteristics. Methods: Within the P4O2 COVID-19 study, patients aged 40–65 years were recruited from five Dutch hospitals. At 3–6 and 12–18 months post COVID-19, medical data were collected, and pulmonary function tests were performed. In between, symptoms were assessed monthly with a questionnaire. Latent class mixed modelling was used to identify symptom progression patterns over time, with multinomial logistic regression to examine associations with patient characteristics. Results: Eighty-eight patients (aged 54.4 years, 48.9% males) were included. Three trajectories were identified for fatigue and dyspnoea: decreasing, high persistent, and low persistent. The odds of "decreasing fatigue" was higher for never smokers and participants in the lifestyle intervention and lower for those having a comorbidity. The odds of "decreasing dyspnoea" was higher for moderate COVID-19 patients and lifestyle intervention participants and lower for males, mild COVID-19 patients, and those with a higher age. Conclusions: Three distinct trajectories were identified for fatigue and dyspnoea, delineating patterns of symptom persistence following COVID-19. Sex, age, smoking status, participation in lifestyle interventions and COVID-19 severity were associated with the likelihood of belonging to different trajectories. These findings highlight the heterogeneity of the long-term symptoms experienced by post COVID-19 patients and emphasise the importance of personalised treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2024

4. Fatigue in severe pediatric asthma patients: Results of the PANDA study.

Author

van Dijk, Yoni E., Keuker, Valerie S. L., Hashimoto, Simone, Rutjes, Niels W., van Muilekom, Maud M., Golebski, Kornel, Van Litsenburg, Raphaële R. L., Terheggen‐Lagro, Suzanne W. J., van Ewijk, Bart E., Gemke, Reinoud J. B. J., Maitland‐van der Zee, Anke H., and Vijverberg, Susanne J. H.

Subjects

ASTHMATICS, FATIGUE (Physiology), DUTCH people, ASTHMA in children, STANDARD deviations, CANCER fatigue

Abstract

Background: Fatigue is a commonly reported clinical symptom, yet research on fatigue in children with severe asthma is missing. We aimed to explore the extent of fatigue in severe pediatric asthma and identify associated factors. Method: This study was conducted within the Pediatric Asthma Non‐Invasive Diagnostic Approaches (PANDA), an observational cohort of 6‐ to 17‐year‐old Dutch children with severe asthma. The Pediatric Quality of Life Inventory Multidimensional Fatigue Scale (PedsQL™‐MFS) was used to measure self‐reported fatigue. Fatigue levels were compared with a general pediatric Dutch population using linear regression, and quantifying the prevalence of "fatigued" (−2 < Standard deviations [SD] ≤ −1) and "severely fatigued" (SD ≤ −2) children. Secondly, we performed linear regression analyses to explore whether fatigue levels were independently associated with asthma attacks, comorbidities, medication, pulmonary function, symptom control, and asthma‐related quality of life (QoL). Results: Severe pediatric asthma patients (n = 78, mean age 11.8 ± 3.1 years) reported significantly more fatigue than Dutch peers (n = 328, mean age 11.8 ± 3.2 years) mean difference in z‐score: −0.68; 95%CI −0.96, −0.40. In the severe asthma group, 28.2% scored as "fatigued" and 15.4% as "severely fatigued," compared with 14.0% and 3.4% in the general population. In pediatric asthma patients, asthma‐related QoL (β = 0.77, p <.01, ΔR2 =.43), symptom control (β = 0.56, p <.01, ΔR2 =.24) and a dysfunctional breathing pattern (β = −0.36, p <.01, ΔR2 =.12) were most strongly associated with fatigue scores. Conclusion: Fatigue is a common symptom in children with severe asthma and is associated with multiple clinical factors and patient‐reported outcomes. It should be considered as an important treatment target. [ABSTRACT FROM AUTHOR]

Published

2024

5. A severe asthma phenotype of excessive airway Haemophilus influenzae relative abundance associated with sputum neutrophilia.

Author

Versi, Ali, Azim, Adnan, Ivan, Fransiskus Xaverius, Abdel‐Aziz, Mahmoud I, Bates, Stewart, Riley, John, Uddin, Mohib, Zounemat Kermani, Nazanin, Maitland‐Van Der Zee, Anke‐H, Dahlen, Sven‐Eric, Djukanovic, Ratko, Chotirmall, Sanjay H, Howarth, Peter, Adcock, Ian M, and Chung, Kian Fan

Subjects

HAEMOPHILUS influenzae, MORAXELLA catarrhalis, CUTIBACTERIUM acnes, ACTINOBACILLUS, HIERARCHICAL clustering (Cluster analysis)

Abstract

Background: Severe asthma (SA) encompasses several clinical phenotypes with a heterogeneous airway microbiome. We determined the phenotypes associated with a low α‐diversity microbiome. Methods: Metagenomic sequencing was performed on sputum samples from SA participants. A threshold of 2 standard deviations below the mean of α‐diversity of mild‐moderate asthma and healthy control subjects was used to define those with an abnormal abundance threshold as relative dominant species (RDS). Findings: Fifty‐one out of 97 SA samples were classified as RDSs with Haemophilus influenzae RDS being most common (n = 16), followed by Actinobacillus unclassified (n = 10), Veillonella unclassified (n = 9), Haemophilus aegyptius (n = 9), Streptococcus pseudopneumoniae (n = 7), Propionibacterium acnes (n = 5), Moraxella catarrhalis (n = 5) and Tropheryma whipplei (n = 5). Haemophilus influenzae RDS had the highest duration of disease, more exacerbations in previous year and greatest number on daily oral corticosteroids. Hierarchical clustering of RDSs revealed a C2 cluster (n = 9) of highest relative abundance of exclusively Haemophilus influenzae RDSs with longer duration of disease and higher sputum neutrophil counts associated with enrichment pathways of MAPK, NF‐κB, TNF, mTOR and necroptosis, compared to the only other cluster, C1, which consisted of 7 Haemophilus influenzae RDSs out of 42. Sputum transcriptomics of C2 cluster compared to C1 RDSs revealed higher expression of neutrophil extracellular trap pathway (NETosis), IL6‐transignalling signature and neutrophil activation. Conclusion: We describe a Haemophilus influenzae cluster of the highest relative abundance associated with neutrophilic inflammation and NETosis indicating a host response to the bacteria. This phenotype of severe asthma may respond to specific antibiotics. [ABSTRACT FROM AUTHOR]

Published

2024

6. International Care programs for Pediatric Post-COVID Condition (Long COVID) and the way forward.

Author

Brackel, Caroline L. H., Noij, Lieke C. E., Vijverberg, Susanne J. H., Legghe, Camille L., Maitland-van der Zee, Anke H., van Goudoever, Johannes B., Buonsenso, Danilo, Munblit, Daniel, Sigfrid, Louise, McFarland, Sammie, Anmyr, Lena, Ashkenazi-Hoffnung, Liat, Bellinat, Ana P. N., Dias, Nathália L. S., Edwards, Amy, Fashina, Tomini, Juraški, Romana Gjergja, Gonçalves, Ana L. N., Hansted, Edita, and Herczeg, Vivien

Published

2024

7. Hemoglobin and Its Relationship with Fatigue in Long-COVID Patients Three to Six Months after SARS-CoV-2 Infection.

Author

Bazdar, Somayeh, Bloemsma, Lizan D., Baalbaki, Nadia, Blankestijn, Jelle M., Cornelissen, Merel E. B., Beijers, Rosanne J. H. C. G., Sondermeijer, Brigitte M., van Wijck, Yolanda, Downward, George S., and Maitland-van der Zee, Anke H.

Subjects

FATIGUE (Physiology), POST-acute COVID-19 syndrome, HEMOGLOBINS, SARS-CoV-2, RANK correlation (Statistics)

Abstract

Background: While some long-term effects of COVID-19 are respiratory in nature, a non-respiratory effect gaining attention has been a decline in hemoglobin, potentially mediated by inflammatory processes. In this study, we examined the correlations between hemoglobin levels and inflammatory biomarkers and evaluated the association between hemoglobin and fatigue in a cohort of Long-COVID patients. Methods: This prospective cohort study in the Netherlands evaluated 95 (mostly hospitalized) patients, aged 40–65 years, 3–6 months post SARS-CoV-2 infection, examining their venous hemoglobin concentration, anemia (hemoglobin < 7.5 mmol/L in women and <8.5 mmol/L in men), inflammatory blood biomarkers, average FSS (Fatigue Severity Score), demographics, and clinical features. Follow-up hemoglobin was compared against hemoglobin during acute infection. Spearman correlation was used for assessing the relationship between hemoglobin concentrations and inflammatory biomarkers, and the association between hemoglobin and fatigue was examined using logistic regression. Results: In total, 11 (16.4%) participants were suffering from anemia 3–6 months after SARS-CoV-2 infection. The mean hemoglobin value increased by 0.3 mmol/L 3–6 months after infection compared to the hemoglobin during the acute phase (p-value = 0.003). Whilst logistic regression showed that a 1 mmol/L greater increase in hemoglobin is related to a decrease in experiencing fatigue in Long-COVID patients (adjusted OR 0.38 [95%CI 0.13–1.09]), we observed no correlations between hemoglobin and any of the inflammatory biomarkers examined. Conclusion: Our results indicate that hemoglobin impairment might play a role in developing Long-COVID fatigue. Further investigation is necessary to identify the precise mechanism causing hemoglobin alteration in these patients. [ABSTRACT FROM AUTHOR]

Published

2024

8. Volatile Organic Compounds in Cellular Headspace after Hyperbaric Oxygen Exposure: An In Vitro Pilot Study.

Author

de Jong, Feiko J. M., Lilien, Thijs A., Fenn, Dominic W., Wingelaar, Thijs T., van Ooij, Pieter-Jan A. M., Maitland-van der Zee, Anke H., Hollmann, Markus W., van Hulst, Rob A., and Brinkman, Paul

Subjects

GAS chromatography/Mass spectrometry (GC-MS), PILOT projects, VOLATILE organic compounds, OXYGEN, COMPRESSED air, EPITHELIAL cells

Abstract

Volatile organic compounds (VOCs) might be associated with pulmonary oxygen toxicity (POT). This pilot study aims to identify VOCs linked to oxidative stress employing an in vitro model of alveolar basal epithelial cells exposed to hyperbaric and hyperoxic conditions. In addition, the feasibility of this in vitro model for POT biomarker research was evaluated. The hyperbaric exposure protocol, similar to the U.S. Navy Treatment Table 6, was conducted on human alveolar basal epithelial cells, and the headspace VOCs were analyzed using gas chromatography–mass spectrometry. Three compounds (nonane [p = 0.005], octanal [p = 0.009], and decane [p = 0.018]), of which nonane and decane were also identified in a previous in vivo study with similar hyperbaric exposure, varied significantly between the intervention group which was exposed to 100% oxygen and the control group which was exposed to compressed air. VOC signal intensities were lower in the intervention group, but cellular stress markers (IL8 and LDH) confirmed increased stress and injury in the intervention group. Despite the observed reductions in compound expression, the model holds promise for POT biomarker exploration, emphasizing the need for further investigation into the complex relationship between VOCs and oxidative stress. [ABSTRACT FROM AUTHOR]

Published

2024

9. Influence of the gut and airway microbiome on asthma development and disease.

Author

Smulders, Tamar, Van Der Schee, Marc P., Maitland‐Van Der Zee, Anke H., Dikkers, Frederik G., and Van Drunen, Cornelis M.

Subjects

GUT microbiome, ASTHMA, NUMBERS of species, INDIVIDUAL differences, IMMUNE system, WHEEZE

Abstract

There are ample data to suggest that early‐life dysbiosis of both the gut and/or airway microbiome can predispose a child to develop along a trajectory toward asthma. Although individual studies show clear associations between dysbiosis and asthma development, it is less clear what (collection of) bacterial species is mechanistically responsible for the observed effects. This is partly due to issues related to the asthma diagnosis and the broad spectrum of anatomical sites, sample techniques, and analysis protocols that are used in different studies. Moreover, there is limited attention for potential differences in the genetics of individuals that would affect the outcome of the interaction between the environment and that individual. Despite these challenges, the first bacterial components were identified that are able to affect the transcriptional state of human cells, ergo the immune system. Such molecules could in the future be the basis for intervention studies that are now (necessarily) restricted to a limited number of bacterial species. For this transition, it might be prudent to develop an ex vivo human model of a local mucosal immune system to better and safer explore the impact of such molecules. With this approach, we might move beyond association toward understanding of causality. [ABSTRACT FROM AUTHOR]

Published

2024

10. Fatigue and symptom-based clusters in post COVID-19 patients: a multicentre, prospective, observational cohort study.

Author

Cornelissen, Merel E. B., Bloemsma, Lizan D., Vaes, Anouk W., Baalbaki, Nadia, Deng, Qichen, Beijers, Rosanne J. H. C. G., Noij, Lieke C. E., Houweling, Laura, Bazdar, Somayeh, Spruit, Martijn A., and Maitland-van der Zee, Anke H.

Subjects

COVID-19, FATIGUE (Physiology), SLEEP interruptions, CHRONIC fatigue syndrome, SELF-organizing maps, CANCER fatigue

Abstract

Background: In the Netherlands, the prevalence of post COVID-19 condition is estimated at 12.7% at 90–150 days after SARS-CoV-2 infection. This study aimed to determine the occurrence of fatigue and other symptoms, to assess how many patients meet the Myalgic Encephalomyelitis/Chronic Fatigue Syndrome (ME/CFS) criteria, to identify symptom-based clusters within the P4O2 COVID-19 cohort and to compare these clusters with clusters in a ME/CFS cohort. Methods: In this multicentre, prospective, observational cohort in the Netherlands, 95 post COVID-19 patients aged 40–65 years were included. Data collection at 3–6 months after infection included demographics, medical history, questionnaires, and a medical examination. Follow-up assessments occurred 9–12 months later, where the same data were collected. Fatigue was determined with the Fatigue Severity Scale (FSS), a score of ≥ 4 means moderate to high fatigue. The frequency and severity of other symptoms and the percentage of patients that meet the ME/CFS criteria were assessed using the DePaul Symptom Questionnaire-2 (DSQ-2). A self-organizing map was used to visualize the clustering of patients based on severity and frequency of 79 symptoms. In a previous study, 337 Dutch ME/CFS patients were clustered based on their symptom scores. The symptom scores of post COVID-19 patients were applied to these clusters to examine whether the same or different clusters were found. Results: According to the FSS, fatigue was reported by 75.9% of the patients at 3–6 months after infection and by 57.1% of the patients 9–12 months later. Post-exertional malaise, sleep disturbances, pain, and neurocognitive symptoms were also frequently reported, according to the DSQ-2. Over half of the patients (52.7%) met the Fukuda criteria for ME/CFS, while fewer patients met other ME/CFS definitions. Clustering revealed specific symptom patterns and showed that post COVID-19 patients occurred in 11 of the clusters that have been observed in the ME/CFS cohort, where 2 clusters had > 10 patients. Conclusions: This study shows persistent fatigue and diverse symptomatology in post COVID-19 patients, up to 12–18 months after SARS-CoV-2 infection. Clustering showed that post COVID-19 patients occurred in 11 of the clusters that have been observed in the ME/CFS cohort. [ABSTRACT FROM AUTHOR]

Published

2024

11. The effects of the COVID‐19 pandemic on PICU admissions for severe asthma exacerbations: A single‐center experience.

Author

Bazdar, Somayeh, van den Berg, Sarah, Rutjes, Niels W., Bloemsma, Lizan D., Downward, George S., De Weger, Letty A., Terheggen‐Lagro, Suzanne W. J., van Wijck, Yolanda, Maitland van der Zee, Anke H., and Kapitein, Berber

Published

2024

12. Haemophilus influenzae and Moraxella catarrhalis in sputum of severe asthma with inflammasome and neutrophil activation.

Author

Versi, Ali, Ivan, Fransiskus Xaverius, Abdel‐Aziz, Mahmoud I., Bates, Stewart, Riley, John, Baribaud, Frederic, Kermani, Nazanin Zounemat, Montuschi, Paolo, Dahlen, Sven‐Erik, Djukanovic, Ratko, Sterk, Peter, Maitland‐Van Der Zee, Anke H., Chotirmall, Sanjay H., Howarth, Peter, Adcock, Ian M., Chung, Kian Fan, Andersson, LI, Auffray, C, Badi, YE, and Bakke, P

Subjects

HAEMOPHILUS influenzae, MORAXELLA catarrhalis, SPUTUM, ASTHMA, ASTHMATICS, HAEMOPHILUS diseases

Abstract

Background: Because of altered airway microbiome in asthma, we analysed the bacterial species in sputum of patients with severe asthma. Methods: Whole genome sequencing was performed on induced sputum from non‐smoking (SAn) and current or ex‐smoker (SAs/ex) severe asthma patients, mild/moderate asthma (MMA) and healthy controls (HC). Data were analysed by asthma severity, inflammatory status and transcriptome‐associated clusters (TACs). Results: α‐diversity at the species level was lower in SAn and SAs/ex, with an increase in Haemophilus influenzae and Moraxella catarrhalis, and Haemophilus influenzae and Tropheryma whipplei, respectively, compared to HC. In neutrophilic asthma, there was greater abundance of Haemophilus influenzae and Moraxella catarrhalis and in eosinophilic asthma, Tropheryma whipplei was increased. There was a reduction in α‐diversity in TAC1 and TAC2 that expressed high levels of Haemophilus influenzae and Tropheryma whipplei, and Haemophilus influenzae and Moraxella catarrhalis, respectively, compared to HC. Sputum neutrophils correlated positively with Moraxella catarrhalis and negatively with Prevotella, Neisseria and Veillonella species and Haemophilus parainfluenzae. Sputum eosinophils correlated positively with Tropheryma whipplei which correlated with pack‐years of smoking. α‐ and β‐diversities were stable at one year. Conclusions: Haemophilus influenzae and Moraxella catarrhalis were more abundant in severe neutrophilic asthma and TAC2 linked to inflammasome and neutrophil activation, while Haemophilus influenzae and Tropheryma whipplei were highest in SAs/ex and in TAC1 associated with highest expression of IL‐13 type 2 and ILC2 signatures with the abundance of Tropheryma whipplei correlating positively with sputum eosinophils. Whether these bacterial species drive the inflammatory response in asthma needs evaluation. [ABSTRACT FROM AUTHOR]

Published

2023

13. Neutrophil extracellular trap production and CCL4L2 expression influence corticosteroid response in asthma.

Author

Tsai, Ching-Hui, Lai, Alan Chuan-Ying, Lin, Yu-Cheng, Chi, Po-Yu, Chen, Yun-Chi, Yang, Yao-Hsu, Chen, Chien-Han, Shen, Sheng-Yeh, Hwang, Tsong-Long, Su, Ming-Wei, Hsu, I-Ling, Huang, Yu-Chi, Maitland-van der Zee, Anke H., McGeachie, Michael J., Tantisira, Kelan G., Chang, Ya-Jen, and Lee, Yungling L.

Subjects

GENE expression, ASTHMA, ASTHMA in children, NEUTROPHILS, LEUKOTRIENE antagonists, ADRENERGIC beta agonists, GENE regulatory networks

Abstract

The association between neutrophil extracellular traps (NETs) and response to inhaled corticosteroids (ICS) in asthma is unclear. To better understand this relationship, we analyzed the blood transcriptomes from children with controlled and uncontrolled asthma in the Taiwanese Consortium of Childhood Asthma Study using weighted gene coexpression network analysis and pathway enrichment methods. We identified 298 uncontrolled asthma-specific differentially expressed genes and one gene module associated with neutrophil-mediated immunity, highlighting a potential role for neutrophils in uncontrolled asthma. We also found that NET abundance was associated with nonresponse to ICS in patients. In a neutrophilic airway inflammation murine model, steroid treatment could not suppress neutrophilic inflammation and airway hyperreactivity. However, NET disruption with deoxyribonuclease I (DNase I) efficiently inhibited airway hyperreactivity and inflammation. Using neutrophil-specific transcriptomic profiles, we found that CCL4L2 was associated with ICS nonresponse in asthma, which was validated in human and murine lung tissue. CCL4L2 expression was also negatively correlated with pulmonary function change after ICS treatment. In summary, steroids fail to suppress neutrophilic airway inflammation, highlighting the potential need to use alternative therapies such as leukotriene receptor antagonists or DNase I that target the neutrophil-associated phenotype. Furthermore, these results highlight CCL4L2 as a potential therapeutic target for individuals with asthma refractory to ICS. Editor's summary: Many individuals with asthma are able to control disease with inhaled corticosteroid (ICS) treatment; however, a subset of patients fail to respond to ICS. To understand why, Tsai et al. identified differentially expressed genes in cells isolated from the blood of children with asthma that did or did not respond to ICS. The authors identified a neutrophil-associated phenotype that was associated with non-response to ICS. Neutrophil extracellular trap (NET) production similarly correlated with ICS responsiveness. In a mouse model of neutrophilic airway hyperreactivity, the authors found that treatment with DNase I, which can disrupt NET formation, reduced disease severity, whereas steroid treatment could not. Last, the authors demonstrate that neutrophil-produced CCL4L2 was also negatively associated with ICS responsiveness. Together, these results highlight both NETs and CCL4L2 as potential drivers and therapeutic targets for ICS-refractory asthma. —Courtney Malo [ABSTRACT FROM AUTHOR]

Published

2023

14. Analysis of Volatile Organic Compounds in Exhaled Breath Following a COMEX-30 Treatment Table.

Author

de Jong, Feiko J. M., Wingelaar, Thijs T., Brinkman, Paul, van Ooij, Pieter-Jan A. M., Maitland-van der Zee, Anke H., Hollmann, Markus W., and van Hulst, Rob A.

Subjects

DECOMPRESSION sickness, VOLATILE organic compounds, HYPERBARIC oxygenation

Abstract

The COMEX-30 hyperbaric treatment table is used to manage decompression sickness in divers but may result in pulmonary oxygen toxicity (POT). Volatile organic compounds (VOCs) in exhaled breath are early markers of hyperoxic stress that may be linked to POT. The present study assessed whether VOCs following COMEX-30 treatment are early markers of hyperoxic stress and/or POT in ten healthy, nonsmoking volunteers. Because more oxygen is inhaled during COMEX-30 treatment than with other treatment tables, this study hypothesized that VOCs exhaled following COMEX-30 treatment are indicators of POT. Breath samples were collected before and 0.5, 2, and 4 h after COMEX-30 treatment. All subjects were followed-up for signs of POT or other symptoms. Nine compounds were identified, with four (nonanal, decanal, ethyl acetate, and tridecane) increasing 33–500% in intensity from before to after COMEX-30 treatment. Seven subjects reported pulmonary symptoms, five reported out-of-proportion tiredness and transient ear fullness, and four had signs of mild dehydration. All VOCs identified following COMEX-30 treatment have been associated with inflammatory responses or pulmonary diseases, such as asthma or lung cancer. Because most subjects reported transient pulmonary symptoms reflecting early-stage POT, the identified VOCs are likely markers of POT, not just hyperbaric hyperoxic exposure. [ABSTRACT FROM AUTHOR]

Published

2023

15. A Systematic Review of Chest Imaging Findings in Long COVID Patients.

Author

Bazdar, Somayeh, Kwee, Anastasia K. A. L., Houweling, Laura, de Wit-van Wijck, Yolanda, Mohamed Hoesein, Firdaus A. A., Downward, George S., Nossent, Esther J., and Maitland-van der Zee, Anke H.

Subjects

POST-acute COVID-19 syndrome, COMPUTED tomography, VIRUS diseases, ENGLISH language

Abstract

Long COVID is the persistence of one or more COVID-19 symptoms after the initial viral infection, and there is evidence supporting its association with lung damage. In this systematic review, we provide an overview of lung imaging and its findings in long COVID patients. A PubMed search was performed on 29 September 2021, for English language studies in which lung imaging was performed in adults suffering from long COVID. Two independent researchers extracted the data. Our search identified 3130 articles, of which 31, representing the imaging findings of 342 long COVID patients, were retained. The most common imaging modality used was computed tomography (CT) (N = 249). A total of 29 different imaging findings were reported, which were broadly categorized into interstitial (fibrotic), pleural, airway, and other parenchymal abnormalities. A direct comparison between cases, in terms of residual lesions, was available for 148 patients, of whom 66 (44.6%) had normal CT findings. Although respiratory symptoms belong to the most common symptoms in long COVID patients, this is not necessarily linked to radiologically detectable lung damage. Therefore, more research is needed on the role of the various types of lung (and other organ) damage which may or may not occur in long COVID. [ABSTRACT FROM AUTHOR]

Published

2023

16. Cisplatin-induced nephrotoxicity in childhood cancer: comparison between two countries.

Author

Zazuli, Zulfan, Op 't Hoog, Catharina J. P., Vijverberg, Susanne J. H., Masereeuw, Rosalinde, Rassekh, Shahrad Rod, Medeiros, Mara, Rivas-Ruiz, Rodolfo, Maitland-van der Zee, Anke H., and Carleton, Bruce C.

Subjects

NEPHROTOXICOLOGY -- Risk factors, CONFIDENCE intervals, POPULATION geography, RETROSPECTIVE studies, ACQUISITION of data, PEDIATRICS, TUMORS in children, RISK assessment, COMPARATIVE studies, CISPLATIN, MEDICAL records, DESCRIPTIVE statistics, ACUTE kidney failure, LONGITUDINAL method, DISEASE risk factors

Abstract

Background: Various definitions used to describe cisplatin nephrotoxicity potentially lead to differences in determination of risk factors. This study evaluated incidence of kidney injury according to commonly used and alternative definitions in two cohorts of children who received cisplatin. Methods: This retrospective cohort study included children from Vancouver, Canada (one center), and Mexico City, Mexico (two centers), treated with cisplatin for a variety of solid tumors. Serum creatinine–based definitions (KDIGO and Pediatric RIFLE (pRIFLE)), electrolyte abnormalities consisted of hypokalemia, hypophosphatemia and hypomagnesemia (based on NCI-CTCAE v5), and an alternative definition (Alt-AKI) were used to describe nephrotoxicity. Incidence with different definitions, definitional overlap, and inter-definition reliability was analyzed. Results: In total, 173 children (100 from Vancouver, 73 from Mexico) were included. In the combined cohort, Alt-AKI criteria detected more patients with cisplatin nephrotoxicity compared to pRIFLE and KDIGO criteria (82.7 vs. 63.6 vs. 44.5%, respectively). Nephrotoxicity and all electrolyte abnormalities were significantly more common in Vancouver cohort than in Mexico City cohort except when using KDIGO definition. The most common electrolyte abnormalities were hypomagnesemia (88.9%, Vancouver) and hypophosphatemia (24.2%, Mexico City). The KDIGO definition provided highest overlap of cases in Vancouver (100%), Mexico (98.6%), and the combined cohort (99.4%). Moderate overall agreement was found among Alt-AKI, KDIGO, and pRIFLE definitions (κ = 0.18, 95% CI 0.1–0.27) in which KDIGO and pRIFLE showed moderate agreement (κ = 0.48, 95% CI 0.36–0.60). Conclusions: Compared to pRIFLE and KDIGO criteria, Alt-AKI criteria detected more patients with cisplatin nephrotoxicity. pRIFLE is more sensitive to detect not only actual kidney injury but also patients at risk of cisplatin nephrotoxicity, while KDIGO seems more useful to detect clinically significant kidney injury. A higher resolution version of the Graphical abstract is available as Supplementary information. [ABSTRACT FROM AUTHOR]

Published

2023

17. How paediatric drug development and use could benefit from OMICs: A c4c expert group white paper.

Author

Neumann, Eva, Schreeck, Filippa, Herberg, Jethro, Jacqz Aigrain, Evelyne, Maitland‐van der Zee, Anke H., Pérez‐Martínez, Antonio, Hawcutt, Daniel B., Schaeffeler, Elke, Rane, Anders, de Wildt, Saskia N., and Schwab, Matthias

Subjects

DRUG development, CLINICAL drug trials, DRUG utilization, PEDIATRICS, TECHNOLOGICAL innovations

Abstract

The safety and efficacy of pharmacotherapy in children, particularly preterms, neonates and infants, is limited by a paucity of good‐quality data from prospective clinical drug trials. A specific challenge is the establishment of valid biomarkers. OMICs technologies may support these efforts by complementary information about targeted and nontargeted molecules through systematic characterization and quantitation of biological samples. OMICs technologies comprise at least genomics, epigenomics, transcriptomics, proteomics, metabolomics and microbiomics in addition to the patient's phenotype. OMICs technologies are in part hypothesis‐generating, allowing an in depth understanding of disease pathophysiology and pharmacological mechanisms. Application of OMICs technologies in paediatrics faces major challenges before routine adoption. First, developmental processes need to be considered, including a subdivision into specific age groups as developmental changes clearly impact OMICs data. Second, compared to the adult population, the number of patients is limited as are the type and amount of necessary biomaterial, especially in neonates and preterms. Thus, advanced trial designs and biostatistical methods, noninvasive biomarkers, innovative biobanking concepts including data and samples from healthy children, as well as analytical approaches (eg liquid biopsies) should be addressed to overcome these obstacles. The ultimate goal is to link OMICs technologies with innovative analysis tools, such as artificial intelligence at an early stage. The use of OMICs data based on a feasible approach will contribute to the identification complex phenotypes and subpopulations of patients to improve the development of medicines for children with potential economic advantages. [ABSTRACT FROM AUTHOR]

Published

2022

18. Real‐life efficacy and safety of elexacaftor/tezacaftor/ivacaftor on severe cystic fibrosis lung disease patients.

Author

Kos, Renate, Neerincx, Anne H., Fenn, Dominic W., Brinkman, Paul, Lub, Rianne, Vonk, Steffie E. M., Roukema, Jolt, Reijers, Monique H., Terheggen‐Lagro, Suzanne W. J., Altenburg, Josje, Majoor, Christof J., Bos, Lieuwe D., Haarman, Eric G., and Maitland‐van der Zee, Anke H.

Subjects

PULMONARY fibrosis, CYSTIC fibrosis, LUNGS, LUNG diseases, WILCOXON signed-rank test

Abstract

Elexacaftor/tezacaftor/ivacaftor (ETI) is a cystic fibrosis (CF) transmembrane conductance regulator modulator, which has shown efficacy in CF patients (≥6 years) with ≥1 Phe508del mutation and a minimal function mutation. In October 2019, ETI became available on compassionate use basis for Dutch CF patients with severe lung disease. Our objective was to investigate safety and efficacy of ETI in this patient group in a real‐life setting. A multicenter longitudinal observational study was conducted to examine changes in FEV1, BMI, and adverse events at initiation and 1, 3, 6, and 12 months after starting ETI. The number of exacerbations was recorded in the 12 months before and the 12 months after ETI treatment. Patients eligible for compassionate use had a FEV1 <40% predicted. Wilcoxon signed‐rank test analyzed changes over time. Twenty subjects were included and followed up for up to 12 months after starting ETI. Treatment was well tolerated with mild side effects reported, namely, rash (15%) and stomach ache (20%) with 80% resolving within 1 month. Mean absolute increase of FEV1 was 11.8/13.7% (p ≤.001) and BMI was 0.49/1.87 kg/m2 (p <.001–0.02) after 1/12 months, respectively. In comparison to the number of exacerbations pretrial, there was a marked reduction in exacerbations after initiation. Our findings show long‐term effects of treatment with ETI in patients with severe CF lung disease in a real‐life setting. Treatment with ETI is associated with increased lung function and BMI, less exacerbations, and only mild side effects. [ABSTRACT FROM AUTHOR]

Published

2022

19. Asthma and Wheeze Severity and the Oropharyngeal Microbiota in Children and Adolescents.

Author

Thorsen, Jonathan, Stokholm, Jakob, Rasmussen, Morten Arendt, Roggenbuck-Wedemeyer, Michael, Vissing, Nadja H, Mortensen, Martin S, Brejnrod, Asker D, Fleming, Louise, Bush, Andrew, Roberts, Graham, Singer, Florian, Frey, Urs, Hedlin, Gunilla, Nordlund, Björn, Murray, Clare S, Abdel-Aziz, Mahmoud I, Hashimoto, Simone, van Aalderen, Wim, Maitland-van der Zee, Anke H, and Shaw, Dominick

Subjects

RESEARCH, ASTHMA, MICROBIOLOGY, PHENOMENOLOGICAL biology, RESEARCH methodology, EVALUATION research, RESPIRATORY organ sounds, COMPARATIVE studies, OROPHARYNX, BACTERIA

Abstract

Rationale: There is a major unmet need for improving the care of children and adolescents with severe asthma and wheeze. Identifying factors contributing to disease severity may lead to improved diagnostics, biomarkers, or therapies. The airway microbiota may be such a key factor. Objectives: To compare the oropharyngeal airway microbiota of children and adolescents with severe and mild/moderate asthma/wheeze. Methods: Oropharyngeal swab samples from school-age and preschool children in the European U-BIOPRED (Unbiased BIOmarkers in the PREDiction of respiratory disease outcomes) multicenter study of severe asthma, all receiving severity-appropriate treatment, were examined using 16S ribosomal RNA gene sequencing. Bacterial taxa were defined as amplicon sequence variants. Results: We analyzed 241 samples from four cohorts: A) 86 school-age children with severe asthma; B) 39 school-age children with mild/moderate asthma; C) 65 preschool children with severe wheeze; and D) 51 preschool children with mild/moderate wheeze. The most common bacteria were Streptococcus (mean relative abundance, 33.5%), Veillonella (10.3%), Haemophilus (7.0%), Prevotella (5.9%), and Rothia (5.5%). Age group (school-age vs. preschool) was associated with the microbiota in β-diversity analysis (F = 3.32, P = 0.011) and in a differential abundance analysis (28 significant amplicon sequence variants). Among all children, we found no significant difference in the microbiota between children with severe and mild/moderate asthma/wheeze in univariable β-diversity analysis (F = 1.99, P = 0.08, N = 241), but a significant difference in a multivariable model (F = 2.66, P = 0.035), including the number of exacerbations in the previous year. Age was also significant when expressed as a microbial maturity score (Spearman Rho, 0.39; P = 4.6 × 10-10); however, this score was not associated with asthma/wheeze severity. Conclusions: There was a modest difference in the oropharyngeal airway microbiota between children with severe and mild/moderate asthma/wheeze across all children but not in individual age groups, and a strong association between the microbiota and age. This suggests the oropharyngeal airway microbiota as an interesting entity in studying asthma severity, but probably without the strength to serve as a biomarker for targeted intervention. [ABSTRACT FROM AUTHOR]

Published

2022

20. Migration and allergic diseases: Findings from a population‐based study in adults in Amsterdam, the Netherlands.

Author

Amoah, Abena S., Prins, Maria, Bel, Elisabeth H. D., Fokkens, Wytske J., Zwinderman, Aeilko H., Yazdanbakhsh, Maria, Maitland‐van der Zee, Anke H., and van Ree, Ronald

Subjects

ALLERGIES, ADULTS, EMIGRATION & immigration, FOOD allergy, ALLERGIC rhinitis, ETHNIC groups, Q fever

Abstract

Additionally, increasing age at the time of migration was inversely associated with nasal allergy and asthma suggesting that older migrants may have had greater exposure to protective factors in their countries of origin prior to migration. Migration-related factors were "migrant generation" (second-generation ethnic minority versus first-generation ethnic minority), "age at the time of migration" and "residence duration in the Netherlands." To the Editor, Although international migration from low- and middle-income countries to high-income countries is associated with changing exposure to allergy risk factors, its role in allergic disease manifestation is understudied.1 We investigated migration-related factors and doctor-diagnosed allergic diseases among adults from five ethnic groups living in Amsterdam, the Netherlands enrolled in the population-based "Healthy Life in an Urban Setting" (HELIUS) study2,3 (see Methodology in Supplementary Material). [Extracted from the article]

Published

2022

21. Pharmacogenomic testing in paediatrics: Clinical implementation strategies.

Author

Barker, Charlotte I. S., Groeneweg, Gabriella, Maitland‐van der Zee, Anke H., Rieder, Michael J., Hawcutt, Daniel B., Hubbard, Tim J., Swen, Jesse J., and Carleton, Bruce C.

Subjects

PEDIATRICS, DRUG efficacy, CONSORTIA, MEDICAL research, CHILDREN'S health, CHILD patients

Abstract

Pharmacogenomics (PGx) relates to the study of genetic factors determining variability in drug response. Implementing PGx testing in paediatric patients can enhance drug safety, helping to improve drug efficacy or reduce the risk of toxicity. Despite its clinical relevance, the implementation of PGx testing in paediatric practice to date has been variable and limited. As with most paediatric pharmacological studies, there are well‐recognised barriers to obtaining high‐quality PGx evidence, particularly when patient numbers may be small, and off‐label or unlicensed prescribing remains widespread. Furthermore, trials enrolling small numbers of children can rarely, in isolation, provide sufficient PGx evidence to change clinical practice, so extrapolation from larger PGx studies in adult patients, where scientifically sound, is essential. This review paper discusses the relevance of PGx to paediatrics and considers implementation strategies from a child health perspective. Examples are provided from Canada, the Netherlands and the UK, with consideration of the different healthcare systems and their distinct approaches to implementation, followed by future recommendations based on these cumulative experiences. Improving the evidence base demonstrating the clinical utility and cost‐effectiveness of paediatric PGx testing will be critical to drive implementation forwards. International, interdisciplinary collaborations will enhance paediatric data collation, interpretation and evidence curation, while also supporting dedicated paediatric PGx educational initiatives. PGx consortia and paediatric clinical research networks will continue to play a central role in the streamlined development of effective PGx implementation strategies to help optimise paediatric pharmacotherapy. [ABSTRACT FROM AUTHOR]

Published

2022

22. Recent advances in the treatment of childhood asthma: a clinical pharmacology perspective.

Author

Alizadeh Bahmani, Amir Hossein, Abdel-Aziz, Mahmoud I., Maitland-van der Zee, Anke H., and Vijverberg, Susanne J.H.

Subjects

ASTHMA in children, CLINICAL pharmacology, INHALERS, TELEMEDICINE, PATIENT compliance, PEDIATRIC therapy, MEDICAL care

Abstract

Childhood asthma is a complex heterogenous inflammatory disease that can pose a large burden on patients and their caregivers. There is a strong need to adapt asthma treatment to the individual patient taking into account underlying inflammatory profiles, moving from a 'one size fits all' approach toward a much-needed personalized approach. This review article aims to provide an overview of recent advances in the management and treatment of pediatric asthma, including novel insights on the molecular heterogeneity of childhood asthma, the emergence of biologicals to treat severe asthma, and innovative e-health and home monitoring techniques to make asthma management more convenient and accessible. Molecular technologies have provided new treatment leads. E-health and home monitoring technologies have helped to gain more insights into disease dynamics and improve adherence to treatment while bringing health care to the patient. However, uncontrolled childhood asthma is still a major unmet clinical need and precision-medicine approaches are still scarce in clinical practice. Advanced omics methods may help researchers or clinicians to more accurately phenotype and treat subtypes of childhood asthma and gain more insight into the complexity of the disease. [ABSTRACT FROM AUTHOR]

Published

2022

23. Diagnostic Performance of Electronic Nose Technology in Sarcoidosis.

Author

van der Sar, Iris G., Moor, Catharina C., Oppenheimer, Judith C., Luijendijk, Megan L., van Daele, Paul L.A., Maitland-van der Zee, Anke H., Brinkman, Paul, and Wijsenbeek, Marlies S.

Subjects

SARCOIDOSIS, ELECTRONIC noses, INTERSTITIAL lung diseases, HYPERSENSITIVITY pneumonitis, PULMONARY fibrosis, VOLATILE organic compounds, SARCOIDOSIS diagnosis, ORGANIC compound analysis, CROSS-sectional method, ELECTRONIC equipment, RESPIRATION, BREATH tests, TECHNOLOGY

Abstract

Background: Diagnosing sarcoidosis can be challenging, and a noninvasive diagnostic method is lacking. The electronic nose (eNose) technology profiles volatile organic compounds in exhaled breath and has potential as a point-of-care diagnostic tool.Research Question: Can eNose technology be used to distinguish accurately between sarcoidosis, interstitial lung disease (ILD), and healthy control subjects, and between sarcoidosis subgroups?Study Design and Methods: In this cross-sectional study, exhaled breath of patients with sarcoidosis and ILD and healthy control subjects was analyzed by using an eNose (SpiroNose). Clinical characteristics were collected from medical files. Partial least squares discriminant and receiver-operating characteristic analyses were applied to a training and independent validation cohort.Results: The study included 252 patients with sarcoidosis, 317 with ILD, and 48 healthy control subjects. In the validation cohorts, eNose distinguished sarcoidosis from control subjects with an area under the curve (AUC) of 1.00 and pulmonary sarcoidosis from other ILD (AUC, 0.87; 95% CI, 0.82-0.93) and hypersensitivity pneumonitis (AUC, 0.88; 95% CI, 0.75-1.00). Exhaled breath of sarcoidosis patients with and without pulmonary involvement, pulmonary fibrosis, multiple organ involvement, pathology-supported diagnosis, and immunosuppressive treatment revealed no distinctive differences. Breath profiles differed between patients with a slightly and highly elevated soluble IL-2 receptor level (median cutoff, 772.0 U/mL; AUC, 0.78; 95% CI, 0.64-0.92).Interpretation: Patients with sarcoidosis can be distinguished from ILD and healthy control subjects by using eNose technology, indicating that this method may facilitate accurate diagnosis in the future. Further research is warranted to understand the value of eNose in monitoring sarcoidosis activity. [ABSTRACT FROM AUTHOR]

Published

2022

24. Primary ciliary dyskinesia in Volendam: Diagnostic and phenotypic features in patients with a CCDC114 mutation.

Author

Kos, Renate, Israëls, Joël, van Gogh, Christine D. L., Altenburg, Josje, Diepenhorst, Sandra, Paff, Tamara, Boon, Elles M. J., Micha, Dimitra, Pals, Gerard, Neerincx, Anne H., Maitland‐van der Zee, Anke H., and Haarman, Eric G.

Published

2022

25. Transcriptome changes during peanut oral immunotherapy and omalizumab treatment.

Author

Björkander, Sophia, Merid, Simon Kebede, Brodin, David, Brandström, Josef, Fagerström‐Billai, Fredrik, van der Heiden, Marieke, Konradsen, Jon R., Kabesch, Michael, van Drunen, Cornelis M., Golebski, Korneliusz, Maitland‐van der Zee, Anke H., Potočnik, Uroš, Vijverberg, Susanne J. H., Nopp, Anna, Nilsson, Caroline, Melén, Erik, and Peters, Rachel

Subjects

PEANUT allergy, OMALIZUMAB, FARNESOID X receptor, PEANUTS, REGULATORY T cells, TRANSCRIPTOMES

Abstract

We thank all FASTX patients for their participation and the research staff at Forskningscentrum, Södersjukhuset. All participants then underwent an open peanut challenge (pOIT start), before starting peanut OIT (pOIT) in combination with continued omalizumab treatment. The x-axis shows the gene ratio of the overlapping genes of our gene list with the pathway gene set. [Extracted from the article]

Published

2022

26. Increased day‐to‐day fluctuations in exhaled breath profiles after a rhinovirus challenge in asthma.

Author

Lammers, Ariana, Brinkman, Paul, te Nijenhuis, Louwrina H., Vries, Rianne, Dagelet, Yennece W. F., Duijvelaar, Erik, Xu, Binbin, Abdel‐Aziz, Mahmoud I., Vijverberg, Susanne J., Neerincx, Anne H., Frey, Urs, Lutter, Rene, Maitland‐van der Zee, Anke H., Sterk, Peter J., and Sinha, Anirban

Subjects

ASTHMA, MANN Whitney U Test, ELECTRONIC noses, RECEIVER operating characteristic curves, ADULTS, WHEEZE

Abstract

Background: Early detection/prediction of flare‐ups in asthma, commonly triggered by viruses, would enable timely treatment. Previous studies on exhaled breath analysis by electronic nose (eNose) technology could discriminate between stable and unstable episodes of asthma, using single/few time‐points. To investigate its monitoring properties during these episodes, we examined day‐to‐day fluctuations in exhaled breath profiles, before and after a rhinovirus‐16 (RV16) challenge, in healthy and asthmatic adults. Methods: In this proof‐of‐concept study, 12 atopic asthmatic and 12 non‐atopic healthy adults were prospectively followed thrice weekly, 60 days before, and 30 days after a RV16 challenge. Exhaled breath profiles were detected using an eNose, consisting of 7 different sensors. Per sensor, individual means were calculated using pre‐challenge visits. Absolute deviations (|%|) from this baseline were derived for all visits. Within‐group comparisons were tested with Mann‐Whitney U tests and receiver operating characteristic (ROC) analysis. Finally, Spearman's correlations between the total change in eNose deviations and fractional exhaled nitric oxide (FeNO), cold‐like symptoms, and pro‐inflammatory cytokines were examined. Results: Both groups had significantly increased eNose fluctuations post‐challenge, which in asthma started 1 day post‐challenge, before the onset of symptoms. Discrimination between pre‐ and post‐challenge reached an area under the ROC curve of 0.82 (95% CI = 0.65–0.99) in healthy and 0.97 (95% CI = 0.91–1.00) in asthmatic adults. The total change in eNose deviations moderately correlated with IL‐8 and TNFα (ρ ≈.50–0.60) in asthmatics. Conclusion: Electronic nose fluctuations rapidly increase after a RV16 challenge, with distinct differences between healthy and asthmatic adults, suggesting that this technology could be useful in monitoring virus‐driven unstable episodes in asthma. [ABSTRACT FROM AUTHOR]

Published

2021

27. Treating severe asthma: Targeting the IL‐5 pathway.

Author

Principe, Stefania, Porsbjerg, Celeste, Bolm Ditlev, Sisse, Kjærsgaard Klein, Ditte, Golebski, Korneliusz, Dyhre‐Petersen, Nanna, van Dijk, Yoni E., van Bragt, Job J.M.H., Dankelman, Lente L.H., Dahlen, Sven‐Erik, Brightling, Christopher E., Vijverberg, Susanne J.H., and Maitland‐van der Zee, Anke H.

Subjects

ASTHMA, NASAL polyps, BIOTHERAPY, CHILD patients, BIOMARKERS, BODY mass index

Abstract

Severe asthma is a heterogeneous disease with different phenotypes based on clinical, functional or inflammatory parameters. In particular, the eosinophilic phenotype is associated with type 2 inflammation and increased levels of interleukin (IL)‐4, IL‐5 and IL‐13). Monoclonal antibodies that target the eosinophilic inflammatory pathways (IL‐5R and IL‐5), namely mepolizumab, reslizumab, and benralizumab, are effective and safe for severe eosinophilic asthma. Eosinophils threshold represents the most indicative biomarker for response to treatment with all three monoclonal antibodies. Improvement in asthma symptoms scores, lung function, the number of exacerbations, history of late‐onset asthma, chronic rhinosinusitis with nasal polyposis, low oral corticosteroids use and low body mass index represent predictive clinical markers of response. Novel Omics studies are emerging with proteomics data and exhaled breath analyses. These may prove useful as biomarkers of response and non‐response biologics. Moreover, future biomarker studies need to be undertaken in paediatric patients affected by severe asthma. The choice of appropriate biologic therapy for severe asthma remains challenging. The importance of finding biomarkers that can predict response continuous an open issue that needs to be further explored. This review describes the clinical effects of targeting the IL‐5 pathway in severe asthma in adult and paediatric patients, focusing on predictors of response and non‐response. [ABSTRACT FROM AUTHOR]

Published

2021

28. Pharmacoepidemiology: A time for a new multidisciplinary approach to precision medicine.

Author

Issa, Amalia M., Carleton, Bruce, Gerhard, Tobias, Filipski, Kelly K., Freedman, Andrew N., Kimmel, Stephen, Liu, Geoffrey, Longo, Cristina, Maitland‐van der Zee, Anke H., Sansbury, Leah, Zhou, Wei, and Bartlett, Gillian

Abstract

The advent of the genomic age has created a rapid increase in complexity for the development and selection of drug treatments. A key component of precision medicine is the use of genetic information to improve therapeutic effectiveness of drugs and prevent potential adverse drug reactions. Pharmacoepidemiology, as a field, uses observational methods to evaluate the safety and effectiveness of drug treatments in populations. Pharmacoepidemiology by virtue of its focus, tradition, and research orientation can provide appropriate study designs and analysis methods for precision medicine. The objective of this manuscript is to demonstrate how pharmacoepidemiology can impact and shape precision medicine and serve as a reference for pharmacoepidemiologists interested in contributing to the science of precision medicine. This paper depicts the state of the science with respect to the need for pharmacoepidemiology and pharmacoepidemiological methods, tools and approaches for precision medicine; the need for and how pharmacoepidemiologists use their skills to engage with the precision medicine community; and recommendations for moving the science of precision medicine pharmacoepidemiology forward. We propose a new integrated multidisciplinary approach dedicated to the emerging science of precision medicine pharmacoepidemiology. [ABSTRACT FROM AUTHOR]

Published

2021

29. Association of endopeptidases, involved in SARS‐CoV‐2 infection, with microbial aggravation in sputum of severe asthma.

Author

Abdel‐Aziz, Mahmoud I., Kermani, Nazanin Zounemat, Neerincx, Anne H., Vijverberg, Susanne J. H., Guo, Yike, Howarth, Peter, Dahlen, Sven‐Erik, Djukanovic, Ratko, Sterk, Peter J., Kraneveld, Aletta D., Maitland‐van der Zee, Anke H., Chung, Kian Fan, and Adcock, Ian M.

Subjects

ENDOPEPTIDASES, ASTHMA, SARS-CoV-2, COUGH, SPUTUM, CELL receptors

Abstract

To the Editor, COVID-19 can be a serious multisystem disease caused by the SARS-CoV-2 coronavirus, and the current pandemic has affected more than 80 million people and caused nearly two million deaths worldwide. Therefore, the aim of this study was to investigate associations of sputum endopeptidases gene expression with metagenomics composition and whether they could be used to stratify asthma patients according to risk of SARS-CoV-2 infection. In contrast, non-T2 asthma, particularly neutrophilic asthma, has been associated with higher ACE2 and endopeptidases (TMPRSS2 and furin) expression as compared with the T2-high phenotype4,5 that might imply a worse outcome with COVID-19 infection. [Extracted from the article]

Published

2021

30. Nonadherence to inhaled corticosteroids: A characteristic of the pediatric obese‐asthma phenotype?

Author

Orriëns, Lynn B., Vijverberg, Susanne J.H., Maitland—van der Zee, Anke H., and Longo, Cristina

Published

2021

31. Early-life antibiotic use and risk of attention-deficit hyperactivity disorder and autism spectrum disorder: results of a discordant twin study.

Author

Slob, Elise M A, Brew, Bronwyn K, Vijverberg, Susanne J H, Dijs, Talitha, Beijsterveldt, Catharina E M van, Koppelman, Gerard H, Bartels, Meike, Dolan, Conor V, Larsson, Henrik, Lundström, Sebastian, Lichtenstein, Paul, Gong, Tong, Zee, Anke H Maitland-van der, Kraneveld, Aletta D, Almqvist, Catarina, Boomsma, Dorret I, van Beijsterveldt, Catharina E M, and Maitland-van der Zee, Anke H

Subjects

AUTISM spectrum disorders, ATTENTION-deficit hyperactivity disorder, TWIN studies, ANTIBIOTICS, TWINS, RESEARCH, RESEARCH methodology, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, LONGITUDINAL method

Abstract

Background: Development of the gut-brain axis in early life may be disturbed by antibiotic use. It has been hypothesized that this disturbance may contribute to development of neurodevelopmental disorders, including autism spectrum disorder and attention-deficit hyperactivity disorder. We aimed to assess the association between antibiotic use in early life and the risk of developing attention-deficit hyperactivity disorder or autism spectrum disorder, while controlling for shared genetic and environmental factors in a discordant twin design.Methods: We conducted a cohort study in twins (7-12 years; 25 781 twins) from the Netherlands Twin Register (NTR) and a replication study in the Childhood and Adolescent Twin Study in Sweden (CATSS; 7946 9-year-old twins). Antibiotic use was recorded before age 2 years. Attention-deficit hyperactivity disorder and autism spectrum disorder were parent-reported in the Netherlands Twin Register and register-based in the Childhood and Adolescent Twin Study in Sweden.Results: Early-life antibiotic use was associated with increased risk of attention-deficit hyperactivity disorder development [pooled odds ratio (OR) 1.10, 95% confidence interval (CI) 1.02-1.17] and autism spectrum disorder (pooled OR 1.15, 95% CI 1.06-1.25) in a case-control design. When restricting to monozygotic twin pairs discordant for the outcome, associations disappeared for both disorders in both cohorts (attention-deficit hyperactivity disorder OR 0.90, 95% CI 0.48-1.69 and OR 0.80, 95% CI 0.37-1.76, and autism spectrum disorder OR 0.66, 95% CI 0.38-1.16 and OR 0.29, 95% CI 0.02-4.50, respectively).Conclusions: Our findings suggest that the association between early-life antibiotic use and risk of attention-deficit hyperactivity and autism spectrum disorder may be confounded by shared familial environment and genetics. [ABSTRACT FROM AUTHOR]

Published

2021

32. Higher prescription of antidepressants and/or anxiolytics among chronic obstructive pulmonary disease patients.

Author

Pelgrim, Charlotte E., van den Heuvel, Jan Maurik, Folkerts, Gert, Garssen, Johan, Maitland-van der Zee, Anke H., and Kraneveld, Aletta D.

Subjects

OBSTRUCTIVE lung diseases, ORAL medication, TRANQUILIZING drugs, DRUG utilization, ANTIDEPRESSANTS

Abstract

Background: Chronic obstructive pulmonary disease (COPD) is often accompanied by psychiatric problems, such as depression and anxiety, affecting both treatment outcomes and mortality. Evidence for the number of COPD patients using medication for these disorders is sparse. In this study, chronic antidepressant (ATD) and anxiolytic (ANX) drug use – to identify depression and anxiety – among COPD patients was compared with subjects with or without other chronic diseases. Methods: The NControl database containing prescription data of 800 pharmacies including 7 million individuals in The Netherlands was used. Patients of age 55+ years who received frequent prescriptions – at least two/year in 5 out of 6 years – for COPD medication, dermatological drugs, disease-modifying antirheumatic drugs (DMARDs), statins and oral glucose-lowering medication were analyzed for concomitant chronic use of ATDs and ANXs between 1 January 2013 and 1 January 2019. All other subjects aged 55+ years were included as a control group (control group 1). This group was further stratified into a group of subjects that received frequent prescriptions of any kind (control group 2). Results: 15.2% of the patients that receive COPD treatment (n = 96,319), 15.3% of subjects that are treated for dermatological problems (n = 62,865), 13.2% of subjects that receive DMARDs (n = 7900), 11.6% of statins users (n = 422,376) and 11.4% of oral glucose-lowering medication users (n = 165,975) are also chronically treated for depression or anxiety, compared with 2.6% (control group 1; n = 3,290,608) and 11.4% (control group 2; n = 757,947). In general, female and 75+ years aged subjects showed a higher risk for using ATDs and ANXs chronically. In the COPD and the dermatological patient group the risk was the highest compared with the other patient groups. Conclusions: The rates of chronic ATD and ANX use and the risk of having depression and/or anxiety are especially high in COPD patients, indicating that psychiatric problems are more common in COPD than in most other chronic diseases. In general, age and gender strongly influence the risk of chronically using ATDs and ANXs. The reviews of this paper are available via the supplemental material section. [ABSTRACT FROM AUTHOR]

Published

2021

33. Higher prescription of antidepressants and/or anxiolytics among chronic obstructive pulmonary disease patients.

Author

Pelgrim, Charlotte E., van den Heuvel, Jan Maurik, Folkerts, Gert, Garssen, Johan, Maitland-van der Zee, Anke H., and Kraneveld, Aletta D.

Subjects

CHRONIC obstructive pulmonary disease, ANTIRHEUMATIC agents, TRANQUILIZING drugs, ORAL medication, ANTIDEPRESSANTS

Abstract

Background: Chronic obstructive pulmonary disease (COPD) is often accompanied by psychiatric problems, such as depression and anxiety, affecting both treatment outcomes and mortality. Evidence for the number of COPD patients using medication for these disorders is sparse. In this study, chronic antidepressant (ATD) and anxiolytic (ANX) drug use – to identify depression and anxiety – among COPD patients was compared with subjects with or without other chronic diseases. Methods: The NControl database containing prescription data of 800 pharmacies including 7 million individuals in The Netherlands was used. Patients of age 55+ years who received frequent prescriptions – at least two/year in 5 out of 6 years – for COPD medication, dermatological drugs, disease-modifying antirheumatic drugs (DMARDs), statins and oral glucose-lowering medication were analyzed for concomitant chronic use of ATDs and ANXs between 1 January 2013 and 1 January 2019. All other subjects aged 55+ years were included as a control group (control group 1). This group was further stratified into a group of subjects that received frequent prescriptions of any kind (control group 2). Results: 15.2% of the patients that receive COPD treatment (n = 96,319), 15.3% of subjects that are treated for dermatological problems (n = 62,865), 13.2% of subjects that receive DMARDs (n = 7900), 11.6% of statins users (n = 422,376) and 11.4% of oral glucose-lowering medication users (n = 165,975) are also chronically treated for depression or anxiety, compared with 2.6% (control group 1; n = 3,290,608) and 11.4% (control group 2; n = 757,947). In general, female and 75+ years aged subjects showed a higher risk for using ATDs and ANXs chronically. In the COPD and the dermatological patient group the risk was the highest compared with the other patient groups. Conclusions: The rates of chronic ATD and ANX use and the risk of having depression and/or anxiety are especially high in COPD patients, indicating that psychiatric problems are more common in COPD than in most other chronic diseases. In general, age and gender strongly influence the risk of chronically using ATDs and ANXs. The reviews of this paper are available via the supplemental material section. [ABSTRACT FROM AUTHOR]

Published

2021

34. Gut microbiota of adults with asthma is broadly similar to non-asthmatics in a large population with varied ethnic origins.

Author

Kullberg, Robert F. J., Haak, Bastiaan W., Abdel-Aziz, Mahmoud I., Davids, Mark, Hugenholtz, Floor, Nieuwdorp, Max, Galenkamp, Henrike, Prins, Maria, Maitland-van der Zee, Anke H., and Wiersinga, W. Joost

Published

2021

35. Exome Sequencing Reveals Common and Rare Variants in F5 Associated With ACE Inhibitor and Angiotensin Receptor Blocker–Induced Angioedema.

Author

Maroteau, Cyrielle, Siddiqui, Moneeza Kalhan, Veluchamy, Abirami, Carr, Fiona, White, Myra, Cassidy, Andrew J., Baranova, Ekaterina V., Rasmussen, Eva R., Eriksson, Niclas, Bloch, Katarzyna M., Brown, Nancy J., Bygum, Anette, Hallberg, Par, Karawajczyk, Malgorzata, Magnusson, Patrik K. E., Yue, Qun‐Ying, Syvänen, Ann‐Christine, Buchwald, Christian, Alfirevic, Ana, and Maitland‐van der Zee, Anke H.

Subjects

ANGIOTENSIN receptors, EXOMES, ANGIONEUROTIC edema, ACTIVATED protein C resistance, ASIANS, ACE inhibitors, ANGIOTENSIN-receptor blockers

Abstract

Angioedema occurring in the head and neck region is a rare and sometimes life‐threatening adverse reaction to angiotensin‐converting enzyme inhibitors (ACEIs) and angiotensin receptor blockers (ARBs). Few studies have investigated the association of common variants with this extreme reaction, but none have explored the combined influence of rare variants yet. Adjudicated cases of ACEI‐induced angioedema (ACEI‐AE) or ARB‐induced angioedema (ARB‐AE) and controls were recruited at five different centers. Sequencing of 1,066 samples (408 ACEI‐AE, ARB‐AE, and 658 controls) was performed using exome‐enriched sequence data. A common variant of the F5 gene that causes an increase in blood clotting (rs6025, p.Arg506Gln, also called factor V Leiden), was significantly associated with both ACEI‐AE and ARB‐AE (odds ratio: 2.85, 95% confidence interval (CI), 1.89–4.25). A burden test analysis of five rare missense variants in F5 was also found to be associated with ACEI‐AE or ARB‐AE, P = 2.09 × 10−3. A combined gene risk score of these variants, and the common variants rs6025 and rs6020, showed that individuals carrying at least one variant had 2.21 (95% CI, 1.49–3.27, P = 6.30 × 10−9) times the odds of having ACEI‐AE or ARB‐AE. The increased risk due to the common Leiden allele was confirmed in a genome‐wide association study from the United States. A high risk of angioedema was also observed for the rs6020 variant that is the main coagulation defect‐causing variant in black African and Asian populations. We found that deleterious missense variants in F5 are associated with an increased risk of ACEI‐AE or ARB‐AE. [ABSTRACT FROM AUTHOR]

Published

2020

36. Impact of a Gap Junction Protein Alpha 4 Variant on Clinical Disease Phenotype in F508del Homozygous Patients With Cystic Fibrosis.

Author

Horn, Tabea, Ludwig, Michael, Eickmeier, Olaf, Neerinex, Anne H., Maitland-van der Zee, Anke H., Smaczny, Christina, Wagner, Thomas O. F., Schubert, Ralf, Zielen, Stefan, Majoor, Christof, Bos, Lieuwe D., and Schmitt-Grohé, Sabina

Subjects

CYSTIC fibrosis, GTPASE-activating protein, CLINICAL trial registries, SINGLE nucleotide polymorphisms, PHENOTYPES, LUNG volume

Abstract

Background: Lung disease phenotype varies widely even in the F508del (homozygous) genotype. Leukocyte-driven inflammation is important for pulmonary disease pathogenesis in cystic fibrosis (CF). Blood cytokines correlate negatively with pulmonary function in F508del homozygous patients, and gap junction proteins (GJA) might be related to the influx of blood cells into the lung and influence disease course. We aimed to assess the relationship between GJA1/GJA4 genotypes and the clinical disease phenotype. Methods: One-hundred-and-sixteen homozygous F508del patients (mean age 27 years, m/f 66/50) were recruited from the CF centers of Bonn, Frankfurt, and Amsterdam. Sequence analysis was performed for GJA1 and GJA4. The clinical disease course was assessed over 3 years using pulmonary function tests, body mass index, Pseudomonas aeruginosa colonization, diabetes mellitus, survival to end-stage lung disease, blood and sputum inflammatory markers. Results: Sequence analysis revealed one clinically relevant single nucleotide polymorphism. In this GJA4 variant (rs41266431), homozygous G variant carriers (n = 84/116; 72.4%) had poorer pulmonary function (FVC% pred: mean 78/86, p < 0.040) and survival to end-stage lung disease was lower (p < 0.029). The frequency of P. aeruginosa colonization was not influenced by the genotype, but in those chronically colonized, those with the G/G genotype had reduced pulmonary function (FVC% pred: mean 67/80, p < 0.049). Serum interleukin-8 (median: 12.4/6.7 pg/ml, p < 0.052) and sputum leukocytes (2305/437.5 pg/ml, p < 0.025) were higher for the G/G genotype. Conclusions: In carriers of the A allele (27.6%) the GJA4 variant is associated with significantly better protection against end-stage lung disease and superior pulmonary function test results in F508del homozygous patients. This SNP has the potential of a modifier gene for phenotyping severity of CF lung disease, in addition to the CFTR genotype. Clinical Trial Registration: The study was registered with ClinicalTrials.gov, number NCT04242420, retrospectively on January 24th, 2020. [ABSTRACT FROM AUTHOR]

Published

2020

37. Cross‐sectional biomarker comparisons in asthma monitoring using a longitudinal design: The eNose premise.

Author

Abdel‐Aziz, Mahmoud I., de Vries, Rianne, Lammers, Ariana, Xu, Binbin, Neerincx, Anne H., Vijverberg, Susanne J. H., Dagelet, Yennece W. F., Kraneveld, Aletta D., Frey, Urs, Lutter, René, Sterk, Peter J., Maitland‐van der Zee, Anke H., and Sinha, Anirban

Subjects

ASTHMA, RECEIVER operating characteristic curves

Published

2020

38. Childhood asthma in the new omics era: challenges and perspectives.

Author

Golebski, Korneliusz, Kabesch, Michael, Melén, Erik, Potočnik, Uroš, van Drunen, Cornelis M., Reinarts, Susanne, Maitland-van der Zee, Anke H., Vijverberg, Susanne J. H., PERMEABLE consortium, and Reinartz, Susanne

Published

2020

39. Omics for the future in asthma.

Author

Abdel-Aziz, Mahmoud I., Neerincx, Anne H., Vijverberg, Susanne J., Kraneveld, Aletta D., and Maitland-van der Zee, Anke H.

Subjects

MORPHOLOGY, ASTHMA, INDIVIDUALIZED medicine, RESEARCH teams, ASTHMATICS

Abstract

Asthma is a common, complex, multifaceted disease. It comprises multiple phenotypes, which might benefit from treatment with different types of innovative targeted therapies. Refining these phenotypes and understanding their underlying biological structure would help to apply precision medicine approaches. Using different omics methods, such as (epi)genomics, transcriptomics, proteomics, metabolomics, microbiomics, and exposomics, allowed to view and investigate asthma from diverse angles. Technological advancement led to a large increase in the application of omics studies in the asthma field. Although the use of omics technologies has reduced the gap between bench to bedside, several design and methodological challenges still need to be tackled before omics can be applied in asthma patient care. Collaborating under a centralized harmonized work frame (such as in consortia, under consistent methodologies) could help worldwide research teams to tackle these challenges. In this review, we discuss the transition of single biomarker research to multi-omics studies. In addition, we deliberate challenges such as the lack of standardization of sampling and analytical methodologies and validation of findings, which comes in between omics and personalized patient care. The future of omics in asthma is encouraging but not completely clear with some unanswered questions, which have not been adequately addressed before. Therefore, we highlight these questions and emphasize on the importance of fulfilling them. [ABSTRACT FROM AUTHOR]

Published

2020

40. Precision medicine in severe pediatric asthma: opportunities and challenges.

Author

Vijverberg, Susanne J. H., Brinkman, Paul, Rutjes, Niels W. P., and Maitland-van der Zee, Anke H.

Published

2020

41. What did we learn from multiple omics studies in asthma?

Author

Ivanova, Olga, Richards, Levi B., Vijverberg, Susanne J., Neerincx, Anne H., Sinha, Anirban, Sterk, Peter J., and Maitland‐van der Zee, Anke H.

Subjects

ASTHMA, HUMAN genome, INDIVIDUALIZED medicine

Abstract

More than a decade has passed since the finalization of the Human Genome Project. Omics technologies made a huge leap from trendy and very expensive to routinely executed and relatively cheap assays. Simultaneously, we understood that omics is not a panacea for every problem in the area of human health and personalized medicine. Whilst in some areas of research omics showed immediate results, in other fields, including asthma, it only allowed us to identify the incredibly complicated molecular processes. Along with their possibilities, omics technologies also bring many issues connected to sample collection, analyses and interpretation. It is often impossible to separate the intrinsic imperfection of omics from asthma heterogeneity. Still, many insights and directions from applied omics were acquired—presumable phenotypic clusters of patients, plausible biomarkers and potential pathways involved. Omics technologies develop rapidly, bringing improvements also to asthma research. These improvements, together with our growing understanding of asthma subphenotypes and underlying cellular processes, will likely play a role in asthma management strategies. [ABSTRACT FROM AUTHOR]

Published

2019

42. FCER2 T2206C variant associated with FENO levels in asthmatic children using inhaled corticosteroids: The PACMAN study.

Author

Karimi, Leila, Vijverberg, Susanne J.H., Farzan, Niloufar, Ghanbari, Mohsen, Verhamme, Katia M.C., and Maitland‐van der Zee, Anke H.

Subjects

GENETIC models, FOREST measurement, CORTICOSTEROIDS, REGRESSION analysis, LINEAR statistical models

Abstract

Background: The FCER2 gene, via encoding of the CD23 receptor, plays an important role in the regulation of IgE responses. A genetic variant of the FCER2 gene (T2206C) was previously shown to be associated with IgE levels in asthmatic children. IgE sensitization has also been linked to increased levels of fractional exhaled nitric oxide (FENO). Objective: To investigate whether the FCER2 T2206C variant influences FENO levels in asthmatic children with a reported use of inhaled corticosteroids (ICS). Methods: This cross‐sectional study involved 593 asthmatic children with a reported use of ICS, availability of FENO measurements and genotyping data on the FCER2 T2206C variant (rs28364072). An additive genetic model was assumed, and the association between the FCER2 T2206C variant and the log‐transformed (ln) FENO levels was evaluated using linear regression analysis, adjusted for age, sex, adapted British Thoracic Society (BTS) treatment steps and atopy. Results: The mean age of the population was 9.1 ± 2.2 years, and the median of FENO levels was 13.0 ppb with an interquartile range (IQR) of (8.0‐27.5 ppb). The minor allele (G) frequency of rs28364072 was 29.6%, and each extra copy of the G allele was significantly associated with a lower level of the geometric mean of FENO (log scale, β = −0.12, 95% CI: −0.23, −0.02). Conclusion and Clinical Relevance: Our results showed that the FCER2 T2206C variant was significantly associated with lower FENO levels in carriers of the G allele. Nevertheless, this SNP contributed little to the variability in FENO levels in this patient population. Our findings contribute to the present knowledge on FENO in asthmatic children; however, future replication studies are required to establish the role of this gene in relation to FENO. [ABSTRACT FROM AUTHOR]

Published

2019

43. The crosstalk between microbiome and asthma: Exploring associations and challenges.

Author

Abdel‐Aziz, Mahmoud I., Vijverberg, Susanne J. H., Neerincx, Anne H., Kraneveld, Aletta D., and Maitland‐van der Zee, Anke H.

Subjects

ASTHMA, RNA sequencing, CROSSTALK, GUT microbiome

Abstract

With the advancement of high‐throughput DNA/RNA sequencing and computational analysis techniques, commensal bacteria are now considered almost as important as pathological ones. Understanding the interaction between these bacterial microbiota, host and asthma is crucial to reveal their role in asthma pathophysiology. Several airway and/or gut microbiome studies have shown associations between certain bacterial taxa and asthma. However, challenges remain before gained knowledge from these studies can be implemented into clinical practice, such as inconsistency between studies in choosing sampling compartments and/or sequencing approaches, variability of results in asthma studies, and not taking into account medication intake and diet composition especially when investigating gut microbiome. Overcoming those challenges will help to better understand the complex asthma disease process. The therapeutic potential of using pro‐ and prebiotics to prevent or reduce risk of asthma exacerbations requires further investigation. This review will focus on methodological issues regarding setting up a microbiome study, recent developments in asthma bacterial microbiome studies, challenges and future therapeutic potential. [ABSTRACT FROM AUTHOR]

Published

2019

44. Drug‐Induced Liver Injury due to Flucloxacillin: Relevance of Multiple Human Leukocyte Antigen Alleles.

Author

Nicoletti, Paola, Aithal, Guruprasad P., Chamberlain, Thomas C., Coulthard, Sally, Alshabeeb, Mohammad, Grove, Jane I., Andrade, Raul J., Bjornsson, Einar, Dillon, John F., Hallberg, Par, Lucena, M. Isabel, Maitland‐van der Zee, Anke H., Martin, Jennifer H., Molokhia, Mariam, Pirmohamed, Munir, Wadelius, Mia, Shen, Yufeng, Nelson, Matthew R., and Daly, Ann K.

Subjects

HLA histocompatibility antigens, LIVER injuries, AMINO acid sequence, ALLELES, ODDS ratio, DISEASE risk factors

Abstract

Some patients prescribed flucloxacillin (~ 0.01%) develop drug‐induced liver injury (DILI). HLA‐B*57:01 is an established genetic risk factor for flucloxacillin DILI. To consolidate this finding, identify additional genetic factors, and assess relevance of risk factors for flucloxacillin DILI in relation to DILI due to other penicillins, we performed a genomewide association study involving 197 flucloxacillin DILI cases and 6,835 controls. We imputed single‐nucleotide polymorphism and human leukocyte antigen (HLA) genotypes. HLA‐B*57:01 was the major risk factor (allelic odds ratio (OR) = 36.62; P = 2.67 × 10−97). HLA‐B*57:03 also showed an association (OR = 79.21; P = 1.2 × 10−6). Within the HLA‐B protein sequence, imputation showed valine97, common to HLA‐B*57:01 and HLA‐B*57:03, had the largest effect (OR = 38.1; P = 9.7 × 10−97). We found no HLA‐B*57 association with DILI due to other isoxazolyl penicillins (n = 6) or amoxicillin (n = 15) and no significant non‐HLA signals for any penicillin‐related DILI. [ABSTRACT FROM AUTHOR]

Published

2019

45. Blood Eosinophil Counts, Withdrawal of Inhaled Corticosteroids and Risk of COPD Exacerbations and Mortality in the Clinical Practice Research Datalink (CPRD).

Author

Oshagbemi, Olorunfemi A., Franssen, Frits M.E., van Kraaij, Suzanne, Braeken, Dionne C.W., Wouters, Emiel F.M., Maitland-van der Zee, Anke H., Driessen, Johanna H.M., and de Vries, Frank

Subjects

BRONCHIECTASIS, MYOCARDIAL infarction, OBSTRUCTIVE lung diseases, ARRHYTHMIA, PULMONARY fibrosis, BLOOD

Abstract

Although recently introduced in the pharmacological treatment algorithm of chronic obstructive pulmonary disease (COPD), there is a need for more data supporting the use of blood eosinophil counts as a biomarker to guide inhaled corticosteroids (ICS) therapy. The aim of this study was to evaluate the risk of moderate and/or severe exacerbations and all-cause mortality in a large primary care population after withdrawal of ICS compared to continued users stratified by elevated blood eosinophil counts. In this population based cohort study, we used data from the Clinical Practice Research Datalink (CPRD) in the United Kingdom. We included subjects' aged 40 years or more who had a diagnosis of COPD. We excluded subjects with a history of asthma, pulmonary fibrosis, cardiac arrhythmia and bronchiectasis, COPD exacerbations occurring within 6 weeks prior to index date, or with a myocardial infarction within 3 months prior to index date. Continuous users were subjects who received their most recent ICS prescription within 3 months before the start of an interval. ICS withdrawals were those who discontinued ICS for more than 3 months. We evaluated the risk of moderate and/or severe exacerbations and all-cause mortality among subjects with various blood eosinophil thresholds who withdrew from ICS compared to continuous ICS users with elevated blood eosinophil levels using Cox regression analysis adjusted for potential confounders. We identified 48,157 subjects diagnosed with COPD between 1 January 2005 to 31 January 2014. Withdrawal of ICS was not associated with an increased risk of moderate-to-severe exacerbations among subjects with absolute blood eosinophil counts ≥0.34 × 109 cells/L [adjusted hazard ratio (adj. HR) 0.72; 95% confidence interval (CI) 0.63–0.81] or relative counts ≥ 4.0% (adj. HR 0.72; 95% CI: 0.66–0.78). Similarly, withdrawal of ICS was not associated with an increased risk of severe exacerbations among subjects with absolute blood eosinophil ≥0.34 × 109 cells/L (adj. HR 0.82; 95% CI: 0.61–1.10) or relative blood eosinophil counts ≥4.0% (adj. HR 0.80; 95% CI: 0.61–1.04). No increased risk of all-cause mortality was observed among subjects who withdrew from ICS irrespective of elevated absolute or relative blood eosinophil counts. In a real-world primary care population, we did not observe an increased risk of moderate and/or severe COPD exacerbations or all-cause mortality among subjects with eosinophilia who withdrew their use of ICS. [ABSTRACT FROM AUTHOR]

Published

2019

46. Pharmacogenetics of inhaled long‐acting beta2‐agonists in asthma: A systematic review.

Author

Slob, Elise M. A., Vijverberg, Susanne J. H., Palmer, Colin N. A., Zazuli, Zulfan, Farzan, Niloufar, Oliveri, Nadia M. B., Pijnenburg, Mariëlle W., Koppelman, Gerard H., and Maitland‐van der Zee, Anke H.

Subjects

ADRENERGIC beta agonists, ASTHMA treatment, ASTHMATICS, PHARMACOGENOMICS, SYSTEMATIC reviews

Abstract

Background: Long‐acting beta2‐agonists (LABA) are recommended in asthma therapy; however, not all asthma patients respond well to LABA. We performed a systematic review on genetic variants associated with LABA response in patients with asthma. Methods: Articles published until April 2017 were searched by two authors using PubMed and EMBASE. Pharmacogenetic studies in patients with asthma and LABA response as an outcome were included. Results: In total, 33 studies were included in this systematic review; eight focused on children (n = 6051). Nineteen studies were clinical trials, while 14 were observational studies. Studies used different outcomes to define LABA response, for example, lung function measurements (FEV1, PEF, MMEF, FVC), exacerbations, quality of life, and asthma symptoms. Most studies (n = 30) focused on the ADRB2 gene, encoding the beta2‐adrenergic receptor. Thirty studies (n = 14 874) addressed ADRB2 rs1042713, 7 ADRB2 rs1042714 (n = 1629), and 3 ADRB2 rs1800888 (n = 1892). The association of ADRB2 rs1042713 and rs1800888 with LABA response heterogeneity was successfully replicated. Other variants were only studied in three studies but not replicated. One study focused on the ADCY9 gene. Five studies and a meta‐analysis found an increased risk of exacerbations in pediatrics using LABA carrying one or two A alleles (OR 1.52 [1.17; 1.99]). These results were not confirmed in adults. Conclusions: ADRB2 rs1042713 variant is most consistently associated with response to LABA in children but not adults. To assess the clinical value of ADRB2 rs1042713 in children with asthma using LABA, a randomized clinical trial with well‐defined outcomes is needed. [ABSTRACT FROM AUTHOR]

Published

2018

47. Prescription patterns of angiotensin‐converting enzyme inhibitors for various indications: A UK population‐based study.

Author

Mahmoudpour, Seyed Hamidreza, Asselbergs, Folkert W., Souverein, Patrick C., de Boer, Anthonius, and Maitland‐van der Zee, Anke H.

Subjects

ANGIOTENSIN converting enzyme, MEDICAL records, ANGIOTENSIN II, ANTIHYPERTENSIVE agents, RETROSPECTIVE studies

Abstract

Aim: Angiotensin‐converting enzyme inhibitors (ACEIs) are widely prescribed for several cardiovascular indications. This study investigated patterns of ACEI use for various indications. Methods: A descriptive, retrospective population‐based study was conducted using data from the UK Clinical Practice Research Datalink. Patients starting ACEIs (2007–2014) were selected and ACEI indications were retrieved from electronically recorded medical records. Stratified by indication, we distinguished between persistent and nonpersistent ACEI use, considering a 6‐month interval between two prescription periods as a maximum for persistent use. Five‐year persistence rates for various indications were calculated using the Kaplan–Meier method and compared in a log‐rank test. Nonpersistent users were subdivided into three groups: (i) stop; (ii) restart; and (iii) switch to an angiotensin II‐receptor blocker. Patients who received ACEIs for hypertension who switched to other classes of antihypertensive medications were further investigated. Results: In total, 254 002 ACEI initiators were identified with hypertension (57.6%), myocardial infarction (MI; 4.2%), renal disease (RD; 3.7%), heart failure (HF; 1.5%), combinations of the above (17.2%) or none of the above (15.8%). Five‐year persistence rates ranged from 43.2% (RD) to 68.2% (MI; P < 0.0001). RD and HF patients used ACEIs for the shortest time (average 23.6 and 25.0 months, respectively). For the nonpersistent group, the percentage of switchers to angiotensin II‐receptor blockers ranged from 27.6% (RD) to 42.2% (MI) and the restarters ranged from 15.0% (HF) to 18.1% (group without indication). Conclusions: Depending on the indication, there are various rates of ACEI nonpersistence. Patients with RD are most likely to discontinue treatment. [ABSTRACT FROM AUTHOR]

Published

2018

48. Use of oral immunosuppressive drugs in the treatment of atopic dermatitis in the Netherlands.

Author

Garritsen, F. M., van den Heuvel, J. M., Bruijnzeel-Koomen, C. A. F. M., Maitland-van der Zee, A. H., van den Broek, M. P. H., and de Bruin-Weller, M. S.

Subjects

IMMUNOSUPPRESSIVE agents, ATOPIC dermatitis, SKIN diseases, PHARMACY databases, CYCLOSPORINE

Abstract

Background Although atopic dermatitis (AD) is a very common skin disease, data on the percentage of patients with really difficult-to-treat AD are scarce. From socio-economic perspective, it is important to have more insight into these numbers, as new very effective, but expensive, treatment options will be available in the near future for difficult-to-treat AD. Estimating the number of patients with AD using oral immunosuppressive drugs can give an impression of the percentage of difficult-to-treat patients in the total AD population. Objective To give an overview of the use of oral immunosuppressive drugs in patients with AD in the Netherlands. Methods Prescription data of oral immunosuppressive drugs in the Netherlands were extracted from a pharmaceutical database (NControl) containing data of 557 million prescriptions and 7.2 million patients. An algorithm, based on the WHO Anatomical Therapeutic Chemical (ATC) codes, was used to identify patients with AD. The prescription of oral immunosuppressive drugs in patients with AD between 1 January 2012 and 1 January 2017 was evaluated. Results Based on the algorithm, 65 943 patients with AD were selected. 943 patients with AD (1.4%) used cyclosporine A, methotrexate, azathioprine or mycophenolic acid. Methotrexate was most commonly used, followed by azathioprine and cyclosporine A. A switch in medication was rarely seen. In the evaluation period, a decrease in the prescription of cyclosporine A was seen, together with an increase in the prescription of methotrexate. In 31% of the patients who stopped treatment, the discontinuation took place within the first months of treatment. Conclusion In this study population, 1.4% of the patients with AD used oral immunosuppressive drugs for their eczema in a 5-year period. Methotrexate was the most commonly used systemic drug in the Netherlands for the treatment of AD. [ABSTRACT FROM AUTHOR]

Published

2018

49. The use of pharmacogenomics, epigenomics, and transcriptomics to improve childhood asthma management: Where do we stand?

Author

Farzan, Niloufar, Vijverberg, Susanne J., Kabesch, Michael, Sterk, Peter J., and Maitland-van der Zee, Anke H.

Published

2018

50. Patterns of topical corticosteroids prescriptions in children with asthma.

Author

Arabkhazaeli, Ali, Vijverberg, Susanne J. H., van der Lee, Maaike, van der Ent, Cornelis K., Bruijnzeel‐Koomen, Carla A., de Bruin‐Weller, Marjolein S., Raaijmakers, Jan A., and Maitland‐van der Zee, Anke H.

Subjects

CORTICOSTEROIDS, DRUG prescribing, ASTHMA in children, DRUG efficacy, DISEASE incidence, CHI-squared test, GENERAL practitioners, ATOPIC dermatitis, PHYSICIANS' attitudes

Abstract

Abstract: Objectives: To study topical corticosteroid use in Dutch asthmatic children using pharmacy dispensing data and to assess whether Dutch physicians prescribe topical corticosteroids in this population according to clinical guidelines. Methods: Medication histories of children using asthma medication were extracted from the pharmacy dispensing system in 100 Dutch community pharmacies. The incidence rate and the potency of topical corticosteroid prescriptions per age were assessed. The topical corticosteroid incidence rates of the different age groups were compared using the Pearson chi‐square test. Generalized linear models were used to study the prescription behavior of general practitioners and atopic dermatitis‐related specialists regarding different classes of topical corticosteroids. Results: Thirty percent of the infants received a topical corticosteroid prescription, compared with 15%‐18% of the children aged 4 and older. Similarly, the mean number of topical corticosteroid prescriptions in infants was 2.2 per year, compared with 1.6‐1.9 in children aged 4 and older. In concordance with the clinical guidelines, we observed that atopic dermatitis‐related specialists more often prescribed first prescriptions of potent and very potent topical corticosteroids than general practitioners (relative risk = 2.55, 95% confidence interval = 1.79‐3.63). Statistically significant differences (P < .01) were found between potencies of prescribed topical corticosteroids. Conclusion: Younger children receive more topical corticosteroid prescriptions than children aged 4 and older, and there is a statistically significantly higher prescription rate of topical corticosteroid for infants. Sometimes general practitioners do not follow guidelines and prescribe more‐potent topical corticosteroids without a prior prescription of the same potency by a specialist. [ABSTRACT FROM AUTHOR]

Published

2018