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Systematic selection between age and household structure for models aimed at emerging epidemic predictions


Numerous epidemic models have been developed to capture aspects of human contact patterns, making model selection challenging when they fit (often-scarce) early epidemic data equally well but differ in predictions. Here we consider the invasion of a novel directly transmissible infection and perform an extensive, systematic and transparent comparison of models with explicit age and/or household structure, to determine the accuracy loss in predictions in the absence of interventions when ignoring either or both social components. We conclude that, with heterogeneous and assortative contact patterns relevant to respiratory infections, the model’s age stratification is crucial for accurate predictions. Conversely, the household structure is only needed if transmission is highly concentrated in households, as suggested by an empirical but robust rule of thumb based on household secondary attack rate. This work serves as a template to guide the simplicity/accuracy trade-off in designing models aimed at initial, rapid assessment of potential epidemic severity.


Patterns of interactions and contacts between individuals in populations are recognised as important factors shaping the spread of infectious diseases1,2. Mathematical models are routinely used in analysis of epidemic data and prediction of epidemic trends3,4. A wealth of different options for how to describe social interactions in mathematical models is available, ranging from assuming homogeneous mixing5,6, through analytically tractable models that focus on households, age structure or other idealised properties of the contact network1,2,7,8, to complex individual-based stochastic simulations1,9,10,11,12. However, few comparative tools exist to guide the initial choice of structure when designing a mathematical modelling study. One common approach is statistical, comparing models by their ability to fit the data, or seeking a trade-off between the quality of data fitting and model parsimony. However, when data are limited, like at the beginning of an emerging epidemic, different models can fit the same data equally well and nevertheless lead to different predictions. These methods would then favour the simplest model, and would therefore not highlight whether further data should be collected to parameterise a more complicated model whose predictions can be significantly different.

Another comparison approach, rather than ranking models or selecting the best one, retains them all and combines their predictions to quantify uncertainty not only owing to stochastic dynamics and unknown parameters/initial conditions13,14, but also to lack of knowledge on the correct model structure. Such multi-model ensemble methods, well established in the field of numerical weather forecast15, have recently started gaining momentum in epidemiology16,17,18, with different modelling groups sometimes asked to perform predictions of the impact of realistic control policies based on shared scenarios10,18,19,20,21. These comparative studies have proven popular with complex models and policy makers concerned with over-reliance on advice from single modelling groups, but so far have provided little insight into the causes of differences between models. In addition, unidentifiability issues owing to the large number of parameters are sometimes not discussed, and often dealt with through an informal and difficult-to-reproduce calibration procedure22. Furthermore, comparing models by fitting them to the same set of data (or small number of shared scenarios23) provides results that are useful in that specific context but often hard to generalise to other settings18,23 or pathogens.

Therefore, here we take a more mathematical approach and we compare a few popular and relatively simple models when varying widely and systematically the constraints they are required to fit (i.e., the hypothetical data we would observe and fit them to). Particular attention is devoted to being as transparent as possible in the details of the process and the unidentifiability issues encountered, and to understand how the different components of model structure interact and cause differences in predictions. In this sense, our approach is complementary to the multi-model ensemble studies discussed above.

To make extensive comparison computationally feasible, we focus on a specific context where numerous analytical results are available: assuming we are observing the early phase of an emerging epidemic of a novel, directly transmissible, human infection, we explore the joint contribution of age stratification and household structure on its spread in a large and fully susceptible population. There is an extensive literature on age stratification in epidemic modelling6,24 and an increasing amount of empirical data on age-specific patterns of mixing25,26,27. There is an equally extensive literature on household structure28,29,30 as well as empirical data on estimation of household transmission parameters31,32,33,34,35,36. Epidemic models with age and household structure are among the most analytically tractable, and are thus particularly suited to rapid use in an emerging epidemic situation.

Our aim is to compare four different models: an age- and household-stratified model (hereafter denoted AH), a pure age-stratified (A), a pure household-stratified (H) and an unstructured (U) homogeneously mixing model. We then test the ability of these different models to predict: the average final size (z), the average peak daily incidence (π) and the average time to the peak daily incidence (t) of a single epidemic wave. Given model AH includes all others as submodels, we compare predictions by assuming model AH perfectly represents reality and measuring other models’ deviations from it. More specifically, we extensively explore the parameter space of model AH and for each parameter combination we compute, in addition to the outputs of interest, those quantities that are most likely to be measured or estimated from early data in the initial phase of the epidemic, namely: the basic reproduction number R0, i.e., the average number of cases a typical case generates in a fully susceptible population (this is not trivial for models with households; see Methods and Supplementary Methods, Sections 1.2.4 and 1.4); the ratio of adults versus children among new incident cases; and the household secondary attack rate (SAR), i.e., the average size of a within-household outbreak. These quantities, hereafter referred to as the observables, are then used to map (i.e., compute deterministically, assuming no error or noise) the parameters of the models A, H and U, the outputs of which are then compared with the assumed-true ones of model AH and considered inaccurate when they differ by more than a specified threshold ε in relative terms. In computing model outputs and observables, we assume permanent immunity following infection, as well as constant parameter values and no demographic changes, i.e., we have in mind a relatively fast infection with negligible disease-induced mortality and no intervention nor behavioural or environmental change. In addition, despite the models used here being stochastic, for maximum computational efficiency we only focus on average values (infinite population limit).

Despite the rather specific scenario and limited range of models, this work provides a simple rule of thumb that, early on in an outbreak of a new emerging infection, can help striking the crucial balance between model simplicity and prediction accuracy when choosing a model aimed at rapid initial assessment of likely epidemic severity in the absence of interventions.



As baseline scenario we consider: age and household structure of Great Britain, random mixing, R0 = 2, adults and children equally infective (relative infectivity ϕ = 1) and an accuracy threshold ε = 5%. We fully explore the models’ behaviour for a within-household infectious-adult-to-susceptible-adult transmission probability paa ranging from 0 to 0.95 and for children from equally to four times as susceptible as adults (relative susceptibility ψ ranging from 1 to 4) in Fig. 1. We then compare models in Fig. 2. Other values of R0 (from 1.1 to 4) and ϕ (from 1 to 2), UK-like contact patterns relevant to respiratory infections and a markedly different social structure (corresponding to Sierra Leone) are then explored in Figs. 3 and 4. Further sensitivity analyses, including intermediate contact patterns and social structures, other thresholds ε (1% and 10%), and the case of children less susceptible/infective than adults (ϕψ < 1), are reported in the Supplementary Discussion (Sections 2.3.1, 2.3.4, 2.1.3 and 2.3.3, respectively).

Fig. 1: Models’ output under baseline scenario.

For models AH (first row: ac), A (second row: df) and H (third row: gi), the average epidemic final size z (first column: a, d and g), average peak daily incidence π (second column: b, e and h) and average time to peak daily incidence t (third column: c, f and i; time expressed in multiples of the generation time TG) are plotted as functions of the within-household transmission probability paa and the relative susceptibility of children versus adults ψ. The top row (model AH) is assumed to be a perfect representation of reality. The outputs of model U are not plotted, as they are independent of both variables on the axes (they depend only on R0), but can be read in the bottom-left corner of panels in each column, where predictions of all models coincide. The baseline scenario assumes: population structure of Great Britain, random mixing (same contact rates for adults and children in all environments, γg = γh = 1, and global assortativity of children θg = 22.73%—within-household random mixing is always assumed), R0 = 2 and children as infectious as adults (ϕ = 1).

Fig. 2: Simplest-model acceptance regions and examples of epidemic dynamics.

Colours refer to regions of parameter space where no (dark blue), each (age: light blue; households: yellow; either, indifferently: green) or both (red) forms of social structure need to be included in the model in order to compute within 5% relative accuracy of the assumed-true outputs of model AH: a the final size; b the peak daily incidence; c the time to peak daily incidence; and d all of them simultaneously (overall simplest-model acceptance regions plot, where simpler models are discarded if at least one of the three outputs is not sufficiently accurate). Parameters are as per baseline scenario (population structure of Great Britain, random mixing, R0 = 2, ϕ = 1). On the right-hand side eh, epidemic dynamics of the four models at different parameter regimes indicated by the corresponding points labelled in orange in panel d: daily incidence (solid line, left axis) and cumulative incidence (dashed line, right axis) are plotted for models AH (red), A (light blue), H (yellow) and U (dark blue). The black dash-dotted line gives the total population size (right axis), to which cumulative incidence should be compared.

Fig. 3: Sensitivity analysis on overall simplest-model acceptance regions.

a Overall simplest-model acceptance regions for various values of R0 (1.5, 2 and 4; increasing from left to right) and the relative infectivity of children versus adults ϕ (1, 1.5 and 2; increasing from top to bottom) for the population structure of Great Britain, assuming baseline random mixing. Simple models are rejected when at least one of the three predicted outputs (final size, peak daily incidence and time to peak incidence) differs in relative terms by more than 5% from those of model AH (the panel corresponding to R0 = 2 and ϕ = 1 is identical to Fig. 2d). The overlaid orange labels cover the zones of the parameter space approximately associated to some realistic infections: (1) H1N1 2009 pandemic influenza; (2) 1918 pandemic influenza; (3) a highly infectious disease, with characteristics similar to measles or chickenpox. b Same plot as in a, but for UK-like contact patterns (γg = γh = 0.75) and assortative mixing (θg = 58%), with overlaid contour lines for the SAR (%, black lines).

Baseline scenario

We first describe the outputs of each model in absolute terms in the baseline scenario. Model U predicts a final size z of 80%, a peak daily incidence π of 5.5% and t = 9.8 generation times to the peak (we chose the generation time37 as the time unit to facilitate translation to other infections). These values are common to all models (Fig. 1, bottom-left corner of all panels) when there is no household transmission (within-household transmission probability paa = 0) and children and adults are equally susceptible (relative susceptibility ψ = 1). For a fair comparison, the parameter explorations for all models are performed at fixed R0, i.e., larger values of the within-household transmission probability paa correspond to suitably smaller values of between-household transmission. Both the final size z (Fig. 1a) and the peak incidence π (Fig. 1b) appear to decrease when increasing age difference in susceptibility (i.e., increasing ψ): this result is known for the final size in the absence of households5,38,39, but appears to hold also for the peak incidence, and to extend to any amount of within-household transmission. Conversely, both outputs increase when transmission is shifted from between to within households (increasing paa at constant R0). Comparing Fig. 1a, d and g and b, e and h, it appears that, for both final size z and peak incidence π, model A is better than model H at mirroring the qualitative behaviour of model AH (though note that model H has only two free parameters, whereas model A has four, of which two shared with model AH: see description of model A in the Methods and Supplementary Discussion, Section 2.1.2). It also appears that the joint contribution of age and household structure in model AH can be roughly decomposed in the separate contribution of the two social structures (Fig. 1a, b contain elements of d and e for increasing ψ, and of g and h for increasing paa), but that models A and H, respectively, underestimate and overestimate both the final size and the peak incidence. Predictions of time to the peak t (Fig. 1c) seem to decrease when increasing both paa and ψ, but are more complex to interpret and overall show limited variation (much variation would come from stochastic delays in the very early epidemic phase, but these are minimised on purpose to detect structural differences in epidemic speed between models). Results are qualitatively similar for other values of R0 and relative infectivity ϕ (see Supplementary Discussion, Section 2.1.2).

In Fig. 2a–c, we highlight the regions where either or both forms of social structure need to be included in the model to accurately capture each of the three outputs of model AH. Those regions are then combined in Fig. 2d into an overall simplest-model-acceptance-region plot, in which a less-structured model is rejected when at least one of the outputs is too inaccurate. Model U appears accurate for both the final size z and peak incidence π in a diagonal region of the parameter space, i.e., when the increase owing to stronger within-household transmission and the decrease owing to larger age differences cancel each other out. The graph for the time to the peak t is more complex, and highlights the presence of a region where at least one structure, no matter which, is needed, but not necessarily both (green area in Fig. 2c).

Four different parameter sets are then arbitrarily chosen, one in each region of the overall plot in Fig. 2d (orange labels e–h). For each choice, Fig. 2 (respectively, panels e–h) compares the full incidence and cumulative incidence curves of the models and suggests that the regions given in Fig. 2d indicate when models U, A and H approximate well not only the three outputs of interest but also the full dynamics of model AH.

Sensitivity analysis

Finally, we explore how results depend on the remaining two parameters of model AH. Figure 3a reports the overall simplest-model acceptance regions for varying values of R0 and the relative infectivity of children versus adults ϕ, still under baseline random mixing. For increasing R0 (left to right), the household structure becomes less relevant for accurate predictions, unless within-household transmission is extremely high. Intuitively, at least for the final size, this is because at large R0 almost all the population ends up infected, leaving very little room for stronger within-household transmission to increase it further (Fig. 1a). Despite not being capped, as the final size is by the total population, the peak incidence shows a similar behaviour. Figure 3a confirms the intuition that, under random mixing, the age structure can be neglected when age classes do not differ much in susceptibility and that the household structure can be neglected when not much transmission occurs in households. Quantifying this intuition, however, is an important result of this analysis. On the other hand, when realistic UK contact patterns25 are assumed, as in Fig. 3b, the age structure becomes absolutely crucial for accurate predictions, whereas the household structure remains important only at large values of within-household transmission.

To facilitate intuition about the quantitative meaning of Fig. 3, we locate points in the parameter space corresponding to some scenarios inspired by real infections. Scenario 1 is characterised by parameters in the ballpark of H1N1 2009 pandemic influenza (points 1): R0 ≈ 1.5, ϕ ≈ 1, ψ ≈ 233 and values of paa from 0.1 to 0.4, corresponding to the wide range of SAR estimates found in the literature35, from  <10%40 up to 40%35. At the low end of this range, Fig. 3 suggests the household structure can be neglected, whereas at the high end the household structure should be retained, at least when mixing is heterogeneous (Fig. 3b, points 1). Scenario 2 has parameter values closer to those estimated for the 1918 influenza pandemic34, with a higher R0 than in 2009, and children apparently not more susceptible but potentially more infectious than adults. We choose R0 ≈ 2, ϕ ≈ 2, ψ ≈ 1 and paa ≈ 0.3 (leading to a SAR of ~30%34) and conclude that the household structure can (just about) be ignored, whereas the age stratification is necessary when mixing is heterogeneous (Fig. 3b, point 2). However, we note that the higher transmissibility seen in the 1918 influenza pandemic compared to the 2009 one might be partially owing to a different demography and social structure, in particular with larger households. For Scenario 3, we imagine the hypothetical invasion in a fully susceptible population of a highly transmissible infection, with characteristics similar to common childhood infections like measles or chickenpox: R0 ≈ 4, ϕ ≈ 1 and a trade-off between ψ and paa owing to the fact that only child-to-child estimates of transmission probability are available in the literature (see Supplementary Methods, Section 1.6.5). This leads to a range of possible points 3 in Fig. 3, all of which suggest the household structure can be ignored, whereas the age stratification is essential. Applications to other topical emerging infections (e.g., SARS, MERS, Ebola) would also be possible, though data scarcity and other limitations highlighted in the Discussion suggest conclusions in these cases would be rather tentative. Furthermore, parameter values for SARS and Ebola, with their marked lower susceptibility of children compared with adults41, would not appear in the range displayed in Fig. 3.

Rule of thumb

Overlaying the contour lines for the SAR onto Fig. 3b reveals how the SAR can be used directly (i.e., without estimating paa) to discriminate whether the household structure is needed or not, somewhat irrespective of the relative infectivity and susceptibility of children, but strongly depending on the value of R0. This dependence is explored more extensively in Fig. 4a, where the values of the SAR along the lines at which model A differ by 5% in relative terms from model AH (the borders between the light blue and red regions in Fig. 3b) are collected for all values of ψ ranging from 1 to 4 and for ϕ =  1, 1.5 and 2, and plotted against R0. The relationship appears approximately linear (Fig. 4a) for a wide range of values of R0, except for R0 close to its threshold value of 1 or for a SAR roughly above 70%. Figures 3b and 4 together allow the formulation of an approximate but simple empirical rule of thumb:

Fig. 4: Criterion for inclusion of household structure for accurate predictions.

Empirical rule of thumb specifying the level of SAR above which a household structure is necessary for output predictions within a 5% relative accuracy for the household structure of a Great Britain (fraction of children = 22.73%, mean household size χ = 2.35) and b Sierra Leone (fraction of children = 53.81%, mean household size χ = 5.85), both with UK-like contact patterns and assortative mixing (though of little relevance, as the same rule of thumb also applies for random mixing: see Supplementary Discussion, Section 2.4). For each R0, data points represent the values of the SAR along the borders between the light blue and red regions in Fig. 3b (more precisely, the values of the SAR at each point of the 5% relative error contour lines, which are not explicitly drawn here to reduce clutter, but are shown as think black lines in Supplementary Fig. 16B) for ϕ = 1, 1.5 and 2 and ψ ranging from 1 to 4. Black data points give SAR values associated with more moderate and realistic differences in susceptibility and infectivity between adults and children (ψϕ ≤ 3) and are typically less widespread than grey data points, which correspond to extreme and unrealistic differences (ψϕ > 3). Regression lines (dashed) fit corresponding-colour data points, excluding R0 = 1.1 and 4, where a linear fit looks unreasonable. The thick black line shows the empirical rule of thumb, with parameters reported in the figure (η1, regression coefficient; η0, intercept), and is empirically chosen to: be closer to the dark than the grey dashed line, reflecting low confidence in extreme differences between adults and children; and provide an acceptable fit for both the SAR values obtained assuming UK-like mixing (here) and random mixing (see Supplementary Discussion, Section 2.4). Note that part of the spread in the data points is owing to the ruggedness of the borders between regions (contour lines in Supplementary Fig. 16B): a smaller step in paa and ψ would reduce the spread but increase the computational cost.

For accurate predictions of expected epidemic final size, peak daily incidence and time to peak daily incidence in a developed country with UK-like contact patterns relevant for respiratory infections, the age structure should always be included in the model and the household structure should be present if SAR ≥ (η1 × R0 + η0)%, where R0 can be estimated from the early growth with standard methods (i.e., in the absence of households), η1 = 24 and η0 = −10.

The coefficients of this linear relationship have been determined empirically to carry more weight from values of the SAR associated to more moderate and realistic differences in susceptibility and infectivity of children versus adults (see Fig. 4 and Supplementary Discussion, Section 2.4), and to provide simultaneously a satisfactory fit for both UK-like mixing patterns (Fig. 4a) and random mixing (Supplementary Fig. 25B). The term “accurate” refers to predictions with a theoretical relative accuracy of 5%, given perfect observations and parameter estimates, and assuming model AH is the truth. The possibility of using standard methods of estimating R0, e.g., from the exponential growth rate r, comes from the observation42 that ignoring age and household structure does not fundamentally undermine the accuracy of such estimates (see also Supplementary Methods, Sections 1.1.2 and 1.1.3).

Despite its simplicity, the linear relationship between the SAR and R0 is surprisingly solid, given the amount of complexity captured. In particular, it appears not to be significantly affected by contact patterns (see Supplementary Fig. 25), and is therefore still informative about whether the household structure is needed or not even in the case of random mixing or other intermediate contact patterns, suggesting it can be broadly exported to other developed countries; and it extends to very different social structures (e.g., Sierra Leone, Fig. 4b) and to other accuracy thresholds (Supplementary Fig. 25), though the line coefficients require suitable modifications investigated in the Supplementary Discussion (Section 2.4).

Finally, although in the rule of thumb described above for a developed country with UK-like contact patterns the age stratification appears essential for almost all parameter values explored (ϕ =  1, 1.5 and 2, ψ from 1 to 4; R0 from 1.1 to 4), this is not always the case in general, e.g., with random mixing, a 10% threshold or other social structures (see Supplementary Discussion, Sections 2.1.2, 2.1.3 and 2.3.4). Although a clear condition determining when the age structure is needed for accurate predictions seems less evident to formulate, we deem it also less essential, given the limited complexity the age structure component adds to the model and the wide availability of age-stratified epidemiological data.


The main aim of this analysis is to provide a deeper understanding of the role played by structural model components on epidemiological predictions. For this reason, unlike multi-model ensemble approaches18,23 where models’ outputs are combined into a median or weighted average43, here outputs are kept separate44 to highlight disagreements between models (in the same spirit as structured decision-making17). Furthermore, rather than only focusing on predictions in a single scenario, models are compared on a wide region of the space of observables (i.e., R0, SAR and the ratio of adults and children in the incidence), and sharp boundaries are identified between regions in this space where models behave similarly and regions where they differ.

Overall, our analysis suggests that the age structure seems to be a more rewarding ingredient to add to the model than the household structure, especially, if measured against the respective cost in terms of mathematical complexity. In other words, if one is not interested in the explicit presence of households (details of local transmission, targeted interventions, etc.), their complex and antagonistic effects—longer and more frequent local contacts, but also stronger saturation effects—may often cancel out to a good approximation. This is more likely to be true for large values of R0. However, it is worth emphasising that ignoring households systematically underestimates epidemic severity, predicting a lower final size, lower peak incidence and a later peak time.

The best retrospective example of how this study could have guided model design is the case of the H1N1 2009 pandemic, because of the early availability of data also at the level of households. With initial parameter estimates33,45 as presented above (R0 ≈ 1.5, ϕ ≈ 1 and ψ ≈ 2, somehow capturing prior immunity in the elderly) and average SAR values of the order of 10–13%33, this study would have strongly discouraged the use of complex households models in favour of purely age-stratified ones. In fact, model A would have predicted a final size of 34% (compared with the 35% of model AH), which is much lower than the 58% of the homogeneously mixing model. Current estimates of the final size from retrospective analysis in Italy are even lower (in the range 15–30%12,46), but such discrepancy is easily imputable to interventions and spontaneous social distancing, and possibly a different demography and more refined age structure of these studies compared with the simple two-class one presented here. Later studies reported higher estimates for the SAR35, but even with SAR values ~40% (corresponding to paa = 0.4), on the high end of the range displayed in Fig. 3b, model A would predict a final size of 37%, still very close to the 40% of model AH (a relative difference just above 5%).

These results apply in particular to the case of children being more susceptible and/or infectious than adults, which is the main one discussed here. The situation is more complex in the opposite case, as sometimes we have found the mapping from model AH to model A to fail (see Supplementary Discussion, Section 2.3.3). The insight is that, when children are less susceptible or infectious than adults, sometimes the mixing imposed by the household structure results in an age-stratified incidence that cannot be reproduced by an age-stratified model alone (with the same contact rates), irrespective of the level of assortative mixing assumed. In this sense, the household structure becomes essential to reconcile observed disease dynamics and measured contact rates of adults and children. More research, in particular, on the implications for public health, is needed in this direction. Except in this region of the parameter space, though, the household structure does appear in general less relevant for accurate predictions than the age structure (Fig. 3). Throughout, we have assumed a 5% accuracy threshold, which is probably optimistic in an emerging epidemic scenario. However, the same result appears even more strikingly at less-stringent accuracy requirements, as the need for household structure drops, whereas the age structure, at least with heterogeneous and assortative mixing patterns, remains essential (see Supplementary Discussion, Section 2.2.2 and Supplementary Fig. 16).

At a methodological level this work highlights how, even in a rather simple context, comparing models that are structurally different—i.e., differing in the number and biological meaning of parameters—is not a straightforward and unambiguous process, and requires making choices on which the conclusions may fundamentally depend, in particular, what to keep fixed across models (we argue these should be observable or directly estimable macro-parameters with a model-independent biological interpretation); how model-specific parameters are derived from these observables (a process that might unravel numerous unidentifiability issues); and how models’ predictions are compared.

The choices we made here, though arguably natural, are not unique. For example, we decided to focus only on predictions in terms of the three selected outputs. Despite being chosen for their public health relevance, other outputs might be of more interest, depending on the question addressed. We then only presented results in terms of aggregate outputs (some comments on age-stratified final size appear in the Supplementary Discussion, Sections 2.1.2 and 2.2.2). Furthermore, we also exploited the fact that model AH includes all the others as submodels and we were therefore able to compare predictions by studying the divergence of the outputs of simpler models from the assumed truth of model AH. Alternative choices would be required in the absence of a full model. Finally, we chose to keep R0 fixed across all model, whereas another perhaps even more natural choice would have been to fix the real-time growth rate r. This would have been feasible in the case of models involving constant transition rates between compartments (analytical methods for computing r in the presence of household can be found, e.g., in8), but the lack of exact results in the case of the time-since-infection modelling framework assumed here (see Methods and Supplementary Methods, Sections 1.1.3, 1.2.9 and 1.4) would have caused significant loss in computational efficiency. A brief exploration (only in the baseline scenario: see Supplementary Discussion, Section 2.3.2) leads to similar results, with simpler models appearing even more likely to be accurate than the constant-R0 comparison suggests. This is in line with previous results42,47 showing that ignoring the household structure in the time-since-infection model used here leads to an overestimation of R0: models with households, therefore, when forced to match the same R0, need to compensate with a slightly larger overall infectivity, and this leads to a larger final size and peak incidence, if instead the models are calibrated on the same r, no compensation in infectivity is needed and models with no households are likely more accurate on a larger region of the parameter space (see Supplementary Discussion, Section 2.3.2). However, not all aspect of the present study can be captured by the simple comparison of R0 and r42,47, given past work is restricted to the exponentially growing phase, whereas the present study investigates also the late epidemic behaviour.

Numerous limitations can be highlighted. The first and most obvious one is the lack of uncertainty: despite models being stochastic, the comparison is performed by deterministically mapping parameters from one model to another, thus ignoring the impact of any randomness, noise or estimation bias on model observables and outputs; in addition, final predictions are deterministic. It would not be difficult to compare the full distributions of model outputs, but more complicated results than binary acceptance/rejection of simpler models based on arbitrary thresholds would likely be harder to present and interpret. A more significant step would be to implement uncertainty in the model-mapping process. However, the choice we made in this study was to trade proper uncertainty management for the ability to perform extensive exploration of the space of observables, as any formal statistical estimation procedure, especially, if Bayesian in nature, would have been computationally challenging, and possibly difficult to automatise. Nevertheless, the role of uncertainty could still be roughly quantified by heuristically considering confidence intervals around each quantity in Fig. 3 (or similar figures, for values that do not appear there), given that boundaries appear to be changing monotonically with parameters: for example, for confidence intervals (1.5, 2) for R0 and (20%, 40%) for the SAR, from Fig. 3 one can still conclude the clear need for age, and the need for household structure in the lowest R0 range only when SAR  >30% and with decreasing and ultimately vanishing need as R0 increases (ϕ and ψ are almost irrelevant).

A second limitation is that we only distinguished between adults and children. Stratification to more than two age groups could lead to some non-trivial unidentifiability problems in mapping relative infectivities and susceptibilities from age-stratified incidence, and would require to rely more extensively on data about age-specific contact patterns25, which has been here kept to a minimum to facilitate generalisability to different population structures. Furthermore, with more parameters, results would be again more difficult to present, so it was deemed less relevant in the first instance. However, for practical purposes, for example, in the case of influenza, it would be relevant to have at least a third age group, i.e., seniors, who make up a substantial fraction of developed countries’ population and typically have lower contact rates25, potentially reduced susceptibility owing to prior immunity33,36,48 and higher risk of severe symptoms49.

Third, we assumed a fully susceptible population, thus fundamentally restricting this framework to emerging infections. Changes in mixing and transmission parameters could account for the limiting cases of perfect (i.e., fully protective) prior immunity distributed uniformly in the population or affecting entire age classes, but a more general and realistic case would require to know how prior immunity is distributed in households. Alternatively, a mechanism to generate such prior immunity (e.g., multiannual simulations run prior to the start of the epidemic) would be needed, but then results would depend on the details of such a complex approach.

Fourth, the assumption of constant parameter values, though essential for analytical results, effectively makes model predictions approximately valid only for fast and relatively mild infections, influenza being the most natural example. Paradoxically, though, most new infections for which the emerging epidemic scenario considered here would be relevant are often highly pathogenic (e.g., SARS41, MERS50, Ebola51), thus eliciting active interventions or spontaneous behavioural change. Outbreak response would likely reduce contact rates over time, (as well as time intervals to notification or hospitalisation52), causing the actual epidemic to deviate from initial forecasts. Analytical results are unlikely to be available for non-constant parameters, but we note that inclusion of assumed changes in parameters over time owing to explored interventions would not compromise the computational efficiency of this approach (they would affect only forward predictions, not the mapping procedure itself—see Methods).

Fundamentally, though, predictions in the presence of interventions are not the main focus of this analysis for two reasons: first, the choice of which interventions to explore would strongly shape the model selection process; and second, the models considered here are arguably too simple for most realistic interventions. To study interventions in specific scenarios, more tailored models and more statistically principled methods for robust uncertainty quantification should be used. structures on epidemic predictions in the absence of interventions, and should be viewed as complementary to these other methods. However, such early predictions would still be highly informative in assessing the impact of interventions (or additional impact after estimates became available) by comparison with the epidemic outcome actually observed. Finally, note that potential factors playing a role only under certain intervention scenarios would not be useful to tease apart models compared in the absence of such interventions; however, this is not a limitation of the current methodology, but rather a typical out-of-sample prediction problem17.

Fifth, the assumption of random mixing within the household could also be questionable in certain contexts. The data used for age-specific mixing patterns25 suggest a focus on respiratory infections, for which within-household random mixing appears reasonable53, but applications to other directly transmissible infections might require different assumptions. Extensions to within-household age-stratified mixing would be possible, but would require estimates dependent on the household composition (see Supplementary Methods, Section 1.2.3), or potentially even disease-specific (e.g., school-age children less at risk to Ebola54, possibly because less likely to care for sick individuals55) and hence likely unavailable and hard to collect prospectively. But even age-stratified mixing would fall short of other potentially important heterogeneities in within-household contact patterns, e.g., specific family members taking on the responsibility of caring for relatives infected with Ebola55.

Sixth, we have focussed on age and households only. Other forms of social structure exist, which in some cases could be more relevant and even reasonably well informed by data (e.g., hospital56 or funeral transmission57). In addition, we have ignored any network, patch or explicit spatial structure, or other even more complex models, owing to scarcity in data, analytical results or both.

Finally, we have assumed the presence of a clearly defined exponentially growing phase. This was not the case for MERS and SARS, owing to small outbreak sizes and/or strongly spatial and localised (hospital-based) spread56, thus questioning the reliability of estimates of R0 and other parameters used here, and hence compromising the applicability of our mapping procedure.

Despite all limitations, though, in the restricted context of an emerging infection that is fast enough or not too severe (e.g., influenza—or Zika, though social mixing patterns are likely less relevant for vector-borne diseases) our comparison can inform a useful trade-off between model simplicity and prediction accuracy. Improvements are certainly possible, but we believe the general approach proposed here should be adopted for comparing models and shed light on how structural model components affect predictions. In the particular case of age and household structure, substantial information is still needed early on in an outbreak of a new emerging infection for an appropriate, scientifically driven model choice. Nevertheless, the present analysis suggests that, in many real-world scenarios, households give limited additional accuracy in overall descriptors of epidemic severity for high cost in terms of model complexity and, despite the risk of slightly underestimating the epidemic severity, are probably worth neglecting in the first instance, when limited information is available and rapid predictions are needed.


Aspects common to all models

All models share the same stochastic, time-since-infection transmission process8,58: each infected individual makes infectious contacts at a rate described by a function βω(τ), where the total infectivity β depends on the ages of the infector and the other contacted person, as well as on the environment (i.e., within or outside the household), and the infectious contact interval distribution ω(τ)59 is a function of the time since infection τ, normalised to integrate to 1, with mean TG (often referred to as the generation time37) and is the same between every pair of individuals, irrespective of age and environment (see Supplementary Methods, Section 1.1.2). After infection, individuals cannot be infected again.

The dynamics of this model, at least in its deterministic form and in the absence of household structure, could be described in terms of a renewal-type integral equation8,58, with β = R0, but we do not present it here because no dynamical equations are solved in this work. Instead, for all models, the observables defined during the exponentially growing phase and used for the mapping (i.e., R0, the incidence ratio of adults and children and the SAR), as well as the final size z, are computed directly using available mathematical results, whereas the peak incidence π and time to the peak t are computed as the average of 100 individual-based stochastic simulations in a population of 100,000 individuals. The epidemics are started with n0 = 50 initial cases, to avoid stochastic extinction and minimise the effect of random delays at the start of the epidemic, and are synchronised at the peak.

Inspired by influenza, we choose a Γ-shaped infectious contact interval distribution ω(τ) with mean TG = 2.85 days and shape parameter α = 98,32. However, this particular choice does not affect the quantities calculated analytically (observables and final size), which are all time-integrated quantities, and hence bears no influence on the mapping procedure, although it does affect the peak incidence π and the time to the peak t. However, to allow generalisations to other infections, the time to the peak is rescaled by a factor TG, thus approximately measuring the average number of generations to the peak.

Although the stochastic simulations are computationally intensive, the forward problem of computing observables and outputs for each model is relatively inexpensive even in the absence of analytical results, as it needs to be performed once for each combination of basic model parameters. Instead, the inverse problem of exploring parameter spaces at fixed observables is in general computationally expensive. In the presence of explicit expressions for the observables, which is rarely the case, one could simply invert them to map parameters directly from one model to another42. In the absence of explicit expressions, iterative methods must be used (see Supplementary Methods, Section 1.1.1), which require solving the forward problem multiple times and might become prohibitive for computationally costly simulations. The efficiency of our approach stems from the fact that the context we have focussed on, though rather specific, is rich in analytical results: in particular, thanks to the latest methodological advances in the computation of R0 for households models47,60, the observables of all models can be obtained without having to integrate the system dynamics. Therefore, the mapping procedure could be performed on all points of a regular grid in the parameter space of model AH (Figs. 1, 2a and 3) that is fine enough to suggest our conclusions, though numerical in nature, hold throughout the explored portion of space.

Model AH (age and households)

Model AH is parameterised as follows. The infection spread between adults (a) and children (c) in each environment x (in the community, x = g for “global”; or in the household, x = h) is parameterised in terms of a next-generation matrix (NGM) of the form

$${K}_{x}=\left(\begin{array}{ll}{k}_{aa}^{x}&{k}_{ac}^{x}\\ {k}_{ca}^{x}&{k}_{cc}^{x}\end{array}\right)={\beta }_{x}\left(\begin{array}{ll}{\gamma }_{x}-\frac{{N}_{c}^{x}}{{N}_{a}^{x}}&\left(1-{\theta }_{x}\right)\phi \\ \psi \left(1-{\theta }_{x}\right)\frac{{N}_{c}^{x}}{{N}_{a}^{x}}&\psi {\theta }_{x}\phi \end{array}\right)$$

(derivation in Supplementary Methods, Sections 1.1.4 and 1.1.5), where \({k}_{ij}^{x}\) gives the average number of infectious contacts an individual in age-class j makes with individuals in age-class i in environment x. In the initial phase of the epidemic all the infectious contacts \({k}_{ij}^{g}\) in the community lead to real infections. In a household, instead, some of the \({k}_{ij}^{h}\) infectious contacts hit previously infected or immune cases.

The NGM Kx incorporates simultaneously both contact and transmission elements. The contact patterns are given by: γx, the ratio of the numbers of daily contacts an adult and a child have in environment x; \({N}_{a}^{x}\) and \({N}_{c}^{x}\), the numbers of adults and children in environment x, respectively; and θx, the assortativity of children in x, defined somewhat non-standardly as the fraction of contacts that a child makes with other children in x and ranging from 0 (fully antiassortative mixing) to 1 (fully assortative mixing). Random mixing is achieved for θx equal to the fraction of other children in the environment. Within-household mixing is always assumed to be random (note that this requires θh to depend on the household composition). We assume frequency-dependent contact patterns in the households, so that the infectious contacts \({k}_{ij}^{h}\) are distributed among all (other) cases of age-class i; that is, in the simple case of all identical individuals, the person-to-person contact rate in a household of size n scales as 1 ∕(n − 1)—see Supplementary Methods, Section 1.2.3, for precise age-stratified details.

The transmission component of the model is parameterised in terms of ψ and ϕ, which represent respectively the relative susceptibility and infectivity of children versus adults, and total infectivities βx. In practice, the within-household total infectivity βh is re-parameterised in terms of paa, defined as the probability that a randomly selected susceptible would be infected directly by a single initial household case, in a randomly selected household with at least two individuals, when adults and children have the same susceptibility and infectivity (ψ = ϕ = 1). In other words, paa is obtained by first computing pn = 1 − exp(−βh ∕(n − 1)) and then averaging pn over the size distribution of a randomly selected household with at least two members. Other similar choices would have been possible, as long as they do not depend on other parameters we are exploring independently, like ψ or ϕ. In the Supplementary Discussion (Sections 2.1.1 and 2.2.1) we comment on more aggregate, but more intuitive epidemiological quantities, such as the SAR or the fraction of total transmission occurring in households. The latter is measured as \(\left({R}_{0}-{R}_{0}^{g}\right)/{R}_{0}\), where \({R}_{0}^{g}\) is the dominant eigenvalue of Kg, and reveals that, at least for the H1N1 2009 pandemic influenza in Great Britain, approximately a third of the total transmission occurs in household (a rule of thumb suggested before8,9,32; see Supplementary Discussion, Sections 2.1.1 and 2.2.1).

Numerical values are as follows. At baseline, the population structure is that of Great Britain61, with a fraction Fc = 22.73% of the population consisting of children and a mean household size χ = 2.35 (see Supplementary Methods, Section 1.6.1, and Supplementary Tables 1–4). Other social structures (South Africa: Fc = 45.92%, χ = 4.27; Sierra Leone: Fc = 53.81%, χ = 5.85) are explored in the Supplementary Methods, Section 1.6.2, Supplementary Tables 47 and Supplementary Discussion, Section 2.3.4. At baseline, contact patterns assume random mixing: γh = γg = 1 (adults and children have the same contact rates everywhere) and θg = Fc = 22.73%, the fraction of children in the population. Parameters for UK-like contact patterns, characterised by strongly assortative mixing, are estimated from the POLYMOD study25 to be γh = γg = 0.75 and θg = 58% (see Supplementary Methods, Section 1.6.3, and Supplementary Table 8), and are used also for other social structures (in the absence of contact pattern data for South Africa and Sierra Leone). Intermediate contact patterns are explored in the Supplementary Discussion (Section 2.3.1).

The observables for model AH are derived as follows. The basic reproduction number R0 is computed using a multitype extension of the technique developed in60 that leads to the construction of a suitable matrix M (details in the Supplementary Methods, Section 1.2.4), the dominant eigenvalue of which is R0.

From M it is also possible to reconstruct the vector \({v}^{{\rm{AH}}}={\left({v}_{a},{v}_{c}\right)}^{\top }\) (superscript denotes transposition, to give a column vector), whose components are the fractions of adults and children in each generation (vAH is constant during the exponentially growing phase), correctly computed by taking into account both household and global transmission (Supplementary Methods, Section 1.2.5). Primary cases in households are infected globally, so arise in proportions given by the components of the vector \({v}_{h}^{{\rm{AH}}}={\left({v}_{h}^{a},{v}_{h}^{c}\right)}^{\top }\), obtained by renormalizing KgvAH so that its components sum to 1.

The SAR is defined as the fraction of initial susceptibles that are infected in a within-household outbreak started by a single individual in a typical household infected during the exponentially growing phase. Its computation is not trivial, because the distribution of infected households during the exponentially growing phase is affected by the age-dependent between-household transmission: if children are more likely to be infected in the population, larger households are also more likely to be infected because they tend to contain more children. We denote by \(\left\{{\pi }_{n}^{a}\right\}\) and \(\left\{{\pi }_{n}^{c}\right\}\) the size distributions of the household of a randomly selected adult and child, respectively, and by μa and μc the average epidemic sizes in the household of a randomly chosen initial adult or child case, respectively. Then the average size of a household epidemic during the exponentially growing phase is \({\mu }^{{\rm{AH}}}={v}_{h}^{a}{\mu }^{a}+{v}_{h}^{c}{\mu }^{c}\). The household SAR is then computed as (μAH − 1)∕(χv − 1), where χv is the average size of a household infected in that phase (see Supplementary Methods, Section 1.2.6).

Finally, the outputs for model AH are derived as follows. The average final size z, in the asymptotic limit of an infinite number of households, is computed using the methodology described in ref. 30 (Supplementary Methods, Section 1.2.7). The peak incidence and the time to the peak are obtained from individual-based stochastic simulations in a synthetic population with the required social structure and contact patterns (Supplementary Methods, Sections 1.2.8 and 1.5). To minimise the convergence time from the initial conditions to the stable proportions of cases of each type during the exponentially growing phase, the n0 initial cases are all chosen as primary cases in different households and consist of adults and children in proportions given by \({v}_{h}^{{\rm{AH}}}\).

Further details about model AH can be found in the Supplementary Methods, Section 1.2.

Model A (age)

Model A is parameterised as follows. The spread between adults and children in model A is described by KA, a NGM of the same form as the one in Eq. (1), but with elements indexed by A (there is only one environment). The contact patterns are given by γA, the ratio of the overall number of contacts an adult and a child have, and the assortativity of children θA. The transmission component of the model is parameterised in terms of an overall transmission parameter βA and the relative susceptibility and infectivity of children versus adults, ψ and ϕ, which are thought of as biological parameters ideally accurately measured via detailed household studies, and are therefore assumed to be the same as in model AH. The presence of four parameters, two of which coincide by construction with those of model AH, makes model A both more flexible and more tightly linked to model AH than to model H (two parameters only). This partly explains why model A is better than model H at mirroring the outputs of model AH in Fig. 1.

Numerical values are inherited by the social structure and mixing patterns of model AH. At baseline (Great Britain61) the fraction of children is 22.73% and adults and children have the same contact rate (γA = 1). UK-like contact patterns are given by γA = 0.75. The assortativity θA is estimated in the mapping procedure (see below).

In terms of observables, the basic reproduction number R0 in model A is computed as the dominant eigenvalue of the NGM KA, and the corresponding eigenvector vA, normalised to have components summing to 1, represents the fraction of adults and children in each generation58.

In terms of outputs, the final size is computed using standard methods5 (Supplementary Methods, Section 1.3). The peak incidence and the time to the peak are again computed using the individual-based stochastic simulation, with no household structure and starting with n0 initially cases, consisting of adults and children in proportions given by the components of the vector vA (to start as close as possible to the stable proportions of adults and children during the exponentially growing phase).

Further details about model A can be found in the Supplementary Methods, Section 1.3.

Model H (households)

The pure households model is parameterised in terms of a global total infectivity \({\beta }_{g}^{{\rm{H}}}\) and a within-household total infectivity \({\beta }_{h}^{{\rm{H}}}\), representing, respectively, the average number of infectious contacts an infective makes in the community and in their household, during their entire infection period. Early on in the epidemic, every infectious contact in the community leads to a new infection. Frequency-dependent contact patterns are assumed within the household, so that the number of infectious contacts toward a single member of a household of size n is \({\beta }_{h}^{{\rm{H}}}/(n-1)\).

Numerical values are again inherited by the household structure of model AH. At baseline, the household size distribution is that of Great Britain, with a mean household size χ = 2.35 (see Supplementary Tables 1–3). Other social structures are also considered (South Africa: χ = 4.27; Sierra Leone: χ = 5.85).

The computation of R0 for model H follows the method of47,60 (Supplementary Methods, Section 1.4). Similarly to model AH, the SAR is computed as (μH − 1)∕(χ − 1), where μH is the average size of a within-household epidemic, computed using standard methods for small populations5,62 and χ is the average household size. However, care needs to be taken in the choice of the correct household size distribution (see below).

The final size is computed using standard analytical techniques28, and the peak incidence and time to the peak are obtained from stochastic simulations starting with n0 cases, all primary cases in different households, divided in adults and children according to the components of \({v}_{h}^{{\rm{AH}}}\) (to start as close as possible to the stable household size distribution of the exponentially growing phase).

Further details about model H can be found in the Supplementary Methods, Section 1.4.

Model U (unstructured)

Given the temporal details of the infection process are fixed by the infectious contact interval distribution ω(τ), the model with pure homogeneous mixing has only one parameter β = R0. The final size is computed standardly as the only positive solution z of \(1-z={{\rm{e}}}^{-{R}_{0}z}\)5, whereas the peak incidence and the time to the peak are obtained via simulations starting with n0 initial cases.

Model-mapping procedure

For each combination of basic parameters for the assumed-true model AH (ψ, ϕ, paa, from which βh is derived, and βg—as well as fixed θg, γg, and γh—we calculate the true epidemic observables R0, vAH, and SAR, as described above. In practice, the parameter space in all figures is explored at constant R0, so that for each choice of paa, ψ, and ϕ we compute the value of βg required to achieve a desired R0. These observables are then used to map the parameters for the other models as follows.

We start by mapping model AH to model A. Parameters ψ and ϕ in model A are assumed to be known and the same as in model AH. Then θA is ideally chosen to match vAH. Unfortunately, there are parameter values for which no suitable value of θA [0, 1] can be found (see Supplementary Methods, Section 1.3). This is often the case for ψ < 1 (Supplementary Discussion, Section 2.3.3). The overall infectivity βA is then chosen to match R0. There are no households in model A, so the SAR is not used.

To map model AH to model H, first \({\beta }_{h}^{{\rm{H}}}\) is computed to match the observed household SAR. The correct household size distribution to use cannot be computed from model H alone, because the distribution of infected households during the exponentially growing phase is affected by the age-dependent transmission as described for model AH. In real scenarios, the within-household infectivity is measured from household studies. In such surveys, the recruitment of households is subject to many constraints, but it ideally monitors a representative portion of the population of infected households. If model AH were an exact description of reality, then households would be recruited with size distribution \(\left\{{\pi }_{n}^{v}\right\}\), where, for each n, \({\pi }_{n}^{v}={v}_{h}^{a}{\pi }_{n}^{a}+{v}_{h}^{c}{\pi }_{n}^{c}\). In practice, instead of matching the same SAR as in model AH, we equivalently compute \({\beta }_{h}^{{\rm{H}}}\) by imposing μH = μAH, with household size distribution \(\left\{{\pi }_{n}^{v}\right\}\) (and hence χ = χv). The global infectivity \({\beta }_{g}^{{\rm{H}}}\) is then computed to match R0. Apart from appearing in the computation of the correct household size distribution for matching the SAR (rather than obtaining such a distribution from a random sample of infected households), vAH is not explicitly used.

Finally, the mapping from model AH to model U is trivial, as model U is only parameterised in terms of R0 and the other observables are not used.

Reporting summary

Further information on research design is available in the Nature Research Reporting Summary linked to this article.

Data availability

Household data for Great Britain (England, Wales and Scotland) are available from 2001 UK census data, table number C084461; source: Office for National Statistics licensed under the Open Government Licence v.1.0. The table can be downloaded from or, or can be requested directly from the Office for National Statistics. UK social contact data are obtained from the POLYMOD study25 (raw data available from the authors upon request). Household data for Sierra Leone are available from the 2008 Sierra Leone Demographic and Health Survey63 and household data for South Africa from the 1998 South Africa Demographic and Health Survey64. Both can be requested from the Demographic and Health Surveys Program65 (free registration). Raw data are only used to generate Supplementary Tables 1, 4, 6 and 8 (see Supplementary Information), from which all other tables, analyses and figures are generated.

Code availability

Numerical codes, output files and figures have been archived at the time of publication with Potential improvements or corrections will be made available at The main code to perform the model mapping is written in MATLAB and has been tested on both R2016a on Mac OSX El Capitan and R2019a on Microsoft Windows 7 Professional (Service Pack 1). The individual-based stochastic simulation is written in C++ and source codes are freely available.


  1. 1.

    Ferguson, N. M. et al. Planning for smallpox outbreaks. Nature 425, 681–685 (2003).

    ADS  CAS  PubMed  Article  PubMed Central  Google Scholar 

  2. 2.

    Riley, S. Large-scale spatial-transmission models of infectious disease. Science 316, 1298–1301 (2007).

    ADS  CAS  PubMed  Article  PubMed Central  Google Scholar 

  3. 3.

    Baguelin, M. et al. Vaccination against pandemic influenza A/H1N1v in England: a real-time economic evaluation. Vaccine 28, 2370–2384 (2010).

    PubMed  Article  PubMed Central  Google Scholar 

  4. 4.

    Flasche, S. et al. Different transmission patterns in the early stages of the influenza A(H1N1)v pandemic: a comparative analysis of 12 European countries. Epidemics 3, 125–133 (2011).

    PubMed  Article  PubMed Central  Google Scholar 

  5. 5.

    Andersson, H. & Britton, T. Stochastic epidemic models and their statistical analysis (Springer, 2000).

  6. 6.

    Keeling, M.J. & Rohani, P. Modeling infectious diseases in humans and animals (Princeton University Press, 2008).

  7. 7.

    Danon, L. et al. Networks and the epidemiology of infectious disease. Interdiscip. Perspect. Infect. Dis. 2011, 284909 (2011).

    PubMed  PubMed Central  Article  Google Scholar 

  8. 8.

    Pellis, L., Ferguson, N. M. & Fraser, C. Epidemic growth rate and household reproduction number in communities of households, schools and workplaces. J. Math. Biol. 63, 691–734 (2010).

    MathSciNet  PubMed  PubMed Central  MATH  Article  Google Scholar 

  9. 9.

    Ferguson, N. M. et al. Strategies for mitigating an influenza pandemic. Nature 442, 448–452 (2006).

    ADS  CAS  PubMed  Article  PubMed Central  Google Scholar 

  10. 10.

    Halloran, M. E. et al. Modeling targeted layered containment of an influenza pandemic in the United States. Proc. Natl. Acad. Sci. USA 105, 4639–4644 (2008).

    ADS  CAS  PubMed  Article  Google Scholar 

  11. 11.

    Ajelli, M. et al. Comparing large-scale computational approaches to epidemic modeling: agent-based versus structured metapopulation models. BMC Infect. Dis. 10, 1 (2010).

    Article  Google Scholar 

  12. 12.

    Ajelli, M., Merler, S., Pugliese, A. & Rizzo, C. Model predictions and evaluation of possible control strategies for the 2009 A/H1N1v influenza pandemic in Italy. Epidemiol. Infect. 139, 68–79 (2011).

    CAS  PubMed  Article  Google Scholar 

  13. 13.

    Shaman, J. & Karspeck, A. Forecasting seasonal outbreaks of influenza. Proceed. Natl. Acad. Sci. 109, 20425–20430 (2012).

    ADS  CAS  Article  Google Scholar 

  14. 14.

    Shaman, J., Karspeck, A., Yang, W., Tamerius, J. & Lipsitch, M. Real-time influenza forecasts during the 2012 - 2013 season. Nat. Commun. 4, 2837 (2013).

    ADS  PubMed  PubMed Central  Article  CAS  Google Scholar 

  15. 15.

    Tebaldi, C. & Knutti, R. The use of the multi-model ensemble in probabilistic climate projections. Philos. Trans. R. Soc. A 365, 2053–2075 (2007).

    ADS  MathSciNet  Article  Google Scholar 

  16. 16.

    Lindström, T., Tildesley, M. & Webb, C. A Bayesian ensemble approach for epidemiological projections. PLoS Comput. Biol. 11, 1–30 (2015).

    Article  CAS  Google Scholar 

  17. 17.

    Webb, C. T. et al. Ensemble modelling and structured decision-making to support emergency disease management. Prev. Vet. Med. 138, 124–133 (2017).

    PubMed  Article  Google Scholar 

  18. 18.

    Hollingsworth, T. D. & Medley, G. F. Learning from multi-model comparisons: collaboration leads to insights, but limitations remain. Epidemics 18, 1–3 (2017).

    CAS  PubMed  Article  Google Scholar 

  19. 19.

    Eaton, J. W. et al. HIV treatment as prevention: systematic comparison of mathematical models of the potential impact of antiretroviral therapy on HIV incidence in South Africa. PLoS Med. 9, e1001245 (2012).

    PubMed  PubMed Central  Article  Google Scholar 

  20. 20.

    Smith, T. et al. Ensemble modeling of the likely public health impact of a pre-erythrocytic malaria vaccine. PLoS Med. 9, e1001157 (2012).

    PubMed  PubMed Central  Article  Google Scholar 

  21. 21.

    Malaria Policy Advisory Committee Meeting. Consensus modelling evidence to support the design of mass drug administration programmes. World Health Organization 1–20 (2015).

  22. 22.

    Gerberry, D. J. An exact approach to calibrating infectious disease models to surveillance data: the case of hiv and hsv-2. Math. Biosci. Eng. 15, 153–179 (2018).

    MathSciNet  PubMed  MATH  Article  Google Scholar 

  23. 23.

    Smith, M. E. et al. Predicting lymphatic filariasis transmission and elimination dynamics using a multi-model ensemble framework. Epidemics 18, 16–28 (2017).

    PubMed  PubMed Central  Article  Google Scholar 

  24. 24.

    Wallinga, J., Teunis, P. & Kretzschmar, M. Using data on social contacts to estimate age-specific transmission parameters for respiratory-spread infectious agents. Am. J. Epidemiol. 164, 936–944 (2006).

    PubMed  Article  Google Scholar 

  25. 25.

    Mossong, J. et al. Social contacts and mixing patterns relevant to the spread of infectious diseases. PLoS Med. 5, e74 (2008).

    PubMed  PubMed Central  Article  Google Scholar 

  26. 26.

    Gregson, S. et al. Sexual mixing patterns and sex-differentials in teenage exposure to HIV infection in rural Zimbabwe. Lancet 359, 1896–1903 (2002).

    PubMed  Article  Google Scholar 

  27. 27.

    Eames, K. T. D., Tilston, N. L., Brooks-Pollock, E. & Edmunds, W. J. Measured dynamic social contact patterns explain the spread of H1N1v influenza. PLoS Comput, Biol. 8, 1–8 (2012).

    MathSciNet  Article  CAS  Google Scholar 

  28. 28.

    Ball, F. G. & Neal, P. A general model for stochastic SIR epidemics with two levels of mixing. Math. Biosci. 180, 73–102 (2002).

    MathSciNet  PubMed  MATH  Article  Google Scholar 

  29. 29.

    House, T. & Keeling, M. J. Deterministic epidemic models with explicit household structure. Math. Biosci. 213, 29–39 (2008).

    MathSciNet  PubMed  MATH  Article  Google Scholar 

  30. 30.

    Ball, F., Britton, T. & Sirl, D. Household epidemic models with varying infection response. J. Math. Biol. 63, 309–337 (2010).

    MathSciNet  PubMed  MATH  Article  PubMed Central  Google Scholar 

  31. 31.

    Simpson, R. E. H. Infectiousness of communicable diseases in the household (measles, chickenpox, and mumps). Lancet 2, 549–554 (1952).

    CAS  PubMed  Article  PubMed Central  Google Scholar 

  32. 32.

    Fraser, C. Estimating individual and household reproduction numbers in an emerging epidemic. PLoS ONE 2, e758 (2007).

    ADS  PubMed  PubMed Central  Article  Google Scholar 

  33. 33.

    Cauchemez, S. et al. Household transmission of 2009 pandemic influenza A (H1N1) virus in the United States. N. Engl. J. Med. 361, 2619–2627 (2009).

    CAS  PubMed  Article  PubMed Central  Google Scholar 

  34. 34.

    Fraser, C., Cummings, D. a. T., Klinkenberg, D., Burke, D. S. & Ferguson, N. M. Influenza transmission in households during the 1918 pandemic. Am. J. Epidemiol. 174, 505–514 (2011).

    PubMed  PubMed Central  Article  Google Scholar 

  35. 35.

    House, T. et al. Estimation of outbreak severity and transmissibility: influenza A (H1N1) pdm09 in households. BMC Med. 10, 117 (2012).

    PubMed  PubMed Central  Article  Google Scholar 

  36. 36.

    Lau, L. L. et al. Household transmission of 2009 pandemic influenza A (H1N1): a systematic review and meta-analysis. Epidemiology 23, 531 (2012).

    PubMed  PubMed Central  Article  Google Scholar 

  37. 37.

    Svensson, A. A note on generation times in epidemic models. Math. Biosci. 208, 300–311 (2007).

    MathSciNet  PubMed  MATH  Article  PubMed Central  Google Scholar 

  38. 38.

    Andreasen, V. The final size of an epidemic and its relation to the basic reproduction number. Bull. Math. Biol. 73, 2305–2321 (2011).

    MathSciNet  PubMed  MATH  Article  PubMed Central  Google Scholar 

  39. 39.

    Miller, J. Epidemic size and probability in populations with heterogeneous infectivity and susceptibility. Phys. Rev. E 76, 1–4 (2007).

    Google Scholar 

  40. 40.

    Cowling, B. J. et al. Comparative epidemiology of pandemic and seasonal influenza A in households. N. Engl. J. Med. 362, 2175–2184 (2010).

    CAS  PubMed  PubMed Central  Article  Google Scholar 

  41. 41.

    World Health Organization et al. Consensus document on the epidemiology of severe acute respiratory syndrome (SARS). (World Health Organization, 2003).

  42. 42.

    Trapman, P. et al. Inferring R 0 in emerging epidemics - the effect of common population structure is small. J. R. Soc. Interface 13, 20160288 (2016).

    PubMed  PubMed Central  Article  Google Scholar 

  43. 43.

    Knutti, R., Furrer, R., Tebaldi, C., Cermak, J. & Meehl, G. A. Challenges in combining projections from multiple climate models. J. Climate 23, 2739–2758 (2010).

    ADS  Article  Google Scholar 

  44. 44.

    Probert, W. J. et al. Decision-making for foot-and-mouth disease control: objectives matter. Epidemics 15, 10–19 (2016).

    PubMed  Article  PubMed Central  Google Scholar 

  45. 45.

    Fraser, C. et al. Pandemic potential of a strain of influenza A (H1N1): early findings. Science 324, 1557–1561 (2009).

    ADS  CAS  PubMed  PubMed Central  Article  Google Scholar 

  46. 46.

    Dorigatti, I., Cauchemez, S., Pugliese, A. & Ferguson, N. M. A new approach to characterising infectious disease transmission dynamics from sentinel surveillance: application to the Italian 2009–2010 A/H1N1 influenza pandemic. Epidemics 4, 9–21 (2012).

    PubMed  Article  PubMed Central  Google Scholar 

  47. 47.

    Ball, F., Pellis, L. & Trapman, P. Reproduction numbers for epidemic models with households and other social structures II: comparisons and implications for vaccination. Math. Biosci. 274, 108–139 (2016).

    MathSciNet  PubMed  MATH  Article  PubMed Central  Google Scholar 

  48. 48.

    Yang, W., Lipsitch, M. & Shaman, J. Inference of seasonal and pandemic influenza transmission dynamics. Proceed. Natl. Acad. Sci. 112, 201415012 (2015).

    Google Scholar 

  49. 49.

    Public Health England. Flu Plan Winter 2017/18 (2017).

  50. 50.

    World Health Organization et al. WHO MERS-CoV global summary and risk assessment. Technical Report (2016).

  51. 51.

    Van Kerkhove, M. D., Bento, A. I., Mills, H. L., Ferguson, N. M. & Donnelly, C. A. A review of epidemiological parameters from Ebola outbreaks to inform early public health decision-making. Sci. Data 2, 1–10 (2015).

    Article  Google Scholar 

  52. 52.

    Ebola, W. H. O., Team, R., March, O. & August, O. Ebola Virus disease in West Africa - the first 9 months of the epidemic and forward projections. N. Engl. J. Med. 371, 1481–1495 (2014).

    Article  CAS  Google Scholar 

  53. 53.

    Goeyvaerts, N. et al. Household members do not contact each other at random: implications for infectious disease modelling. BioRxiv 285, 220202 (2017).

    Google Scholar 

  54. 54.

    Bower, H. et al. Exposure-specific and age-specific attack rates for Ebola virus disease in Ebola-affected households, Sierra Leone. Emerg. Infect. Dis. 22, 1403–1411 (2016).

    PubMed  PubMed Central  Article  Google Scholar 

  55. 55.

    Dowell, S. F. et al. Transmission of Ebola hemorrhagic fever: a study of risk factors in family members, Kikwit, Democratic Republic of the Congo, 1995. J. Infect. Dis. 179, 87–91 (1999).

    Article  Google Scholar 

  56. 56.

    Riley, S. et al. Transmission dynamics of the etiological agent of SARS in Hong Kong: impact of public health interventions. Science 300, 1961–1966 (2003).

    ADS  CAS  PubMed  Article  Google Scholar 

  57. 57.

    Agua-Agum, J. et al. Exposure patterns driving Ebola transmission in West Africa: a retrospective observational study. PLoS Med. 13, 1–23 (2016).

    Google Scholar 

  58. 58.

    Diekmann, O., Heesterbeek, H. & Britton, T. Mathematical tools for understanding infectious disease dynamics (Princeton University Press, 2012).

  59. 59.

    Kenah, E. Contact intervals, survival analysis of epidemic data, and estimation of R 0. Biostatistics 12, 548–566 (2011).

    PubMed  MATH  Article  Google Scholar 

  60. 60.

    Pellis, L., Ball, F. G. & Trapman, P. Reproduction numbers for epidemic models with households and other social structures. I. Definition and calculation of R 0. Math. Biosci. 235, 85–97 (2012).

    MathSciNet  PubMed  PubMed Central  MATH  Article  Google Scholar 

  61. 61.

    Office for National Statistics. Table C0844, UK census (2001). Available at:

  62. 62.

    House, T., Ross, J. V. & Sirl, D. How big is an outbreak likely to be? Methods for epidemic final-size calculation. Proc. R. Soc. A Math. Phys. Eng. Sci. 469, 20120436 (2013).

  63. 63.

    Statistics Sierra Leone (SSL) and ICF Macro. Sierra Leone Demographic and Health Survey 2008 [Dataset]. SLPR51FL.SAV. Calverton, Maryland, USA: SSL and ICF Macro [Producers]. ICF [Distributor] (2009).

  64. 64.

    Department of Health/South Africa and Macro International. South Africa De- mographic and Health Survey 1998 [Dataset]. ZAPR31FL.SAV. Pretoria, South Africa: Department of Health/South Africa [Producer]. ICF [Distributor] (2002).

  65. 65.

    ICF. The DHS Program. Funded by USAID. [Accessed January, 22, 2020].

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We acknowledge the MRC Methodology Grant G0800596. L.P. acknowledges the EPSRC (grant EP/J002437/1) and the Wellcome Trust and Royal Society (grant 202562/Z/16/Z); S.C. acknowledges funding from the NIGMS MIDAS initiative, the French Government’s Investissement d’Avenir program, Laboratoire d’Excellence “Integrative Biology of Emerging Infectious Diseases” (grant number ANR-10-LABX-62-IBEID), the AXA Research Fund and Grand Prix Robert Debré; and N.M.F. acknowledges Centre funding from the MRC and DFID, Health Protection Research Unit funding from NIHR, Institute funding from Community Jameel and grant funding from the Bill and Melinda Gates Foundation. We also thank Niel Hens for support with the analysis of the POLYMOD data, the members of the Zeeman Institute at the University of Warwick for useful discussions, and the anonymous reviewers for their insightful and constructive comments.

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L.P., S.C., N.M.F., C.F. designed the study. L.P. developed the mathematical methods and numerical codes, performed the analyses and wrote the paper and supplementary material. S.C., N.M.F. and C.F. commented on the manuscript.

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Correspondence to Lorenzo Pellis.

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Pellis, L., Cauchemez, S., Ferguson, N.M. et al. Systematic selection between age and household structure for models aimed at emerging epidemic predictions. Nat Commun 11, 906 (2020).

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