Análise das repetições CA do gene IGF1, VNTR do gene da insulina e região promotora P4 do gene IGF2 em indivíduos nascidos pequenos para idade gestacional / Analysis of the CA repeats of IGF1 gene, VNTR of insulin gene polymorphism and P4 Promoter region of IGF2 gene in children born small for gestational age

Rocio Riatto Della Coletta

22 February 2008

Introdução: Polimorfismos na região promotora dos genes da insulina, IGF2 e IGF1 podem estar relacionados a uma diminuição da expressão desses genes na vida fetal que, por sua vez, pode causar restrição do crescimento intra-uterino e maior risco de hipospádia. Na vida pós-natal, perda completa ou parcial da expressão desses genes pode resultar em ausência de recuperação estatural e menores concentrações séricas de IGF1 na criança, além de um maior risco de diabetes melito tipo 2 e síndrome de resistência à insulina no adulto. Objetivos: Analisar em crianças nascidas pequenas para idade gestacional (PIG) com ou sem recuperação estatural (RE): 1) a freqüência alélica e genotípica dos polimorfismos VNTR-INS e das repetições CA do gene IGF1; 2) a região promotora P4 do gene IGF2; 3) a influência do VNTR INS e das repetições CA do gene IGF1 na sensibilidade à insulina e nas concentrações séricas de IGF1, respectivamente. Pacientes: Foram estudados 142 indivíduos nascidos PIG com (n= 66) e sem recuperação (n= 76) estatural selecionados de três diferentes centros (HC-FMUSP, Santa Casa de São Paulo e HC-UFPR) e um grupo controle constituído de 297 indivíduos nascidos adequados para idade gestacional (AIG). Métodos: Extração de DNA genômico; amplificação por PCR das regiões contendo os polimorfismos VNTR INS e repetições CA do IGF1 e da região promotora P4; digestão por enzima de restrição; software Genescan; seqüenciamento automático; avaliação bioquímica e hormonal da glicemia, insulina e IGF1, extração de RNA, PCR em tempo real e análise estatística com SPSS 13.0 (Statistical Package fo Social Sciences). Resultados: A média do Z-altura, Z-IMC (índice de massa corpórea), Z-altura paterno e ZEA (estatura alvo) foram maiores nas crianças PIG que tiveram recuperação estatural, com o Z-PC (perímetro cefálico) maior nas crianças sem recuperação estatural. O Z-IGF1 sérico foi significantemente mais elevado em crianças que apresentaram RE (p<0,05). A distribuição e genotipica das repetições CA do gene IGF1 e do VNTR INS foi semelhante estatisticamente entre os grupos AIG e PIG, e entre os PIG com e sem RE; não foi observada associação entre esse polimorfismo e as variáveis clínicas e laboratoriais do estudo. O estudo da região promotora P4 do gene IGF2 identificou um novo polimorfismo de 9-12 repetições C na posição -1982, antes do sítio de início de transcrição do exon 2, e este apresentou distribuição semelhante entre os grupos PIG e AIG. Foi identificada também uma troca C/T em heterozigose no nono nucleotídeo do alelo 11C em quatro crianças nascidas PIG. Contudo, a quantificação da expressão do gene IGF2 em duas dessas crianças não demonstrou perda da expressão desse gene. Conclusões: Não observamos influência dos polimorfismos acima descritos no crescimento pré e pós-natal, na presença de resistência à insulina, nem em concentrações séricas de IGF1 dos indivíduos nascidos PIG. Identificamos uma nova variante na região promotora P4 do gene IGF2, contudo estudos preliminares não demonstraram influência desse polimorfismo sobre o crescimento intra-uterino. / Introduction: Polymorphisms in the promoter region of insulin (INS), IGF2 and IGF1 genes may decrease their expression during fetal life and afterward could be related to intra-uterine fetal growth retardation and greater risk of hypospadia development. In post-natal life, decreased expression of these genes can result in lack of stature recovery and in lower IGF1 serum levels in children, as well as in higher risk for type 2 diabetes mellitus and metabolic syndrome in adults. Objectives: The aims of the present study were: (1) to analyze the allelic and the genotypic frequency of the insulin (INS) gene variable number of tandem repeats (VNTR) and the IGF1 gene CA repeats; (2) to analyze the P4 promoter region of IGF2 gene (3) to test the contribution of INS VNTR, IGF1 gene CA repeats on insulin sensitivity and IGF1 serum levels in children born SGA with and without catch up, respectively. Patients: We studied 142 individuals born SGA with catch up (n = 66) and without catch up (n = 76) selected from three different centers (HCFMUSP, Santa Casa de Sao Paulo and HC-UFPR). The control group consisted of 297 children born appropriate for gestational age (AGA). Methods: Extraction of genomic DNA, PCR-amplification of the VNTR of insulin gene, CA repeats of IGF1 and IGF2 gene P4 promoter region; restriction analysis; Genescan software; automatic sequencing. Blood measurements of serum level of glucose, insulin and IGF1. Statistical analysis (Statistical Package for Social Sciences software). Results: Regarding birth parameters, the average of Z-height, Z-BMI (body mass index) and Z-height paternal and Z- EA (target height) were higher in children born SGA who had catch up. Interestingly, we observed that the Z-PC was higher in children born SGA without catch up. In addition, the Z-IGF1 serum levels were significantly higher in children who had catch up (p <0.05). The molecular analysis of IGF1 gene CA repeats and of INS gene VNTR locus did not show a statistically significant difference in the allelic and genotypic distribution of these polymorphisms between adequate for gestational age (AGA) and SGA groups nor between SGA with and without catch up. Similarly, we have not found an association of these polymorphisms with clinical or laboratory variables of this study. A novel polymorphism in the P4 promoter region of the IGF2 gene was identified. It was characterized by cytosine repeats (9-12) at position -1982 before transcription initiation site of exon 2 of IGF2 gene. Yet, we have identified a heterozygous substitution of cytosine for thymine at the nucleotide position 9 in the allele 11C in four children born SGA. This change was also absent in the control population. Quantization of IGF2 gene expression in two of these children did show loss of expression of this gene in patients carrying the variant 9C/T. Conclusions: We have not observed an association of the above described polymorphisms with pre and post natal growth, or with the occurrence of insulin resistance in individuals born SGA. IGF-1 levels did not seem to be associated with the polymorphisms either. A new variant in the P4 promoter region of IGF2 gene was identified, however preliminary studies showed no influence on intra-uterine growth.

Fator de crescimento insulin-like I

Fator de crescimento insulin-like II

Insulina

Resistência à insulina

Retardo do crescimento fetal

Fetal growth retardation

Infant small for gestational age

Insulin

Insulin resistance

Insulin- like growth factor II

Insulin-like growth factor I

Les méthodes de procréation médicale assistées et les risques adverses périnataux : l’impact du programme de remboursement universel du Québec.

Gorgui, Jessica

12 1900

L'infertilité affecte 11-15 % des Canadiennes et 8-20 % des couples ont de la difficulté à concevoir spontanément. Par conséquent, le recours à la procréation médicalement assistée (PMA) ne cesse d'augmenter, cependant la controverse demeure quant à ses risques sur la santé maternelle et celle des enfants. La PMA comprend les techniques de procréation assistée (TRA) (fécondation in vitro [FIV], insémination intra-utérine [IIU]) et les stimulateurs ovariens (SO), avec plus de 5 millions d'enfants issu d’une FIV au monde. La PMA a précédemment été associée à un risque accru d’issues adverses de grossesse incluant l’hypertension gestationnelle, les saignements utérins ainsi que les issues adverses affectant la santé de l’enfant, notamment les grossesses multiples, la prématurité, et le faible poids à la naissance sur lesquelles nous allons nous concentrer dans cette thèse de doctorat. Entre 05/08/2010-15/11/2015, le Québec fut la 1ère province Canadienne à financer un programme de remboursement universel pour la PMA, visant à augmenter le taux de natalité au Québec et réduire les grossesses multiples et leurs dépenses de santé associées en implémentant le transfert d'embryon unique. Le programme a été interrompu en 2015 dû aux dépenses de santé plus élevées que prévu. Nous avons identifié plusieurs lacunes de connaissances, que nous avons cherché à combler dans ce programme doctoral. Premièrement, aucun registre n’a été mis en place pour évaluer l'impact du programme sur les mères et les enfants. Deuxièmement, les études se concentrent sur les TRA ou combinent toutes les méthodes non-FIV, ce qui a des implications cliniques limitées. Les SO sont sous-analysées mais ont des implications cliniques importantes car ils constituent un traitement de première ligne pour l'infertilité. Enfin, les grossesses singleton sont moins évaluées alors qu’il est devenu évident qu'elles comportent des risques périnataux cliniquement importants. Cette thèse de doctorat est composée d'une revue de la littérature publiée et de trois études épidémiologiques effectuées dans la Cohorte des Grossesses du Québec (CQG). L'étude 1 quantifie les variations des tendances trimestrielles des issues obstétricales et périnatales 5 ans avant et pendant le programme québécois, et quantifie le risque de multiplicité associé au programme et à la PMA dans l’ensemble et par sous-types (SO seuls, TRA seuls, SO/TRA combinés) pendant ses années actives. Nous avons aussi étudié le rôle des grossesses multiples comme modificateur d'effet dans l'association entre la PMA et la prématurité. Entre 2005-2015, nous avons observé une augmentation de la prévalence de multiplicité par un facteur de 10. Les grossesses multiples ont augmenté significativement pendant le programme (rapport de cotes ajusté [RCa] 6,09, intervalle de confiance à 95 % [IC95%] 5,23-7,09) par rapport aux 5 ans avant. La PMA a significativement augmenté le risque de multiplicité (RCa 4,65, IC95% 3,84-5,62) par rapport à la conception spontanée. Les SO seuls augmentaient le plus le risque de multiplicité (RCa 6,28, IC95 % 4,56-8,64) par rapport à la conception spontanée. L’étude 2 quantifie le risque de prématurité associé à la PMA dans l'ensemble et par sous-type parmi les grossesses singleton survenues pendant le programme et dans une cohorte restreinte de grossesses PMA pour évaluer l'impact d’un biais d'indication (l’infertilité ou la sous-fertilité) potentiel. La PMA dans l’ensemble (RCa 1,46, IC95 % 1,25-1,72) et par sous-types : OS seul (RCa 1,47, IC95% 1,04-2,07), TRA seul (RCa 1,76, IC95% 1,01-3,06) et SO/TRA combinés (RCa 1,43, IC95% 1,19-1,73) étaient associées à un risque accru de prématurité par rapport à la conception spontanée. Enfin, l’étude 3 quantifie le risque de naitre petit/très petit pour l'âge gestationnel associé à la PMA dans l’ensemble et par sous-types. Connaissant l'association PMA/prématurité, nous avons aussi évalué le rôle de la prématurité comme modificateur d'effet dans l'association entre PMA et le fait de naitre petit ou très petit pour l'âge gestationnel. Bien qu'aucune association n'ait été observée entre la PMA et le fait de naitre petit ou très petit pour l'âge gestationnel, la PMA était associée à un risque accru de naitre petit ou très petit pour l'âge gestationnel (RCa 1,69, IC95 % 1,08-2,66) chez les prématurés spécifiquement. Nos résultats démontrent une augmentation significative des grossesses multiples pendant le programme, au-delà des seuils visés. Les SO seuls augmentent particulièrement les grossesses multiples, une technique de PMA ne pouvant être contrôlée par le transfert d’embryon unique. La PMA augmente le risque de prématurité, en particulier chez les singletons. Nos résultats confirment en outre qu’elle augmente également le risque de naitre petit pour l’âge gestationnel, en particulier chez singletons prématurés. / Infertility affects 11-15% of Canadian women, while 8-20% of couples report having difficulties conceiving spontaneously. As such, the use of medically assisted reproduction (MAR) has steadily increased, however controversy remains with regards to its risks on the health of mothers and children. MAR includes assisted reproductive technology (ART) (i.e. in vitro fertilization [IVF], intrauterine insemination [IUI]) and ovarian stimulators (OS), with over 5 million children born through IVF alone worldwide. MARs have previously been associated with an increased risk of adverse pregnancy outcomes including gestational hypertension, uterine bleeding as well as adverse child health outcomes including multiplicity, prematurity, and low birth weight. Perinatal outcomes will be the focus in this doctoral thesis. Between 05/08/2010-15/11/2015, Quebec was the first Canadian province to fund a universal MAR reimbursement program, which aimed to reduce multiplicity and associated health expenditures with the practice of single embryo transfers in the context of IVF and increase Quebec’s birth rate. The program was halted in 2015 following a higher than expected healthcare expenditure. We identified several knowledge gaps, which we have aimed to fill through this doctoral program. First, no database exists to assess the impact of Quebec’s universal MAR program on mothers and children. Second, evidence focuses on ART or combine all non-IVF (e.g. OS) methods together, which has limited clinical implications. OS are under analysed but carry clinical implications as they are a first line therapy for infertility. Lastly, singleton pregnancies are not always evaluated when it has become evident that they carry clinically relevant perinatal risks. This doctoral thesis is composed of a published literature review as well as three epidemiological studies conducted within the Quebec Pregnancy Cohort (QPC). Study 1 aimed to quantify the changes in quarterly trends of obstetrical and perinatal outcomes 5 years before and during the universal program in Quebec through an interrupted time series analysis, as well as quantify the risk of multiplicity in association with the program itself and MAR conceptions specifically during the active program years. In this first study we also aimed to evaluate the role of multiplicity as an effect modifier in the association between MAR conception and prematurity. Between 2005-2015, we observed a 10-fold increase in multiplicity. Multiplicity increased by 6-fold during the program (adjusted odds ratio [aOR] 6.09, 95% confidence interval [CI] 5.23-7.09) compared to 5 years prior. MAR significantly increased the risk of multiplicity by 4.7-fold (aOR 4.65, 95%CI 3.84-5.62) compared to spontaneous conception. OS alone increased the risk of multiplicity the most (aOR 6.28, 95%CI 4.56-8.64) compared to spontaneous conception. In Study 2, we quantified the risk of prematurity associated with MAR conceptions overall and by subtype (eg. OS alone, ART alone, OS/ART combined) among singleton pregnancies occurring during the program as well as in a restricted cohort of MAR-exposed pregnancies to evaluate the impact of indication (infertility/subfertility) bias. MAR conception was associated with an increased prematurity risk (aOR 1.46, 95%CI 1.25-1.72). All MAR types were associated with increased prematurity risk when compared to spontaneous conception: OS alone (aOR 1.47, 95%CI 1.04-2.07), ART alone (aOR 1.76, 95%CI 1.01-3.06), and OS/ART combined (aOR 1.43, 95%CI 1.19-1.73). Lastly, in Study 3, we aimed to quantify the risk of being born small/very small for gestational age (SGA, VSGA) associated with MAR overall and by subtype. In this study, knowing the MAR/prematurity association, we assessed the role of prematurity as an effect modifier in the association between MAR and SGA/VSGA. While no association was observed between MAR and SGA/VSGA, MAR was associated with an increased SGA risk (aOR 1.69, 95%CI 1.08-2.66) among preterms. Our findings show a significant increase of multiplicity during the program years, well above the thresholds targeted by the program administrators. OS alone particularly increases multiplicity the most, an MAR technique that cannot be controlled through single embryo transfer. MARs increase the risk of preterm, particularly among singleton pregnancies. Our results further confirm that they also increase the risk of SGA, specifically among preterm singleton pregnancies.

procréation médicale assistée

stimulants ovariens

fertilisation in vitro

prélèvement d'ovocytes

insémination intra-utérine

prématurité

petit poids à la naissance

multiplicité

Medically assisted reproduction

Ovarian stimulators

In vitro fertilisation

Egg harvesting

Intra-uterine insemination

Prematurity

Small for gestational age

Multiplicity

Estudo eletrofisiológico longitudinal da via auditiva em lactentes nascidos pequenos para a idade gestacional / Longitudinal electrophysiological study of the hearing pathway in small for gestational age infants

Angrisani, Rosanna Mariangela Giaffredo

13 December 2013

A adequação do peso ao nascimento é um fator de risco para atrasos de desenvolvimento. Dentre outras causas de morbidade e mortalidade, encontra-se a prematuridade e a Restrição de Crescimento Intrauterino (RCIU). O termo \"Pequeno para a Idade Gestacional\" (PIG) é utilizado muitas vezes, como indicador de RCIU, cujo feto pode ter sido submetido a agravos em diferentes momentos da gestação. A literatura aponta o PIG como risco para atraso no desenvolvimento neuropsicomotor, incluindo a linguagem. Objetivo: Acompanhar a maturação da via auditiva em lactentes nascidos PIG, comparando-os aos lactentes nascidos Adequados para Idade Gestacional (AIG) a termo e pré-termo, por meio do estudo das respostas do PEATE por estímulo click e tone burst (TB) nos seis primeiros meses de vida. Método: Estudo longitudinal, observacional de caráter multicêntrico. Foram avaliados 172 lactentes nascidos PIG e AIG, a termo e pré-termo, nos períodos neonatal, aos três e aos seis meses, por meio do PEATE com estímulo tipo click e tone burst em 0,5 kHz e 1 kHz, a 80dBnNA. Resultados: no período neonatal, os RN T/PIG não se diferenciaram dos RN T/AIG quanto às respostas do PEATE, o mesmo ocorrendo entre PT/PIG e PT/AIG. Ao se comparar o grupo T e PT/PIG, observou-se diferença entre as latências das ondas III, V e intervalos interpicos (Itpc) I-III e I-V, com latências maiores nos PT/PIG; não foram evidenciadas diferenças com TB nas frequências avaliadas. Na comparação do grupo T e PT/AIG, observou-se diferença entre as latências das ondas III, V e nos Itpc III-V e I-V e latências maiores nos PT/AIG. Não houve diferenças no TB nas frequências avaliadas. Aos três meses, não houve diferenças entre os T/PIG e T/AIG; na comparação PT/PIG e PT/AIG, houve diferenças no Itpc III-V, com latência menor no grupo PT/PIG. Não houve diferenças entre T/PIG e PT/PIG; o grupo AIG mostrou diferença entre T e PT nas latências da onda V e Itpc I-V. Na terceira coleta, aos seis meses, os T/PIG e T/AIG evidenciaram diferenças significativas entre as latências da onda III e Itpc I-III, o mesmo não ocorrendo quando se comparou PT/PIG e PT/AIG, os quais se diferenciaram somente no Itpc III-V. Ao se comparar T/PIG e PT/PIG, verificou-se diferenças relevantes somente no TB 0,5 kHz. Conclusão: Os achados do presente estudo permitiram concluir que o processo maturacional da via auditiva em lactentes nascidos PIG ocorre em diferente velocidade quando comparado ao de lactentes AIG; os PIG têm maturação acelerada, principalmente nos três primeiros meses, caracterizando desta forma um período de recuperação do ponto de vista da audição; a prematuridade influencia mais a maturação do sistema nervoso auditivo central que o fator peso ao nascer no período neonatal; a maturação ocorreu no sentido caudo-rostral nos dois grupos. O PEATE com TB em 0,5 kHz e em 1 kHz evidenciou o processo maturacional, porém não de modo tão detalhado quanto o fez com o estímulo tipo click. As crianças PIG devem ser monitoradas até pelo menos os três anos de idade / The appropriateness of weight at birth is a risk factor for developmental delays. Prematurity and intrauterine growth restriction (IUGR) are among other causes of morbidity and mortality. The term \"small for gestational age\" (SGA) is often used as an indicator of IUGR, when the fetus may have been subjected to restrictions at different periods of pregnancy. The literature points SGA as a risk for neuropsychological developmental delay, including language. Objective: to monitor the maturation of the auditory pathway in SGA infants, comparing to term and preterm appropriate for gestational age (AGA) infants, through the analysis of the ABR responses to click and tone burst stimulus in the first six months of life. Method: A longitudinal, observational and multicenter study was conducted. A total of 172 SGA and AGA infants, term and preterm, were evaluated in the neonatal period and at three and six months of age through the ABR with click and tone burst stimulus with 0.5 kHz and 1 kHz at 80dBHL. Results: in the neonatal period, the term SGA infants did not differ from term AGA infants for ABR responses. The same was observed between preterm SGA and preterm AGA infants. When comparing the term and preterm SGA groups, there was a difference between the latencies of waves III, V and interpeak intervals (lTPI) I-III and I-V, with longer latencies in preterm SGA; there were no differences with the tone burst stimuli in the analyzed frequencies. When comparing the AGA term and preterm groups, differences were observed on latencies of waves III, V and ITPI III-V and I-V, with longer latencies for preterm infants. There were no differences in the frequencies evaluated with the tone burst stimuli. At three months of age, there were no differences between the term SGA and AGA; when comparing preterm SGA and AGA, differences were found for ITPI III-V, with shorter latencies in preterm SGA. SGA term and preterm infants did not differ; there were differences between term and preterm AGA in latencies of wave V and ITPI I-V. In the third data collection, at six months of age, term SGA and AGA infants significantly differed on latencies of wave III and ITPI I-III, which did not occur when comparing preterm SGA and AGA infants, who differed only regarding ITPI III-V. Significant differences were only observed when comparing term and preterm SGA infants regarding the tone burst stimuli at 0.5 kHz. Conclusion: The findings of this study showed that the maturational process of the auditory pathway in SGA infants occurs at different speed when compared to AGA infants; SGA infants have accelerated maturation, especially in the first three months of age, thus characterizing a recovery period from the hearing standpoint; in the neonatal period, the maturation of the central auditory nervous system is more influenced by prematurity than birth weight; maturation occurred in caudo-rostral direction in the two groups. The ABR with tone burst at 0.5 kHz and 1 kHz evidenced maturational process, but not in such detail as with the click stimuli. The SGA infants should be monitored until at least three years of age

Audição

Estudos longitudinais

Evoked potentials auditory brain stem

Hearing

Hearing disorders

Infant

Infant newborn/growth e development

Infant premature/growth and development

Lactente

Longitudinal studies

Nascimento a termo

Prematuro/crescimento e desenvolvimento

Term birth

Transtornos da audição

Estudo eletrofisiológico longitudinal da via auditiva em lactentes nascidos pequenos para a idade gestacional / Longitudinal electrophysiological study of the hearing pathway in small for gestational age infants

Rosanna Mariangela Giaffredo Angrisani

13 December 2013

A adequação do peso ao nascimento é um fator de risco para atrasos de desenvolvimento. Dentre outras causas de morbidade e mortalidade, encontra-se a prematuridade e a Restrição de Crescimento Intrauterino (RCIU). O termo \"Pequeno para a Idade Gestacional\" (PIG) é utilizado muitas vezes, como indicador de RCIU, cujo feto pode ter sido submetido a agravos em diferentes momentos da gestação. A literatura aponta o PIG como risco para atraso no desenvolvimento neuropsicomotor, incluindo a linguagem. Objetivo: Acompanhar a maturação da via auditiva em lactentes nascidos PIG, comparando-os aos lactentes nascidos Adequados para Idade Gestacional (AIG) a termo e pré-termo, por meio do estudo das respostas do PEATE por estímulo click e tone burst (TB) nos seis primeiros meses de vida. Método: Estudo longitudinal, observacional de caráter multicêntrico. Foram avaliados 172 lactentes nascidos PIG e AIG, a termo e pré-termo, nos períodos neonatal, aos três e aos seis meses, por meio do PEATE com estímulo tipo click e tone burst em 0,5 kHz e 1 kHz, a 80dBnNA. Resultados: no período neonatal, os RN T/PIG não se diferenciaram dos RN T/AIG quanto às respostas do PEATE, o mesmo ocorrendo entre PT/PIG e PT/AIG. Ao se comparar o grupo T e PT/PIG, observou-se diferença entre as latências das ondas III, V e intervalos interpicos (Itpc) I-III e I-V, com latências maiores nos PT/PIG; não foram evidenciadas diferenças com TB nas frequências avaliadas. Na comparação do grupo T e PT/AIG, observou-se diferença entre as latências das ondas III, V e nos Itpc III-V e I-V e latências maiores nos PT/AIG. Não houve diferenças no TB nas frequências avaliadas. Aos três meses, não houve diferenças entre os T/PIG e T/AIG; na comparação PT/PIG e PT/AIG, houve diferenças no Itpc III-V, com latência menor no grupo PT/PIG. Não houve diferenças entre T/PIG e PT/PIG; o grupo AIG mostrou diferença entre T e PT nas latências da onda V e Itpc I-V. Na terceira coleta, aos seis meses, os T/PIG e T/AIG evidenciaram diferenças significativas entre as latências da onda III e Itpc I-III, o mesmo não ocorrendo quando se comparou PT/PIG e PT/AIG, os quais se diferenciaram somente no Itpc III-V. Ao se comparar T/PIG e PT/PIG, verificou-se diferenças relevantes somente no TB 0,5 kHz. Conclusão: Os achados do presente estudo permitiram concluir que o processo maturacional da via auditiva em lactentes nascidos PIG ocorre em diferente velocidade quando comparado ao de lactentes AIG; os PIG têm maturação acelerada, principalmente nos três primeiros meses, caracterizando desta forma um período de recuperação do ponto de vista da audição; a prematuridade influencia mais a maturação do sistema nervoso auditivo central que o fator peso ao nascer no período neonatal; a maturação ocorreu no sentido caudo-rostral nos dois grupos. O PEATE com TB em 0,5 kHz e em 1 kHz evidenciou o processo maturacional, porém não de modo tão detalhado quanto o fez com o estímulo tipo click. As crianças PIG devem ser monitoradas até pelo menos os três anos de idade / The appropriateness of weight at birth is a risk factor for developmental delays. Prematurity and intrauterine growth restriction (IUGR) are among other causes of morbidity and mortality. The term \"small for gestational age\" (SGA) is often used as an indicator of IUGR, when the fetus may have been subjected to restrictions at different periods of pregnancy. The literature points SGA as a risk for neuropsychological developmental delay, including language. Objective: to monitor the maturation of the auditory pathway in SGA infants, comparing to term and preterm appropriate for gestational age (AGA) infants, through the analysis of the ABR responses to click and tone burst stimulus in the first six months of life. Method: A longitudinal, observational and multicenter study was conducted. A total of 172 SGA and AGA infants, term and preterm, were evaluated in the neonatal period and at three and six months of age through the ABR with click and tone burst stimulus with 0.5 kHz and 1 kHz at 80dBHL. Results: in the neonatal period, the term SGA infants did not differ from term AGA infants for ABR responses. The same was observed between preterm SGA and preterm AGA infants. When comparing the term and preterm SGA groups, there was a difference between the latencies of waves III, V and interpeak intervals (lTPI) I-III and I-V, with longer latencies in preterm SGA; there were no differences with the tone burst stimuli in the analyzed frequencies. When comparing the AGA term and preterm groups, differences were observed on latencies of waves III, V and ITPI III-V and I-V, with longer latencies for preterm infants. There were no differences in the frequencies evaluated with the tone burst stimuli. At three months of age, there were no differences between the term SGA and AGA; when comparing preterm SGA and AGA, differences were found for ITPI III-V, with shorter latencies in preterm SGA. SGA term and preterm infants did not differ; there were differences between term and preterm AGA in latencies of wave V and ITPI I-V. In the third data collection, at six months of age, term SGA and AGA infants significantly differed on latencies of wave III and ITPI I-III, which did not occur when comparing preterm SGA and AGA infants, who differed only regarding ITPI III-V. Significant differences were only observed when comparing term and preterm SGA infants regarding the tone burst stimuli at 0.5 kHz. Conclusion: The findings of this study showed that the maturational process of the auditory pathway in SGA infants occurs at different speed when compared to AGA infants; SGA infants have accelerated maturation, especially in the first three months of age, thus characterizing a recovery period from the hearing standpoint; in the neonatal period, the maturation of the central auditory nervous system is more influenced by prematurity than birth weight; maturation occurred in caudo-rostral direction in the two groups. The ABR with tone burst at 0.5 kHz and 1 kHz evidenced maturational process, but not in such detail as with the click stimuli. The SGA infants should be monitored until at least three years of age

Audição

Estudos longitudinais

Lactente

Nascimento a termo

Prematuro/crescimento e desenvolvimento

Transtornos da audição

Evoked potentials auditory brain stem

Hearing

Hearing disorders

Infant

Infant newborn/growth e development

Infant premature/growth and development

Longitudinal studies

Term birth