Copyright
©The Author(s) 2017.
World J Respirol. Mar 28, 2017; 7(1): 1-16
Published online Mar 28, 2017. doi: 10.5320/wjr.v7.i1.1
Published online Mar 28, 2017. doi: 10.5320/wjr.v7.i1.1
Table 1 Summary of studies dividing patients as HRCT defined phenotypes and their significant differences clinical and physiological (P < 0.05)
| Ref. | HRCT defined phenotypes | Variables studied | Significant variable difference |
| Kitaguchi et al[8], 2006 | A: Little or none of either emphysema or BWT E: Emphysema but no BWT M: Emphysema and BWT | Gas exchange Gas transfer Lung function Response to beta-agonist Response to treatment with ICS Sputum cell differentiation | A: ↑ BMI ↑DLCO ↓ hyperinflation ↑ reversibility ↑response to ICS ↑ % of sputum eosinophils E: No response to ICS M: ↑ response to ICS ↑ % of sputum eosinophils |
| Fujimoto et al[9], 2006 | A: Little or none of either emphysema or BWT E: Emphysema but no BWT M: Emphysema and BWT | Exacerbation rates Gas exchange Gas transfer Hospital admissions Lung function Response to beta-agonist Symptoms | M: ↑ volume of sputum, exacerbation rate and admission to hospital |
| Pistolesi et al[10], 2008 | From derivation set, created new validation set Group A and B | CT parameters Gas exchange Gas transfer Lung function | A: ↓ FEV1, ↑ TLC ↓ DLCO. ↑ pixel index (threshold -950HU) B: ↑ BMI purulent sputum worse bronchial wall thickening |
| Han et al[7], 2011 | Emphysema predominant or Airway predominant | BWT Exacerbation rates lung function % emphysema | Emphysema Predominant (> 35% -950HU): ↓ FEV1 and 6MWD ↑ SGRQ and MRC grade For every 5% ↑ in emphysema, 1.18 fold ↑ exacerbation frequency Airways predominant: For 1 mm ↑ in segmental BWT 1.84 fold ↑ in exacerbation frequency |
| Subramanian et al[3], 2016 | Emphysema dominant, airways disease dominant, mixed pathology and mild disease | Blood parameters CT parameters Gas exchange Gas transfer Lung volumes Spirometry | Compared with airway disease dominant group, emphysema dominant group had ↑ lung volumes, ↓ gas transfer ↓ pO2 + pCO2↓BMI ↑Hb No difference between age, and smoking history between the groups |
| Da Silva et al[2], 2016 | Emphysema or airways disease | Clinical + functional evaluation HRCT | Emphysema group: ↑ airflow obstruction ↓ BMI ↓ 6MWD |
Table 2 Treatment of chronic obstructive pulmonary disease as defined by computed tomography phenotypes
| CT phenotype | CT defining features | Clinical features | Findings | Treatments | Ref. |
| Emphysema | ↓ Perc15 Emphysema Centrilobular Panlobular Paraseptal Bullous | Health status | ↓ BMI[2] ↑ SGRQ + MRC[7] | Rehabilitation Nutritional support Palliative care | GOLD 2016[5] |
| Exercise tolerance | ↓ 6MWD[2] ↓ pO2↓ pCO2[3] | Rehabilitation Maintenance of physical activity Oxygen | GOLD 2016[5] | ||
| Lung function | ↑ TLC ↓ KCO ↓ FEV1/FVC | LAMA/LABA LVRS/BVLS Transplant Bullectomy[11] LVRS[11] | GOLD 2016[5] NICE 2010[11] | ||
| Symptoms | ↑ Hb[3] No significant response to ICS[8] | Theophylline Rehabilitation typically MRC > 3 | GOLD 2016[5] NICE 2010[11] | ||
| Airways disease | Exacerbation frequency/ severity | ↑ Exacerbations hospital admissions[7] | LABA/phosphodiesterase-4 inhibitor LAMA/phosphodiesterase-4 inhibitor Mucolytics Add in ICS Prophylactic antibiotics | GOLD 2016[5] NICE 2010[11] Brown et al[12], 2007 Fabbri et al[13], 2009 Calverley et al[14], 2009 Herath et al[15], 2013 | |
| Lower wall area/body Surface area ratio (WA/BSA) Lower luminal area/BSA Higher %WA | Symptoms | Significant response to ICS+ Significantly higher % of sputum eosinophils[8] Peribronchial thickening[10] Air trapping | Physiotherapy and active breathing techniques Mucolytics Roflumilast Bronchodilators | NICE 2010[11] |
Table 3 Table to summarise studies performed in alpha one antitrypsin deficiency and chronic obstructive pulmonary disease directly comparing the most accurate measure of computed tomography density
| Condition | Type of study | 910 | 950 | Perc15 | Conclusion of superior measure | Ref. |
| Alpha one | RCT | x | x | 950 | Parr et al[29] | |
| RCT | x | x | 950 and Perc15 | Parr et al[30] | ||
| RCT | x | x | x | Perc15 | Parr et al[26] | |
| Review | x | x | x | Perc15 | Hogg et al[28] | |
| Chronic obstructive pulmonary disease | RCT | x | x | x | Perc15 | Shaker et al[31] |
| Review | x | x | Perc15 | Dirksen et al[27] | ||
| RCT | x | x | 950 | Chong et al[32] |
Table 4 Summary of interventional drug trials using computed tomography measures as an outcome measure
| Ref. | Study design | Pt N° | Duration | CT measure | Drug | Result |
| Usual COPD | ||||||
| Shaker et al[75] | RCT | 254 | 2-4 yr | Perc15 and -910HU | Budesonide or placebo | Annual fall in Perc15 ↑in the placebo arm vs budesonide (P = 0.09) Annual increase in -910HU↓in the budesonide arm (P = 0.02) |
| Hoshino et al[76] | RCT | 54 | 16 wk | %WA, LA, BWT | Tiotropium, Indacaterol or both | Combination therapy resulted in a ↓in %WA and wall thickness (P < 0.01) |
| Nordenmark et al[77] | RCT | 36 | 12 wk | BWT, air trapping index and %WA | Reversible neutrophil elastase inhibitor 60 mg BD | No difference |
| Shimizu et al[78] | Inter-ventional trial | 23 | 1 wk | Airway inner luminal area | SFC | Ct detected the significant change in airway inner luminal area r = 0.65, P < 0.001 |
| Alpha 1 Antitrypsin deficiency | ||||||
| Stolk et al[79] | RCT | 262 | 1 yr | Perc15 | Parlovarotene | No benefit on lung density |
| Mao et al[80] | RCT-pilot study | 20 | 9 mo | -910HU | ATRA | No benefit |
| Roth et al[81] | RCT feasibility study | 148 | 9 mo | -910HU | Patients received ATRA either LD, HD, 13-cRA or placebo | No definitive clinical benefits |
| Dirksen et al[82] | RCT | 32 | 3 yr | Perc15 | Alpha1-antitrysin | CT analysis showed a non-significant trend towards a favourable effect. CT lung density twice as sensitive as PFTs |
| Dirksen et al[72] (EXACTLE) | RCT | 77 | 2-2.5 yr | Perc15 | Prolastin | CT densitometry more sensitive measure for the detection of emphysema progression than PFTs or health status indices |
| Chapman et al[73] | RCT | 180 | 2 yr | Perc15 | Alpha 1 proteinase inhibitor | Annual rate of density decline at TLC ↓in treatment group (P = 0.03) |
Table 5 Magnetic resonance imaging modalities to phenotype and treat chronic obstructive pulmonary disease
| Phenotype | MRI modality | Findings | Suggested treatments |
| Airways disease | Hyperpolarised MRI | Detailed anatomical information of airway inflammation, oedema and mucus plugging[84,85] | Nebulised antibiotics Chest clearance techniques[83] |
| Regional information re. lung volumes, e.g., focal bronchoconstriction | Broncho-thermoplasty[91] BVRS | ||
| Emphysema | Hyperpolarised MRI | Global high ADC[87] | Early disease detection |
| Low PaO2[92] | Future alpha one augmentation therapy1 | ||
| Oxygen enhanced MRI | ↑↓Relative enhancement signal[93,94] | Targets for resection | |
| Early emphysema detection | |||
| Dynamic contrast MRI | Global microvascular reduction blood flow[95] | Lifestyle moderation | |
| Focal defects, small pulmonary emboli | Anticoagulation | ||
| Increased pulmonary pressure | Treat as pulmonary hypertension |
Table 6 Studies correlating magnetic resonance imaging with other clinical variables
Table 7 Summary of studies comparing magnetic resonance imaging and computed tomography in chronic obstructive pulmonary disease
| Ref. | Year | Pt No. | Variables | Results |
| Ley et al[96] | 2004 | 13 | ADC and EI vs FEV1 | ADC vs FEV1, R = 0.7 EI vs FEV1, R = 0.5 MLD vs FEV1, R = 0.4 |
| Ohno et al[93] | 2008 | 71 | O2 enhanced MRI (mean wash in time and relative enhancement ratio), CT defined lung volumes vs lung function | Mean wash in time vs FEV1, r = -0.74 Relative Enhancement Ratio vs KCO, r = 0.66 CT lung volume vs FEV1, r = 0.61 CT lung volume vs KCO, r = 0.56 |
| Van Beek et al[98] | 2009 | 94 | ADC and MLD vs FEV1/FVC and DLCO | ADC vs Fev1/fvc, r = 0.5 MLD vs Fev1/fvc, r = 0.52 ADC vs DLCO, r = 0.59 MLD vs DLCO, r = 0.29 |
| Diaz et al[38] | 2009 | 27 | ADC and EI vs FEV1 and DLCO | ADC vs FEV1, r = 0.67 EI vs FEV1, r = 0.55 ADC vs DLCO, r = -0.82 Perc15 vs DLCO, r = 0.6 |
| Quirk et al[114] | 2011 | 30 | Hyperpolarised He vs CT density in at risk smokers | Lung morphometry vs %LAA 950: Significant difference seen in those still smoke, not on CT |
| Xia et al[101] | 2014 | 55 | +ve rate of Perfusion defects vs CT changes | Early COPD: MRI detected 8/8, vs CT 3/8 P = 0.003 Mod. COPD: MRI detected 9/9, vs CT 7/9 P = 0.47 |
| Hueper et al[95] | 2015 | 144 | DCE-MRI vs CT density | PMBF vs %LAA 950: Evidence of non-linearity, P = 0.015 |
Table 8 Practical considerations for positron emission tomography vs single photon emission computed tomography
| Modality | Advantages | Disadvantages |
| PET | Increased resolution | Cyclotron and radiopharmaceutical preparation Rapid repeat testing not possible[87] |
| SPECT | Lower cost More widely available. Dynamic SPECT give time course of ventilation | Lower spatial and contrast resolution |
Table 9 Studies correlating single photon emission computed tomography with other clinical variables
Table 10 Demonstration of how optical coherence tomography could phenotype in chronic obstructive pulmonary disease
| Condition | OCT method | Findings | Suggested treatments |
| Chronic bronchitis | Endoscopic | Increased volume of submucosal glands; central airway inflammation[133-135] | Investigations directed towards asthma overlap syndrome; targeted inhaled steroids |
| Emphysema | Anatomical OCT | Can visualise collapsibility dynamically[136] | Bronchodilators; smoking cessation |
- Citation: Crossley D, Turner A, Subramanian D. Phenotyping emphysema and airways disease: Clinical value of quantitative radiological techniques. World J Respirol 2017; 7(1): 1-16
- URL: https://www.wjgnet.com/2218-6255/full/v7/i1/1.htm
- DOI: https://dx.doi.org/10.5320/wjr.v7.i1.1