Post on 11-Jan-2016
HPN COMPLICATIONS
Metabolic • liver abnormalities• Gallbladder sludge &
stones• metabolic bone disease• trace element and /or
vitamins deficiencies• manganese toxicity• renal function impairment
B Messing. Approved centre for Intestinal failure. Paris1 title, 6 sub titles, 25 materials + 4 additional
HPN-long term ComplicationsHPN-long term Complications
• Renal function impairment
* in SBS : avoid hyperoxaluria and oxalate-Ca renal stone Up to 25% of patients if steatorrhea and colon. Prevention : oral Ca and food with low oxalate content
Serious Renal Impairment Is Associated With Long-Term Parenteral Nutrition
- 33 (13M, 20 W) adult 51 (21-79) yr old - on Long-term HPN : 8.3±4.4 yrs- Protein load : 1.28± 0.32 g.Kg.d- Nephrotoxic drug : 3.4±4.0% of all HPN days- Bacteriemia/fungemia : 2.3 (0.5±0.5 / yr) episode - Cr clearance (CrCl) decline was 3.5±6.3% per year
- age + 3 above factors : 50% change in CrCl- age + infection factor : idem- excessive urinary phosphate excretion (? aciduria)- but no association with amino acid content of TPN - this decline in renal function is largely unexplained
From L.-A. Buchman; A. Moukarzel, M.-E. Ament et al. JPEN 1993;17: 438-444
Buchman JPEN 1993; 17: 438-44
HPN - ComplicationsHPN - Complications
• deficiencies of trace elements • manganese toxicity • deficiencies of vitamins
Healing of Zn deficiency after a few days of IV supplements BM 0094
TRACE-METAL DEFICIENCIES during (H)PN
Blood & MRIExtrapyramidal syndrome+Mn*
Porotic ±painful osteopathy +Al*
Liver thesaurismosis, perls+Fe
UrGoitre (nil po)+I
Acrodermatitis, diarrhea, hair loss, - NB++Zn
Heme-SynthaseAplastic anemia ± mild leucopenia++Cu
Xanthine ox
Sulfite ox
Coma, ? Met, Uric acidNeuromyelopathie
?Mo
Diabetes-Cr
Glutathion peroxydaseCardiomyopathie / failure++Se
Perls,ferritine
* Excess and toxicity (chronic dehydration, renal insufficiency, cholestasis) (Chonic Zn deficit : altered growth in children with nanism) Mo 0.62±0.29 (Clin Chemistry 2001; 47(2)279 BM. 0093
blood, Ur
Zn blood, Ur, hair
Cr blood
Mn toxicity :Brain MRI / hypersignal in T1, basal ganglia + white matter BM 0099
Vitamin deficiencies and (H)PNDeficiency Presentation
B1, Thiamine Wermicke's encephalopathy
Cardio myopathy,
Refractory lactic acidosis
Folique (B9) Megaloblastic anemia ± cytopenia
B12 Irritability, megaloblastic anemia Cordonal posterior Syndrome
PP, Niacin, Dermatosis (pellagra), Diarrhea, Demencia
B6 Sideroblastic anemia, convulsions
B2 Cheilosis, red swollen tongue, folliculitis
Biotin Dermatitis, alopecia, hypotonia in 1 child
BM 0097
Vitamin deficiency during (H)PNDeficiency Presentation
Vitamin A Night blindness, xerophammia,dark field adaptation, defective bone mineralization
Vitamin E In vitro plateled hyper-aggregation and H2O2 - induced RBC hemolysis.
Signs and symptoms suggestive of subacute combined degeneration (postero-lateral columns) in the presence of normal B12,ophthalmoplegia
Vitamin D Osteomalacia
Vitamin K Bleeding tendencies,defective II,VII,IX,XII
Bone mineralization (Gla proteins)
Vitamin C Scurvy, bleeding sore gums,
peri joint and bone hemorrhages
BM 0096
HPN-LD ComplicationsHPN-LD Complications
• Multifactorial metabolic bone disease
Contributing factors of *Metabolic bone disease associated with HPN
Contributing factors of *Metabolic bone disease associated with HPN
- PN dependent - Patient ’s dependentContinuous > cyclic SteroidsAl in hydrolysates (past) ImmobilisationAl in additives Inflammation / sepsisToo much Ca Age of disease occurrence
Inappropriate vitamine DVitamin K deficit Vitamin K antagonistsVitamin A deficit
Decreased BMI or LBM Mg deficiency Physical inactivityP deficiency Tobacco use
* patchy osteomalacia; low remodeling (resorption> formation)
Metabolic bone disease & LT-HPN- Cross sectional study Cohen-Solal 2003 Pironi 2002 - median age (yr) 52 52- patients (n) 88 165- bone pain 35%- Bone fragility fractures 10% 10%- osteoporosis (T score < 2.5 BMD) 67% 41%- Associated Factors (Z score)
sex - post menopausalage at PN start younger younger BMI + +diseases steroids -
- Longitudinal study Cohen-Solal 2003 Pironi 2004 - patients (n) 56 65- HPN duration (month) 66±15 18±5- BMD evolution (Z score)
Lumbar (trabecular) Increased increased p =0.04
better ≥ 21 yr oldFemoral (cortical) NS change NS change
Cohen-Solal M et al JBMR 2003; Pironi L et al Clin Nutr 2002 & 2004
0 2 4 6 8 10
-2.5
-2
-1.5
-1
-0.5
0
0.5
Lu
mb
ar
sp
ine
Z-
Sc
ore
15y
35y
55y
21y
0 2 4 6 8 10
-2.5
-2
-1.5
-1
-0.5
0
0.5
15y
35y
55y
21y
Figure 2 : Mean change of lumbar spine Z-Score during long term HPN among 56 patients with or without osteoporosis according to the age at IF onset.
To illustrate the results, we chose 3 ages equally spaced within the age-range of our patients, and we calculated the evolution, using the regression equation. As the duration of treatment decreased linearly with age, we did not extrapolate the evolution above the duration of follow-up. The negative evolution under HPN in young patients became positive with aging, and the change was reversed when the patients reached the age of 21. Similar evolutions were observed among patients with osteoporosis. However their Z-Scores were much lower (all values were reduced by 1.1 SD).
With osteoporosisWithout osteoporosis
Duration of HPN (years) Duration of HPN (years)
Cohen-Solql M et al JBMR 2003
Haderslev KV et al AJCN 2002; 76: 482-8.IV Pamidronate (1500 mg/3mo) vs placebo in 20 HPN patients with a T score < 1.
Metabolic bone disease & LT-HPN• Osteomalacia :
- Check vit D metabolites & Ca, P and Mg balances• Low remodeling bone :
- ibid & reinforces Ca, Mg, Vit D metabolites orally- Avoid too much N & Ca IV (calciuria & lower PTH)- Check Al in Blood & in All-in-One (& in renal risk patients ++)
- Check DEXA & BMD at PN start & annually- Check bone markers : osteocalcin & cross laps / deoxypyridinoline
• Specific treatments of osteoporosis :- Biphoshonates ° : positive moderate results at lumbar site,be careful with Ca & vit D status before treatment to avoid deficits
- Near future : trophic factors (GLP2*) or rH-PTH** * Haderslev KV Scand J Gastroenterol 2002; ° Haderslev KV et al Am J Clin Nutr 2002, D ’aoust L et al Clin Nutr 2002 (A)** Khosla S. N Eng J Med. 2003 (editorial)