ARIZONA study: is the risk of post-herpetic neuralgia and its burden increased in the most elderly patients?

644 GPs enrolled in the ARIZONA study 1,517 patients aged 50 years and over, of whom 1,358 satisfied the inclusion criteria. Out of these 1,517 patients, 609 (45%) were 70+ and were included in the present complementary analysis: 383 patients (62.9%) were between 70 and 79 years of age and 226 (37.1%) were 80+; respectively, 220 (36.1%), 163 (26.8%), 137 (22.5%), and 89 patients (14.6%) belonged to the 70–74, 75–79, 80–84, and 85+ age-groups.

Table 1 presents the main baseline characteristics of the elderly patients in each of the four age-groups. In all age-groups, there were more women than men. Comorbidity (mainly cardiovascular disease) was frequent in all age groups (>70%).

Table 2 presents HZ characteristics at baseline. The time-interval between rash onset and HZ diagnosis was commonly ≤2 days in all age-groups. Rash severity did not qualitatively or quantitatively increase with age after 70 years. Ophthalmic zoster location was more frequent in the most elderly patients although the difference between age-groups was not significant (p = 0.57): the frequency of ophthalmic zoster ranged from 5.5% in the 70–74 age-group to 9.0% in the 85+ age-group.

HZ-related pain, whose onset always slightly preceded rash onset in all age-groups, was frequent at baseline (reported by about 80% of patients, n = 486). It was of moderate intensity without difference between age-groups: mean NPSI score around 30 and mean worst pain ZBPI severity score around 5 in all age-groups (Table 2). Burning pain was the main descriptor (data not shown).

98.5% of patients had at least one medical prescription, mainly antiviral drugs (94.7%) and analgesics (86.5%). The percentage of patients under treatment did not differ with age.

Results are presented in Table 3. At baseline, HRQoL, and mood were impaired in all age-groups: mean ZBPI interference scores were around 3, mean SF-12 PCS and MCS scores were below 50, and mean HADS depression scores close to 8.

No significant difference was found in mean ZBPI interference scores between the four age-groups (p = 0.582).

As regards HRQoL, SF-12 PCS scores decreased significantly with age (p < 0.001), indicating greater HRQoL impairment in the most elderly patients. The low SF-12 PCS scores observed in the 85+ age-group were mainly due to the scores of the ‘physical functioning’ and ‘vitality’ dimensions. No statistically significant difference in SF-12 MCS scores was observed between the four age groups (p = 0.413).

As regards mood, HADS depression scores increased significantly with age (p < 0.001), indicating greater mood impairment in the most elderly patients. No statistically significant differences in HADS anxiety scores were observed between the four age groups (p = 0.237).

Figure 1 presents the percentage of patients who reported HZ-related pain from day 0 to month 12. Prevalence of HZ-related pain dramatically decreased between day 0 and month 3 in all age-groups: overall, 66 patients (14.3%) had PHN at month 3. Prevalence of PHN slightly decreased from months 3 to 12: 30 patients (7.6%) had PHN at month 12. At months 3, 6 and 12, the percentage of patients with PHN was always higher in the 85+ than in the other age-groups. However, no statistically significant difference was found between the four age-groups (p = 0.58, p = 0.34, and p = 0.24, respectively).Figure 2 presents mean NPSI scores from day 0 to month 12 in each age-group in patients who reported HZ-related pain (day 0) or PHN (months 3, 6 and 12). Pain intensity assessed by NPSI decreased significantly between day 0 and month 3, and then decreased slightly between months 3 and 12 in all age-groups except for the 85+ age-group at month 6 and the 80–84 age-group at month 12, leading to a statistically significant interaction between time and age (p = 0.01).

During follow-up, ZBPI interference scores in patients with HZ-related (day 0) or PHN (months 3 to 12) remained high (around 3), with no difference between age-groups (data not shown).Figure 3 presents mean SF-12 PCS and MCS scores from day 0 to month 12 in each age-group. SF-12 PCS scores increased slightly, from day 0 to month 12, in all age groups (p < 0.001), indicating slight improvement in HRQoL. These results were always driven by the ‘physical functioning’ and ‘vitality’ scores (data not shown). In addition, at each time point, SF-12 PCS scores were lower in the 85+ age-group than in the other age-groups (p < 0.001), indicating greater HRQoL impairment in the most elderly patients. Comparison within the 85+ age-group found a significant difference in SF-12 PCS scores between patients with and without PHN at month 3 (mean +/− SD: 27.0 +/− 11.26 and 37.6 +/− 12.26, respectively; p = 0.015), but not at months 6 and 12 (p = 0.956, and p = 0.919, respectively), indicating that impact of age and its comorbidities prevails over consequences of PHN. Regarding SF-12 MCS summary scores, from day 0 to month 12, SF-12 MCS scores increased in all age-groups (p < 0.001), indicating an improvement in HRQoL, without statistically significant difference in SF-12 MCS scores according to age (p = 0.27).Figure 4 presents mean HADS depression and anxiety scores from day 0 to month 12 in each age-group. HADS depression scores decreased from day 0 to month 12, in all age-groups (p < 0.001), indicating mood improvement. In addition, at each time point, HADS depression scores were greater in the 85+ age-group than in the other age-groups (p < 0.001), indicating greater mood impairment in the most elderly patients. Comparison within the 85+ age-group found no significant difference in HADS depression scores between patients with and without PHN at months 3, 6, and 12 (p = 0.52, p = 0.83, and p = 1.00, respectively), indicating that the impact of age prevails over consequences of PHN. However, when patients were classified into two age-groups, in the 80+ age-group, HADS depression scores significantly differed between patients with and without PHN at months 3 and 12 (p = 0.01, and p = 0.04, respectively) but not at month 6 (p = 0.30). HADS anxiety scores decreased from day 0 to month 12, in all age-groups (p < 0.001), indicating mood improvement, without statistically significant difference according to age (p = 0.60).

Older age has long been considered as a risk factor for severe pain during the acute phase of HZ infection [3]. In the entire ARIZONA cohort, we showed that at baseline the proportions of patients with extensive rash or haemorrhagic or necrotic lesions were higher in patients 70+. By contrast, no difference between groups of patients was observed in the frequency or severity of HZ-related pain at inclusion [16]. In the MASTER study [23‐25], older age also ‘emerged as an independent predictor of greater severity-of-illness over 180 days, but not during the first 90 days after rash onset’. According to the authors, this result indicated that younger patients were as likely as older patients to experience considerable burden during the acute phase of HZ, but had a lower risk of developing PHN and consequently experiencing lower severity-of-illness over the entire episode. The present results confirm that, in patients 70+, the incidence of HZ-pain during the acute phase was large and similar in all age groups: regardless of age, approximately 80% of them reported HZ-related pain. Our data also indicate that there is no specific age cut-off after 70 years of age at which the frequency or intensity of pain during the acute phase of HZ infection is further increased. However, this analysis shows that the ophthalmic location of HZ infection tended to increase with age, from 5.5% in the 70+ group to 9% in the 85+ group.

Depending on the time-frame used in the literature, PHN occurs in 5% to more than 30% of patients [26]. Several possible risk-factors such as age, immunodepression, prodromal pain, and ophthalmic zoster have been considered [25]. PHN, defined as HZ-related pain persisting ≥3 months, was reported by about 30% of 70+ patients in an Icelandic study [27], 13% of 70+ patients in the ARIZONA study, and 45% of patients in the MASTER study [23‐25]. After one year, 15% of 70+ patients in the Icelandic and 8% of the same age class in the ARIZONA study still had pain. The percentage of subjects with PHN was lower in the ARIZONA study than in the MASTER study. In the ARIZONA study [16], however, antiviral drugs were prescribed to 94.1% of patients for a median 7 days, which may have contributed to reduce the intensity of acute pain, accelerate vesicular rash healing and reduce acute-phase viral excretion duration [28]; conversely, in the MASTER study [23], only 26% of included patients received antiviral medication at the recommended dose and time. Although the efficacy of antiviral medication in PHN prevention is controversial [29], it may thus be hypothesised that early initiation of adequate treatment may have contributed to the lower prevalence of related pain at 3 months as compared with the MASTER study [23‐25]. These findings nevertheless support the need for preventive vaccine strategies in elderly patients since more than 1 in 10 patients will develop PHN even with adequate treatment. Vaccination was shown to reduce the incidence of HZ and PHN and the HZ burden of illness (a composite end point sensitive to the incidence, severity and duration of HZ pain), to have a good safety profile [17, 30], and to be cost effective in elderly patients [31, 32]. Centers of Disease Control and Prevention (CDC) recommended HZ vaccine for prevention of HZ and its complications among adults aged 60 years or more [33].

According to the literature, older age is an independent factor of PHN [3‐7]. The ARIZONA study showed that older age (70+) at baseline was an independent predictive factor for PHN [16]. Severity of HZ-related pain was comparable for 70+ patients and younger, but the prevalence was significantly higher for 70+ patients at months 1, 3, 6, and 9 and close to significance at month 12. The present data showed that the percentage of patients with persistent HZ-related pain at months 3, 6, and 12 was systematically but not statistically significantly higher in the most elderly patients (i.e. 85+).

Pain intensity appeared to remain constant in patients with persistent HZ-related pain (regardless of age). This additional result was partly consistent with that of the Canadian MASTER study, which found that mean pain intensity decreased during the first month of the disease and then remained stable from months 1 to 6 [23]. In addition, no clear difference in the severity of PHN was observed according to age. This can possibly be partly explained by a negative influence of age on perceived degree of pain, as shown in acute myocardial ischemia as being a possible cause for delayed treatment in elderly patients, with a similar cut-off at 69 years [34].

It has been previously described that the PCS score of the SF-12 shows impairment with age, and that HZ infection severely impacts HRQoL [35, 36]. In addition, it has been recently showed that an episode of HZ could lead to comorbidity decompensation and could jeopardize the health status of an older person with concomitant diabetes, COPD, or cardiovascular disease [37]. An impairment of HRQoL due to both age and PHN could thus be expected in the oldest patients in the ARIZONA study. In fact, only the physical component of HRQoL as assessed by the SF-12 PCS and depression as assessed by the HADS were impacted by age. Indeed, the difference over 8 points of baseline SF-12 PCS score between 85+ and 70–74 age groups exceeds the minimal important difference of 3 points, by a meaningful [12].

However, the absence of significant difference can also be explained by some of the limitations in this our study. A selection bias cannot be ruled out as only data from patients who agreed to participate in the study were collected. However, the mean number of included patients per GP was consistent with the mean number of patients seen in general practice for HZ according to the French GPs Sentinelles network (https://​websenti.​u707.​jussieu.​fr/​sentiweb/​?​page=​presentation), indicating that almost all patients seen for HZ by a GP agreed to participate in the study. The second limitation is the small sample size and heterogeneity of the different age-groups (although as a whole, the sample size of ARIZONA cohort was large, with over 1,350 patients), which may not be sufficient to detect any effect. However, similar results were usually observed when patients were classified into two larger age-groups (70–79 and 80+). Finally, although the frailty risk increases with age, the population of 70+ patients is probably highly heterogeneous: both well and frail patients with various chronic diseases are included in each age-group. That is why it is difficult to separate influence of HZ and age and chronic diseases. Further longitudinal studies with a large number of very old patients assessing chronological and physiological ages or frailty are thus needed to evaluate HZ and PHN burden in the 70+. Indeed, beyond the age of 70 years, HZ and PHN can impair frail patients. In the model by Rockwood et al., frailty can be thought of as a dynamic balance between assets which help maintain a person’s independence and deficits which threatens a person’s self-sufficiency or functional capacity. In frail elderly, HZ and PHN can tip the balance in favour of the deficit [38].