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Learning About Your DNA and Childbearing
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Subsections on this page:
Resources
Please consider privacy issues if you're planning
to have your DNA analyzed. I recommend organizing a group
purchase of kits so that it's hard to know who got which kit
and then registering the kits through an anonymous email
address. Or you might ask your midwife to serve as an
anonymizing intermediary.
MTHFR and
your Pregnancy - This is an excellent presentation of the
issues
What
Is MTHFR...in simple terms! with Dr. Eric Berg DC - Really
great video that breaks the MTHFR mutation down into understandable
terms.
Folic
Acid vs Folate — What's the Difference?
Folic acid is completely man-made whereas folate is a natural
nutrient from food primarily greens. Some manufacturers of vitamins
for example will label folate and then after the word folate state
that it is indeed folic acid. in this instance it is folic acid, not
natural folate, and they are using folate as an all-encompassing
term.
Foods that are processed such as breads, pasta, cookies just to name
a few are going to have folic acid added to them. If you read a
label and it says folate only, and there is nowhere in the
ingredients list what type of folate it is you can contact the
company to verify what they are using in their product. Another way
to tell if folic acid is in it is if it says enriched.
Doctors are prescribing folic acid and even EXTRA folic acid as a
solution to this mutation.
RULE # 1 of the mutation is NEVER ingest folic acid. NEVER! It is
like poison to us. If your doctor prescribed you folic acid knowing
that the gene is specifically responsible for breaking down folic
acid (as this is basic genetics 101), knowing the mutation creates a
deficiency in the ability to convert folic acid to methylfolate,
they are an idiot. That is all.
If you have methylation issues or don't know your methylation
status, it's particularly important during pregnancy to make sure
that you're getting the bioactive forms of supplements. In
addition, it's important to avoid the inactive forms because they
can block receptors for many days. Be warned that many
processed foods, including mainstream breads, are supplemented with
inactive folic acid, sometimes also called folate.
As a general recommendation for most women, good prenatal vitamins
with bioactive forms of B9 (folate) and B12 are available from Thorne
(Basic Prenatal). Their Vitamin B6 is provided as pyridoxal
5-phosphate, the bioactive form of B6, instead of the more common
Pyridoxine HCl form which sometimes cannot be converted into P-5-P
in cases of nutritional inadequacies, certain medications,
compromised liver function, and enzyme defects.
I used to recommend the Metagenics (Wellness
Essentials® Pregnancy or Fem
Prenatal®). Unfortunately, the Metagenics formulas
have inactive Vitamin B6 from pyridoxine HCl, which can contribute
to the nausea of pregnancy. (Some people also really like NATURELO
Prenatal Whole Food Multivitamin and Best Nest. I have heard that
Smarty pants is owned by Merck, and Garden of Life was just bought
out by Nestle.)
You can get the biologically active forms of B vitamins from Thorne's
Methyl-Guard Plus®:
Riboflavin (as Riboflavin 5'-Phosphate Sodium) 90 mg
Vitamin B6 (as Pyridoxal 5'-Phosphate) 45 mg
Folate (as L-5-Methyltetrahydrofolate from L-5-Methyltetrahydrofolic
Acid, Glucosamine Salt) 3 mg
Vitamin B12 (as Methylcobalamin) 3 mg
Biologically Active Forms
Levomefolic acid (INN)
(also known as 5-MTHF, L-methylfolate and 5-methyltetrahydrofolate
and (6S)-5-methyltetrahydrofolate, and (6S)-5-MTHF)
is the primary biologically active form of folic
acid
Calcium folinate (also called, Folinic acid or called
5-formyltetrahydrofolate) [The bio-inactive C-6 isomer,
[6R]-5-formyl-tetrahydrofolate (5-HCO-H4F), is not found in Nature.
An oral dose of 13.5µmol of [6R]-5-HCO-H4F in humans results
in the appearance of the naturally occurring
[6S]-5-methyl-tetrahydrofolate and relatively large amounts of other
bioactive folates in plasma. from Biochemical
Journal.]
Riboflavin 5'-Phosphate Sodium (Vitamin B2)
Vitamin B6 (as Pyridoxal 5'-Phosphate)
Vitamin B12 (as Methylcobalamin or Adenosylcobalamin).
Methylcobalamin and adenosylcobalamin have different functions thus
providing a total solution when combined for those with B12
deficiency. They are both natural.. [Information from seekinghealth.com]
Inactive Forms
Folic Acid, possible anything labeled just Folate
Vitamin B6 (as Pyridoxine HCl)
Vitamin B12 (as Cyanocobalamin or Hydroxocobalamin) -
Hydroxocobalamin is a natural form of B12 but is not bioactive; it
requires methylation so it not a good choice for those who have
methylation or neurological dysfunction. Cyanocobalamin is
synthetic and requires methylation to be utilized and eliminated
from the body.
Please note that Floradix Iron + Herbs has synthetic B6 and B12. I
was shocked that such a revered pregnancy remedy for anemia isn't as
natural as I thought. Gaia
Herbs PlantForce® Liquid Iron is free from synthetic
(non-bioactive) additives.
What
is Methylation and Why Should You Care About it by Alan
Miller, ND [1/12/18] from the Thorne web site - this is an
excellent, short overview of methylation issues.
I absolutely rail at the recent 23AndMe nonsense blog article about
how methylation couldn't be a real issue because humans wouldn't
have evolved to have so many disease states from one gene.
Newsflash: the disease states come from ingesting the synthetic
forms of the vitamins, combined with common genes. Everyone agrees
that we did not evolve with synthetic vitamins!
MTHFR,
Folic Acid and Folate: Should I Eat It? BY JOE (MSC
NUTRITION), DIETITIAN [Last Updated 6th August, 2017]
MTHFR mutations are well-known genetic variations that can impact
folate metabolism.
I could not find a reliable source that lists the exact ratios, but
many websites suggest these are the top food sources of
L-methylfolate (methylated folate):
Romaine (Cos) Lettuce
Sprouted legumes (buckwheat, mung beans, chickpeas, etc)
Broccoli and cauliflower
Asparagus
Kale and spinach
Cabbage
Fermented foods such as miso and kefir
Berries like strawberries and raspberries
Citrus fruits like oranges and grapefruits
The
MTHFR Variant—What Is It? - a very good explanation, from Best Nest Wellness, a
company that makes prenatal vitamins with bioactive forms of folate
and B12. I don't understand why it has the non-bioactive form of B6
when the bioactive form can help reduce nausea.
Methylfolate
Vs. Folic Acid: What Your Doctor Hasn’t Told You
Preparing For Pregnancy With MTHFR Mutations [Updated on 8
Jan, 2014]
Excessive
Folate, B12 in Pregnancy Dramatically Ups Autism Risk
[3/12/16] - Excessive levels of plasma folate and vitamin B12 during
pregnancy have been linked to a dramatic increase in autism risk in
offspring, new research shows. . . . Dr Fallin said that
the team was not able to determine whether excessive plasma folate
and vitamin B12 levels corresponded to a certain level of intake of
both supplements during pregnancy.
[ED: This provides a helpful direction for more focused
research. It seems there may be a common cause between high
folate levels in pregnant women and autism in their children.
I posit that the common cause is problems with their methylation
genes. Women with genetic methylation problems will run higher
levels of serum folate and B12 because their bodies can't clear
it. Even though their serum levels are high, they may actually
be deficient in the bioactive forms which can get into the
cells. There's an increased likelihood that their children
will also have genetic methylation problems, which affects their
ability to clear environmental toxins, which could cause
neurological damage leading to autism. Similar research would
benefit significantly from looking at the MTHFR genes of study
participants and their children.]
Your
MTHFR Status: How Much Mercury is Detoxified vs. Stored? -
This great graphic does a really good job of explaining how
different combinations of MTHFR gene variations affect your body's
ability to handle mercury.
How
to Test for MTHFR Mutations and What to Do if You Have Them
Dr. Amy
Myers offers a link to allow you to order the dnalife SNP testing;
this uses a mouth swab instead of saliva, so you can use it with
your newborn.
Folic acid handling by the human gut: implications for food
fortification and supplementation. [free
full text]
Patanwala I1, King MJ1, Barrett DA1, Rose J1, Jackson R1, Hudson M1,
Philo M1, Dainty JR1, Wright AJ1, Finglas PM1, Jones DE1.
Am J Clin Nutr. 2014 Aug;100(2):593-9. doi:
10.3945/ajcn.113.080507. Epub 2014 Jun 18.
Conclusions: The human gut appears to have a very efficient capacity
to convert reduced dietary folates to 5-MTHF but limited ability to
reduce folic acid.
I haven't been able to verify this, but I read that stork bites are
also likely signs of midline defects related to MTHFR.
Maximized Genetics
performs a number of DNA tests from a cheek swab, which can be done
on a breastfeeding newborn.
23andMe
Offers New Genetic Report on Type 2 Diabetes [3/10/19] - The
genes for gestational diabetes and Type II diabetes are related,
although this is not totally specific to gestational diabetes.
The
Plight of Thyroid Patients - People with MTHFR mutations may
not be able to metabolize Synthroid and generics properly. This is
an excellent explanation of the issues.
IS
FOLIC ACID IN YOUR PRENATAL MAKING YOU & BABY SICK?
[10/8/19] By Jacqueline
Methylated Prenatal
Vitamins
I generally like supplements from Thorne and Metagenics. They're the
high-quality supplements recommended by chiropractors and
naturopaths. I particularly like that they are not part of any
multi-level marketing scheme. However, it seems that many fine
supplements providers still have some prenatal vitamins that have
non-bioactive components. These can be problematic for the 40%
or so of women who have methylation issues, as discussed in the rest
of this web page.
For example, some people say that if you take whole foods
supplements, then you can be sure you're getting the natural form of
folate. But New Chapter lists their folate in Perfect
Prenatal™ Multivitamin as "Folate (as folic acid from culture
media)"; this sounds like it might not be bioactive.
There's a new set of high-end prenatal vitamins with bioactive forms
of folate, B6 and B12 available from Best Nest Wellness.
As I write this, the following products have only methylated forms
of B6, B9/folate, and B12: Mama
Bird™ Prenatal Multi+, Mama
Bird™ AM/PM Prenatal Multi+, Mama
Bird™ AM/PM Prenatal Multi+ Iodine & Iron Free
Be sure to click on "Supplement Facts" for any item you're
considering purchasing. You want to see
L-5-Methyltetrahydrofolate (folate), Methylcobalamin (B12) and
Pyridoxal-t-Phosphate (B6).
Getting Your DNA Tested
Please note that as of May, 2018, 23andMe says that it doesn't
provide MTHFR analysis, but they do seem to be providing the raw
data needed to assess your methylation genes.
Conditions
NOT Included In 23andMe - "23andMe does not offer diagnostic
testing." They explicitly say that their current 23andMe reports do
not include "MTHFR analysis, such as a targeted mutation analysis,
methylation analysis or detox profile".
I believe this has always been true of 23andMe. And I know they've
had issues with the FDA about medical interpretation. I just wish
they would be more explicit about exactly which parts of which genes
they report on.
I am troubled by the ways in which 23andMe is distancing itself from
the value of information about MTHFR genes. Is there a better
all-purpose DNA analyzer that seems to be more supportive of
learning one's MTHFR status?
I believe that knowledge is power and that our intelligence allows
us to use knowledge to save ourselves untold miseries. For
example, some people have an unfortunate gene that causes myopathy
(including unreversible muscle degeneration); simply knowing
this allows you to avoid statins or modify your use. Most
pregnant women already have their DNA tested to see if they carry
the gene for cystic fibrosis, and couples in certain demographics
may have their DNA tested to assess their risks of creating a child
with a severe, life-threatening condition. Reproductive
technologies can help couples to make sure they pass on a good gene
to their baby.
In addition to some of the major mutations, there are also less
obvious mutations that affect the way your body processes your
prenatal vitamins. For about 10% of women, their prenatal
vitamins may actually INCREASE their risk of having a baby with
tongue tie or other midline defects. This is how the issue of
DNA testing and the MTHFR gene came to the attention of midwives; a
baby with a tongue tie cannot nurse well, causing untold miseries
for the mother and baby; surgical correction may be an option, but
it can be expensive, very difficult, and may not work well.
Most women who have reached childbearing age will not have any major
surprises if they get a full DNA analysis. Still, some women I
talk to "don't want to know".
So, it's important for you to know that you can just have your MTHFR
gene tested, or you can have your full DNA analyzed but only get a
methylation report, including your MTHFR gene status.
23AndMe offers a
provider program, which includes a complimentary kit for the
provider, herself. 23AndMe provides raw data that can be
interpreted at other sites:
Genetic Genie - Methylation
and detox analysis from 23andMe results
MTHFR Support offers a Pregnancy
Forum and Find A
Practitioner feature.
I really like the comprehensive methylation report from Genetic
Genie, and I also really enjoyed the tons of information I got from
Promethease.com offering
medical interpretation of the results from 23AndMe. I also
like their extensive list of prenatal screens for genetic
diseases. But they've recently raised their price to around
$200. (You can get a discount for group purchases.)
There is a less expensive alternative that just looks at a couple of
pairs in the MTHFR gene: 677 and 1298; this is available from SpectraCell
Laboratories; I've heard the cost is $40.
StrateGene
is a genetic analysis program that uses the raw data from
23andMe. One of my midwife friends liked it in combination
with everything else.
1. Focuses on SNPs that have potential clinical implications
2. Provides the biochemical pathways for each gene - not just the
isolated SNP
3. Identifies factors which influence SNPs, kinetic impact, and
potential associated symptoms and conditions
4. Includes a full bibliography with supporting research
MTHFR from
pointofreturn.com - This is a nice explanation of MTHFR issues, and
they list four different places that will give methylation reports
from the 23AndMe raw data.
As of May, 2021, Sequencing
is a new provider of DNA testing. They claim to provide more
comprehensive testing than any other provider. I don't have any
experience with them.
Carrier
Screening for Rare Diseases & Syndromes | DNA Tests - they
screen for a very large number of rare diseases.
Their web pages also list many
other providers of DNA tests.
MTHFR and Fertility
Tips
for TTC with MTHFR
MTHFR and Tongue Tie
See also: Tongue Tie and
Lip Tie
MTHFR Gene
Mutations: A Beginner’s Guide
Find a Doctor who
can help with MTHFR issues. Increasingly, midwives seem
to be more aware of the MTHFR issue because of the association with
tongue tie and breastfeeding issues. So you might be able to
find a midwife locally who can help guide you through testing and
adjusting your diet and supplements. The editor of these web
pages is available for phone consulting to provide you with relevant
information - contact
Ronnie Falcao, LM MS CPM.
The
MTHFR Gene Mutation And How To Rewire Your Genetics - The
Bulletproof Executive has an excellent explanation of MTHFR issues.
Preparing
For Pregnancy With MTHFR Mutations from mthfrliving.com
Folic
Acid and Folate Facts and Fallacies - synthetic folic acid
isn't absorbed well. The natural form is folate or L-5
methyltetrahydrofolate.
TONGUE TIE - IS FOLIC ACID TO BLAME? - This is a simple
explanation of how synthetic folic acid may be related to tongue
tie.
The little
known (but crucial) difference between folate and folic acid
[3/9/12] from Chris Kresser's blog
The form of folate that can enter the main folate metabolic cycle is
tetrahydrofolate (THF). (2) Unlike natural folates, which are
metabolized to THF in the mucosa of the small intestine, folic acid
undergoes initial reduction and methylation in the liver, where
conversion to the THF form requires dihydrofolate reductase. The low
activity of this enzyme in the human liver, combined with a high
intake of folic acid, may result in unnatural levels of
unmetabolized folic acid entering the systemic circulation.
In his lectures, Dr Neil Rawlins implies that for some people with
methylation problems, even natural folate may not be
assimilable. He says that berries are the only natural foods
that contain the form that can be assimilated by those with the
worst methylation problems.
When people have the MTHFR gene mutation, they do not turn folic
acid into folate. In addition, the folic acid plugs the receptor
sites in cells with an unusable form for these people. With the
unusable folic acid in the receptor cites, the body is prevented
from being able to use the folate that they do consume through
natural food.
Folate
vs Folic Acid, MTHFR, and Why I Regret Taking My Prenatal Vitamin
- Here's another version of Cara's web page on folic acid; it's a
very accessible discussion of why synthetic folic acid causes
problems for some women.
Methylation Resources
Dr Neil
Rawlins - MTHFR - Sept 2011 - One-hour YouTube video
about the methylation genes and recommended supplements. Great
Start Video!
About the MTHFR gene
from the NIH's Genetics Home
Reference
Folic
Acid and Folate Facts and Fallacies - synthetic folic acid is
thought to cause cancer and may contribute to asthma in
children. The natural form is folate or L-5
methyltetrahydrofolate.
And, most importantly, an estimated 33 % of people are genetically
deficient in the enzyme that converts synthetic folic acid form for
it to be used by your body.
So, pregnant mamas, make sure you're getting natural folate, either
through better supplements or through superior nutrition.
Any synthetic folic acid in your diet or supplements actually blocks
the absorption of natural folate, thus compounding the
problem. Synthetic folic acid is common in prenatal vitamins,
many multivitamins and processed foods.
Dr Ghaheri believes that ties form at around gestation week 12-13,
not super early as once thought. So it might not be too late to
prevent a tongue tie in your baby.
MTHFR and Hyperemesis
People with a double defective MTHFR C677T gene combination will not
be able to metabolize the usual (inactive) form of vitamin B6, which
is pyridoxine HCl. This also means that pharmaceutical
combinations such as Diclegis and
Dilectin also will not be helpful. They could theoretically
make the hyperemesis worse by blocking receptors for the
active form.
The active form of vitamin B 6 is pyridoxal 5'-phosphate, which is
contained in Thorne's Methyl-Guard Plus.
Anyone with hyperemesis would do well to
get their genes tested to see if this is an issue for you, or
just switch to Thorne's Methyl-Guard Plus and stop taking inactive
forms of the B vitamins.
Treatment for Hyperemesis Caused by MTHFR/Methylation Issues
1) Stop intake of all forms of non-bioactive supplements or
supplemented foods. Many processed foods such as bread and
cereal are supplemented with non-bioactive folic acid, or they may
even call it folate. At the top of this web page, there are
lists of terms used for bioactive or non-bioactive forms of the
supplements.
2) Stop intake of all prenatal vitamins or other supplements and
nausea medications which contain non-bioactive vitamins; this
includes Diclegis and Dilectin.
3) Supplement with bioactive forms of B6, which is pyridoxal
5'-phosphate; make sure it's from a very reputable supplements
source. I like Methyl-Guard
Plus or Pyridoxal
5'-Phosphate 180's from Thorne. The amount of B6 in Diclegis
is 10 mg, so this seems like a good goal. B vitamins are
excreted fairly rapidly, so it is unlikely that you would be able to
take in excessive amounts.
If the nausea is so bad that you're having trouble keeping the
capsules down, you could try opening a capsule (or half capsule,
depending on taste) into an ice cube compartment and then freezing
it. Most moms will be able to suck on the frozen ice
cube. And you can absorb the dissolved vitamins through the
mucous membranes of your mouth, so you don't even have to swallow
it!
4) KEEP YOUR BOWELS MOVING - This is a problem with any case of
hyperemesis. You can't keep food down, so your bowel activity slows,
so you're not excreting the high levels of pregnancy hormones as
quickly as you should be. You may actually be re-absorbing
hormones from your gut to cause higher levels of the hormones which
cause hyperemesis. The best remedy is probably maltitol, a
pregnancy-safe natural sweetener which has laxative effects. Again,
you can sweeten ice cubes with it. Start out slowly . . .
maybe one teaspoon maltitol every six hours or so and increase as
needed to achieve the desired result.
It can take up to two weeks for your body to clear out the
non-bioactive form of B6, so don't expect a full recovery
immediately. But you should start to see some mild improvement
within a few days and some significant improvement within a week.
GDF15 and IGFBP
and Hyperemesis
Two genes
likely play key role in extreme nausea and vomiting during
pregnancy | YouTube video from UCLA Health News [3/21/18]
A new study led by researchers at UCLA and published in the journal
Nature Communications has identified two genes associated with
hyperemesis gravidarum, whose cause has not been determined in
previous studies. The genes, known as GDF15 and IGFBP7, are both
involved in the development of the placenta and play important roles
in early pregnancy and appetite regulation.
These genes are expressed at high levels in the placenta. They've
shown that the associated proteins are abnormally high in women with
HG.
They say there's no evidence that HCG and elevated estrogen are
related to HG, which seems to contradict long-established teachings.
No relevant therapies are found yet.
Two
genes likely play key role in extreme nausea and vomiting during
pregnancy - UCLA-led study will help scientists better
understand debilitating condition [3/21/18] - research by Marlena
Schoenberg Fejzo, the study’s first author, said. She is an
associate researcher at the David Geffen School of Medicine at UCLA.
Placenta and
appetite genes GDF15 and IGFBP7 are associated with hyperemesis
gravidarum. [Full
text from Nature Communications]
Fejzo MS1,2, Sazonova OV3, Sathirapongsasuti JF3,
Hallgrímsdóttir IB3,4, Vacic V3, MacGibbon KW5,
Schoenberg FP6, Mancuso N7, Slamon DJ8, Mullin PM9; 23andMe Research
Team.
Nat Commun. 2018 Mar 21;9(1):1178. doi:
10.1038/s41467-018-03258-0.
Abstract: Hyperemesis gravidarum (HG), severe nausea and vomiting of
pregnancy, occurs in 0.3-2% of pregnancies and is associated with
maternal and fetal morbidity. The cause of HG remains unknown, but
familial aggregation and results of twin studies suggest that
understanding the genetic contribution is essential for
comprehending the disease etiology. Here, we conduct a genome-wide
association study (GWAS) for binary (HG) and ordinal (severity of
nausea and vomiting) phenotypes of pregnancy complications. Two
loci, chr19p13.11 and chr4q12, are genome-wide significant
(p < 5 × 10-8) in both association scans and are replicated
in an independent cohort. The genes implicated at these two loci are
GDF15 and IGFBP7 respectively, both known to be involved in
placentation, appetite, and cachexia. While proving the casual roles
of GDF15 and IGFBP7 in nausea and vomiting of pregnancy requires
further study, this GWAS provides insights into the genetic risk
factors contributing to the disease.
MTHFR and Vaccination Reactions
Genetic basis
for adverse events after smallpox vaccination. [full
text]
Reif DM1, McKinney BA, Motsinger AA, Chanock SJ, Edwards KM, Rock
MT, Moore JH, Crowe JE.
J Infect Dis. 2008 Jul 1;198(1):16-22. doi: 10.1086/588670.
Identifying genetic factors associated with the development of
adverse events might allow screening before vaccinia virus
administration. Two independent clinical trials of the smallpox
vaccine (Aventis Pasteur) were conducted in healthy, vaccinia
virus-naive adult volunteers. Volunteers were assessed repeatedly
for local and systemic adverse events (AEs) associated with the
receipt of vaccine and underwent genotyping for 1,442
singlenucleotide polymorphisms (SNPs). In the first study, 36 SNPs
in 26 genes were associated with systemic AEs (P <or= .05); these
26 genes were tested in the second study. In the final analysis, 3
SNPs were consistently associated with AEs in both studies. The
presence of a nonsynonymous SNP in the methylenetetrahydrofolate
reductase (MTHFR)gene was associated with the risk ofAEin both
trials (odds ratio [OR], 2.3 [95% confidence interval {CI}, 1.1-5.2]
[P = .04] and OR, 4.1 [95% CI, 1.4 -11.4] [P<.01]). Two SNPs in
the interferon regulatory factor-1 (IRF1) gene were associated with
the risk of AE in both sample sets (OR, 3.2 [95% CI, 1.1-9.8] [P =
.03] andOR, 3.0 [95% CI, 1.1- 8.3] [P = .03]). Genetic
polymorphisms in genes expressing an enzyme previously associated
with adverse reactions to a variety of pharmacologic agents
(MTHFR) and an immunological transcription factor (IRF1) were
associated with AEs after smallpox vaccination in 2 independent
study samples.
MTHFR and Newborn Screening
In the California Newborn Screening's list of Disorders
Detectable by NBS Program as of January 1, 2012, they
include remethylation defects (MTHFR, MTR, MTRR, Cbl D v1,
Cbl G deficiencies) .
The Newborn Screen is not a genetic test of the MTHFR gene.
Instead, it measures chemicals in the baby's blood that would
indicate very severe problems with remethylation. The rate of
babies identified by this specific tests is only 0.27%, whereas the
genetic average for people with homozygous defects is closer to 10%.
Newborn
screening for homocystinurias and methylation disorders:
systematic review and proposed guidelines. [full text]
Huemer M1,2,3, Kožich V4, Rinaldo P5, Baumgartner MR6,7, Merinero
B8, Pasquini E9, Ribes A10, Blom HJ11.
J Inherit Metab Dis. 2015 Nov;38(6):1007-19. doi:
10.1007/s10545-015-9830-z. Epub 2015 Mar 12.
Newborn screening (NBS) is justified if early intervention is
effective in a disorder generally not detected early in life on a
clinical basis, and if sensitive and specific biochemical markers
exist. Experience with NBS for homocystinurias and methylation
disorders is limited. However, there is robust evidence for the
success of early treatment with diet, betaine and/or pyridoxine for
CBS deficiency and good evidence for the success of early betaine
treatment in severe MTHFR deficiency. These conditions can be
screened in dried blood spots by determining methionine (Met),
methionine-to-phenylanine (Met/Phe) ratio, and total homocysteine
(tHcy) as a second tier marker. Therefore, we recommend NBS
for cystathionine beta-synthase and severe MTHFR deficiency. Weaker
evidence is available for the disorders of intracellular cobalamin
metabolism. Early treatment is clearly of advantage for patients
with the late-onset cblC defect. In the early-onset type, survival
and non-neurological symptoms improve but the effect on
neurocognitive development is uncertain. The cblC defect can be
screened by measuring propionylcarnitine,
propionylcarnitine-to-acetylcarnitine ratio combined with the second
tier markers methylmalonic acid and tHcy. For the cblE and cblG
defects, evidence for the benefit of early treatment is weaker; and
data on performance of Met, Met/Phe and tHcy even more limited.
Individuals homozygous or compound heterozygous for MAT1A mutations
may benefit from detection by NBS using Met, which on the other hand
also detects asymptomatic heterozygotes. Clinical and laboratory
data is insufficient to develop any recommendation on NBS for the
cblD, cblF, cblJ defects, glycineN-methyltransferase-,
S-adenosylhomocysteinehydrolase- and adenosine kinase deficiency.
Two-tier approach to the newborn screening of
methylenetetrahydrofolate reductase deficiency and other
remethylation disorders with tandem mass spectrometry. [full
text]
Tortorelli S1, Turgeon CT, Lim JS, Baumgart S, Day-Salvatore DL,
Abdenur J, Bernstein JA, Lorey F, Lichter-Konecki U, Oglesbee D,
Raymond K, Matern D, Schimmenti L, Rinaldo P, Gavrilov DK.
J Pediatr. 2010 Aug;157(2):271-5. doi:
10.1016/j.jpeds.2010.02.027. Epub 2010 Apr 14.
RESULTS: A total of 86 333 NBS samples were tested between January
2007 and March 2008, and 233 of them (0.27%) met the criteria
for second-tier testing of tHcy.
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