InvestorsHub Logo
Boards
News
Market Data
Markets
Discover
Discover
Subscribe Login/Register
S&P 500
5,460.48
(
-0.41%
)
US TECH 100
19,181.60
(
-0.43%
)
Dow Jones
39,118.86
(
-0.12%
)
Brent Oil
84.85
(
0.00%
)
Bitcoin
60,887.67
(
0.95%
)

Replies to post #115083 on Avid Bioservices Inc (CDMO)

Replies to #115083 on Avid Bioservices Inc (CDMO)

north40000

03/06/13 11:14 AM

#115085 RE: RRdog #115083

Note particularly[lol] where the following message was posted:

http://investorshub.advfn.com/boards/read_msg.aspx?message_id=85350560

I will remain a neutral observer on this topic over there.
The identified poster is prolific, usually quite informative with absence of expression of personal opinion

Protector

03/06/13 11:41 AM

#115090 RE: RRdog #115083

RRDog, smart and good post.

However, be careful with:

The small molecule value may lie in its ability to also access PS targets inside the cell that have not migrated to the surface.



I ventured there when FTM and goodJohn were in a deep scientific discussion (incl localized and systemic action, activating the immune response, etc, etc of Bavi) and according KT I projected something that was not really what the MOA said (and indeed that was so) when I advance the theory and a mechanism (maybe not the right one but say at least an attempt to support the statement) that Bavi could enter the cell and how it could exist there and remove some of it's activity latency ones something got wrong with the cell because it would already be in place (don't confound with FTM's vaccine post).

But Bavi targeting PS inside the cell wasn't very well accepted on the board (as was my sabotage post in January, as was my Bavi activity latency in Viral post in 2010 after gov contract ended, etc I am getting used to it :) ). Bavi was sabotaged, Bavi's latency is becoming more visual also in oncology (pancreatic ECOG 2 patients) and for Bavi entering the cell we'll have to wait some to know the verdict.

Remember, it was said you need the presence of blood to have all needed molecules to allow Bavi to bind with PS. Since there is no blood inside the cell Bavi can't bind to the PS on the inside of the cell membrane (which was what I claimed could happen to explain how it remained there). Maybe it doesn't bind there but ones past the receptor gate and inside the cell just manages to stay there and floats in the cytoplasm without being destroyed/consumed. Then when the cell is damaged the rest of the story remains the same, Bavi is at its post and can immediately bind with the PS ones blood is present.

Just saying, you know, not asking anybody to believe me. I am a real positive but a pseudo-scientist :)

freethemice

03/06/13 1:58 PM

#115113 RE: RRdog #115083

I don't understand what they mean here since PGN650 is the Fab part of PGN635 and is used
in the 125I-PGN650 imaging molecule. It is not a "better" bavi since it can not bind to
macrophages, DCs using the Fc-gamma receptor, since it doesn't have one.

md1225

03/06/13 2:46 PM

#115127 RE: RRdog #115083

great post RRdog!