SDL Quiz
what drug helps relieve carnitine deficiency
levocarnitine
von-elevated TAGS
excess pyruvate is converted to acetyl Coa which can be used to make fatty acids glyceralehyde excess (from glycolysis) can also be used to make glycerol from glycerol 3 phosphatase these two combine to form TAG's
MSUD- phenotype
failure to thrive, seizures, irritability, little interest in feeding
carnitine deficiency- why hepatomegaly, why low ketone bodiesm hyperammonemia
fatty acids being transported to the liver during fasting for FA oxidation build up in the liver cells because they are unable to be oxidized no FA oxidation-no production of ketone bodies patient is breaking down amino acids to produce energy in the fasting state as an alternative to FA oxidation resulting in higher output of ammonia
what key features of achondroplasia would be seen in an ultrasound
frontal bossing, macrocephaly, short femur length
VCLFAD- intermittant hypoglycemia, hepatomegaly
if the body is in starvation mode and oxidizes s/m chain fatty acids, it will be unable to oxidize vlc and therefore unable to produce glucose these unoxidized vlcfa are sent to the liver where they accumulate since they cannot be oxidizes in liver perioxisomes
what diet for angelman should be used to manage the seizures
keto
how does coronary artery disease increase in patients with familial hyper
oxidized LDL hanging out in the arteries and unable to enter the cells are taken up by SRA receptors on macrophages, these cells accumulate to form foam cells. these foam cells can eventually create a plaque within the arteries
Management of disorder
PT/OT/ST; behavioral programs/care
causative gene for achondroplasia- what chromosome, location, function
FGFR3 4 P16 -tyrosine kinase receptor that binds to fibroblast growth factors and triggers signaling cascades in this disorder= FGF unable to bind to receptor leading to uncontrolled/uncoordinated processes in the bone growth plates=stunted growth
what gene causes von gierke disease, where is it located, inheritance
G6PC1 chromosome 17 glucose-6-phophatase AR
advantage to having high HDL in patients with hyperchol
HDL can take up cholesterol and return it to the liver to be processed, increased HDL will decrease the amount of cholesterol circulating
tay sachs- gene, structure of protein, organelle affected, what accumulates
HEXA, two domains/heterodimer w alpha/beta subunit, GM2 gangliosides AR
beckman weidemann syndrome overview
IGF2 (maternal imprinting), CDKN1C (paternal imprinting) get by: methylation at maternal Ic1 (activating IGF2), UPD paternal, mutation at maternal CDKN1C, demethylation at maternal IC2 (inactivating CDKN1C) -macroglossia, macrosomia, omphalocele, hypoglycemia, ear creases/pits
Angelman Syndrome
slow growth, microcephalic, autism like, jerky movements, happy and laughs a lot
why do statins not work in patients with familial hypercholesteolemia
statins work to stop the production of cholesterol but that is not the issue in these patients, these medications wont reduce the amount of LDL in the patient's blood
methyl malonic- what action should physician take according to american college of medical genetics algorithm
test- urine Orangic acids, plasma Acylcarnitine
what does TAGS in the normal limits indicate
there is not an issue with TAG breakdown so can rule out lipoprotein lipase disorder, VLDL disorder
why would a Y-specific primer sequencing report be done in patients with turners what would a negative test indicate?
to see if the child has mosaicism in which some cells have the 46XY karyotype patient is not at risk for gonadal blastoma which occurs in mosaic patients
edema of feet, redundant skin on back of neck, small, dont go into puberty, girls, ovarian dysgenesis
turners syndrome one X chromosome or isochromosome x
otc- urine uracil levels
would be high- orotic acid can be converted to uracil via ump synthase
von gierke disease type 1a phenotype
-abdominal distension -irritability -doll like face, round cheeks -thin extremities -malnourished/emaciated
biochem mechanism for patients with familial hyperchol
-absence of LDL receptors -altered LDL receptors that cant bind LDL -B100 protein defect that makes LDL unable to bind with the cell to be taken in
what prenatal test are preformed to assess for down syndrome, name all of the test that could diagnose this condition
-chorionic villus sampling -aminocentesis -karyotype g-banding, array CGH, SNP array, FISH
what are therapies and psychosocial supports for children with turners
-growth hormone administration -estrogen for secondary sex characteristics
ways to get angelman
-maternal deletion -UBE3A mutation -paternal UPD -imprinting defect where maternal is silenced also
a women is having spontaneous abortions and the test reveals the fetus has monsomy 21, explain
-monosomy 21 is not typically compatible with life -woman is having non-disjunction within the gametes with chromosome 21
huntingtons- expansion fragile x friedreich ataxia spinocerebrallar ataxia myotonic dystrophy type 1 and 2
1. CAG repeat in exons- 9-35 normal, 40+ HD 2. CGG in 5UTR FMR1 gene 3. AR, FRDA, GAA repeat intron 4. ATXN1, CAG repeat 5. DMPK, CTG repeat 50-100 mild, over 1000, c.19; CNBP, CCTG 75 repeats, c.3
MSUD variations- 1. classic severe 2. intermediate 3. intermittent 4. thiamine-responsive
1. death by 3 months of age, not responsive to treatment 2. responsive to controlled diet, severe developmental and neurological delay 3. controlled diet, actue episodes of ataxia lethargy, semi coma 4. total cute in response to thiamine
pharm intervention for familial hyper-primary and secondary
1. ezemtimibe-limits absorption of cholesterol (typically combined with statins to keep cholesterol levels low) 2. PCSK9 inhibitors- help liver absorb more cholesterol lowering the amount circling in the blood 1. bile acid sequestrits- block bile acid absorption from the stomach (allows cholesterol attached to be excreted rather than reabsorbed) 2. niacin/nicotinic (decreases FFA release) can raise HDL and lower LDL
gene for VLCFAD, inheritance pattern,
ACADVL, AR
what influences the development of downs syndrome
AMA
genes defective in familial hyper, homozygote versus heterozygote
APOB gene, LDLR gene, PCSK9 homo can have a worse manifestation with heart attacks in childhood heterozygotes have better outlook
carnitine deficiency- inheritance, gene
AR OCTN2- SLC22A5
maple syrup urine disease-gene, inheritance, mechanism
BCKDHa/b- branched chain alphaketo dehydrogenase -trouble metabolizing branched AA- leucine, isoleucine, valine AR
angelman- chromosome, location/gene, how disease comes about
CNV on chromosome 15q11-13, acrocentric, long arm-q UBE3A- mutation leads to disruption in ub protein degradation paternal imprinted, maternal
methyl malonic- gene, variant, present, inheritance
MMA AR missense vomiting, sleeping a lot, dehydrated, acidosis, not gaining weight high forehead, broad nasal bridge, wide appearing eyes, long smooth philtrum
prader willi overview
SNURF gene maternal imprinted, paternal expressed hypotonia, obesity, impaired satiety, failure to thrive
carnitine deficiency symptoms
abdominal pain, vomiting, myotonia, muscle weakness
methyl malonic- ACT SHEET for physicians
ascertain current clinical status, consult pediatric metabolic specialists' same day, evaluate newborn for serious conditions and transfer to hospital if needed, confirm diagnostic testing, provide family with basic information regarding the disorder
in what populations is tay sachs disease high
ashkenazi jews, french canadians, cajun
OTC- why glutamine levels high, inheritance patttern
body is acidic (excess ammonia)- packs up NH3 and glutamate to make glutamine and transports kidney who use glutaminase to release NH3 and glutamate, nh3 then neutralizes some acid by combing to form NH4 which is then excreted x-linked dominant
hypoglycemia in carnitine deficiency
cannot transport acetly coa into mitochondria- aka fatty acid oxidation (which is providing fuel for gluconeogenesis) is blocked
tay sachs phenotype
cherry red macula, psychomotor degeneration, seizures, hypotonia, dementia, increased startle response
pathway affected by methylmalonic aciduria
cobalmin is unable to enter mitochondria and be converted to its active form and used as a coenzyme for methyl malonyl-coa mutase, therefore methylmalonyl cannot be converted to propionyl COA
what surveillance should be done for someone with downs syndrome
congenital heart defects, leukemia, hypothyroidism, hearing loss, spinal cord injuries, developmental/intellectual disabilities, improper growth, respiratory infections
besides achondroplasia-what other disorders are associated with variants in the FGFR3 gene
crouzon syndrome, LADD syndrome, muenke syndrome, SADDAN, hypochondroplasia, thanatophoric dysplasia types 1/2
methylmalon- nutritional guidelines, nutrients/medicine for condition
decrease intake of amino acids/odd chain number FA vitamin b12- hydroxycobalamin -active form of B12
clinical presentation of downs
depressed nose, up slanting palpebral fissures, small ears, short neck, short broad hands/feet
turners and chronic disease
elevated chance of patient developing T2D-must work to prevent/manage this disease in these patients since they are already at risk for CD issues
methylmalonic aciduria NBS secreening
elevated propionyl CA
silver russell overview
get by: maternal UPD, demethyl at paternal IG1 (turn off IGF2), -small for age, body asymmetry, feeding difficulties,
what would you expect to find on a histological slide of a patient with turners syndrome
gonadal dysgenesis- streaks of CT instead of ovaries
methyl malon- main complications for long term surviving patients
growth delay, ID, kidney disease, pancreatitis
von- elevated serum lactic acid/elevated pyruvate
high G6p sends it back down glycolysis producing lots of pyruvate which is then shunted to lactate
von- elevated uric acid levels
high action in pentose phosphate pathway leading to de novo synthesis of purine nucleotides which are not needed and are catabolized to uric acid
von gierke explanation- low fasting blood glucose
liver and kidney unable to convert glucose 6p to glucose to be transmitted into the blood to be used my muscle during times of fasting
nutritional treatment for vlcfa
low fat diet, inclusion of odd chain FA in diet, injection of IV glucose, triheptanoin (medium odd chain fatty acid supplement as a source of FA's and calories)
what key prenatal signs should you look for on an ultrasound that would lead to turners
lymphedema, hydrops, heart/kindey defects
best way to manage von gierke, why does this disease occur in fasted state
maintain normal blood glucose concentration body cannot complete glycogenolysis or gluconeogenesis
methylmalonic acidemia- involved with what
methyl malonic acid is an intermediate in the catabolism of methionine, isoleucine, valine, threonine, and odd chain FA form propionyl CA to methyl manoyl to succinyl Coa
most commo pathogenic variant for achondroplasia, how does one normally get it
missense- C1138G>A mostly de novo, paternal age effects, AD- dominant version is lethal
huntingtons disease, inheritance pattern, gene, location, what type
neurological decline, cortex degeneration, personality changes, motor abnormalities, hyperreflexia, dementia autosomal dominant, typically paternally transmitted, GOF HTT, chromosome 4p16.3, submetacentric
does maternal age contribute to a child being born with turners
no, a majority of turners patients are caused by absence of paternal X
how does downs arise what chromosome and what type of chromosome is this
non disjunction in meiosis one (homologous chromosomes fail to separate) or two (sisters fail to separate), translocation chromosome 21-acrocentric (13-14, 21/22) metacentric- 1,3,16,19,20
why would a turners syndrome patient be short
only one copy of the SHOX gene
two medications for OTC- hyperammonia treatmentq
phenylbutrye- binds glutamine benzoate- binds glycine both fast track to liver to excret excess ammonmium- can bypass urea cycle
turners- more live births or prenatal losses
prenatal losses
Huntington's and HTT gene mechanism
protein assists with mRNA moving/transcription/translation- gain of function so increases and aggregates protein leading to issues with proper transport and maturation of proteins
