Impact of perinatal different intrauterine environments on child growth and development in the first six months of life - IVAPSA birth cohort: rationale, design, and methods

Food intake estimate will be assessed by 24 h recall applied for both mother and child in different occasions and by an 88-itens Food Frequency Questionnaire (FFQ), validated for the pregnant women in Brazil [56]. The quantitative analysis of macronutrients and micronutrients consumed will be calculated with the use of NutriBase^® software (Versão NB7 Network) [Phoenix, AZ, USD].

Physical activity during pregnancy will be assessed by the International Physical Activity Questionnaire (IPAQ) short form. The items in the IPAQ short form were structured to provide separate scores on walking, moderate-intensity and vigorous-intensity activity [57]. This instrument is proposed by the World Health Organization (WHO) to determine physical activity levels, and was used in different studies having a good correlation with actual activity levels [58].

Anthropometric measurements will be measured in duplicate to ensure minimum inter- and intra-observer variability, and taken through the use of standard techniques and calibrated equipment.

Body weight of the mothers and infants will be measured in kilograms with a portable digital electronic scale (Marte^®) accurate to the nearest 50 g, wearing minimal clothing and without shoes. The infants will be weight in the arms of mothers, for the scale tare. The infant's weight will be then calculated by subtracting the total body weight of the mother from the weight of both mother and child.

Stature of mothers and infants will be measured with an extensible portable stadiometer (Alturexata^®). The infant's recumbent length will be measured in a supine position, placed on a flat, stable surface such as a table. The mother height will be measured using a height board mounted at a right angle between a level floor and against a straight, vertical surface such as a wall or pillar.

Weight in kilograms and height in meters when used to calculate body mass index (BMI). Body weight and a weight gain of the pregnant women will be reported from the charts. The gestational weight gain and prepregnancy BMI will be classified according to the recommendations of the Institute of Medicine [59]. The nutritional status of infants will be evaluated using age specific values of height, weight and BMI using the World Health Organization [60] growth chart.

Arm circumference, head and waist circumference will be measured with an inextensible tape measure. The arm circumference of mothers and infants will be measured always at the left arm at the medium point between the acromium and olecranum. Head circumference of infants will be measured at the largest occipitofrontal circumference. The waist circumference of mothers will be measured midway between the costal margin and iliac crest.

The subscapular and triceps skinfolds will be assessed using a caliper (Lange^®). In infants skinfold thickness will be measured starting at 3 months. Triceps skinfold of mothers and infants will be measured at the same levels as the arm circumference and subscapular skinfold will be measured and at the lower angle of the scapula, in the axis of the skin crease.

The arm and head circumference, subscapular and triceps skinfolds of infants will be evaluated using age specific using the World Health Organization [61] growth chart.

The women will be advised to wash their hands with soap and water before milking and washing their breasts with water [96, 97]. The collection procedure will be performed by the mothers, under appropriate supervision provided by the researcher. Milk was collected, under supervision, by manual expression directly into a plastic recipient. To express breast milk by hand mothers or researchers will be have to massage in the breast by starting at the top of the breast in circular manner with the C shape position. After collection, samples will be properly transported and stored at -80°C at the Translational Pediatrics Laboratory until analysis.

Fatty acids will be determined in phospholipids, triglyceride, and cholesterol ester fractions. Lipids will be extracted from serum with chloroform-methanol (2:1 by volume) according to the method of Folch et al., 1957 [98]. Fatty acid fractions will be separated by thin-layer chromatography using a silica gel plate and mobile-phase development, using a mixture of hexane, diethyl ether, and acetic acid glacial [99]. Fractions will be visualized by iodine vapor. Phospholipids, triglyceride, and cholesterol ester bands were scraped into separate tubes, and lipids were extracted from silica with chloroform-methanol and converted into fatty acid methyl esters by boron trifluoride catalysis [100]. The methyl esters will be then separated and measured by gas chromatography on specific capillary column. Analysis was performed on a Hewlett-Packard 6890 gas chromatograph equipped with a flame ionization detector. Helium will be used as carrier gas and nitrogen as make-up gas. The injection port temperature will be 200°C and the detector temperature 250°C. The column temperature will be held at 160°C for 5 min and increased to 190°C at a rate of 2°C/min; it was then held at this temperature for 2 min, and increased again to 220°C at a rate of 1°C/min. The identity of each fatty acid peak will be ascertained by comparison of peak retention time with a previously characterized mixture of 20 fatty acids. The relative amount of each fatty acid (% of total fatty acid) will be quantified by integrating the area under the peak and dividing the result by the total area for all fatty acids.

Total carbohydrates from milk will be determined by phenol-sulfuric acid assay, using the [101] method in a microplate format. Protein concentration will be quantified using bicinchoninic acid (BCA) protein assay. Milk leptin and corticosterone levels will be analyzed by ELISA using commercial kits.

The DNA will be extracted from saliva samples collected from mothers and their children at the postpartum interview using the Isohelix DNA Buccal Swabs^® (SK-2, Isohelix, United Kingdon). Mothers will be instructed to first rinse with 100 ml of distilled water and the collection is made by scraping the inner face of the cheeks with sterile cytological brushes, with circular movements repeated about 30 times. Then the brushes have their outer portion of the stems cut and placed in 2 ml microtubes. The samples will be stored in the refrigerator for a period of 2 to 30 days before extraction.

For the DNA extraction, 200 μl TES (10 mM Tris HCl, pH 7.6, 1 mM EDTA, 0.6% SDS) and 5 μl of proteinase K (10 mg/mL) are added to the tubes containing the swab and incubated for 2 h at 42 C. Then, the brush is removed and it is added 42 μl of saturated NaCl (6 M), stirring by hand with vigor. The sample will be centrifuged for 1 minute at 15,000 g, the supernatant transferred to a new tube and added 2 times the volume of absolute ethanol. The tubes are agitated and centrifuged for 1 minute at 15,000 g. The pure ethanol is discarded and will be added 1 ml of 70% ethanol by inverting the tubes several times to wash the pellet. Then tubes are centrifuged again for 1 minute at 15,000 g and the supernatant is discarded. Rinsing with 70% ethanol is repeated and, after discarding the supernatant, the tubes remain open for 30 minutes to evaporate residual ethanol. The DNA is dissolved in 60 μl TE 10:0,1 (10 mM Tris HCl, 0.1 mMEDTA).

Proopiomelanocortin gene (Pomc), Fat Mass- and Obesity-Associated gene (FTO, rs9939609 gene containing the risk A allele) and Dopamine receptor D4 gene (Drd4) expression will be measured by real-time quantitative reverse transcription-polymerase chain reaction (RT-PCR) using an inventoried TaqMan FAM/MGB assay (Applied Biosystems). Expression values will be normalized by GAPD endogenous control expression using a TaqMan VIC/MGB endogenous control inventoried assay (Applied Biosystems, 4352340E). Quantification will be carried out by Nanodrop. Reactions will be performed in ABI Prism 7500 sequence detection instrument, which directly detects the RT-PCR product without downstream processing. Reactions will be carried out in a total volume of 12 ml containing 6 ml of 2x TaqMan Gene Expression Master Mix (containing ROX, Amplitaq Gold DNA polimerase, AmpErase UNG, dATP, dCTP, dGTP, dUTP, and MgCl2), 0.6 ml of 20x TaqMan Gene Expression Assay, 0.6 ml of 20x TaqMan Endegenous Control, 3.8 ml of water and 1 ml of DNA solution. Cycling program consists of 2 min at 50°C and 10 min at 95°C, followed by 40 cycles of 15 s at 95°C and 1 min at 60°C. All reactions will be performed in triplicates. Relative expression levels will be determined by the ddCt method [101, 102].