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ANTI FIBROTIC POTENTIAL OF NONI

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Excessive Production and deposition of Collagens (elastin and laminin) ... Altered ECM Major producer of fibrotic neomatrix. Altered ECM ... THANKING YOU ... – PowerPoint PPT presentation

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Title: ANTI FIBROTIC POTENTIAL OF NONI


1
ANTI FIBROTIC POTENTIAL OF NONI
2
Liver Fibrosis
  • Liver Fibrosis is Characterized by
  • Excessive Scarring
  • Excessive Production and deposition of Collagens
  • (elastin and laminin)
  • 3. Decreased Collagenolytic activity (1)
  • 4. Altered Extra cellular matrix ( ECM )

3
Biochemical Marker Hydroxy Proline ( HP)
Altered ECM Major producer of fibrotic neomatrix
Altered ECM excess collagen -
Triple Helix structure
Stabilized by
Hydroxy Proline
4
Altered ECM
Degraded by
Matrix Metallo Proteinase (MMP) 2 3
Inhibited by
Tissue Inhibitors of MMP ( TIMPS)
In fibrosis
Excessive Production of TIMPS
TIMPS expression correlates with HP
5
INDUCTION
Liver fibrosis results of repeated repair of
chronic liver damage. Chronic Liver injury
chemicals CCl4. Single dose Liver
Damage Repeated doses Chronic Liver damage.
6
Materials and Methods
Animals - Male Albino Wistar rats Groups I -
Normal II - CCL4 -1 ml/kg mixed with equal
volume of liquid paraffin twice a week for 4
weeks (4) III - 5 ml
of diluted Noni extract in divided
doses.
7
Biochemical Parameters
Aspartate Transaminase (AST IU/L) Alanine
Transaminase (ALT IU/L) Alkaline
Phosphatase ( ALP IU/L) Total
Bilirubin (TBL mg/dl) Hydroxyproline (HP
mg/g of liver)
Other Parameters Body Weight
Liver Weight
8
Effect of Noni on biochemical Parameter
AST ( IU/L)
ALT ( IU/L)
TBL (mg/dl)
ALP ( IU/L)
HP (µg/g of liver tissue)
GROUPS
Groups
I
159 6
47 2
215 7
0.48 .01
53 3
II
289 11
102 5
396 8
1.6 .08
124 7
III
175 8a
61 4a
235 12a
0.7 0.3a
77 3a
  • Significantly different from Group I
  • a Significantly different from Group - II

9
Effect of Noni on liver and Body weight
Body Weight
GROUPS
Liver Weight on Day 28
Day 28
Day 1
I
163 4
3.4 0.3
164 3
165 3
II
1482
4.5 0.06
3.8 0.05a
III
164 2
159 2a
  • Significantly different from Group I
  • a Significantly different from Group - II

10
DISCUSSION
  • Hepatic stellate cells of Liver are associated
    with fibrosis
  • Normally Vit A stores
  • Chronic injury proliferation

Excessive secretion of collagen
Altered ECM
HP
11
  • Level of HP correlates with the extent of
    fibrosis
  • Scope for future study
  • CCL4 ? CCL3 (free radical) ? Lipid peroxidation

Liver damage
  • Antioxidant potential ? confirms the
    antifibrotic potential

12
CONCLUSION
  • AST, ALT, ALP, TBL levels confirm the hepato
    protective potential
  • HP level in group III indicate the antifibrotic
    potential of NONI

13
references
  • Okazaki, I., Maruyama, K.,1974. Collagenase
    activity in experimental hepatic fibrosis. Nature
    252, 49-50.
  • Arthur, M.J.P., 1997. Matrix degradation in liver
    and a role in injury and repair. Hepatalogy 26,
    1069-1071.
  • Ohuchi, E., Imai, E., Fijii, Y., 1997. Membrane
    type I matrix metalloproteinases digests
    interstitial collagens and other extra cellular
    matrix macromolecules.J.Biol.Chem.272,2446-2451.
  • Bickel, M., Baader, E., Brocks, D.G., Engelbart,
    K., Gunzler, V., Schmidts, H.L., Vogel, G.H.,
    1991.Beneficial effects of inhibitors of propyl
    4-hydroxylase in CCl4 induced fibrosis of liver
    in rats.J.Hepatol.13 (Suppl.3),26-33.

14
THANKING YOU
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