Caffeine in preterm infants: where are we in 2020?

Neurological effects

A number of studies have suggested that caffeine intake in preterm infants may have a neuroprotective effect, although researches on animal models have shown contrasting results, probably impacted by the species examined, dose of caffeine used, neurodevelopmental stage at the time of administration and duration of exposure (figure 1) [23, 41–43].

In preterm infants, enhanced cerebral cortical activity, observed as increases in amplitude and periods of continuity on electroencephalography recordings, is seen within 2 h of administration of caffeine [25, 26], suggesting an effect on neurological function. Furthermore, at 36 weeks post-menstrual age (PMA) infants treated with caffeine therapy had a higher amplitude-integrated electroencephalography score compared to the control group (p<0.001), without an increase in seizure activity [26]. The most comprehensive study to date exploring the long-term effects of caffeine in preterm infants is the CAP trial, whose primary objective was to determine whether survival without neurodevelopmental disability at a corrected age of 18–21 months was altered if AOP was treated with caffeine [33]. 2006 infants (birthweight 500–1250 g) were enrolled and randomly assigned to receive either caffeine (20 mg·kg⁻¹ intravenously as loading dose followed by a maintenance dose of 5 mg·kg⁻¹ per day) or placebo. The caffeine group had a reduced likelihood of death or clinical disability (40.2% versus 46.2%; p=0.008), together with a reduced incidence of cerebral palsy (4.4% versus 7.3%; p=0.009) and of cognitive delay (33.8% versus 38.3%; p=0.04) [27]. The results of the subsequent follow-up at 5 years of age showed no significant difference between caffeine treatment and placebo in the composite outcome of death or disability (21.1% versus 24.8%; p=0.09) [28], but a significant improvement of gross motor function in the caffeine group (odds ratio adjusted for centre 0.64, p=0.006). The long-term follow-up at 11 years of age confirmed previous results of reduced risk of motor impairment (19.7% versus 27.5%; p=0.009), with no significant difference in the rates of functional impairment (31.7% versus 37.6%; p=0.07), academic performance and behavioural problems (10.9% versus 8.3%; p=0.22) [29, 30].

Prolonged treatment with caffeine reduces hypoxaemia events in premature infants [44], the severity and duration of which are probably associated with adverse neurodevelopmental outcomes [45, 46]. Overall neonatal caffeine therapy, at the doses used in the CAP trial, appears to be safe into middle-school age, with no adverse effects on general motor function, intelligence, attention and behaviour.

Caffeine for apnoea, ventilatory support and extubation

Methylxanthines have been used for >40 years in neonatal medicine to reduce the frequency of apnoea, but, apart from the CAP trial, studies and systematic reviews comparing caffeine versus placebo have mainly addressed short-term respiratory outcomes, such as apnoea prophylaxis (one review, two trials), apnoea treatment (one review, three trials), extubation success (one review, two trials) and ventilator support (intermittent positive pressure ventilation (IPPV) and/or mechanical ventilation) (five trials), with a consequent uncertainty of the long-term benefit/risk ratio of this therapy [15, 33, 47].

The Cochrane review published in 2010 [35], included, in addition to the CAP trial, two studies evaluating the effects of prophylactic caffeine on short-term outcomes. The review concluded against the support of the use of prophylactic caffeine for preterm infants at risk of apnoea, but only one study reported apnoea (as defined by duration >20 s with bradycardia <100 bpm or cyanosis) as an outcome in the results [48].

However, a single-centre RCT [49] on premature infants (birthweight <1200 g) demonstrated a reduction in apnoea episodes (as a breathing pause for ≤20 s with bradycardia and/or cyanosis) in the caffeine-treated group compared to placebo (15.4% versus 61.5%, 95% CI 0.097–0.647; p=0.001), with the more immature infants having the greater benefit of prophylactic caffeine on the incidence and severity of apnoea. The limitations of this study, which was published after the 2010 Cochrane review, are the monocentric setting, the small sample size (26 infants in the treatment group versus 26 in the placebo group) and the unprecise detection of apnoea (daily neonatal intensive care unit reports and monitor downloads). In general, the definition of prophylactic caffeine in terms of hours of life at first administration can be debated, as it is supposed that apnoea events can occur from the first hour of life, and studies comparing caffeine in the delivery room versus placebo to reduce the incidence of apnoea are lacking.

Another Cochrane review published in 2010 [15] evaluated the effects of methylxanthine treatment on the incidence of apnoea (American Academy of Pediatrics 2003 definition [50]) and included three trials on caffeine. The analysis of the two trials [51, 52] on caffeine, without considering the CAP trial, found significantly less treatment failure (relative risk 0.46, 95% CI 0.27–0.78, number needed to treat 3) as defined by <50% reduction in apnoea, or use of IPPV, or death during the study period (by 5 and 10 days from starting treatment).

Finally, the last Cochrane review of the series summarised the effects of prophylactic methylxanthine treatment to improve the chances of successful extubation, with failed extubation defined within 1 week of commencing treatment, if unable to wean from IPPV and extubate, or reintubation for IPPV, or need for use of continuous positive airways pressure (CPAP) [36]. Overall analysis of the six included trials showed that methylxanthine treatment results in an absolute reduction of 27% in the incidence of failed extubation. However, although all trials had the aim of improving the chances of successful extubation, protocols differed considerably, and only two trials compared caffeine versus placebo [33, 53].

The large CAP trial was included in each of the three Cochrane reviews, but did not report on apnoea outcomes and extubation success, although recruited infants received caffeine for any one of the three indications (prophylaxis for apnoea (22%), treatment of apnoea (40%) or prophylaxis for extubation (38%)).

However, the CAP trial clearly demonstrated that caffeine treatment within the first 10 days of life determined a reduction in each of the three levels of respiratory support (need for endotracheal tube, any positive pressure ventilation (PPV), supplemental oxygen) of 1 week compared to placebo (p<0.001), with no difference according to the indication for starting treatment. Interestingly, the positive results on respiratory support, together with the significantly reduced rate of BPD, surgical closure of patent ductus arteriosus (PDA) and of use of postnatal steroids, explained 55% of caffeine effect on the primary neurological outcomes at 18–21 months of age (with the most important variable being earlier discontinuation of PPV), suggesting a direct neuroprotective effect of the drug [33].

As a result of these findings, caffeine is the drug of choice to reduce apnoea rates, need for IPPV, ventilatory support, extubation failure and PDA ligation in preterm infants. However, the role of caffeine on longer term clinical outcomes, such as apnoea incidence till 34 corrected gestational weeks, infant respiratory morbidity within the first year of age, need for oxygen treatment after discharge and lung function up until adult age needs to be further investigated in appropriately designed RCTs.

BPD and long-term pulmonary outcomes

Caffeine is one of the few known drugs proven to reduce the risk of BPD at 36 weeks PMA. However, most of the studies evaluating this outcome have been limited in number, have used different definitions of BPD and have not reported longer-term pulmonary outcomes. The main data stem from the results of the CAP trial. Other studies have compared different timing of caffeine treatment or different doses of the drug, and have been conducted mainly retrospectively.

In the Cochrane review on methylxanthines for extubation [36] two trials, the first comparing caffeine versus placebo [53] and the second comparing caffeine, theophylline and placebo, reported rates of BPD defined as oxygen supplementation at 28 days of life in the first, but undefined in the second. Therefore, conclusions on this outcome could not be performed.

In the CAP trial [33], caffeine use led to a 36% decrease in BPD at 36 weeks PMA as defined by Shennan et al. [54], although the definition of BPD is continuously put into question and debate [55, 56]. Interestingly, the post hoc subgroup analysis of the CAP data showed an influence of postnatal age at onset of caffeine treatment on BPD reduction [34], and these findings were confirmed by subsequent cohort studies (further details in section on Benefits of early caffeine administration) [32, 57]. Encouragingly, the effect of caffeine therapy on BPD in the neonatal period seems to have positive repercussions on later lung function as well, as demonstrated by the results of the follow-up at 11 years in Australian former CAP study participants. In this study, expiratory flows were improved by 0.5 sd in children randomised to caffeine (forced expiratory volume at 1 s mean z-score −1.00 versus −1.53, 95% CI 0.14–0.94; p=0.008), with 11% versus 28% with forced vital capacity values below the fifth centile [37]. However, when the respiratory outcomes were adjusted for the higher incidence of BPD in the placebo group, the independent effect of caffeine was lost. As suggested in a comment by Jobe [58] after the publishing of these results, caffeine is extremely useful in minimising apnoea of prematurity with associated improved lung and motor function at 11 years of age. Nevertheless, it is not a lung drug per se, as it minimises interventions for respiratory control abnormalities in the very preterm infant that result in lung injury persisting into childhood.

Overall, studies have demonstrated that caffeine is effective in reducing BPD rates, especially when administered in the first 3 days of life (see later). A follow-up of the CAP trial has shown a positive long-term effect of caffeine on lung function. However, further trials are needed in order to draw more conclusions on the long-term benefits of caffeine in terms of respiratory outcomes, and to target the appropriate population for early treatment.

Benefits of early caffeine administration

A post hoc subgroup analysis of results from the CAP trial suggested an influence of postnatal age at onset of caffeine treatment on BPD reduction, with a decrease in the rate of BPD by 52% in those with early treatment (1–3 days of life) in contrast with a reduction of only 23% if started after day 3 [34]. Since the publication of the results of the CAP trial caffeine has been administered closer and closer to birth, sometimes even in the delivery room [12]. The 2019 European consensus guidelines on the management of neonatal respiratory distress syndrome in preterm infants and the recently published National Institute for Health and Care Excellence recommendations on preterm infants emphasise the role of the timing of caffeine initiation, suggesting that earlier treatment is associated with increased benefit [59, 60]. Nonetheless, no formal guidance specifying the exact timing of therapy commencement has been provided so far.

A retrospective cohort study on 140 infants (birthweight <1250 g) by Patel et al. [61] in 2013 demonstrated that early caffeine initiation (<3 days of life) was associated with a reduced rate of death or BPD, decreased requirement of PDA treatment and shorter duration of mechanical ventilation compared to later caffeine initiation (≥3 days of life). Infants with birthweight <750 g, considered to be at the highest risk for BPD or death, showed the strongest association between early caffeine initiation and decreased incidence of this combined outcome. These results were confirmed by two retrospective studies conducted in 2014. The first study included 29 070 VLBW infants [32], half of whom received early caffeine treatment and were matched on baseline demographics to infants in the late caffeine group. Infants in the early caffeine group had a reduced rate of the composite outcome of death or BPD, less PDA requiring treatment and fewer days of mechanical ventilation. Although infants born at <24 GW treated with early caffeine showed increased odds of death, this result was attributed to survival bias (need to survive to receive later caffeine), as many very preterm infants die in the first 48 h [32]. The second study by Lodha et al. [57] from the Canadian Neonatal Network also showed decreased odds of death or BPD in the group treated with early caffeine (<2 days of life), with most of this effect stemming from the reduction of BPD. In addition, they found a reduced incidence of PDA and duration of mechanical ventilations. Importantly, follow-up of 2108 infants in this study at 18–24 months corrected age demonstrated lower odds of neurodevelopmental impairment in the early caffeine group [62].

Three prospective studies have also suggested benefits of early caffeine administration. A small pilot double-blinded, randomised, placebo-controlled trial conducted in 2015 on 21 infants (<29 GW) randomised to early prophylactic use of caffeine (<2 h of age) or to later caffeine initiation (at 12 h of age), reported improved blood pressure and systemic blood flow (significantly higher superior vena cava flow and right ventricular output) in the early group, and a trend towards reduced rates of intubation by 12 h of age (27% versus 70%; p=0.08), but no reduction in the number of days of mechanical ventilation [40]. More recently, a prospective cohort study on 986 infants (≤32 GW) with respiratory distress syndrome demonstrated that early caffeine treatment (<24 h after birth) compared to later treatment (≥2 days) was associated with a significantly reduced need for invasive ventilation, total duration of mechanical ventilations and significantly lower odds of intraventricular haemorrhage (IVH) and PDA, but no difference in the incidence of BPD and mortality rates [63]. Finally, in a small cohort randomised study, Dekker et al. [12] demonstrated benefits of caffeine administered in the delivery room on minute volumes and tidal volumes at 7–9 min after birth compared to caffeine given after arrival in the neonatal intensive care unit.

Three systematic reviews and meta-analyses have summarised the results of all the studies published so far comparing early versus late caffeine administration. The first, conducted by Park et al. [64] in 2015 included VLBW infants (birthweight <1500 g) treated with early use of caffeine (0–2 days of life) versus late use (≥3 days of life). This meta-analysis of five studies [32, 34, 61, 65, 66] concluded that early caffeine use was associated with a decreased incidence of death, BPD and the composite measure of the two, while the duration of mechanical ventilation was not significantly reduced. The second review and meta-analysis by Kua and Lee [67], published in 2017, selected 14 studies in which early caffeine (<3 days of life) was compared with late caffeine, placebo or theophylline. The meta-analysis of the five cohort studies [34, 57, 61, 65, 68] comparing early versus late caffeine showed reduced rates of BPD, PDA, PDA requiring surgical intervention, brain injury and duration of mechanical ventilation in the early caffeine group, but an increased rate of death, which was not confirmed by the pooled analysis of two randomised control trials [34, 69]. A more recent systematic review and meta-analysis by Pakvasa et al. [70] has explored the effect of both timing of caffeine initiation and dose of caffeine therapy on clinical outcomes (primary: BPD as defined by each specific study or by the need for oxygen at 36 weeks PMA; secondary: death, BPD or death, PDA, necrotising enterocolitis, retinopathy of prematurity, duration of mechanical ventilation and neurodevelopmental impairment). The analysis of the five included observational studies [32, 57, 61, 66, 71] demonstrated a decreased risk of BPD with earlier initiation of caffeine (<3 days of life), while only one RCT comparing early versus routine use of caffeine was identified, and therefore meta-analysis could not be performed [34].

The clinical benefits of beginning caffeine treatment before 3 days of age has been summarised recently by Dobson and Hunt [72], showing the reduced incidence of BPD (with moderate quality of evidence according to the Grading of Recommendations Assessment, Development and Evaluation system), death or BPD, IVH, necrotising enterocolitis, need for treatment of PDA, retinopathy of prematurity and use of postnatal steroids (all of which with low quality of evidence) with the early treatment.

Contrasting results on early caffeine administration

A retrospective analysis conducted by Patel et al. [73] on VLBW infants (birthweight <1500 g) receiving initial CPAP (on day of life 0) compared the effect of early caffeine (day of life 0) versus routine caffeine (day of life 1–6). The results demonstrated no difference in CPAP failure defined as invasive mechanical ventilation or surfactant therapy on day of life 1–6 (22% versus 21%, adjusted odds ratio (aOR) 1.05), in exposure to a maximal inspiratory oxygen fraction >0.3 in the first week of life (27% versus 32%, aOR 1.05) and in the total duration of CPAP therapy (median 3 versus 2 days, aOR 1.02). The authors hypothesised that mechanisms influencing CPAP failure might be different from those influencing the risk of BPD or duration of respiratory support.

In a recent single-centre double-blinded placebo-controlled trial [74], preterm infants (23–30 GW) requiring mechanical ventilations in the first five postnatal days were randomised to receive an early caffeine loading dose of 20 mg·kg⁻¹ followed by 5 mg·kg⁻¹ per day or placebo until considered ready for extubation (the control group then received a pre-extubation bolus of caffeine, whereas the intervention group received a pre-extubation bolus of placebo). Caffeine treatment did not reduce age of first successful extubation (>24 h) nor total duration of mechanical ventilation, incidence of BPD, severe BPD or the composites of BPD or death. Furthermore, a nonsignificant trend towards higher mortality in the early caffeine group led to a cautious decision to stop the trial (22% versus 12%; p=0.22). However, one-third of the deaths in the caffeine group occurred after the first successful extubation, when both groups were receiving caffeine. Furthermore, a recent external analysis of the study [75] highlights that, given the early termination of the trial, the differences in prognostic variables for mortality between groups (gender, Apgar score at 5 min and birthweight) and the imprecision in the estimates of the treatment effect of early caffeine on mortality, no confident conclusions can be determined regarding the effect of early caffeine on mortality.

Currently there are two main ongoing trials exploring the use of early caffeine initiation (data sourced from ClinicalTrials.gov database (https://clinicaltrials.gov)). The first is a double-blind, randomised, placebo-controlled trial evaluating the need for endotracheal intubation within the first 12 h of life and the cardiac output in neonates born at <32 GW receiving caffeine either within 2 h after birth or at 12 h after birth (clinicaltrials.gov identifier NCT0308647). The second is a randomised, double-blind controlled trial of extremely low birthweight newborns (birthweight ≤1000 g and <28 GW) aiming to evaluate the cumulative incidence of death and BPD between groups receiving caffeine (20 mg·kg⁻¹ i.v. bolus, then i.v. or by mouth 5 mg·kg⁻¹ daily for 14 days), or placebo (dextrose) within 24 h of life and then for the subsequent 14 days (clinicaltrials.gov identifier NCT02524249). The results of these trials will be able to shed further light on the best timing for caffeine administration in order to potentially reduce these short- and long-term outcomes.

Table 1 summarises the studies conducted to date in this area. Overall, caffeine administered within the first 3 days of life seems to provide a reduction in BPD rates, PDA and IVH, but does not reduce the risk of CPAP and extubation failure. In addition, there are still contrasting results of the effect of early caffeine initiation on duration of mechanical ventilation and death. There is an urgent need for RCTs addressing this issue, as most results stem from retrospective studies or trials with small sample sizes.

Caffeine metabolism and pharmacokinetics

Most of the studies investigating the metabolism of caffeine in premature newborns were conducted between the 1970s and the 1990s by Aranda and co-workers [93, 94]. Using high-performance liquid chromatography (HPLC), these authors were able to show a strict correlation between administered dose of drug and plasma level [77], as well as between plasma and cerebrospinal fluid levels [95]. The route of caffeine administration does not affect its pharmacokinetics, as there is almost complete bioavailability after its oral or i.v. administration. Oral caffeine citrate is rapidly and completely absorbed by the gastrointestinal tract, as there is almost no first-pass metabolism, with the peak plasma concentration often reached in <1 h [96].

Caffeine metabolism occurs in the liver, mainly by CYP1A2, with a subsequent N-demethylation at positions 1, 3 and 7 and hydroxylation at position 8. In preterm neonates, ∼86% of caffeine citrate is excreted unchanged in the urine [97], as the processes of caffeine metabolism maturates progressively through time (N7-demethylation at the post-natal age of ∼4 months [98], acetylation by N-acetyltransferase (NAT2) completely developed by 1 year of postnatal age [99] and 8-hydroxylation activity starting as early as 1 month of age [100]). Thus, the maturity of the hepatic enzymes, dependent mainly by the postnatal age regardless of birthweight and gestational age, affects the plasma half-life of the drug [98, 101].

Due to this difference in metabolism, and to the slow urinary excretion of unmetabolised drug at the earlier gestational ages, the serum half-life of caffeine in infants ranges from 40 to 230 h (>17-fold greater than that in adults), decreasing with the advance of PMA to ∼2–4 h by 6–8 months [102]. Of note, because of the long half-life, caffeine may persist in an infant's plasma for some days after cessation of therapy [102, 103].

Elimination of caffeine occurs mainly by renal excretion in the first weeks of life, which is slower in premature and term neonates compared with older children and adults, because of immaturity of renal functions [96]. Clearance of caffeine in neonates is influenced by gestational age, postconceptional age, parenteral nutrition and comorbidities [96, 99, 100, 103, 104], with values ranging from 0.08  to 0.13 mL·kg⁻¹·min⁻¹ compared to that of adults and older children of 1.5 and 4.4 mL·kg⁻¹·min⁻¹, respectively [100, 105].

These data highlight that extremely premature infants do not behave as “little adults” with respect to caffeine pharmacokinetics, as caffeine metabolism and urinary elimination are strongly determined by the maturity of liver enzymes and renal function, which are influenced by gestational and postnatal age and by the presence of morbidities affecting these organs.

Therapeutic drug monitoring

Caffeine dosing and therapeutic drug monitoring (TDM) vary from practice to practice. Caffeine has a wider therapeutic range than theophylline, therefore the role of TDM for the control of therapeutic ranges of caffeine has often been challenged [106]. A therapeutic level of caffeine is considered between 5 and 25 mg·L⁻¹ (or µg·mL⁻¹), while toxic levels are reached with >40–50 mg·L⁻¹ [107, 108]. An observational study by Natarajan et al. [109] in neonates born between 23 and 32 GW found that caffeine citrate doses of 2.5–10.9 mg·kg⁻¹ (median 5 mg·kg⁻¹), obtained plasma levels ranging between 5.1 and 20 mg·L⁻¹ in 94.8% of cases (within the normal therapeutic ranges), independent of gestation, thus indicating against the necessity of TDM. However, in the subgroup of infants in whom caffeine plasma concentrations were obtained for lack of clinical efficacy, three-quarters of the levels were within the normal range (15 mg·L⁻¹), which suggests that higher doses and plasma concentrations may be required for optimal efficacy in some preterm neonates. In addition, the numbers of infants with renal or hepatic dysfunction in the study were small at the time of caffeine level, and no data on relation to efficacy with regard to apnoea was reported. Importantly, another study demonstrated that a standardised regimen leads to a high variation of serum levels of caffeine metabolites in infants <33 GW, with no correlation between episodes of apnoea and caffeine serum concentrations in the post-extubation period [110]. Therefore, caffeine TDM may help dose individualisation in order to minimise the incidence of toxic adverse effects, optimise efficacy and the performance of diagnostic tests, especially for patients who are unresponsive to therapy (breakthrough apnoea, bradycardia or desaturations without other obvious disease-related aetiologies) [106, 111, 112]. In addition, a retrospective chart review of infants born ≤29 GW demonstrated that those with an average caffeine concentration >14.5 μg·mL⁻¹ had lower incidence of chronic lung disease and PDA, lesser number of days on ventilator and oxygen, less need for diuretics and lower length of stay and total hospital charges (all p<0.05) [113]. If these findings are confirmed prospectively, it could become useful to introduce TDM in routine practice.

Caffeine levels can be measured in plasma, saliva or urine by enzyme immunoassay technique, which is simple, convenient and rapid, or using HPLC, which is the most accurate technique for caffeine TDM in the clinical setting [114, 115]. In recent years, minimally invasive techniques have been proposed for the detection of caffeine levels, with promising results. In 2013, Patel et al. [116] used dried blood spots (DBS) to measure caffeine dosage with liquid chromatography triple quadrupole mass spectrometry from 67 preterm infants at random time intervals following either oral or i.v. doses. The study showed a good agreement between pharmacokinetic parameters estimated using DBS samples and historical caffeine pharmacokinetic parameters based on plasma samples.

In 2016, Bruschettini et al. [117] confirmed the importance of limiting the size of blood samples to avoid anaemia due to blood sampling for TDM in preterm infants and highlighted the advantages of DBS over conventional sampling techniques. To overcome the problem of haematocrit, alternative strategies based on new microfluidic sampling procedures or volumetric microsampling devices have been described and proved to be a reliable sampling approach for caffeine [118, 119]; however, the drawback is the use of expensive devices for routine TDM analyses or for pharmacokinetic studies. To overcome the problem of blood sample size, invasiveness and cost, in 2017, Chaabane et al. [120] determined caffeine concentrations in both saliva and serum of preterm infants (mean gestational age 32.2±0.7 weeks), showing a proportional increase in both saliva and serum caffeine concentration to the administered dose, with the saliva caffeine concentrations strongly correlating with those from serum.

Despite different studies exploring the best minimally invasive and cost-effective methods to monitor therapeutic ranges of caffeine in clinical practice, few have tried to develop a pharmacokinetic model to adjust caffeine dosage and none has investigated the relationship between caffeine biofluid levels in the first weeks of life and clinical outcomes, such as apnoea frequency [121, 122]. Interestingly, in 2017 Koch et al. [122] developed simulation models of caffeine concentrations, proposing the need of adjusting the maintenance doses through time in preterm neonates, with the administration of 6 mg·kg⁻¹·day⁻¹ in the second week of life, 7 mg·kg⁻¹·day⁻¹ in weeks 3–4 and 8 mg·kg⁻¹·day⁻¹ in weeks 5–8.

Further studies are needed to determine whether caffeine dosage can be optimised for the individual patient through TDM in particular situations. Drug levels could be performed minimising the drawn blood volume (for instance with DBS) or, even better, non-invasively (for example in urine or saliva samples). Prospective pharmacokinetic studies of caffeine with relation to both clinical outcomes (apnoea episodes, extubation failure, respiratory support at 36 weeks PMA, respiratory morbidity in the first year of life), and adverse events (tachycardia, hypoglycaemia, seizures, weight loss, neurodevelopment at 2 and 5 years) should be conducted in order to identify the appropriate dosage of the drug.