Epidemiology and clinical presentation of the four human parainfluenza virus types

Samples in this study were taken as part of standard care. The First Affiliated Hospital of Guangzhou Medical University Ethics Committee approved the experimental design and patient involvement in this study. Written informed consent was obtained from the patient for publication of this report and any accompanying images.

Throat swab samples were collected from patients with ARTI (presenting with at least two of the following symptoms: cough, pharyngeal discomfort, nasal obstruction, coryza, sneeze, dyspnoea) at three hospitals in Guangzhou, southern China between July 2009 and August 2011. The samples were refrigerated at 2 to 8°C and transported on ice to State Key Laboratory of Respiratory Diseases and analysed every working day or stored at −80°C before testing. Over 97 samples were collected and tested during each month in our study.

Clinical presentations were collected and categorized retrospectively into the following six groups from the patients’ medical records using designed presentation cards: URTI, LRTI, systemic influenza-like symptoms, gastrointestinal illness, neurologic symptom and others. Patients with nasal obstruction, coryza, sneeze, cough, pharyngeal discomfort, or hoarseness were categorized as having URTI. Patients with pneumonia, bronchopneumonia, increasing lung markings, dyspnoea, or abnormal pulmonary breath sound were categorized as having LRTI. Patients with high fever (≥38°C), chills, dizziness, headache, myalgia or debilitation were categorized as having systemic influenza-like symptoms. Patients with vomiting, poor appetite, or diarrhoea were categorized as having gastrointestinal illness. Patients with convulsion were categorized as having an neurologic symptom. Patients with other symptoms, including but not limited to rash, were classified as “others”. Some patients were assigned to multiple clinical presentation groups. Pneumonia and bronchopneumonia were diagnosed by chest radiography. Pneumonia was defined as an acute illness with radiographic pulmonary shadowing which was at least segmental or present in one lobe (excluding the bronchi); bronchopneumonia was defined as inflammation of the walls of the smaller bronchial tubes, with varying amounts of pulmonary consolidation due to spread of the inflammation into peribronchiolar alveoli and the alveolar ducts. Other clinical symptoms were identified by common medical examinations and clinical descriptions.

DNA or RNA from respiratory samples was extracted using QIAamp DNA Mini Kit or QIAamp Viral RNA Mini Kit (Qiagen Co. Ltd., Shanghai, China) in accordance with the manufacturer’s protocols. The four types of HPIV were tested by TaqMan real-time PCR as previously reported [19], and 13 other common respiratory pathogens were also selected for TaqMan real-time PCR testing, including influenza A virus (infA), influenza B virus (infB), respiratory syncytial virus (RSV), adenovirus (ADV), enterovirus (EV), human metapneumovirus (HMPV), four strains of human coronavirus (HCoV-229E, OC43, NL63 and HKU1), human bocavirus (HBoV), Mycoplasma pneumoniae (MP), and Chlamydophila pneumoniae (CP) [19].

For comparisons of categorical data, χ² test and Fisher’s exact test were used where appropriate. All tests were two-tailed and p<0.05 was considered statistically significant.

We tested 4755 samples for HPIV and 13 other respiratory pathogens between July 2009 and August 2011 in Guangzhou, southern China. The median age was 4.75 (interquartile range, 1.00 to 25.00), and ranged from one day to 91 years. Pathogens were detected in 2439/4755 (51.3%) samples, and were detected in a higher proportion of samples from children (<14 years old) (1503/2793; 53.8%) than from adults (≥14 years old) (936/1962; 47.7%) (p<0.001). The pathogens identified most frequently were infA (833/4755; 17.5%), RSV (524/4755; 11.0%) and MP (274/4755; 5.8%) (Table 1).

HPIVs were identified in 178/4755 (3.7%) samples. Ninety-nine (2.1%) samples were positive for HPIV-3, 58 (1.2%) for HPIV-1, 19 (0.4%) for HPIV-2 and 8 (0.2%) for HPIV-4 (Table 1). Some samples were positive for multiple HPIV types, therefore the sum of these segments is more than 178. The age of patients positive for HPIV ranged from one month to 78 years. The male to female ratio was 139:39 in HPIV-positive patients and 2759:1818 in HPIV-negative patients (p<0.001). The child to adult ratio was 162:12 in HPIV-positive patients and 2627:1950 in HPIV-negative patients (p<0.001). The distribution and co-infection status of HPIV-positive patients are shown in Figure 1 according to different age groups. The large majority (160/178; 88.9%) of HPIV-positive samples were from paediatric patients younger than 5 years old (Figure 1), but no infant under one month of age was HPIV positive.

HPIV-3 was isolated from patients aged one month to 78 years. HPIV-3 was isolated predominantly from patients under 5 years of age, and the highest frequency was found in those aged 7–12 months (27/406; 6.7%). HPIV-1 was isolated from patients aged one month to 47 years, and HPIV-2 was isolated from patients aged 2 months to 41 years old. HPIV-1-positive patients were more evenly distributed across ages than HPIV-3-positive patients, but like HPIV-3 the highest frequency of HPIV-1 was detected from patients aged 7–12 months (9/406; 2.2%). HPIV-2 was not isolated as frequently as HPIV-3 or HPIV-1, but the highest frequencies of HPIV-2 were found in patients’ age groups of 0–3 months (4/316; 1.3%) and 4–6 months (3/274; 1.1%). Only 8 (0.2%) patients were HPIV-4 positive in this study, and patient age ranged from 5 months to 8 years.

66 of 178 (37.1%) HPIVs-positive-patients were co-infected with other 11/13 concerned pathogens except HCoV-HKU1 and CP. Pathogens with the highest frequency of co-infection with HPIV were RSV (18/66; 27.3%) and MP (18/66; 27.3%), followed by EV (13/66; 19.7%) and HCoV-OC43 (10/66; 15.2%) (Table 1). The vast majority of co-infections were in children (64/66; 97.0%), especially in patients under 5 years of age (63/66; 95.5%) (Figure 1). The co-infection rate of HPIV-2 was 63.2% (12/19), the rate of HPIV-4 was 50% (4/8) the rate of HPIV-1 was 39.7% (23/58) and the rate of HPIV-3 was 33.3% (33/99) (Table 1).

In general, detection of HPIVs increased as autumn turned to winter (September 2009 to November 2009; September 2010 to October 2010) and summer turned to autumn (April 2011 to July 2011). HPIV-3 and HPIV-1, the two most frequently isolated types, predominantly drove these seasonal trends. HPIV-2 and HPIV-4 had different seasonal patterns, and were mainly isolated as winter turned to spring (December 2010 to March 2011) (Figure 2).

4447 of 4755 (93.5%) patients, and 174 of 178 (97.8%) HPIVs-positive patients’ clinical presentations were analyzed. Patients with incomplete clinical data available were excluded from the clinical data analysis. We compared the clinical characteristics of HPIV-positive to HPIV-negative patients, characteristics of each of the HPIV types, and characteristics of single HPIV infections to co-infections (Table 2).

Significant differences were seen between HPIV-positive and HPIV-negative patients for pharyngeal discomfort (p<0.001), hoarseness (p=0.015), “Abnormal pulmonary breathing sound” (p<0.001), “Dyspnoea” (p<0.001), “Pneumonia” (p=0.01), and “Diarrhoea” (p<0.001) (Table 2). In HPIV-positive samples, the proportion of patients with “Bronchopneumonia” was 13.8% (24/174) and the proportion with “Increasing lung marking” was 5.7% (10/174), although these proportions were not significantly different from HPIV-negative patients (p=0.079 and 0.056). HPIV-positive patients were less likely than HPIV-negative patients to present with each of the six symptoms of “Systemic influenza-like symptoms” (p<0.001) (Table 2).

The only significant difference in clinical characteristics between patients solely infected with HPIV and those co-infected was “Hoarseness” (p=0.037), present in 7 patients with “single HPIV” but no co-infected patient (Table 2).

The only significant difference in clinical presentation between HPIV types was “Expectoration,” in which 49/97 (50.5%) HPIV-3 positive patients, 9/18 (50%) HPIV-2 positive patients, 11/57 (19.3%) HPIV-1 positive patients and 1/8 (12.5%) HPIV-4 positive patients presented with the symptom (p<0.001) (Table 2).

Within HPIV-positive patients, 10/10 (100%) adult patients presented with systemic influenza-like symptoms, while 90/164 (54.9%) paediatric patients presented with these symptoms (p=0.005).