Alpha-1-antitrypsin deficient man presenting with lung function decline associated with dust exposure: a case report

A 68-year-old Caucasian man presented with an initial complaint of dyspnea on exertion that had developed five years prior and had progressed to shortness of breath while walking up one flight of stairs. He was a former cigarette smoker from ages 14 to 30 years, with a maximum of one and a half packs per day (less than 25 pack-years total) and no reported respiratory symptoms during that period. He experienced significant inorganic dust exposure while grinding large concrete aquarium exhibition tanks over a period of 10 years, ending six years prior to presentation. Less dusty work exposure continued until his retirement at age 67. He had no other significant exposure to dusts or fumes.

His medical history was notable only for a prior traumatic cervical spine injury. His physical examination revealed pulmonary auscultation that was remarkable for a prolonged expiratory phase without wheezes or rhonchi. The remainder of his physical examination was otherwise unremarkable, except for a left-sided paresis (most notable in the upper extremity) consistent with his prior spinal injury.

Pulmonary function testing at presentation demonstrated airflow obstruction: forced expiratory volume in one second (FEV₁) was 2.10 litres (61% of the predicted value), forced vital capacity (FVC) was 3.60 litres (81% of the predicted value), the FEV₁:FVC ratio was 0.58, forced expiratory flow over 25% to 75% of the expired volume (FEF_25-75) was 0.85 litres per second (28% of the predicted value), total lung capacity (TLC) measured by plethysmography was 6.40 litres (93% of the predicted value), and residual lung volume (RV) was 2.91 litres (123% of the predicted value). There was minimal response to an inhaled bronchodilator. The diffusing capacity of the lung for carbon monoxide (D_LCO) (hemoglobin-adjusted) was 18.5 ml/min/mmHg (59% of the predicted value), and the D_LCO adjusted for alveolar volume (VA) was 3.2 (69% of the predicted value). A computed tomography scan of the chest demonstrated bilateral lower-lobe-predominant emphysema (Figure 1). A serum A1AT assay (electrophoresis with agarose immunofixation) indicated a PiZZ phenotype, with a quantified value of 24 U (normal ≥ 90 U). Treatment was initiated with a combination of inhaled fluticasone and salmeterol twice daily, tiotropium once daily and albuterol as needed.

Data available from a program of periodic employment-based spirometric monitoring dating back 16 years prior to presentation, along with nearly five years of subsequent follow-up, are shown in Figure 2. Taking into account 18 serial measurements taken over 241 months, analyzed by least squares regression, the patient's FEV₁ fell by 77 ml/year, FVC fell by 54 ml/year and FEF_25-75 fell by 110 ml/s/year overall. Using National Institute for Occupational Safety and Health (NIOSH) Spirometry Longitudinal Data Analysis (SPIROLA) software for analysis of lung function time trends [6], the change in FEV₁ measured during the period of employment (-128 ml/year) demonstrated an accelerated decline relative to the projected normal age-related decrease of FEV₁ (-42 ml/year) [7]. The trajectory of plotted lung function crosses below the age-based 95th percentile lower limit of normal (LLN) approximately midway in this occupational exposure period. After the patient's retirement, his FEV₁ remained below the LLN, but the slope of its decline (46 ml/year) shifted closer to the normal age-related trajectory. The within-person variation in FEV₁ remained within the SPIROLA-based normal range. The overall slope of the FVC was steeper than the normal age-predicted decline, but only crossed the LLN later in follow-up.

To further assess the pattern of change over time, we remodeled the data in Figure 2 in a "break-point" analysis, jointly estimating linear regression parameter estimates for lung function decline over the periods before and after the patient's retirement. For FEV₁, the parameter estimate before retirement was negative (in the direction of loss) and significant (P < 0.05), but positive, albeit non-significantly, after his retirement (P = 0.7). For FVC, the parameter estimate for the period before the patient's retirement was close to zero (P > 0.99), and post-retirement the parameter estimate deflected negatively (P < 0.05). For FEF_25-75, the pre-retirement parameter estimate was significantly negative and then positive after the breakpoint (P < 0.01 for each).

A repeat CT scan of the chest after almost five years of follow-up showed progression of panlobular severe emphysema and areas of scarring in the bilateral bases (not shown). Repeat pulmonary function testing demonstrated a TLC volume by plethysmography of 6.37 litres (94% of the predicted value), RV of 3.10 litres (126% of the predicted value), a RV:TLC ratio of 49%, and D_LCO adjusted for alveolar volume of 2.8 (63% of the predicted value). To date, the patient has not wished to initiate A1AT replacement therapy. The patient was recognized by his employer's workers' compensation carrier as having COPD attributable in part to his occupational exposure, along with co-attribution to non-work-related factors (A1AT deficiency and cigarette smoking).