Recognition of the existence of interstitial lung disease (ILD) dates back more than 100 years when Sir William Osler described ‘cirrhosis of the lungs’ and recognized the diversity of its forms and the difficulty of classifying these disorders (1). Various terminologies were coined over the span of the twentieth century as various leaders in the field described patients whose lungs displayed changes of interstitial inflammation and fibrosis. Hamman and Rich (1944) described four cases of rapidly progressive, diffuse alveolar wall thickening without identifiable cause, which led to use of the term, ‘Hamman–Rich syndrome’ for either acute-onset or chronic fibrotic ILD. Subsequently, diffuse pulmonary fibrosis was linked to forms of connective tissue disease (CTD) and other causes, such as exposure to organic or inorganic dusts and pneumotoxic drug reactions, but many forms remained unexplained by any associations. Terms such as ‘chronic idiopathic interstitial fibrosis’, ‘diffuse fibrosing alveolitis’ or ‘idiopathic pulmonary fibrosis’ were used to designate fibrotic ILD of unknown aetiology, and these disorders were thought to occur as a consequence of alveolar wall inflammation (‘alveolitis’). The term ‘diffuse fibrosing alveolitis’ was coined by Scadding (2) to describe widespread fibrotic change beyond the level of the terminal bronchioles, and Scadding subdivided entities according to known or unknown associations and patterns of fibrosis (Figure 1.1). Liebow and Carrington (3,4) published a classification system for chronic idiopathic interstitial pneumonias that was based on histopathologic changes; one of the five subgroups that they described was termed ‘usual’ interstitial pneumonia (UIP), and the Hamman–Rich syndrome was felt to be an acute form of UIP (Figure 1.1).