Luisa Brussino

Respiratory function in systemic lupus erythematosus: relation with activity and severity

OBJECTIVES To determine whether patients with primary Sjögrens syndrome (SS), diagnosed according to San Diego criteria, had improvement in their laboratory or clinical features during treatment with hydroxychloroquine (6-7 mg/kg/day) for at least two years. METHODS The study population included 50 consecutive patients with primary SS who were diagnosed according to San Diego criteria, and in whom hydroxychloroquine was suggested as treatment. This group included 10 patients who were early dropouts (side effects or desire not to take antimalarial drugs) and 40 patients who received drugs for at least two years (range 24-48 months). In a subset of SS patients, values for ESR (westergren) and quantitative immunoglobulins were available for comparison. Improvement with therapy was defined as: (a) > or = 20% improvement in variables of tear flow (Schirmers test I) or corneal integrity (rose Bengal): (b) > or = 20% salivary function (flow rate); and (c) improvement in at least two of the following measures: physicians assessment of global disease activity by > or = 20%, patient assessment of improvement in pain or fatigue by > or = 20%, and ESR improved by > or = 20 mm/hr. RESULTS In a retrospective study of SS patients who completed the trial, a significant improvement was noted in ocular symptoms (pain and dryness) in patients (55 and 57%) and improved corneal integrity (rose Bengal straining) in 53% of patients. The Schirmers test was improved by > or = 2 mm/5 minutes in 50% in patients. Improvement was noted in oral symptoms (pain and dryness) in patients (57 and 60%) and salivary flow rate was increased in 82% of patients. In a subset of SS patients evaluated, the ESR improved by > or = 20 mm/hr in 17/32 patients (53%) and quantitative IgG level by > or = 20% in 8/13 patients (61%). Physician global assessment of overall patient status and patient assessment of overall status indicated improvement in over 62% of patients. CONCLUSION In a retrospective study of patients fulfilling San Diego Criteria for SS, we found: (a) sustained improvement of local symptoms (painful eyes, painful mouth) and improvement of systemic manifestations (arthralgias and myalgias) after treatment with hydroxychloroquine 6-7 mg/kg/day over mean three-year follow-up; (b) laboratory analysis showed a significant improvement in their ESR and their quantitative IgG levels; (c) no significant late toxicity was observed in this study cohort. A prospective study of hydroxychloroquine in patients fulfilling San Diego criteria for SS is indicated.The objective of this study was to examine the relation between respiratory function tests, disease activity and disease severity in ambulatory patients with systemic lupus erythematosus (SLE) who did not present with overt respiratory problems. Lung volumes, maximal expiratory flows at 50% and 25% of vital capacity (MEF50 and MEF25), bronchial threshold to methacholine (PD15FEV 1), transfer factor CO (KCO) were measured in 24 consecutive SLE outpatients (22 women, age 41 ± 14.8 years) and in 24 healthy controls matched for age and sex. In SLE patients alveolar-arterial oxygen gradient (AaO2) was also measured. Disease activity was assessed by European Consensus Lupus Activity Measurement (ECLAM) scoring system and disease severity by Lupus Severity of Disease Index. In comparison to controls SLE patients showed a significant decrease of total lung capacity (TLC) (91.7 ± 16.5 vs 102.7 ± 12.9% predicted, P < 0.01), MEF25 (58.4 ± 25.2 vs 73.5 ± 19.5% predicted, P < 0.005), PD15FEV1 (2164 ± 1122 vs 4230 ± 1014 μg methacholine, P < 0.0001) and KCO (77.1 ± 20.5 vs 96.3 ± 12.4% predicted, P < 0.001). AaO2 (mean value 13.2 ± 8.4) was abnormally high (>20 mm Hg) in 12 patients. The ECLAM score of activity was inversely related with KCO (r = 0.48, P < 0.02). The severity index was significantly related with FEV1/VC ratio (r = 0.43, P < 0.05), MEF50 (r = 0.51, P < 0.01), MEF25 (r = 0.40, P < 0.05) and PD15FEV1 (r = 0.51, P < 0.01). In eight patients, evaluated also after treatment intensification, there was a significant increase in KCO (from 71.8 ± 24.7 to 84.9 ± 22.3% predicted, P < 0.01) along with a decrease in ECLAM score (from 3.0 ± 1.34 to 0.69 ± 0.75, P < 0.01). The relation between disease activity and KCO suggests a relation between systemic and alveolar inflammation whereas the relation between severity index, airway patency and reactivity indices suggests a cumulative damage to the airways in SLE patients, even in the absence of overt respiratory manifestations.

Exhaled Nitric Oxide and Impaired Oxygenation in Cirrhotic Patients before and after Liver Transplantation

Abnormalities of arterial oxygenation are common in patients with cirrhosis [1], and a widened alveolar-arterial oxygen gradient is reported in more than half of these patients at pretransplantation assessment of pulmonary function [2, 3]. Increasing evidence suggests that the abnormal gas exchange in cirrhotic patients is primarily due to intrapulmonary vasodilatations, which cause ventilation-perfusion mismatch and impaired diffusion [4]. Increased circulation of a pulmonary vasodilator seems to be the favored mechanism for intrapulmonary vasodilatations, and recent evidence points to nitric oxide as the most important vasodilating substance [5]. Increased nitric oxide output in exhaled air has been reported in patients with advanced cirrhosis [6], and a correlation between exhaled nitric oxide concentrations and alveolar-arterial oxygen gradient was recently shown in 45 patients with cirrhosis [7]. After successful liver transplantation, oxygenation has been reported to improve in most patients [3]. In a limited series of three patients with full-blown hepatopulmonary syndrome characterized by severe hypoxemia and evidence of intrapulmonary shunting, the increased amount of exhaled nitric oxide reportedly decreased to within the normal range in one patient after successful liver transplantation [8]. To further investigate the association between nitric oxide produced in the lung and oxygenation abnormalities in patients with cirrhosis, we sought to determine exhaled nitric oxide and oxygenation measures before and after liver transplantation in a selected group of patients with cirrhosis who did not have obvious cardiorespiratory diseases. Methods Patients Twenty patients who underwent successful orthotopic liver transplantation at our hospital from August 1995 to February 1997 were recruited for our study. These patients came from a group of 45 patients who were evaluated at the Outpatient Clinic for Liver Cirrhosis during a scheduled visit [7]. All patients gave their informed consent to participate in the study, which was approved by the ethical committee. Included patients had to have been evaluated within 8 weeks before transplantation. Exclusion criteria were respiratory and cardiovascular disease, including clinically significant pleural effusion (larger than costophrenic angle on chest radiography); tense ascites; inability to perform lung function tests; current smoking habit or a smoking history of more than 10 packs per year (1 pack per year = 20 cigarettes per day for 1 year); forced vital capacity (FVC) and FEV (1) less than 80% of predicted; FEV1/FVC 100 less than 70%; and an airway infection in the previous 4 weeks. All patients were reevaluated 3 to 12 months after transplantation. Laboratory Testing Patients underwent the following studies: pulmonary function tests, arterial blood gas analysis done while patients were breathing room air in a seated position, contrast-enhanced echocardiography, and measurement of nitric oxide in exhaled air. The hepatopulmonary syndrome was defined as an alveolar-arterial oxygen gradient greater than 15 mm Hg and echocardiographic evidence of intrapulmonary vasodilatations [4]. Lung volumes and carbon monoxide diffusing capacity were obtained according to standardized procedures [9, 10]. The reference values of Quanjer were used [11]. Arterial blood gas samples were obtained by percutaneous radial artery puncture while patients were seated and breathing room air. The alveolar oxygen tension was calculated by using the ideal air Equation and assuming a respiratory exchange ratio of 0.8. The alveolar-arterial oxygen difference was then derived. A gradient less than 15 mm Hg was considered normal. Exhaled nitric oxide was measured on a chemiluminescence analyzer (Dasibi Environmental Corp., Glendale, California) that is sensitive to nitric oxide from 1 to 4000 parts per billion (ppb) by volume, adapted for on-line recording of nitric oxide concentration, at a sample gas flow of 250 mL/min according to European Respiratory Society recommendations [12]. The analyzer was calibrated daily against standard gas mixtures. While seated and wearing a noseclip, patients were asked to inhale nitric oxide-free air (<5 ppb) and to perform a slow expiratory vital capacity test over 20 to 30 seconds with a flow of 5 to 15 L/min against a low resistance (5 to 20 cm H2O). Exhaled air was sampled for nitric oxide analysis by way of a Teflon tubing side arm attached to the mouthpiece. Nitric oxide concentration, flow, and pressure were simultaneously displayed against time on a computer screen. Three successive reproducible recordings were made at 2-minute intervals, and the mean values of the plateau (the last part of expiration) of nitric oxide concentration (expressed in ppb) were recorded. Because of flow dependence of exhaled nitric oxide concentration [13], flow rates at which nitric oxide measurements were performed in each patient before and after transplantation were compared and found to not be statistically significantly different (10.2 2.37 L/min compared with 10.6 2.28 L/min). Twenty nonsmoking healthy persons (mean age, 44.6 11.2 years; 12 men) served as normal controls for exhaled nitric oxide concentrations. Saline contrast-enhanced echocardiography was done by use of a peripheral intravenous line, as reported elsewhere [14]. A positive result on contrast-enhanced echocardiography (that is, indicating intrapulmonary right-to-left shunt) was defined as the delayed appearance (three to six beats after the initial appearance of contrast in the right side of the heart) of microbubbles in the left side of the heart. Statistical Analysis The variability of the outcomes (decrease in alveolar-arterial oxygen gradient and exhaled nitric oxide concentration after transplantation) was estimated from previous studies [3, 8]. The sample size was calculated on the basis of an expected 50% decrease in the outcomes after transplantation compared with pretransplantation values, for a two-tailed value of 0.05 and a value of 0.20. Means and SDs were calculated for each variable. The Student t-test for paired data was used to compare data before and after transplantation; the McNemar test was used when appropriate. Regression analysis was performed by using the least-squares method. A P value of 0.05 or less was considered statistically significant. Role of the Funding Source Our funding source had no role in the collection, analysis, or interpretation of the data or in the submission of the paper for publication. Results Eighteen patients (mean age, 48.3 7 years; 14 men) completed the study. Two patients died after surgery (1 of pneumonia and 1 of stroke) 72 and 85 days after transplantation. Cirrhosis was alcoholic in 7 patients; viral in 8 patients; and autoimmune, cryptogenic, and associated with Wilson disease in 1 patient each. According to the Child-Pugh classification [15], 4 patients had class A cirrhosis, 4 had class B cirrhosis, and 10 had class C cirrhosis. Fifteen patients (83.3%) had esophageal varices. Patients were reevaluated 8.5 3.5 months (range, 3 to 12 months) after transplantation. Post-transplantation lung volumes and diffusion did not significantly differ from pretransplantation values: Total lung capacity increased from 95.4% 9.6% of predicted to 96.7% 10.4% of predicted, FEV1 increased from 100.3% 13.3% of predicted to 103% 13.2% of predicted, FEV1/FVC 100 decreased from 80.5% 4.5% of predicted to 79.5% 4.2% of predicted, and the diffusing capacity of the lung for carbon monoxide divided by alveolar volume decreased from 76.5% 20.9% of predicted to 71.6% 17.2% of predicted. Arterial blood gas data, exhaled nitric oxide concentrations, and findings on echocardiographic evaluation of intrapulmonary shunts before and after transplantation are given in Table 1. Before transplantation, the mean exhaled nitric oxide concentration was significantly higher in patients than in controls (13 4.9 ppb compared with 5.75 1.9 ppb; P < 0.001). Table 1. Arterial Blood Gas Analyses, Exhaled Nitric Oxide Concentrations, and Patients with the Hepatopulmonary Syndrome before and after Liver Transplantation* After transplantation, the alveolar-arterial oxygen gradient significantly decreased (from 17.3 7.1 mm Hg before transplantation to 9 5.2 mm Hg; P < 0.001), as did the exhaled nitric oxide concentration (from 13 4.9 ppb to 6.2 2.8 ppb; P < 0.001). The decrease in exhaled nitric oxide concentration after liver transplantation was significantly correlated with the decrease in alveolar-arterial oxygen gradient (r = 0.56; P = 0.014) (Figure 1). Figure 1. Correlation between the differences in alveolar-arterial oxygen gradient and exhaled nitric oxide concentrations before and after liver transplantation. Before transplantation, intrapulmonary shunts were detected by contrast-enhanced echocardiography in five patients, all of whom met the criteria for the hepatopulmonary syndrome and had an alveolar-arterial oxygen gradient greater than 15 mm Hg. In these patients, the pretransplantation exhaled nitric oxide concentration was significantly higher than that in patients without the hepatopulmonary syndrome (18 5.48 ppb compared with 11.07 3.2 ppb; P < 0.005). After transplantation, the hepatopulmonary syndrome was no longer evident; the alveolar-arterial oxygen gradient returned to normal in all affected patients, even the two patients in whom contrast-enhanced echocardiography still showed intrapulmonary vasodilatations. Discussion We found a highly significant decrease in exhaled nitric oxide concentrations after liver transplantation that was correlated with the decrease in alveolar-arterial oxygen gradient. As in other investigations [1-3], respiratory function assessment done before liver transplantation revealed a high prevalence of widened alveolar-arterial oxygen gradient in our patients with advanced liver disease. The high concentration of exhaled nitric oxide in our pati

Are asthma-like symptoms due to bronchial or extrathoracic airway dysfunction?

Patients with asthma-like symptoms may not have asthma but obstruction of the extrathoracic airway (EA). To evaluate if dysfunction of the EA causes asthma-like symptoms, we assessed bronchial and EA responsiveness to inhaled histamine in 441 patients who presented with at least one of three key symptoms--cough, wheeze, dyspnoea--but had neither documented asthma nor bronchial obstruction. The histamine concentrations causing a 20% fall in forced expiratory volume in 1 s (PC20FEV1) and a 25% fall in maximal mid-inspiratory flow (PC25MIF50) were used as respective thresholds of bronchial and EA responsiveness. Values 8 mg/mL or less indicated bronchial (B-HR) or EA hyper-responsiveness (EA-HR). The influence of concurrent upper respiratory tract diseases, such as post-nasal drip (PND), pharyngitis, laryngitis and sinusitis, was also assessed. We found four response patterns to the histamine challenge: EA-HR in 26.5% of the patients, B-HR in 11.1%, combined EA-HR and B-HR in 40.6%, and no-HR in 21.8%. Cough was reported by 79% of the patients, wheeze by 53%, and dyspnoea by 40%. Patients with cough as the sole presenting symptom (34.2%), as compared with those with wheeze and/or dyspnoea (20%), had significantly greater probability of having EA-HR (OR 5.35, 95% CI 3.25-8.82) and lower probability of having B-HR (OR 0.45, CI 0.28-0.70); patients with cough plus wheeze and/or dyspnoea (45.8%) had significantly greater probability of having both EA-HR and B-HR than either those with cough alone (OR 2.48, CI 1.49-4.13), or those with wheeze and/or dyspnoea but not cough (OR 1.74, CI 1.36-2.22). EA-HR alone or combined with B-HR was strongly associated with EA diseases, particularly pharyngitis and PND. Cough was significantly associated with PND, either when it was the sole symptom (OR 2.16, CI 1.14-4.09) or when it was combined with wheeze and/or dyspnoea (OR 3.53, CI 1.97-6.33). Our results suggest that extrathoracic airway dysfunction may account for asthma-like symptoms, particularly chronic cough. This abnormality seems to be sustained by chronic diseases of the upper respiratory tract.

Tooth loss and obstructive sleep apnoea

BackgroundComplete tooth loss (edentulism) produces anatomical changes that may impair upper airway size and function. The aim of this study was to evaluate whether edentulism favours the occurrence of obstructive sleep apnoea (OSA).MethodsPolysomnography was performed in 48 edentulous subjects on two consecutive nights, one slept with and the other without dentures. Upper airway size was assessed by cephalometry and by recording forced mid-inspiratory airflow rate (FIF50). Exhaled nitric oxide (eNO) and oral NO (oNO), were measured as markers of airway and oropharyngeal inflammation.ResultsThe apnoea/hypopnoea index (AHI) without dentures was significantly higher than with dentures (17·4 ± 3·6 versus 11·0 ± 2·3. p = 0·002), and was inversely related to FIF50 (p = 0·017) and directly related to eNO (p = 0·042). Sleeping with dentures, 23 subjects (48%) had an AHI over 5, consistent with OSA, but sleeping without dentures the number of subjects with abnormal AHI rose to 34 (71%). At cephalometry, removing dentures produced a significant decrease in retropharyngeal space (from 1·522 ± 0·33 cm to 1·27 ± 0·42 cm, p = 0·006). Both morning eNO and oNO were higher after the night slept without dentures (eNO 46·1 ± 8·2 ppb versus 33·7 ± 6·3 ppb, p = 0·035, oNO 84·6 ± 13·7 ppb versus 59·2 ± 17·4 ppb, p = 0·001).ConclusionThese findings suggest that complete tooth loss favours upper airway obstruction during sleep. This untoward effect seems to be due to decrease in retropharyngeal space and is associated with increased oral and exhaled NO concentration.

Damage of the pharyngeal mucosa and hyperresponsiveness of airway in sinusitis

BACKGROUND In sinusitis bronchoconstriction is supposed to originate from pharyngobronchial reflexes triggered by seeding of the inflammatory process into the pharynx. OBJECTIVE Our aim was to evaluate whether in sinusitis bronchial and extrathoracic airway (EA) dysfunction correlate with morphologic abnormalities of the pharyngeal mucosa. METHODS We performed histamine inhalation challenge, nasal lavage, and nasopharyngeal biopsies in 24 nonasthmatic patients with exacerbation of chronic sinusitis. The histamine PC20 was the threshold of bronchial responsiveness, and that causing 25% fall in maximal midinspiratory flow was the threshold of EA responsiveness (PC25MIF50). Thresholds of 8 mg/ml or less were assumed to indicate bronchial hyperresponsiveness (BHR) or EA hyperresponsiveness (EAHR). PC20 and PC25MIF50 values were related to clinical data, nasal lavage fluid eosinophils, pharyngeal epithelium and basement membrane thickness, and density of submucosal vessels and nervous fibers. RESULTS The PC20 was closely related to PC25MIF50 (p = 0.0004). Ten patients had EAHR, 9 had combined EAHR and BHR, and 5 had neither EAHR nor BHR. EAHR was strongly associated with epithelial thinning, and BHR with long-standing sinusitis, a lower PC25MIF50, increased submucosal nerve density and increased nasal lavage fluid eosinophils. CONCLUSIONS Our findings suggest that in nonasthmatic patients with sinusitis, pharyngeal damage may contribute to airway dysfunction by favoring the access of irritants to submucosal nerve endings, with activation of constrictive reflexes to the EA. Proliferation of sensory neurons, consequent to long-lasting pharyngeal inflammation, may cause more severe EA narrowing and activate pharyngobronchial reflexes.

Oral nitric oxide during plaque deposition

Background Nitric oxide (NO) is one of the most powerful antibacterial compounds. We investigated if NO oral production increases during dental plaque deposition.

Effect of pleurotomy on pulmonary function after coronary artery bypass grafting with internal mammary artery

Coronary artery by-pass grafting with internal mammary artery (IMA) has become the graft conduit of choice, due to improved survival and its long term patency rate. However, some studies have shown that, in comparison with saphenous vein grafts, after IMA grafting, there is increased postoperative impairment of pulmonary function, possibly due to the frequent performance of pleurotomy. In 57 consecutive patients, admitted for elective CABG with IMA, we prospectively evaluated the early (2nd and 6th day) postoperative chest X-ray complications and the late (2 months) respiratory function tests changes. Thirty-two patients had been subjected to pleurotomy (group 1) and 25 not (group 2). The incidence of pulmonary atelectasis and pleural effusion in 2nd and in 6th postoperative days was not different in the two groups: 22 vs. 19%, 74 vs. 52% in 2nd, and 29 vs. 19%, 48 vs. 38% in 6th postoperative day respectively. The incidence of elevated hemidiaphragm in 6th postoperative day was not different in the two groups (18.5 vs. 14%). Two months after surgery the mean values of spirometric tests were significantly lower than the preoperative values: VC from 88.5 +/- 1.26 to 80 +/- 1.65% of predicted, P < 0.001, FEV1 from 96.1 +/- 1.27 to 84.7 +/- 1.73% of predicted, P < 0.001, MEF50 from 84.9 +/- 3.14 to 69.2 +/- 3.18% of predicted, P < 0.001. No significant changes were detected in RV and in AaPO2.(ABSTRACT TRUNCATED AT 250 WORDS)

Oxidative stress and airway inflammation after allergen challenge evaluated by exhaled breath condensate analysis.

Background Allergen exposure may increase airway oxidative stress, which causes lipid membrane peroxidation and an increased formation of 8‐isoprostane.

Chronic cough and irritable larynx.

BACKGROUND Perennial rhinitis (PR), chronic rhinosinusitis (CRS), or both, asthma, and gastroesophageal reflux disease (GERD) are the most frequent triggers of chronic cough (CC). Extrathoracic airway receptors might be involved in all 3 conditions because asthma is often associated with PR/CRS and gastroesophageal refluxate might reach the upper airway. We previously found that most patients with rhinosinusitis, postnasal drip, and pharyngolaryngitis show laryngeal hyperresponsiveness (LHR; ie, vocal cord adduction on histamine challenge) that is consistent with an irritable larynx. OBJECTIVE We sought to evaluate the role of LHR in patients with CC. METHODS LHR and bronchial hyperresponsiveness (BHR) to histamine were assessed in 372 patients with CC and in 52 asthmatic control subjects without cough (asthma/CC-). In 172 patients the challenge was repeated after treatment for the underlying cause of cough. RESULTS The primary trigger of CC was PR/CRS in 208 (56%) patients, asthma in 41 (11%) patients (asthma/CC+), GERD in 62 (17%) patients, and unexplained chronic cough (UNEX) in 61 (16%) patients. LHR prevalence was 76% in patients with PR/CRS, 77% in patients with GERD, 66% in patients with UNEX, 93% in asthma/CC+ patients, and 11% in asthma/CC- patients. Upper airway disease was found in most (95%) asthma/CC+ patients and in 6% of asthma/CC- patients. BHR discriminated asthmatic patients and atopy discriminated patients with PR/CRS from patients with GERD and UNEX. Absence of LHR discriminated asthmatic patients without cough. After treatment, LHR resolved in 63% of the patients and improved in 11%, and BHR resolved in 57% and improved in 18%. CONCLUSIONS An irritable larynx is common in patients with CC and indicates upper airway involvement, whether from rhinitis/sinusitis, gastric reflux, or idiopathic sensory neuropathy.

Increased oral nitric oxide in obstructive sleep apnoea

BACKGROUND Hypoxia and snoring-related mechanical trauma contribute to airway inflammation in obstructive sleep apnoea (OSA). Increased exhaled nitric oxide (FENO), an airway inflammation marker, has been reported in OSA patients. We propose the measure of NO in the oral cavity (oNO) as marker of oropharyngeal inflammation in OSA. METHODS We compared oNO and FENO of 39 OSA patients with those of 26 mild asthmatics (ASTHMA), 15 patients with chronic rhinitis or rhinosinusitis (CRS) and 24 healthy subjects. A special device was used for oNO measurement. Apnoea/hypopnoea index (AHI), oxygen desaturation index, mean and nadir SaO2 were calculated from the polysomnography. RESULTS oNO was significantly increased in OSA (104.2 95%CI 80.2-135.5ppb) as compared to ASTHMA (71.9 95%CI 56.3-91.9ppb; p=0.015), CRS (54.4 95%CI 40.2-73.7ppb; p=0.009) and healthy subjects (63.6 95%CI 59-73ppb; p<0.001). oNO was directly related to AHI (r=0.466, p=0.003) and to minutes slept with SaO2 <90% (r=0.471, p=0.011) and it was inversely related to nadirSaO2 (r=-0.393, p=0.018). FENO was highest in asthmatics (40.3 95%CI 32.5-50.1ppb) and only slightly elevated in OSA (23.1 95%CI 19,8-28.3ppb) and CRS (22.8 95%CI 16.8-32.5ppb). CONCLUSIONS The finding that oral NO is increased in OSA and is related to upper airway obstructive episodes and to hypoxemia severity, strengthens the clinical and pathogenic role of oral inflammation in OSA.