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Volume 17, Issue 10 (October 2019)
IJRM 2019, 17(10): 763-770 |
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Żółkowska J, Hozyasz K. Low increase in phenylalanine tolerance during pregnancies in PKU woman with high prepregnancy BMI and postconceptional initiation of diet: A case report. IJRM 2019; 17 (10) :763-770
URL: http://ijrm.ir/article-1-1699-en.html
URL: http://ijrm.ir/article-1-1699-en.html
1- PKU Polyclinic, Institute of Mother and Child, Warsaw, Poland.
2- Institute of Health Sciences, State School of Higher Education, Biała Podlaska, Poland. , khozyasz@gmail.com
2- Institute of Health Sciences, State School of Higher Education, Biała Podlaska, Poland. , khozyasz@gmail.com
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1. Introduction
Classical phenylketonuria (PKU, OMIM 261600), caused by a deficiency of the biopterin-dependent cytosolic enzyme phenylalanine hydroxylase (PAH, EC 1.14.16.1), is the relatively frequent inborn error of metabolism. Over the last half century, population newborn screening has made PKU one of the most spectacular examples of diseases whose manifestations can be prophylactically managed via early intervention (1-3). In PKU, the essential aromatic amino acid phenylalanine (with the formula C9H11NO2, Phe), cannot be converted to 4-hydroxyphenylalanine (tyrosine) and therefore pathologically accumulates. Dietary intervention restricting Phe intake has converted PKU to a disease with essentially normal neurodevelopment and social integration (1-3). Phe tolerance (mg/day) is the amount of this amino acid in food that those with PKU can eat and maintain acceptable blood Phe levels. Clinical determination of Phe tolerance relies on the systematic assessment of blood Phe levels in relations to Phe intake from detailed menus provided by the patient. A protein substitute free of Phe, but nutritionally complete in all other amino acids, minerals, vitamins, and trace elements is an essential part of dietary management.
Pregnant women with PKU need appropriate management to avoid raised levels of Phe with teratogenic properties, leading to a host of birth defects, especially microcephaly and congenital heart disease (so-called maternal PKU syndrome) (2, 3). Therefore, having a pregnant patient with PKU is an important public health problem with direct impacts on the offspring’s health and quality of life (4). With that in mind, PKU women intending to get pregnant are advised to use a restricted low-Phe diet that starts at least 4 wk before conception to prevent teratogenic effects of increased Phe. However, the Phe intake should ensure the necessary amount of the amino acid needed to support the protein turnover for current body mass of mother and fetus/es. During pregnancy, the Phe tolerance may improve to some extent because of the increased fetal activity of PAH. It should be noted that there are limited pieces of evidence for the practical management of pregnant PKU patient (3, 5, 6). For example, the prediction of phenylalanine tolerance changes during the course of pregnancy is not clear.
The purpose of this case report is to describe phenylketonuric woman with a very low increase of Phe tolerance during pregnancies.
2. Case Presentation
A Caucasian patient of Polish origin was diagnosed with classical PKU at one month of age and remained on phenylalanine-restricted diet until the age of 17 years (IQ 105), however, her metabolic control during adolescence was not fully satisfactory. She became a food technologist. The patient has had two pregnancies and did not follow phenylalanine-restricted diet prior to the conception in both and the cases; her whole blood phenylalanine concentrations on normal diet were above 1,200 µmol/L. She returned to dietary phenylalanine restriction when she was almost five wk pregnant and worked with a metabolic dietitian (J.Ż.) to stabilize blood Phe levels. Dietary treatment included supplements and nutritional mixtures specifically devised for pregnant PKU patients (Table I), which were taken in 3-5 doses per day. Whole blood Phe concentration has been measured using the tandem mass spectrometer technique (Ms/Ms) at least twice a week and a target range of phenylalanine of 120-360 µmol/L was applied. If the blood Phe concentration remained above acceptable range, Phe intake was slowly decreased. The Phe intake was increased without delay if the blood Phe concentration was ≤ 120 µml/L (3). The Phe tolerance was empirically determined based on the analysis of fluctuations of the patient’s blood Phe concentration in relation to dietary Phe intake. Apart from the metabolic physicians and dietary care, the pregnancies were managed in the normal way by the obstetricians. It should be noted that the patient’s prepregnancy BMI was high (Table I). Moreover, her mean total weight gain for pregnancies was 14.5 kg.
There were no obstetric complications throughout the pregnancies and the babies were born by normal delivery, see Table II for birth measurements. None of the infants had PKU or any degree of persistent hyperphenylalaninemia. The neurodevelopment of offspring was normal over a follow-up periods of at least three years.
During the courses of the first and second pregnancies, the Phe tolerance increased 3.9- and 2.3-times, respectively (Table III). Table I and Figures 1 and 2 show what might not be considered as “satisfactory” metabolic control throughout pregnancies since a huge number of assessments of phenylalanine concentration was above the target range. Tables IV and V present a puzzling picture of the lack of association between maternal weight gain, as well as fetal weight gain, and the phenylalanine tolerance changes.
_97-112/Table_1.jpg)
_97-112/Table_2.jpg)
_97-112/Table_3.jpg)
_97-112/Table_4.jpg)
_97-112/Table_5.jpg)
_97-112/Figure_1.jpg)
_97-112/Figure_2.jpg)
Ethical consideration
The patient had given a written consent before participating in the program of care for pregnant PKU patients developed by the Polish PKU Consensus.
3.Discussion
Poor reproductive outcome is observed in PKU women when dietary treatment is started late or when blood Phe levels remain elevated. Hyperphenylalaninemia in women may affect amino acid composition of uterine fluid (7). Maillot and colleagues (5) demonstrated that the proportion of time when the Phe concentrations in blood are within the target range is greater in pregnant PKU patients who started diet preconceptionally than postconceptionally. Ideally, all PKU patients wishing to become pregnant should do so in a planned way. Unfortunately, both pregnancies in our patient were unplanned. In Poland, in the general population, a high number of conceptions is unplanned (8, 9).
It has been demonstrated that after unsatisfied pregnancy dietary treatment, infants have commonly smaller anthropometric measurements at birth as well as impaired subsequent cognitive development (2, 3, 5). In our case, the high number of Phe assessments above 360 µmol/L was mostly not caused by a lack of patient’s compliance and we observed normal neurodevelopment of patient’s offspring. The Phe blood levels exceeded the desirable upper limit in spite of a low Phe intake similar to the case of PKU mother with PKU-affected fetus described by Kohlschütter and colleagues (10).
We suspect that the patient’s low Phe tolerance might be related to her sever PKU phenotype (11) and the high prepregnancy BMI, as well as the high BMI during the course of pregnancies. Early body fat percentage strongly influence maternal and fetal health (12). In the study by MacLeod and colleagues (13), efforts to increase and maintain lean weight seem to increase the Phe tolerance in adult (non-pregnant) PKU patients. However, to our knowledge, there have been no studies indicating an effect of high preconceptional BMI and high BMI during the course of pregnancy on the limitation of Phe tolerance increase.
In the present case, good metabolic control was not achieved even in late pregnancy, time when increased phenylalanine requirement is expected due to the fetal growth and its phenylalanine hydroxylase activity in developing liver tissue (3, 6, 10, 14, 15). There was no impacting increase of Phe tolerance expressed as mg/kg of pregnant woman’s body weight (b.w.) in both the pregnancies of our patient. In 1988, Hyánek and colleagues (15) reported mean increase of Phe tolerance 3 mg/kg b.w. (26%) during the last three months of pregnancy in a group of five women with PKU (six pregnancies), who returned to a low phenylalanine diet from the 5th or 6th month of pregnancy. The Phe tolerances in the first, second, and third trimesters of three PKU women (diet before conception, six and eight wk gestation) from the New England Maternal PKU Project were 450 mg (10 mg/kg b.w.), 720 mg (14 mg/kg b.w.), 1,300 mg (24 mg/kg b.w.); 800 mg (9mg/kg b.w.), 1,000 mg (14 mg/kg b.w.) 1,400 mg (14 mg/kg b.w.), and 675 mg (11 mg/kg b.w.), 1,300 mg (19 mg/kg b.w.), 1,500 mg (19 mg/kg b.w.), respectively (16). In one case, where the dietary treatment started 10 wk before conception, Thompson and colleagues (17) showed an increase of Phe tolerance from 6 mg/kg b.w. up to 30 mg/kg b.w. In our previous study, in two singleton pregnancies of PKU women (PKU genotypes: p.Q383X/p.R408W and p.R281L/p.R408W) on diet initiated preconceptionally, the mean Phe tolerance increased 12.1 mg/kg (172%) from 14 gestation wk to the pre-delivery week (18). Interestingly, the American College of Medical Genetics Guidelines on PKU (ACMG Practice Guidelines) recommended relatively high Phe intake for pregnant phenylketonurics: 265-770 mg in trimester 1, 400-1650 mg in trimester 2, and 700-2275 in trimester 3 (2), although based on the study of 23 pregnant patients with good metabolic control, Acosta et al. (19) provided data on the mean Phe tolerance in trimesters 1, 2, and 3 of 609 ± 220mg, 824 ± 411mg, and 1248 ± 513mg, respectively. The PKU patient (p.R408W/p.R261Q) reported by Duran and colleagues (20), who began the Phe-restricted diet at 13 wk of gestation had Phe tolerance of 300 mg in the second trimester. In two PKU patients (PKU genotypes: p.194del/p.P281L and p.165T/p.R408W) described by Kohlschütter and colleagues (10) in trimester 3, the Phe tolerance increased 900 mg (100%) and 500 mg (50%), respectively. Interestingly, in a pregnancy of the patient with the genotype p.R408W/p.R261Q with a fetus homozygous for PKU (genotype: p.R408W/p.R408W), the Phe tolerance increase was approximately 200 mg in trimester 3, and during the course of whole pregnancy, the Phe intake could not be increased above 400-500 mg/day without risking high Phe blood concentrations (10), which was majorly below the lowest recommended value of Phe intake for trimester 3 as per the ACMG Practice Guidelines (2). In the European guidelines on PKU (3), there is a suggestion based on the Kohlschütter and colleagues study (10) that” a low Phe tolerance in the third trimester of (treated) pregnancy may indicate foetal PKU.” Levy and colleagues (21) compared sibs with or without PKU from untreated pregnancies in phenylketonuric mother and observed no effect of the fetal genetic PKU status on maternal metabolic control as well as offspring outcomes. We would like to stress that described PKU woman gave birth to two healthy children and the Phe intake could not be increased above 470 mg/day in both the pregnancies; the increase in the Phe tolerance in the third trimester was below 200 mg. In the patient presented by us, the late third trimester Phe tolerance in the second pregnancy was 15% lower compared to the first pregnancy. It is known that the Phe tolerance may vary highly even between pregnancies in the same patient (3). Hyánek and colleagues (15) reported the Phe tolerance in two pregnancies of a PKU patient before conception and during the 5th, 6th, 8th, and 9th month of pregnancy: 10.0, 11.0, 13.0, 15.0, 15.5 mg/kg b.w. and 6.8, 7.8, 9.0, 10.0, 11.0 mg/kg b.w., respectively.
Conclusion
In conclusion, both the pregnancies of the presented PKU patient were difficult to manage because the expected increase of Phe tolerance did not take place. This case report does not confirm the observation that a lack of impacting Phe tolerance increase in pregnancy is a marker of fetal PKU affection.
Conflict of Interest
The authors deny any conflict of interest related to this study.
Classical phenylketonuria (PKU, OMIM 261600), caused by a deficiency of the biopterin-dependent cytosolic enzyme phenylalanine hydroxylase (PAH, EC 1.14.16.1), is the relatively frequent inborn error of metabolism. Over the last half century, population newborn screening has made PKU one of the most spectacular examples of diseases whose manifestations can be prophylactically managed via early intervention (1-3). In PKU, the essential aromatic amino acid phenylalanine (with the formula C9H11NO2, Phe), cannot be converted to 4-hydroxyphenylalanine (tyrosine) and therefore pathologically accumulates. Dietary intervention restricting Phe intake has converted PKU to a disease with essentially normal neurodevelopment and social integration (1-3). Phe tolerance (mg/day) is the amount of this amino acid in food that those with PKU can eat and maintain acceptable blood Phe levels. Clinical determination of Phe tolerance relies on the systematic assessment of blood Phe levels in relations to Phe intake from detailed menus provided by the patient. A protein substitute free of Phe, but nutritionally complete in all other amino acids, minerals, vitamins, and trace elements is an essential part of dietary management.
Pregnant women with PKU need appropriate management to avoid raised levels of Phe with teratogenic properties, leading to a host of birth defects, especially microcephaly and congenital heart disease (so-called maternal PKU syndrome) (2, 3). Therefore, having a pregnant patient with PKU is an important public health problem with direct impacts on the offspring’s health and quality of life (4). With that in mind, PKU women intending to get pregnant are advised to use a restricted low-Phe diet that starts at least 4 wk before conception to prevent teratogenic effects of increased Phe. However, the Phe intake should ensure the necessary amount of the amino acid needed to support the protein turnover for current body mass of mother and fetus/es. During pregnancy, the Phe tolerance may improve to some extent because of the increased fetal activity of PAH. It should be noted that there are limited pieces of evidence for the practical management of pregnant PKU patient (3, 5, 6). For example, the prediction of phenylalanine tolerance changes during the course of pregnancy is not clear.
The purpose of this case report is to describe phenylketonuric woman with a very low increase of Phe tolerance during pregnancies.
2. Case Presentation
A Caucasian patient of Polish origin was diagnosed with classical PKU at one month of age and remained on phenylalanine-restricted diet until the age of 17 years (IQ 105), however, her metabolic control during adolescence was not fully satisfactory. She became a food technologist. The patient has had two pregnancies and did not follow phenylalanine-restricted diet prior to the conception in both and the cases; her whole blood phenylalanine concentrations on normal diet were above 1,200 µmol/L. She returned to dietary phenylalanine restriction when she was almost five wk pregnant and worked with a metabolic dietitian (J.Ż.) to stabilize blood Phe levels. Dietary treatment included supplements and nutritional mixtures specifically devised for pregnant PKU patients (Table I), which were taken in 3-5 doses per day. Whole blood Phe concentration has been measured using the tandem mass spectrometer technique (Ms/Ms) at least twice a week and a target range of phenylalanine of 120-360 µmol/L was applied. If the blood Phe concentration remained above acceptable range, Phe intake was slowly decreased. The Phe intake was increased without delay if the blood Phe concentration was ≤ 120 µml/L (3). The Phe tolerance was empirically determined based on the analysis of fluctuations of the patient’s blood Phe concentration in relation to dietary Phe intake. Apart from the metabolic physicians and dietary care, the pregnancies were managed in the normal way by the obstetricians. It should be noted that the patient’s prepregnancy BMI was high (Table I). Moreover, her mean total weight gain for pregnancies was 14.5 kg.
There were no obstetric complications throughout the pregnancies and the babies were born by normal delivery, see Table II for birth measurements. None of the infants had PKU or any degree of persistent hyperphenylalaninemia. The neurodevelopment of offspring was normal over a follow-up periods of at least three years.
During the courses of the first and second pregnancies, the Phe tolerance increased 3.9- and 2.3-times, respectively (Table III). Table I and Figures 1 and 2 show what might not be considered as “satisfactory” metabolic control throughout pregnancies since a huge number of assessments of phenylalanine concentration was above the target range. Tables IV and V present a puzzling picture of the lack of association between maternal weight gain, as well as fetal weight gain, and the phenylalanine tolerance changes.
Ethical consideration
The patient had given a written consent before participating in the program of care for pregnant PKU patients developed by the Polish PKU Consensus.
3.Discussion
Poor reproductive outcome is observed in PKU women when dietary treatment is started late or when blood Phe levels remain elevated. Hyperphenylalaninemia in women may affect amino acid composition of uterine fluid (7). Maillot and colleagues (5) demonstrated that the proportion of time when the Phe concentrations in blood are within the target range is greater in pregnant PKU patients who started diet preconceptionally than postconceptionally. Ideally, all PKU patients wishing to become pregnant should do so in a planned way. Unfortunately, both pregnancies in our patient were unplanned. In Poland, in the general population, a high number of conceptions is unplanned (8, 9).
It has been demonstrated that after unsatisfied pregnancy dietary treatment, infants have commonly smaller anthropometric measurements at birth as well as impaired subsequent cognitive development (2, 3, 5). In our case, the high number of Phe assessments above 360 µmol/L was mostly not caused by a lack of patient’s compliance and we observed normal neurodevelopment of patient’s offspring. The Phe blood levels exceeded the desirable upper limit in spite of a low Phe intake similar to the case of PKU mother with PKU-affected fetus described by Kohlschütter and colleagues (10).
We suspect that the patient’s low Phe tolerance might be related to her sever PKU phenotype (11) and the high prepregnancy BMI, as well as the high BMI during the course of pregnancies. Early body fat percentage strongly influence maternal and fetal health (12). In the study by MacLeod and colleagues (13), efforts to increase and maintain lean weight seem to increase the Phe tolerance in adult (non-pregnant) PKU patients. However, to our knowledge, there have been no studies indicating an effect of high preconceptional BMI and high BMI during the course of pregnancy on the limitation of Phe tolerance increase.
In the present case, good metabolic control was not achieved even in late pregnancy, time when increased phenylalanine requirement is expected due to the fetal growth and its phenylalanine hydroxylase activity in developing liver tissue (3, 6, 10, 14, 15). There was no impacting increase of Phe tolerance expressed as mg/kg of pregnant woman’s body weight (b.w.) in both the pregnancies of our patient. In 1988, Hyánek and colleagues (15) reported mean increase of Phe tolerance 3 mg/kg b.w. (26%) during the last three months of pregnancy in a group of five women with PKU (six pregnancies), who returned to a low phenylalanine diet from the 5th or 6th month of pregnancy. The Phe tolerances in the first, second, and third trimesters of three PKU women (diet before conception, six and eight wk gestation) from the New England Maternal PKU Project were 450 mg (10 mg/kg b.w.), 720 mg (14 mg/kg b.w.), 1,300 mg (24 mg/kg b.w.); 800 mg (9mg/kg b.w.), 1,000 mg (14 mg/kg b.w.) 1,400 mg (14 mg/kg b.w.), and 675 mg (11 mg/kg b.w.), 1,300 mg (19 mg/kg b.w.), 1,500 mg (19 mg/kg b.w.), respectively (16). In one case, where the dietary treatment started 10 wk before conception, Thompson and colleagues (17) showed an increase of Phe tolerance from 6 mg/kg b.w. up to 30 mg/kg b.w. In our previous study, in two singleton pregnancies of PKU women (PKU genotypes: p.Q383X/p.R408W and p.R281L/p.R408W) on diet initiated preconceptionally, the mean Phe tolerance increased 12.1 mg/kg (172%) from 14 gestation wk to the pre-delivery week (18). Interestingly, the American College of Medical Genetics Guidelines on PKU (ACMG Practice Guidelines) recommended relatively high Phe intake for pregnant phenylketonurics: 265-770 mg in trimester 1, 400-1650 mg in trimester 2, and 700-2275 in trimester 3 (2), although based on the study of 23 pregnant patients with good metabolic control, Acosta et al. (19) provided data on the mean Phe tolerance in trimesters 1, 2, and 3 of 609 ± 220mg, 824 ± 411mg, and 1248 ± 513mg, respectively. The PKU patient (p.R408W/p.R261Q) reported by Duran and colleagues (20), who began the Phe-restricted diet at 13 wk of gestation had Phe tolerance of 300 mg in the second trimester. In two PKU patients (PKU genotypes: p.194del/p.P281L and p.165T/p.R408W) described by Kohlschütter and colleagues (10) in trimester 3, the Phe tolerance increased 900 mg (100%) and 500 mg (50%), respectively. Interestingly, in a pregnancy of the patient with the genotype p.R408W/p.R261Q with a fetus homozygous for PKU (genotype: p.R408W/p.R408W), the Phe tolerance increase was approximately 200 mg in trimester 3, and during the course of whole pregnancy, the Phe intake could not be increased above 400-500 mg/day without risking high Phe blood concentrations (10), which was majorly below the lowest recommended value of Phe intake for trimester 3 as per the ACMG Practice Guidelines (2). In the European guidelines on PKU (3), there is a suggestion based on the Kohlschütter and colleagues study (10) that” a low Phe tolerance in the third trimester of (treated) pregnancy may indicate foetal PKU.” Levy and colleagues (21) compared sibs with or without PKU from untreated pregnancies in phenylketonuric mother and observed no effect of the fetal genetic PKU status on maternal metabolic control as well as offspring outcomes. We would like to stress that described PKU woman gave birth to two healthy children and the Phe intake could not be increased above 470 mg/day in both the pregnancies; the increase in the Phe tolerance in the third trimester was below 200 mg. In the patient presented by us, the late third trimester Phe tolerance in the second pregnancy was 15% lower compared to the first pregnancy. It is known that the Phe tolerance may vary highly even between pregnancies in the same patient (3). Hyánek and colleagues (15) reported the Phe tolerance in two pregnancies of a PKU patient before conception and during the 5th, 6th, 8th, and 9th month of pregnancy: 10.0, 11.0, 13.0, 15.0, 15.5 mg/kg b.w. and 6.8, 7.8, 9.0, 10.0, 11.0 mg/kg b.w., respectively.
Conclusion
In conclusion, both the pregnancies of the presented PKU patient were difficult to manage because the expected increase of Phe tolerance did not take place. This case report does not confirm the observation that a lack of impacting Phe tolerance increase in pregnancy is a marker of fetal PKU affection.
Conflict of Interest
The authors deny any conflict of interest related to this study.
Type of Study: Case Report |
References
1. Morovatdar N, Badiee Aval S, Hosseini Yazdi SMR, Norouzi F, Mina T. The epidemiological and clinical study of phenylketonuria (PKU) patients in Khorasan, North-eastern Iran. Iranian Journal of Neonatology 2015; 6: 18-22
2. Vockley J, Andersson HC, Antshel KM, Braverman NE, Burton BK, Frazier DM, et al. Phenylalanine hydroxylase deficiency: diagnosis and management guideline. Genet Med 2014; 16: 188-200. [DOI:10.1038/gim.2013.157] [PMID]
3. Van Wegberg AMJ, MacDonald A, Ahring K, Belanger-Quintana A, Blau N, Bosch AM, et al. The complete European guidelines on phenylketonuria: diagnosis and treatment. Orphanet J Rare Dis 2017; 12: 162. [DOI:10.1186/s13023-017-0685-2] [PMID] [PMCID]
4. Resta R. Generation n+1: Projected numbers of babies born to women with PKU compared to babies with PKU in the United States in 2009. Am J Med Genet 2012; 158A: 1118-1123. [DOI:10.1002/ajmg.a.35312] [PMID]
5. Maillot F, Lilburn M, Baudin J, Morley DW, Lee PJ. Factors influencing outcomes in the offspring of mothers with phenylketonuria during pregnancy: the importance of variation in maternal blood phenylalanine. Am J Clin Nutr 2008; 88: 700-705. [DOI:10.1093/ajcn/88.3.700] [PMID]
6. Żółkowska J, Hozyasz KK, Nowacka M. Prevention of maternal phenylketonuria syndrome. Dietary management in the preconception period and during pregnancy. Pediatr Med Rodz 2018; 14: 47-53. [DOI:10.15557/PiMR.2018.0004]
7. Kermack AJ, Finn-Sell S, Cheong YC, Brook N, Eckert JJ, Macklon NS, et al. Amino acid composition of human uterine fluid: association with age, lifestyle and gynaecological pathology. Hum Reprod 2015; 30: 917-924. [DOI:10.1093/humrep/dev008] [PMID] [PMCID]
8. Kurzawińska G, Magiełda J, Romała A, Bartkowiak-Wieczorek J, Barlik M, Drews K, et al. Demographic factors determining folic acid supplementation in pregnant and childbearing age women. Ginekol Pol 2018; 89: 211-216. [DOI:10.5603/GP.a2018.0036] [PMID]
9. Karwowska P, Gryko W. Health 2020 and action plan for public health - new understanding of public health. Health Prob Civil 2017; 11: 5-9. [DOI:10.5114/hpc.2017.65523]
10. Kohlschütter B, Ellerbrok M, Merkel M, Tchirikov M, Zschocke J, Santer R, et al. Phenylalanine tolerance in three phenylketonuric women pregnant with fetuses of different genetic PKU status. J Inherit Metab Dis 2009; 32 (Suppl.): S1-S4. [DOI:10.1007/s10545-008-0910-1] [PMID]
11. Guldberg P1, Rey F, Zschocke J, Romano V, François B, Michiels L, et al. A european multicenter study of phenylalanine deficiency: classification of 105 mutations and a general system for genotype-based prediction of metabolic phenotype. Am J Hum Genet 1998; 63: 71-79. [DOI:10.1086/301920] [PMID] [PMCID]
12. Sween LK, Althouse AD, Roberts JM. Early-pregnancy percent body fat in relations to preeclampsia risk in obese women. Am J Obstet Gynecol 2015; 212: 84. e1-e7. [DOI:10.1016/j.ajog.2014.07.055] [PMID]
13. MacLeod EL, Gleason ST, van Calcar SC, Ney DM. Reassessment of phenylalanine tolerance in adults with phenylketonuria is needed as body mass changes. Mol Genet Metab 2009; 98: 331-337. [DOI:10.1016/j.ymgme.2009.07.016] [PMID] [PMCID]
14. Delvalle JA, Greengard O. Phenylalanine hydroxylase and tyrosine aminotransferase in human fetal and adult liver. Pediatr Res 1977; 11: 2-5. [DOI:10.1203/00006450-197711010-00002] [PMID]
15. Hyánek J, Viletová H, Soukup J, Kobilková J, Kubik M, Kunová V. Changes in phenylalanine tolerance while monitoring the dietetic treatment of pregnant women suffering from hyperphenylalaninaemia. J Inherit Metab Dis 1988; 11: 427-428. [DOI:10.1007/BF01800434] [PMID]
16. Rohr FJ, Doherty LB, Waisbren SE, Bailey IV, Ampola MG, Benacerraf B, et al. New england maternal pku project: prospective study of untreated and treated pregnancies and their outcomes. J Pediatr 1987; 110: 391-398. [DOI:10.1016/S0022-3476(87)80500-0]
17. Thompson GN, Francis DE, Kirby DM, Compton R. Pregnancy in phenylketonuria: dietary treatment aimed at normalizing maternal plasma phenylalanine concentration. Arch Dis Child 1991; 66: 1346-1349. [DOI:10.1136/adc.66.11.1346] [PMID] [PMCID]
18. Żółkowska J, Hozyasz KK, Nowacka M. Singleton and twin pregnancies of PKU patients - individual variability of phenylalanine tolerance: Experience of a single treatment center (preliminary report). Dev Period Med 2017; 21: 344-360.
19. Acosta PB, Matalon K, Castiglioni L, Rohr FJ, Wenz E, Austin V, Azen C. Intake of major nutrients by women in the Maternal Phenylketonuria (MPKU) Study and effects on plasma phenylalanine concentrations. Am J Clin Nutr 2001; 73: 792-796. [DOI:10.1093/ajcn/73.4.792] [PMID]
20. Duran GP, Rohr FJ, Slonim A, Güttler F, Levy HL. Necessity of complete intake of phenylalanine-free amino acid mixture for metabolic control of phenylketonuria. J Am Diet Assoc 1999; 99: 1559-1563. [DOI:10.1016/S0002-8223(99)00382-X]
21. Levy HL, Lobbregt D, Sansaricq C, Snyderman SE. Comparison of phenylketonuric and nonphenylketonuric sibs from untreated pregnancies in a mother with phenylketonuria. Am J Med Genet 1992; 44: 439-442. [DOI:10.1002/ajmg.1320440411] [PMID]
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