Hostname: page-component-8448b6f56d-jr42d Total loading time: 0 Render date: 2024-04-18T20:17:07.400Z Has data issue: false hasContentIssue false
  • English
  • Français

Specific probiotics in reducing the risk of acute infections in infancy – a randomised, double-blind, placebo-controlled study

Published online by Cambridge University Press:  06 November 2008

Samuli Rautava ,
Seppo Salminen  and
Erika Isolauri
Samuli Rautava*
Affiliation:
Department of Paediatrics, University of Turku, Turku, Finland
Seppo Salminen
Affiliation:
Department of Biochemistry and Food Chemistry, University of Turku, Turku, Finland
Erika Isolauri
Affiliation:
Department of Paediatrics, University of Turku, Turku, Finland
*
*Corresponding author: Dr Samuli Rautava, fax +358 2 3131460, email samrau@utu.fi
Rights & Permissions [Opens in a new window]

Abstract

A randomised, double-blind, placebo-controlled study was conducted to determine whether probiotics might be effective in reducing the risk of infections in infancy. Infants requiring formula before the age of 2 months were recruited from community well-baby clinics. Infant formula supplemented with the probiotics Lactobacillus rhamnosus GG and Bifidobacterium lactis Bb-12 or placebo was administered daily until the age of 12 months. Incidence of early infections (before the age of 7 months) and incidence of recurrent (three or more) infections during the first year of life were recorded as the main outcome measures of the study. During the first 7 months of life, seven out of thirty-two (22 %) infants receiving probiotics and twenty out of forty (50 %) infants receiving placebo experienced acute otitis media (risk ratio (RR) 0·44 (95 % CI 0·21, 0·90); P = 0·014) and antibiotics were prescribed for ten out of thirty-two (31 %) infants receiving probiotics and twenty-four out of forty (60 %) infants receiving placebo (RR 0·52 (95 % CI 0·29, 0·92); P = 0·015). During the first year of life, nine out of thirty-two (28 %) infants receiving probiotics and twenty-two out of forty (55 %) infants receiving placebo encountered recurrent respiratory infections (RR 0·51 (95 % CI 0·27, 0·95); P = 0·022). These data suggest that probiotics may offer a safe means of reducing the risk of early acute otitis media and antibiotic use and the risk of recurrent respiratory infections during the first year of life. Further clinical trials are warranted.

Keywords

Acute otitis mediaInfantsProbiotics
Type
Full Papers
Information
British Journal of Nutrition , Volume 101 , Issue 11 , 14 June 2009 , pp. 1722 - 1726
Copyright
Copyright © The Authors 2008

Infectious disease is the most important cause of morbidity in infants. In developed countries, infants experience three to six respiratory tract infections during the first year of life(Reference Monto1, Reference Vesa, Kleemola and Blomqvist2) and 40 % of them suffer from at least one episode of acute otitis media (AOM), the most common reason for antibiotic use(Reference Alho, Koivu and Sorri3). Widespread use of antibiotics has led to increasing microbial resistance. In addition to increased caution in prescribing antimicrobial agents, new means of reducing the risk of infectious disease in infancy are called for.

The infant's developing immune system is dependent on contact with environmental antigens to achieve adequate and appropriate immune competence. Breast-feeding and the intestinal microbiota are considered the most important sources of maturational stimuli(Reference Holt and Jones4). On this basis, specific strains from the healthy intestinal microbiota have been used as probiotics, defined as ‘specific live or inactivated microbial cultures that have documented targets in reducing the risk of human disease or in their nutritional management’(Reference Isolauri, Rautava and Kalliomäki5).

Breast milk provides crucial protection against microbial invaders in the form of antibodies and non-specific antimicrobial factors(Reference Bernt and Walker6). In addition, breast milk may contain viable lactobacilli(Reference Martin, Langa and Reviriego7) and factors that promote the growth of bifidobacteria in the infant's intestine(Reference Beerens, Romond and Neut8, Reference Liepke, Adermann and Raida9), which may contribute to healthy immunological maturation. We therefore hypothesised that administering specific probiotics may promote the maturing effect of gut microbiota in infants devoid of the recommended exclusive breast-feeding. Such nutritional intervention could reduce the incidence of acute infections and need for antibiotic treatment during the first year of life.

Methods

The infants participating in this randomised, double-blind, placebo-controlled clinical trial were recruited in Turku, Finland, between September 2000 and May 2002.

At recruitment, reliable data regarding the occurrence of respiratory tract infections or AOM in infants who were not exclusively breast-fed were not available. Based on a rough estimate for statistical power, our initial aim was to recruit 200 infants. Due to the baby-friendly hospital initiative and the strong policy of promoting breast-feeding, which is of utmost importance in well-baby clinics, advertising the study with formula supplementation at an early age was not acceptable. Thus information regarding the study was given only when the need of formula was imminent. Recruitment was therefore slow and a pragmatic deadline for enrolment was set at the end of May 2002. All families who were interested in participating and contacted the research nurse during the recruitment period were assessed for eligibility (Fig. 1).

Fig. 1 The study profile. GI, gastrointestinal.

The sole inclusion criterion for the study was need for infant formula before the age of 2 months. Infants with chronic disease were excluded. The study was found ethically acceptable by the Turku University Central Hospital Ethical Committee. Written informed consent was obtained from the infants' parents.

In all, eighty-one infants were randomised by block randomisation with individual codes to receive either 1 × 1010 colony-forming units of both Lactobacillus rhamnosus (Lactobacillus GG, American type culture collection 53103; Valio Ltd, Helsinki, Finland) and Bifidobacterium lactis Bb-12 (Chr. Hansen A/S, Hoersholm, Denmark) or placebo (microcrystalline cellulose) daily until the age of 12 months. These strains were chosen because of documented safety properties and a long history of safe use both in infant studies and in food products. In addition, we have previously demonstrated that these two strains have synergistic effects in vitro, with Lactobacillus GG increasing the adherence of B. lactis Bb-12(Reference Ouwehand, Isoauri and Kirjavainen10). The random allocation was generated independently from the investigators by the manufacturer of the capsules (Chr. Hansen A/S). All investigations were performed double blind; the code was opened after all the infants had completed the study and data had been edited. The daily probiotics or placebo were provided in visually identical capsules (Chr. Hansen A/S), the contents of which were supplemented to infant formula (Enfamil; Mead Johnson Nutritionals, Evansville, IN, USA) given at one feeding. Administration of the supplemented formula was commenced after recruitment when the need of formula arose and the formula was to be used as the sole infant formula during the study period. At recruitment, maternal use of commercially available products containing probiotics was discouraged. Such products were not available for infants in Finland at the time of the study.

To ascertain that the probiotics remained viable during storage, microbiological analysis of a random sample of capsules was performed by a microbiologist in a blinded fashion. Viable counts between 1 × 109 and 1 × 1010 per capsule were found for both Lactobacillus GG and B. lactis Bb-12.

The infants were followed up until the age of 12 months. Clinical examination of the infants was performed at scheduled visits at the ages of 3, 7 and 12 months. The follow-up was completed by seventy-two of the eighty-one (89 %) infants enrolled (Fig. 1). All infections during the study period were recorded in special diaries by the family or the family physician. Respiratory infections, doctor-diagnosed AOM, gastrointestinal infections and the number of treatments with antibiotic agents were separately recorded in detail. AOM was defined as an acute, short-course inflammation in the middle ear that can be clinically verified, accompanied by at least one of the following features: rhinitis, cough, fever, sore throat, earache, hypacusis, restlessness at night, irritability, loss of appetite, vomiting or diarrhoea. Purulent otorrhoea through a perforated tympanic membrane or tympanostomy tube was also considered to constitute AOM.

The primary outcome measure for the study was the incidence of early respiratory infections, doctor-diagnosed AOM and gastrointestinal infections defined as infections occurring before the age of 7 months. The incidence of recurrent (defined as three or more occurrences) respective infections during the first year of life was considered a secondary outcome measure. Early or recurrent need for antibiotics was interpreted to reflect suspected early or recurrent bacterial infections, respectively, and thus recorded. In Finland, antibiotics are available only through prescription by licensed physicians. Tympanostomy before the age of 12 months was interpreted to indicate frequent ear infections.

All adverse effects were recorded in detail and the infants in whom symptoms were suspected to be related to the study products were subjected to an elimination and re-exposure procedure.

The data are expressed as means with range and risk ratios with 95 % CI to accurately depict statistical power(Reference Schulz and Grimes11). The comparisons between the groups were conducted using the χ2 test. Subjects lost to follow-up were excluded from the analyses. A complete intention-to-treat approach was not possible because the mean age of the nine subjects lost to follow-up was 2·9 (range 1·5–7·0) months and no evaluation after randomisation was performed in eight out of nine of these infants. Imputation techniques were not considered satisfactory solutions to estimate the missing outcome variables due to the proportion of lost-to-follow-up cases and relatively small sample size.

Results

The baseline characteristics were similar in infants receiving probiotics and placebo (Table 1).

Table 1 Baseline characteristics and history

(Mean values and ranges or numbers and percentages)

The effect of probiotics on the incidence of early and recurrent infections

The study probiotics reduced the risk of early AOM and need for antibiotic treatment during the first 7 months of life. The results are presented in detail in Table 2. Probiotics also reduced significantly the incidence of recurrent respiratory infections during the first 12 months of life (Table 3). None of the infants in the study experienced more than two gastrointestinal infections during the study period. In addition, the administration of probiotics tended to reduce the need for tympanostomy, performed either to prevent recurrent AOM or to treat secretory otitis media: none of the infants receiving probiotics required tympanostomy during the first year of life, whereas the procedure was performed on four out of forty (10 %) infants receiving placebo (P = 0·066).

Table 2 Incidence of infections during the first 7 months of life

RR, risk ratio; AOM, acute otitis media.

Table 3 Incidence of recurrent infections (three or more episodes) and use of medical interventions during the first 12 months of life

RR, risk ratio; AOM, acute otitis media.

* Calculated assuming one positive case in probiotic group.

Adverse effects

No serious adverse effects resulting from probiotic supplementation were detected during the study. In addition to the infants who discontinued the intervention (Fig. 1), gastrointestinal symptoms that the parents related to the study product were reported in four infants who completed the study. One infant experienced vomiting after accidental ingestion of a several-fold dosage of the study product daily. The vomiting subsided when supplementation was discontinued and the infant was able to continue the intervention with the appropriate dosage shortly thereafter. The infant was discovered to have received probiotics when the follow-up was completed and the code opened. The remaining three out of four infants with gastrointestinal symptoms, including vomiting, flatulence and increased fussing, were subjected to an elimination and re-exposure procedure and two out of three of these infants subsequently continued with the intervention. When the code was opened after the follow-up was completed, all three of these infants were discovered to have received placebo.

Discussion

A significant reduction in the incidence of early and recurrent infections and the use of antibiotics during the first year of life was achieved by probiotic supplementation in the present study. The effect was most prominent with regard to respiratory infections and AOM, the most prevalent infections in infancy. In contrast, no statistically significant effect was detected on the occurrence of gastrointestinal infections. The relatively small number of patients is an obvious limitation of the study and was reflected in the wide CI of the results. The possibility that all true differences between the infants receiving probiotics and placebo do not display statistical significance cannot be excluded. Nonetheless, probiotics appeared to confer significant protection against early infections, the importance of which culminates in the fact that the children developing frequent infections, including AOM, experience their first infection early(Reference Nokso-Koivisto, Pitkäranta and Blomqvist12, Reference Klein13).

According to a recent survey, only 51 % of infants in Finland are exclusively breast-fed at the age of 2 months, and the proportion of those exclusively breast-fed declines rapidly thereafter(Reference Hasunen14). Lack of breast-feeding and parental smoking are among the most important risk factors for recurrent infections in infancy in developed countries(Reference Klein13). The present study demonstrates the tendency for risk factors to cluster in certain families, as at least one of the parents smoked in more than half of the families participating in the study. This may restrict the applicability of the present results to the general population on the one hand and underscores the importance of continuing counselling with regard to health-promoting lifestyle on the other.

The efficacy of Lactobacillus GG(Reference Oberhelman, Gilman and Sheen15, Reference Szajewska, Kotowska and Mrukowicz16) and bifidobacteria(Reference Chouraqui, Van Egroo and Fichot17, Reference Saavedra, Bauman and Oung18) in reducing the risk of infectious disease has previously been most comprehensively documented in the context of viral diarrhoea. There are limited data on the effects of probiotics in reducing the risk of respiratory tract infections and the present study is the first to suggest protection against AOM. In an older age group, a modest reduction in the severity of respiratory tract infections and absence from day care was achieved with milk supplemented with Lactobacillus GG whereas the occurrence of infections was not significantly reduced(Reference Hatakka, Savilahti and Ponka19). In a recent study, the combination of Lactobacillus GG and three other probiotic bacteria failed to reduce the occurrence of AOM but appeared to protect against recurrent respiratory tract infections in children with a history of recurrent AOM(Reference Weizman, Asli and Alsheikh20). In the present study, probiotic supplementation was commenced in the first months of life before the first occurrence of AOM. According to our interpretation, it is crucial that children are subjected to intervention in early infancy, as the maturing immune system might be more amenable to probiotic modification. Nonetheless, it has been reported that B. lactis Bb-12 or L. reuteri (ATCC 55730) do not confer protection against respiratory tract infections in infancy, but it should be noted that the follow-up in the study only lasted 12 weeks(Reference Hatakka, Plomgren and Pohjavuori21).

There are numerous potential mechanisms through which probiotics might mediate their protective effect against infectious disease. Specific probiotics have direct anti-pathogenic effects by promoting mucosal barrier functions(Reference Isolauri, Majamaa and Arvola22) and inhibiting mucosal pathogen adherence by inducing mucin secretion(Reference Mack, Michail and Wei23). Lactobacilli have been shown to be potent inducers of innate immune responses against microbial pathogens(Reference Perdigón, de Macias and Alvarez24). Both Lactobacillus GG and B. lactis Bb-12 have been documented to augment humoral immune responses(Reference Fukushima, Kawata and Hara25, Reference Rautava, Arvilommi and Isoaluri26), especially during viral infections(Reference Kaila, Isolauri and Soppi27). Indeed, contact with environmental and intestinal microbes appears to be essential for normal immunological maturation(Reference Holt and Jones4).

It is conceivable that the protection against AOM provided by probiotics in the present study may have been mediated via both reduction of colonisation by pathogens by local inhibition and immunomodulation throughout the common mucosa-associated immune system. Nasopharyngeal colonisation by the predominant causative agents of AOM, Streptococcus pneumoniae, Haemophilus influenzae or Moraxella catarrhalis (Reference Kilpi, Herva and Kaijalainen28), before the age of 3 months is associated with an increased risk of AOM(Reference Faden, Duffy and Wasielewski29). Probiotics, such as Lactobacillus GG and bifidobacteria, have been shown to reduce nasal colonisation with pathogenic bacteria, including S. pneumoniae in adults(Reference Glück and Gebbers30). The effect may be immunologically mediated, as no indication of nasal colonisation by the probiotic strains was detected in the study in contrast to a previous study indicating that ingested Lactobacillus GG briefly colonise the mouth(Reference Meurman, Antila and Salminen31). Indeed, we have previously demonstrated that ingestion of Lactobacillus GG leads to favourable changes at mucosal sites beyond the intestine(Reference Rautava, Kalliomäki and Isolauri32). According to a recent study, however, Lactobacillus GG in combination with three other probiotics does not reduce nasopharyngeal carriage of S. pneumoniae, H. influenzae or M. catarrhalis in infants suffering from recurrent AOM(Reference Weizman, Asli and Alsheikh20). It is not known whether probiotics have the potential to reduce initial nasal colonisation by these pathogens in early infancy.

Respiratory infections are a major cause of infant morbidity and still a prominent cause of infant death in many areas. AOM is the most common reason for consulting a doctor in children and more prescriptions for antibiotics are written for AOM than any other disease in infancy(Reference Klein13), thus potentially contributing to the rise in microbial resistance to antibiotic agents. Based on the present study, the probiotic combination of Lactobacillus GG and B. lactis Bb-12 may offer a safe and inexpensive means of reducing the continuing burden of these infections and the need for antibiotic treatment in full-term infants who require formula at an early age. Clinical trials with larger numbers of infants are required to corroborate these results.

Acknowledgements

All authors participated in designing the trial, analysis of the results and writing of the report with full access to all the data in the study, and take responsibility for the integrity of the data and the accuracy of the data analysis. Ms Sari Laksio, RN, provided and cared for the infants participating in the study. Dr Arthur C. Ouwehand, PhD, conducted the viability assessments of the probiotics in the capsules. Statistical consultation was provided by Tuija Poussa, MSc, and Jouni Alin, BSc.

Lactobacillus GG was acquired without cost from Valio Ltd and Chr. Hansen A/S (Hoersholm, Denmark) provided B. lactis Bb-12 and manufactured the probiotic and placebo capsules without cost. The infant formula was provided without cost by MeadJohnson Nutritionals. The study was funded by the Microbes and Man research programme, the Academy of Finland and the Bristol-Myer Squibb MeadJohnson Foundation Unrestricted Research Grant. The funding sources had no involvement in study design, in the collection, analysis and interpretation of data, in the writing of the report or in the decision to submit the paper for publication.

References

1Monto, AS (2002) Epidemiology of viral respiratory infections. Am J Med 112, 4S12S.CrossRefGoogle ScholarPubMed
2Vesa, S, Kleemola, M, Blomqvist, S, et al. (2001) Epidemiology of documented viral respiratory infections and acute otitis media in a cohort of children followed from two to twenty-four months of age. Pediatr Infect Dis J 20, 574581.CrossRefGoogle Scholar
3Alho, OP, Koivu, M, Sorri, M, et al. (1991) The occurrence of acute otitis media in infants. A life-table analysis. Int J Pediatr Otorhinolaryngol 21, 714.CrossRefGoogle ScholarPubMed
4Holt, PG & Jones, CA (2000) The development of the immune system during pregnancy and early life. Allergy 55, 688697.CrossRefGoogle ScholarPubMed
5Isolauri, E, Rautava, S, Kalliomäki, M, et al. (2002) Role of probiotics in food hypersensitivity. Curr Opin Allergy Clin Immunol 2, 263271.CrossRefGoogle ScholarPubMed
6Bernt, KM & Walker, WA (1999) Human milk as a carrier of biochemical messages. Acta Paediatr Suppl 88, 2741.CrossRefGoogle ScholarPubMed
7Martin, R, Langa, S, Reviriego, C, et al. (2003) Human milk is a source of lactic acid bacteria for the infant. J Pediatr 143, 754758.CrossRefGoogle ScholarPubMed
8Beerens, H, Romond, C & Neut, C (1980) Influence of breast-feeding on the bifid flora of the newborn intestine. Am J Clin Nutr 33, 24342439.CrossRefGoogle ScholarPubMed
9Liepke, C, Adermann, K, Raida, M, et al. (2002) Human milk provides peptides highly stimulating the growth of bifidobacteria. Eur J Biochem 269, 712718.CrossRefGoogle ScholarPubMed
10Ouwehand, AC, Isoauri, E, Kirjavainen, PV, et al. (2000) The mucus binding of Bifidobacterium lactis Bb12 is enhanced in the presence of Lactobacillus GG and Lact. delbrueckii subsp. bulgaricus. Lett Appl Microbiol 30, 1013.CrossRefGoogle ScholarPubMed
11Schulz, KF & Grimes, DA (2005) Sample size calculations in randomized trials: mandatory and mystical. Lancet 365, 13481353.CrossRefGoogle ScholarPubMed
12Nokso-Koivisto, J, Pitkäranta, A, Blomqvist, S, et al. (2002) Viral etiology of frequently recurring respiratory tract infections in children. Clin Inf Dis 35, 540546.CrossRefGoogle ScholarPubMed
13Klein, JO (2001) The burden of otitis media. Vaccine 19, S2S8.CrossRefGoogle Scholar
14Hasunen, K (2001) Infant feeding in Finland 2000. In Reports of the Ministry of Social Affairs and Health, vol. 12, pp. 12362115. Helsinki: Ministry of Social Affairs and Health.Google Scholar
15Oberhelman, RA, Gilman, RH, Sheen, P, et al. (1999) A placebo-controlled trial of Lactobacillus GG to prevent diarrhea in undernourished Peruvian children. J Pediatr 134, 1520.CrossRefGoogle ScholarPubMed
16Szajewska, H, Kotowska, M, Mrukowicz, JZ, et al. (2001) Efficacy of Lactobacillus GG in prevention of nosocomial diarrhea in infants. J Pediatr 138, 361365.CrossRefGoogle ScholarPubMed
17Chouraqui, JP, Van Egroo, LD & Fichot, MC (2004) Acidified milk formula supplemented with Bifidobacterium lactis: impact on infant diarrhea in residential care settings. J Pediatr Gastroenterol Nutr 38, 288292.Google ScholarPubMed
18Saavedra, JM, Bauman, NA, Oung, I, et al. (1994) Feeding of Bifidobacterium bifidum and Streptococcus thermophilus to infants in hospital for prevention of diarrhoea and shedding of rotavirus. Lancet 344, 10461049.CrossRefGoogle ScholarPubMed
19Hatakka, K, Savilahti, E, Ponka, A, et al. (2001) Effect of long term consumption of probiotic milk on infections in children attending day care centres: double blind, randomised trial. BMJ 322, 13271331.CrossRefGoogle ScholarPubMed
20Weizman, Z, Asli, G & Alsheikh, A (2005) Effect of a probiotic infant formula on infections in child care centers: comparison of two probiotic agents. Pediatrics 115, 59.CrossRefGoogle ScholarPubMed
21Hatakka, K, Plomgren, K, Pohjavuori, S, et al. (2007) Treatment of acute otitis media with probiotics in otitis-prone children – a double-blind, placebo-controlled randomised study. Clin Nutr 26, 314321.CrossRefGoogle ScholarPubMed
22Isolauri, E, Majamaa, H, Arvola, T, et al. (1993) Lactobacillus casei strain GG reverses increased intestinal permeability induced by cow milk in suckling rats. Gastroenterology 105, 16431650.CrossRefGoogle ScholarPubMed
23Mack, DR, Michail, S, Wei, S, et al. (1999) Probiotics inhibit enteropathogenic E. coli adherence in vitro by inducing intestinal mucin gene expression. Am J Physiol 276, G941G950.Google ScholarPubMed
24Perdigón, G, de Macias, ME, Alvarez, S, et al. (1986) Effect of perorally administered lactobacilli on macrophage activation in mice. Infect Immun 53, 404410.CrossRefGoogle ScholarPubMed
25Fukushima, Y, Kawata, Y, Hara, H, et al. (1998) Effect of a probiotic formula on intestinal immunoglobulin A production in healthy children. Int J Food Microbiol 42, 3944.CrossRefGoogle ScholarPubMed
26Rautava, S, Arvilommi, H & Isoaluri, E (2006) Specific probiotics in enhancing maturation of IgA responses in formula-fed infants. Pediatr Res 60, 221224.CrossRefGoogle ScholarPubMed
27Kaila, M, Isolauri, E, Soppi, E, et al. (1992) Enhancement of the circulating antibody secreting cell response in human diarrhea by a human Lactobacillus strain. Pediatr Res 32, 141144.CrossRefGoogle ScholarPubMed
28Kilpi, T, Herva, E, Kaijalainen, T, et al. (2001) Bacteriology of acute otitis media in a cohort of Finnish children followed for the first two years of life. Pediatr Infect Dis J 20, 654662.CrossRefGoogle Scholar
29Faden, H, Duffy, L, Wasielewski, R, et al. (1997) Relationship between nasopharyngeal colonization and the development of otitis media in children. J Infect Dis 175, 14401445.CrossRefGoogle ScholarPubMed
30Glück, U & Gebbers, JO (2003) Ingested probiotics reduce nasal colonization with pathogenic bacteria (Staphylococcus aureus, Streptococcus pneumoniae, and β-hemolytic streptococci). Am J Clin Nutr 77, 517520.CrossRefGoogle ScholarPubMed
31Meurman, JH, Antila, H & Salminen, S (1994) Recovery of Lactobacillus strain GG (ATCC 53103) from saliva of healthy volunteers after consumption of yoghurt prepared with the bacterium. Microbiol Ecol Health Dis 7, 295298.CrossRefGoogle Scholar
32Rautava, S, Kalliomäki, M & Isolauri, E (2002) Probiotics during pregnancy and breast-feeding might confer immunomodulatory protection against atopic disease in the infant. J Allergy Clin Immunol 109, 119121.CrossRefGoogle ScholarPubMed
Figure 0

Fig. 1 The study profile. GI, gastrointestinal.

Figure 1

Table 1 Baseline characteristics and history(Mean values and ranges or numbers and percentages)

Figure 2

Table 2 Incidence of infections during the first 7 months of life

Figure 3

Table 3 Incidence of recurrent infections (three or more episodes) and use of medical interventions during the first 12 months of life