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Lecture 8 Toxic Responses in the Kidney?

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Lecture 8 Toxic Responses in the Kidney Anatomical arrangement and organization of the nephrons within the kidney 1 million nephrons in each human ... – PowerPoint PPT presentation

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Title: Lecture 8 Toxic Responses in the Kidney?


1
Lecture 8Toxic Responses in the Kidney?
2
Anatomical?? arrangement and organization of the
nephrons??? within the kidney
  • 1 million nephrons in each human kidney
  • Renal blood flow???? (RBF)
  • 94 to cortex??
  • 5 outer medulla??
  • 1 inner medulla

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What causes kidney stones? Kidney stones form
when there is a decrease in urine volume and/or
an excess of stone-forming substances in the
urine. The most common type of kidney stone
contains calcium in combination with either
oxalate or phosphate. Dehydration?? from reduced
fluid intake or strenuous exercise???? without
adequate fluid replacement increases the risk of
kidney stones. High sugar or salt
diets. Kidney stones can also result from
infection in the urinary tract???? these are
known as struvite or infection stones.
8
Three Basic functions of the nephron
  • Filtration?? at the glomerulus ???
  • Tubular reabsorption??????
  • Tubular secretion?????
  • Amount excreted in urine amount filtered
    reabsorbed secreted by tubules

9
Organization of the Glomerulus
  • Solute up to 10000 M.W. pass through the filter
    freely
  • Diffusion is restricted and ceases around 70000
    M.W. to 100000 M.W.
  • For creatinine???? P x GFR UV
  • P Plasma, U Urine
  • V volume of urine
  • GFRglomerulus filtration rate??????

10
Tubular reabsorption??????
  • Urea??
  • Only 30-70 of the filtered load is excreted
  • Glucose
  • All are reabsorbed
  • Calcium
  • 60 of the filtered (ionized form) is reabsorbed
  • Phosphate 95 reabsorbed
  • Uric acid?? mostly reabsorbed
  • Amino acids 98 reabsorbed

11
Tubular secretion?????
  • Foreign substances
  • Secretion is active, show saturation kinetics
  • Physiological substances
  • Metabolic end-products

12
Major transport mechanisms for solutes and water
across the renal proximal tubules?????
  • 2/3 of the filtered water and sodium are
    reabsorbed per minute
  • Amount reabsorbed are influenced by the balance
    of hydrostatic and osmotic forces in the
    peritubular capillaries?????????.
  • ? colloid osmotic????? or ? hydrostatic
    pressures??? in peritubular capillaries ? ?
    reabsorption

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Loops of Henle?????
  • Run deep into the medulla passing through a
    region of increasing osmolality??? .
  • Thin ascending limb??
  • Impermeable to water, highly permeable to Sodium
    and chloride and moderately permeable to urea
  • NaCl diffuses from tubules back to cortex
  • Thick ascending limb
  • Distal tubules????

14
Major transport pathways in the thick ascending
limb of the loop of Henle
  • Reabsorb NaCl from the tubular fluid by
    energy-dependent process
  • Impermeable to water
  • Luminal fluid becomes hypo-osmotic

15
Distal tubules????
  • NaCl is reabsorbed
  • Early part is impermeable to water
  • Permeability of the last part is determined by
    ADH (antidiuretic hormone?????)

16
Effects of Nephrotoxins???
  • Act on the vascular elements or portion of
    nephron
  • Vasoconstriction???? and ischemia??
  • Decreased glomerular filtration and tubular
    transport
  • Affect the glomerulus directly ? flitration
    dysfunction????
  • Affect tubular activities

17
Nephrotoxins on kidney function
  • Acute toxicity ? alter renal function extensively
  • If it is sublethal??? and of short duration ?
    recovery?? to normal function rapidly
  • Chronic low dose over long period ? extensive
    renal damage
  • Marked changes in renal function may not be
    detected due to the compensatory capacity???? of
    the kidney.

18
Common examples of nephrotoxins Heavy metals
such as lead, mercury, cadmium, and arsenic
exposure to these metals is most often
occupational environments. Nonsteroidal
anti-infalmmatory drugs (NSAIDS????????) such as
ibuprofen???(??????) , naproxen??? , and
ketoprofen??? possibly acetaminophen. Certain
antibiotic medications, notably streptomycin???
and gentamicin???? . Organic solvents such as
benzene.
19
Heavy Metals
  • Exposure to most heavy metals ? renal toxicity
  • Necrotic??? proximal tubules containing
    proteinaceous??? casts
  • Ischemia produced by vasoconstriction ? ? GFR
  • ? dose ? renal failure, renal necrosis, ? BUN
    (Blood urea nitrogen), death
  • Protective mechanism against low-dose heavy-metal
    toxicity was exhausted ? cellular damage

20
Heavy Metal (II)
  • Mercury
  • Elemental, inorganic and organic mercury are
    nephrotoxic
  • Low dose ? affect proximal tubule ? secret
    organic ions
  • Platinum
  • A complication of cisplatin (an antitumor drug)
    therapy
  • Damage to proximal tubule, ion loss ? not able to
    produce concentrated urine
  • Alter GFR, affect distal tubule and collecting
    duct functions

21
Heavy Metals (III)
  • Cadmium
  • Toxicity ? ? synthesis of metal binding protein
    metallothionein in liver
  • The complex ? toxicity to other organs but ?
    nephrotoxicity
  • Toxicity is localized to proximal tubule ? ?
    reabsorption, ion loss (phosphate)
  • Presence of low and high M.W. proteins in urine
    (GFR defects)
  • Other Metals
  • Toxicity observed for chromium (potassium
    dichromate), arsenic, gold, iron, antimony,
    thallium and lead

22
Halogenated Hydrocarbons???
  • Both hepatotoxic??? and nephrotoxic
  • Nephrotoxic metabolites produced
  • Directly by the kidney
  • Produced in the liver and transported to the
    kidney
  • Non-nephrotoxic metabolite produced in the liver
    then transported to the kidney ? further
    biotransformation ? nephrotoxin

23
Carbon Tetrachloride???? and Chloroform??
  • Damage primarily to proximal tubules, secondarily
    to the entire nephron
  • Proximal tubular necrosis
  • Glucosurea, aminoacidurea, proteinurea and ?
    secretion of organic ions
  • Glomerular or distal tubular functions are not
    apparently affected
  • At high dose ? renal necrosis, renal failure, ?
    BUN, dealth

24
Hexachlorobutadiene?????
  • Widespread environmental pollutant
  • Potent nephrotoxic with little hepatic toxicity
  • Low dose ? affect proximal tubules
  • Failure to reabsorb tubular filtrate (glucosurea,
    proteinurea, aminoacidurea)
  • ? secretion of organic ions
  • Necrotic proximal tubules
  • High dose ? renal failure, renal necrosis, ? BUN,
    death

25
Other halogenated hydrocarbons
  • Bromobenzene
  • Hepatoxic and nephrotoxic
  • Nephrotoxic metabolites from liver ? to kidney ?
    damage the kidney tissue directly
  • 2-Bromoethylamine (BEA)
  • Necrosis of loop of Henle and collecting duct
  • Sclerosis of juxtamedullary glomeruli and urinary
    concentration defects
  • Methoxyflurane
  • Produce medullary necrosis and renal failure
  • Not able to produce concentrated urine, ion loss,
    ? BUN and renal failure

26
Analgesics???
  • In humans, chronic ingestion of high doses of
    analgesics (aspirin????, phenacetin???? ,
    acetaminophen??????) ? medullary interstitial
    inflammation, fibrosis, renal failure.
  • Vasoconstriction of the vasa recta???? ? ischemic
    medullary damage
  • Neprotoxic metabolites produced by liver ?
    transport to kidney ? cortical tissue damage

27
Antibiotics???
  • Certain antibiotics (neomycin, gentamicin,
    tobramycin, netilmicin, kanamycin, amikacin and
    streptomycin) possess aminoglycoside side chains
    ? nephrotoxic
  • Damage primarily at the proximal convoluted
    tubule and glomerulus.
  • Changes in the endothelial pore size ? filtration
    dysfunction
  • Tetracyclines??? ? medullary toxins
  • Failure to produce concentrated urine
  • Glucosuria??, aminoaciduria???? , proteinuria???

28
Environment contaminants
  • Herbicides???
  • Affect renal capacity to secrete organic ions
  • Polychlorinated Biphenyls???? (PCB) and
    Polybrominated Biphenyls???? (PBB)
  • Enhance drug metabolizing enzyme systems in
    kidneys ? potential hazard
  • Tetrachlorodibenzo-?-dioxin??? (TCDD)
  • Enhance renal drug metabolizing enzymes, but no
    direct effect on the kidneys shown
  • Mycotoxins????
  • In contaminated animal and human foods ?
    proximal tubular dysfunction and ?organic ion
    transport
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