Introduction
While international trading and tourism has huge sociological and economic benefits, it also markedly increases the vulnerability of national populations to emerging and re-emerging infectious diseases. In particular, the ability to travel between almost any two points on the planet within 24 h provides the potential for epidemics to rapidly evolve into pandemics [Reference Fricker and Steffen1–Reference Tatem3]. On the 31 December 2019, the Wuhan Municipal Health Commission reported the first cluster of individuals infected with coronavirus disease-2019 (COVID-19), at the time being an unknown pneumonia inducing disease [4]. By the end of January 2020, cases of COVID-19 had been reported in 26 countries outside of China [5]. Less than 6 weeks later, with cases being reported in 114 countries and territories, the World Health Organisation declared the COVID-19 outbreak a pandemic [6].
The World Health Organisation (WHO) recommends in its International Health Regulations [7] that all WHO States should have the capability to implement some form of screening at international points of entry during times of outbreak. Such screening has previously involved using thermal cameras to scan for signs of fever and asking travellers to self-declare any signs of symptoms via a questionnaire. These methods are both less than perfect and have led many to suggest that screening at the point of entry alone is not a worthwhile endeavour [Reference Priest8, Reference Bitar, Goubar and Desenclos9]. This is supported by fact that health officials in Canada, Australia and Singapore failed to detect a single severe acute respiratory syndrome (SARS) case during the 2003 outbreak while border screening was being enforced (by means of a self-reporting questionnaire and visual and temperature screening) [Reference St. John10–Reference Wilder-Smith, Goh and Paton12]. To investigate these claims, we use mathematical modelling to simulate an idealised border screening process, through which we calculate the maximum detection rates that might be expected by the implementation of a perfect border screening programme (being able to detect 100% of infected travellers who have fully incubated) across a range of scenarios. The detection rates obtained then describe the upper limit of protection that such a programme might provide against disease ingress during an ongoing outbreak. Thus, as real-world screening methods will always be less than perfect (due to non-compliance, false negatives, travellers obscuring symptomologies, etc), these upper limits then allow us to assess the value of a simple test at the point of entry as a method of safeguarding a nation against importations. We present a simple mechanistic model that represents the process of a COVID-19 infected traveller attempting to undertake international travel and gain entry to some destination country where such a hypothetically perfect border screening policy is being enforced. The model is then run repeatedly utilising Monte Carlo simulation, capturing the stochastic nature of the various processes involved, to calculate the likelihood that an infected person would be detectable upon arrival at the border of the destination country. The model we produce is easily extendable to other diseases and as such, we apply our model to simulated outbreaks of influenza, SARS and Ebola for comparison.
Assumptions
Work presented in the following is based upon the subsequent set of assumptions:
• All simulated individuals are assumed to have been infected prior to travelling,
• The distribution of time of infection, D exp, is uniform across the ranges 0–72, 0–168 and 0–336 h prior to flying, simulating where an infection has occurred during a short break, a holiday or more longer-term travel
• Border screening only detects travellers following a period of incubation; prior to completion of this they are not detectable
• Exit screening is being enforced in the country of origin so persons who have become detectable before boarding their flight do not fly
• All persons travelling only take direct flight from their country of origin to the destination country
• The distribution of flight times, D flight, are uniform across the ranges 3–5, 7–9 and 11–13 h to represent short, medium and long-haul flights respectively.
• All people attempting to cross the border are screened
• Screening does not produce false negatives
• The number of infected persons remains constant throughout the simulation (transmission and death are neglected)
• Screening detects all infected persons who have incubated; we do not consider ‘recovery’
• Infected people do not attempt to ‘game’ the system by concealing signs of infection
We reiterate that the presented model assumes a ‘perfect’ border screening process (as defined above) is being used, so the above assumptions have been chosen to reflect this.
Methods
Our model uses Monte Carlo methods to approximate the likelihood that infected travellers, attempting to travel from country A to country B, would be detected on arrival to country B following a range of infection and travelling scenarios. We simulate a large number of infected travellers, each of which is assigned a time of infection (t exp), an incubation period (t inc) and a flight time (tflight), sampled from the distributions D exp, D inc and D flight respectively. These distributions are given as parameters to the model and represent the scenario being considered (note that the disease being considered is characterised in the model solely through the incubation period distribution provided here). For each traveller, these values are compared to determine whether they would become detectable prior to departure, during transit or post-arrival. Results are then compiled, disregarding the travellers that would be detectable prior to departure, to determine what probability that infected travellers would be detectable (and thus detected) by a perfect screening process deployed at country B's border given that they manage to board their flight. More explicitly:
• If t inc < t exp, the traveller has become detectable before boarding their flight and therefore does not travel (either by not being well enough to fly, or being picked up at exit screening); they exit the model being recorded as a non-flier
• If t exp < t inc < t exp + tflight, the traveller has become detectable in transit and will therefore be detected by screening at country B's border; they exit the model being recorded as a border-detection
• Else t inc > t exp + tflight, and the traveller has not become detectable prior to arriving at country B's border and thus crosses into country B undetected; they exit the model being recorded as undetected.
This is visualised in Figure 1:
Each scenario is evaluated by simulating 1 000 000 infected individuals. We then take the ratio of border detections against the number of infected persons who manage to board their flight to get an approximate probability that border screening will capture infected travellers. A pseudo-code breakdown of this algorithm is included in the Supplementary Text, while the Python package used to implement the above model has been made openly available online [13].
Screening for COVID-19
The below results were obtained by applying our model to COVID-19 across all combinations of travel and infection scenarios described above. The incubation period distribution has been modelled using a log-normal distribution with parameters μ = 1.6112 and σ = 0.47238, which was obtained by parameterising results taken from [Reference Linton14] (method of parameterisation is included in the Supplementary Text) (Table 1).
Screening for influenza, SARS and Ebola
We repeat the above for simulated outbreaks of influenza, SARS and Ebola, while also including results for COVID-19. As the rest of the method remains applicable, we need only substitute in incubation period distributions for each of these diseases. These have been taken from [Reference Nishiura, Wilson and Baker15], [Reference Kuk and Ma16] and [Reference Pettey17] for influenza, SARS and Ebola respectively (for the derivation of gamma distribution parameters see Supplementary Text). For brevity, we have averaged the results across flight time ranges for each disease (a table containing a full set of results is included in Supplementary Text) (Table 2)
Discussion
With our best-considered scenario suggesting that screening for COVID-19 would detect less than 9% of infected travellers under ideal conditions, it is clear that our model seems to indicate that the implementation of a single-test screening process, of any kind, is not sufficient to cause a significant reduction in the expected number of infected travellers entering a destination country during the COVID-19 pandemic. Recall also that this is assuming 100% compliance and use of a perfect test, so detection rates in the real world are expected to be even less. Detection rates also decrease with shorter average flight time, meaning screening would be even less effective on travellers arriving via short-haul flights (which would presumably be the most numerous). The intuitive reason for such minimal detection rates would be, considering the average incubation time of COVID-19, that the amount of extra time afforded to individuals by their flight is not substantial enough to expect a notable proportion of infected travellers to complete their incubation period and become detectable prior to arrival (hence also the decrease with shorter flight times) (Fig. 2).
This argument also appears to be supported by the results obtained when applying our model to outbreaks of influenza, SARS and Ebola; detection rates for which are plotted in the above graph. Comparing detection rates between COVID-19 and SARS first (being related diseases that have similar incubation periods), we see that detection rates are roughly in the same ballpark across all scenarios, with screening still detecting less than 10% in the best case. However, when we consider COVID-19 against influenza or Ebola (both have markedly shorter and longer average incubation periods respectively), we see from the above that in the best case we may expect to detect just under 35% of influenza cases and 3% of Ebola cases. What this could indicate is that a single-test border screening process might present a viable intervention for diseases that have very short incubation periods (on the scale of hours), or that incorporating some additional step that provides travellers with additional time in which they might incubate (such as isolating on arrival) might make this a more successful undertaking. However, a reduction of at most 9% of arriving COVID-19 cases would be a hard sell to any public health team considering the potential cost. We would therefore conclude by stating that the results presented here suggest that border screening, as described in this paper, does not present the potential to serve as a suitable intervention to prevent the ingress of further COVID-19 cases. Furthermore, while a possible 35% detection rate for influenza might seem sizeable in comparison to the results from the COVID-19 modelling, it still does not offer a reduction on the scale that might be desired to fully safeguard a nation from the threat of an external outbreak, with a similar conclusion being reached on all of the other of the diseases considered.
The model we described and used to obtain these results is technically simple and can therefore be rapidly evaluated with modern computation. Additionally, this simplicity allows our model to remain flexible, and easily amended to consider other diseases, infections and travelling scenarios. While such considerations were explicitly disregarded during this work, one disadvantage is that the model does not allow for the consideration of the effects of personal behaviours (i.e. infected persons attempting to obscure signs of their infection during screening) or disease dynamics (i.e. the infection of fellow travellers during transit). However, our work seeks to provide an upper bound to the potential benefit of border screening, and as such considerations would act to only decrease expected detection rates, neglecting these aspects are appropriate for the aims of this work. For the consideration of more realistic scenarios, these factors could be readily implemented in future versions of this model.
Conclusion
In this paper, we have presented a simple and adaptable Monte Carlo-based model which can be rapidly evaluated across a range of outbreak scenarios. We then used this model to assess the maximum protective effect that border screening could provide nations from international travellers infected with COVID-19. Our model assumed the implementation of a hypothetical screening process with the ability to detect 100% of incubated cases and was applied across a range of infection and travel scenarios. Despite this, our model indicated that nations could not expect border screening alone to detect more than 9% of arriving travellers infected with COVID-19. In addition to this, we also applied the presented model to simulated outbreaks of influenza, SARS and Ebola; yielding maximum detection rates of 34.8%, 9.7% and 3.0% respectively. Furthermore, while real-world screening methods are less than perfect, observed detection rates through a single point of entry test would reasonably fall below these values in a live scenario. Our model also allowed us to infer that border screening might expect to be more effective when testing for diseases with shorter incubation periods, however as mentioned above, results indicated that screening alone still did not offer sufficient protection from international outbreaks. This model may in future be developed by incorporating some aspect of disease transmission and/or behavioural aspects in infected travellers.
Data availability statement
All results described in the work, in addition to technical descriptions of methods used, are made available in the Supplementary Material. The Python package used to implement these methods and obtain our results has been made accessible online [13].
Supplementary material
The supplementary material for this article can be found at https://doi.org/10.1017/S0950268821002387.