C Macaubas’s research while affiliated with Stanford University and other places

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Publications (29)


Enhancement of vaccine-specific cellular immunity in infants by passively acquired maternal antibody
  • Article

October 2004

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19 Reads

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23 Citations

Vaccine

J Rowe

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C Macaubas

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[...]

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P G Holt

The known protective effects of passively acquired maternal antibody on the resistance of newborns to infections have prompted widespread interest in maternal vaccination. However, a range of animal model and human studies indicate potential inhibitory effects of maternal antibody on vaccine-specific humoral responses in infants. In the present study we have examined the relationship between maternally acquired TT-specific IgG present before DTaP vaccination and subsequent TT-specific T-cell memory responses at 12 and 18 months, in a cohort of 118 infants. We demonstrate a strong positive association between TT-specific cellular immunity as evidenced by increased IL-4, IL-5 and IL-13 responses, and maternal TT-specific IgG.



Association between antenatal cytokine production and the development of atopy and asthma at age 6 years

October 2003

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29 Reads

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205 Citations

The Lancet

Various lines of evidence suggest that antenatal factors are important in determining susceptibility to atopy and asthma. One possible mechanism is cytokines, production of which in the placenta is high throughout gestation and which protect placental integrity via control of local immunological homoeostasis. We investigated antenatal cytokine concentrations in a prospective birth cohort, intensively monitored for atopy and asthma outcomes at age 6 years. Cryopreserved cord-blood serum samples from 407 children were assayed for interleukins 4, 5, 6, 10, 12, and 13, interferon gamma, and tumour necrosis factor alpha (TNFalpha). Associations between family, antenatal, and perinatal factors, cord-blood cytokine concentrations, and atopy or asthma outcomes were analysed by logistic regression. Causal effects of cytokines on outcomes were estimated by propensity scores based on family, antenatal, and perinatal factors. Detectable cord-blood concentrations of interleukin 4 and interferon gamma were each associated with lower risk of physician-diagnosed asthma (adjusted odds ratios 0.60 [95% CI 0.37-0.99] and 0.60 [0.37-0.97] respectively), current asthma (0.59 [0.33-1.00] and 0.39 [0.22-0.71]), and current wheeze (0.55 [0.32-0.93] and 0.52 [0.31-0.90]) and atopy (sensitisation to some inhalant allergens) outcomes at 6 years. High concentrations of TNFalpha were associated with lower risk of atopy but not with asthma risk. These associations were broadly unaltered by propensity-score adjustment. Maternal smoking was associated with higher risk of both wheeze at 6 years and lower concentrations of interleukin 4 and interferon gamma in cord blood. The mechanism underlying attenuated T-helper-1/T-helper-2 cytokine production in high-risk children also apparently operates in control of cytokine production in the fetoplacental unit. The finding that this mechanism is dysregulated by maternal smoking suggests it is a target for antenatal environmental factors relevant to asthma aetiology.


Reciprocal patterns of allergen-induced GATA-3 expression in peripheral blood mononuclear cells from atopics vs. non-atopics

February 2002

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49 Reads

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27 Citations

Clinical & Experimental Allergy

T helper (Th)2 cytokines are considered to play a central role in the induction and expression of allergic disease. However, the relative importance of individual cytokines is unclear, and overall disease pathogenesis appears to involve the coordinate activities of a range of Th2 cytokines acting in sequence or in parallel. The present study examines an alternative approach to the study of cytokine gene function in atopy, focusing instead upon T cell transcription factors (TFs) which play a role in the regulation of multiple cytokine genes. To investigate the allergen-induced expression of the TF GATA-3 and c-Maf in peripheral blood mononuclear cells (PBMCs) and in cytokine-driven Th polarization. PBMC from house dust mite (HDM)-atopic and non-atopics were stimulated in vitro with allergen or anti-CD3/IL-2. TF expression was analysed by semiquantitative RT-PCR and major findings were validated by real-time PCR. Cell separations were performed to analyse the contribution of CD45RO+ cells. CD4+ cord blood cells were Th1 or Th2 polarized in vitro by exogenous cytokines and TF expression analysed by Northern blot and real-time PCR. Results We demonstrate for the first time that during differentiation of CD4+ CD45RA+ naïve human T cells towards Th2 commitment, and during allergen-specific reactivation of peripheral CD4+ CD45RO+ Th2 memory cells in established atopics, expression of the Th2-associated TF GATA-3 is rapidly up-regulated, whereas T cells from non-atopics display equally rapid GATA-3 down-regulation under identical conditions of allergen stimulation. These findings identify Th2-associated TFs as key determinants of the atopic phenotype, suggesting their unique potential as therapeutic targets for disease control.


"Bystander" amplification of PBMC cytokine responses to seasonal allergen in polysensitized atopic children

December 2001

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52 Reads

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26 Citations

Atopic children show increased expression and production of the Th2-associated cytokines IL-4, IL-5, IL-13, and IL-9 from PBMCs after stimulation with allergen, but it has previously not been clearly determined whether the Th2-cytokine production is restricted to the inhalant allergen the child is sensitized to, and whether perennial or seasonal allergens induce different cytokine responses. Our purpose was to determine whether in vitro Th2 cytokine production is specific to the sensitizing allergen, and to compare the cytokine responses to a perennial and a seasonal allergen in monosensitized and polysensitized children. Using semiquantitative RT-PCR, we analyzed the expression of the cytokines IL-4, IL-5, IL-13, IL-9, IL-10, and IFN-gamma after stimulation of PBMCs with house-dust-mite (HDM) or ryegrass allergen. The cells were sampled from groups of 6-year-old children sensitized to either HDM (n=20) or ryegrass (n=24), or to both allergens (n=20), as well as from a nonatopic group (n=20). After stimulation with HDM allergen, PBMCs from children sensitized only to HDM expressed increased mRNA levels of the Th2 cytokines, but not of IL-10 and IFN-gamma, whereas ryegrass stimulation did not result in increased cytokine expression. PBMCs from children sensitized to HDM and ryegrass expressed increased Th2 cytokines after stimulation with either of the two allergens. In contrast, PBMCs from children sensitized only to ryegrass did not express increased levels after stimulation with either of the allergens. The expression of Th2 cytokines after in vitro stimulation of PBMCs from atopic children is specific to the sensitizing allergen, indicating that atopic status per se does not affect the type of T-cell response. In addition, T cells specific to seasonal allergens circulate in the blood out of season only if the child is concomitantly sensitized to a perennial allergen.


Heterogeneity in Diphtheria-Tetanus–Acellular Pertussis Vaccine–Specific Cellular Immunity during Infancy: Relationship to Variations in the Kinetics of Postnatal Maturation of Systemic Th1 Function

August 2001

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24 Reads

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133 Citations

The Journal of Infectious Diseases

Cellular immunity to vaccines is highly variable during infancy. This study addressed the hypothesis that these responses are governed by the pace of maturational changes in adaptive immune competence, in particular, cellular functions that underlie the postnatal transition from Th2 to Th1 “bias.” Tetanus-specific cytokine responses were tracked in peripheral blood mononuclear cells collected from infants at months 2, 4, 6, 12, and 18. These were compared with polyclonal responses. Results show that the Th2 component of the vaccine response develops rapidly and remains stable, unlike interferon (IFN)–γ production, which also is initiated early but commonly declines after the final priming dose at 6 months. However, between 12 and 18 months, the IFN-γ component of the vaccine-specific response has a spontaneous resurgence that coincides with a parallel increase in overall IFN-γ production capacity. The Th2 component of vaccine-specific responses was more prominent in children with atopic family history


In utero and neonatal concerns in allergy

June 2001

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13 Reads

Current Opinion in Otolaryngology & Head and Neck Surgery

The increase in asthma and allergic diseases in the past decades has particularly affected children, who develop symptoms at increasingly younger ages. Understanding early life events involved in the immune response to allergens is central to the development of new strategies for the management and eventually the prevention of atopic diseases. There is accumulating evidence that immune response to allergens may be initiated before birth. Maternal influence during pregnancy and environmental factors may all contribute in various degrees to shaping the initial fetal response to allergens in susceptible people.


Regulation of Cytokine Production in T-Cell Responses to Inhalant Allergen:GATA-3 Expression Distinguishesbetween Th1- and Th2-Polarized Immunity

January 2001

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5 Reads

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22 Citations

International Archives of Allergy and Immunology

The precise nature of allergen-specific cytokine responses in atopics versus non-atopics, in particular the 'Th1 polarity' of responses in non-atopics, remains controversial. This is due in part to the relative insensitivity of cytokine detection systems, and associated variations in kinetics of cytokine production and catabolism in in vitro culture systems. As an alternative to cytokine measurement, this study focuses on expression of the transcription factor GATA-3 for analysis of allergen-specific Th cell responses. Cord blood mononuclear cells were Th1- or Th2-polarized by culture in IL-12- or IL-4-employing established methods; PBMC from house dust mite (HDM)-sensitive atopics and controls were stimulated overnight with HDM; cytokine production was measured by ELISA and GATA-3 mRNA expression by PCR. Cytokine-driven Th2 polarization of naive T cells is associated with marked upregulation of GATA-3 expression, whereas a reciprocal expression pattern accompanies differentiation towards the Th1 cytokine phenotype. In T cells from HDM skin prick test-positive (HDM-SPT+/HDM-IgE+) volunteers, overnight stimulation results in marked upregulation of GATA-3 expression, compared to an equally marked downregulation of expression in T cells from SPT-/IgE- subjects. In subjects who are HDM-SPT+ but IgE-, GATA-3 expression levels remained relatively stable during culture with HDM. Upregulation of GATA-3 expression in PBMC is a hallmark of the early phase of Th2 recall responses to specific allergen in atopics. The reciprocal expression pattern observed in HDM-specific recall responses of non-atopics provides independent confirmation of the presence of underlying Th1-like immunity in these subjects. The parallel findings in neonatal T cells suggest that the same approach may be utilized for monitoring the progress of allergen-specific Th1/Th2 memory development during early childhood, and hence in assessment of risk for future allergic disease.



TT-specific cytokine production by PBMC. The data shown illustrate TT-specific cytokine responses in infants undergoing DTaP vaccination, as detailed in Materials and Methods. The results are presented as box plots. The limits of the boxes represent the 25th and 75th percentiles of the results. The enclosed line represents the median (50th percentile), and the bars represent the 10th and 90th percentiles. (A) The cytokine protein content of culture supernatants was assayed by ELISA and expressed as picograms per milliliter. (B) Cytokine-specific mRNA was determined by semiquantitative reverse transcription-PCR and is presented as a ratio relative to β-actin. The data are expressed as delta values (treatment minus control) from those positively responding to TT (a twofold increase above control production was defined as a positive cytokine response; percentages are shown in parentheses). The significance of differences between test and control cultures within the overall study population, and between the various sampling points, was determined using the Wilcoxon matched-pairs signed rank test for paired responses (∗, P < 0.05; ∗∗, P < 0.01; ∗∗∗, P < 0.0001).
PHA induction of cytokine production by PBMC. The data shown illustrate parallel PHA-induced cytokine responses in the PBMC samples used in the experiment in Fig. 1, as detailed in Materials and Methods. The results are presented for positive responders (the percentage of each age group that was positive is shown in parentheses) as box plots, as in Fig. 1. Differences between groups were analyzed as in Fig. 1.
Antigen-Specific Responses to Diphtheria-Tetanus-Acellular Pertussis Vaccine in Human Infants Are Initially Th2 Polarized
  • Article
  • Full-text available

July 2000

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44 Reads

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117 Citations

Immune responses to exogenous antigens in infant experimental animals display various degrees of Th2 polarization. Preliminary evidence from small human studies suggest a similar age-dependent response pattern to vaccines, but detailed investigations on vaccine immunity during infancy have not yet been undertaken. We report below the results of a comprehensive prospective study on responses to the tetanus component of the diphtheria, tetanus, acellular pertussis (DTaP) vaccine in a cohort of 55 healthy children, employing peripheral blood mononuclear cells (PBMC) collected at the 2-, 4-, and 6-month vaccinations and at 12 months. Antigen-specific production of interleukin-4 (IL-4), IL-5, IL-6, IL-9, IL-10, IL-13, and gamma interferon (IFN-γ) was determined at each sample point, in parallel with polyclonal (phytohemagglutinin PHA-induced) cytokine responses. Our results indicate early and persistent Th2 responses to the vaccine, in contrast to a more delayed and transient pattern of IFN-γ production. This initial disparity between the Th1 and Th2 components of the vaccine response was mirrored by patterns of polyclonally induced cytokine production, suggesting that the delayed maturation of the Th1 component of the vaccine response during infancy is secondary to developmental processes occurring within the overall Th cell system.

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Citations (26)


... However, at birth they have immunoglobulin G from the mother, which crosses through the placenta, and of course there is the secretory IgA from the breast milk. These passively transferred antibodies can protect newborns until 18 months of age, although their response is usually short and with low-affinity [19,20]. This is one of the reasons why most of the admitted patients are around two years of age. ...

Reference:

Total IgE Distribution in Food Allergy Suspected Patients in Republic of Macedonia (2001-2011)
Th-1/Th-2 Switch Regulation in Immune Responses to Inhaled Antigens
  • Citing Chapter
  • January 1997

Advances in Experimental Medicine and Biology

... In our study, pneumococcal serotype diversity and phenotype were associated with NTHi cocolonization among children 2–18 months old [4, 5]. Immune maturation over these ages reverses the neonatal CD4 + /CD8 + lymphocyte balances [33] amid changes in T-helper type 1 (Th1), Th2, and interferon γ profiles [34, 35]. CD4 + T-cell responses mediate immunity to pneumococcal and NTHi carriage [36][37][38] , and their diminishing prominence among older children may underlie the disappearance of species associations. ...

Antigen-specific responses to diphtherial-tetanus-acellular pertussis vaccine in human infants are initially Th2 polarised
  • Citing Article
  • January 2000

... For example, detectable levels of interleukin 4 and interferonγ in cord blood were associated with reduced incidences of asthma and atopy during childhood. 20 Increased expression of CCL22, which encodes a Th2-associated chemokine, in cord blood was found in neonates who later developed allergy. 21 The maternal environment and exposures during pregnancy affect the fetus through the placenta, which is a transient, fetal organ that works in close contact with maternal tissue. ...

Association between antenatal cytokine production and the development of atopy and asthma at age 6 years
  • Citing Article
  • October 2003

The Lancet

... Allergic diseases have a complex background where genetics, environmental factors, and timing play a role. Factors early in life and during the fetal period are thought to be important influences on the risk of sensitization later in life [4,5]. ...

TH2-polarized immunological memory to inhalant allergens in atopics is established during infancy and early childhood
  • Citing Article
  • November 1997

Clinical & Experimental Allergy

... La reactividad hacia alergenos específicos es evidente en la circulación periférica del feto hacia la semana 22 de la gestación (24). Se considera que la exposición y reacción primaria de la respuesta inmune puede iniciarse antes de ese momento. ...

Ciba Foundation Symposium 206 - The Rising Trends in Asthma
  • Citing Article
  • February 1997

Ciba Foundation symposium

... These result were consistent with the cohort study [10] which explained that the CD14-159C influential in the development of atopy in early childhood. CD14 has an important role in Th2 into Th1 response switch during fetal and early birth [11][12][13], this system failures which may be associated with the development of atopy in early life [14][15][16]. ...

Th-1/Th-2 switch regulation in immune responses to inhaled antigens. Role of dendritic cells in the aetiology of allergic respiratory disease
  • Citing Article
  • February 1997

Advances in Experimental Medicine and Biology

... [2] Atopic individuals have a persistent T-h2 response, which make them more vulnerable for pruritus and eczematization. [3][4][5] One small study was undertaken to see the benefit of oral Ketotifen and Vitamin D over conventional therapy in the management of PU. Ketotifen is a second-generation noncompetitive H 1 -antihistamine and mast cell stabilizer. ...

TH2-polarized immunological memory to inhalant allergens in atopics is established during infancy and early childhood
  • Citing Article
  • December 1997

Clinical & Experimental Allergy

... The observed difference did not apply to the older patients. That phenomenon possibly reflected the more severe impact of food allergy on child development in case of the early onset of allergy, which was also suggested in previous studies [9][10][11]. ...

Development of long term tolerance versus sensitisation to environmental allergens during the perinatal period
  • Citing Article
  • January 1998

Current Opinion in Immunology

... Allergen-specific IgE, allergen-specific lymphocytes, liver-resident dendritic cells, and sinusoidal endothelial cells were reported as sources of immune cells. Other possible mechanisms are the action of tacrolimus [9] and immature gastrointestinal and immune system [10]. Tacrolimus promotes Th2 responses to induce IgE secretion from B cells and increases intestinal permeability [9]. ...

Transplacental Priming of the Human Immune System to Environmental Allergens: Universal Skewing of Initial T Cell Responses Toward the Th2 Cytokine Profile

The Journal of Immunology