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Psoriasis Club › HealthHealth Boards › Psoriasis In The News v
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Psoriasis clear 66 months after one subcutaneous injection of trial drug BI 655066

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Psoriasis clear 66 months after one subcutaneous injection of trial drug BI 655066
Fred Offline
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#1
News  Sat-01-11-2014, 17:57 PM
New drug BI 655066 moves on to phase 11 trial after showing psoriasis clearance for 66 months after one single dose Dr. James G. Krueger reported at the annual congress of the European Academy of Dermatology and Venereology. Yes you heard it right 66 months that's 5.5 Years. eek

Quicky version:

Key clinical point: Up to 66 months after receiving a single subcutaneous injection of a biologic agent that selectively blocks interleukin-23, six patients with moderate to severe chronic plaque psoriasis at baseline remained PASI 100 responders with clear skin.

Major finding: The PASI 75 response rate 12 weeks after receiving a single dose of the investigational agent BI 655066 was 87%, and the PASI 90 rate was 58%.

Data source: This was a first-in-humans, proof-of-concept study involving 39 psoriasis patients.


Longer version:
Quote:
“For me, this is one of the most interesting features of this proof-of-concept study,” he added. “If this kind of activity is confirmed in the ongoing phase IIb trial, I think this represents the potential for very long-term disease modification. This could become an important agent in the future to treat psoriasis.”

BI 655066 is a monoclonal antibody that specifically targets the p19 subunit of interleukin (IL)-23. Unlike ustekinumab (Stelara), which blocks both IL-23 and IL-12, BI 655066 selectively blocks only IL-23, which Dr. Krueger believes is the central driving force in activating and sustaining the T-cell subsets responsible for the hyperproliferative and inflammatory reactions that define psoriasis.
“This study is all about testing for the specific pathogenic contribution of IL-23 to psoriasis in a first-in-humans study.

Our findings really emphasize the importance of IL-23 in driving the key pathways of psoriasis,” observed Dr. Krueger, professor of investigative dermatology and director of the Milstein Medical Research Program at Rockefeller University, New York.
The study included 39 patients with moderate to severe plaque psoriasis. Their baseline PASI was 18, and they averaged more than a 20-year history of psoriasis. Twenty-four patients were randomized 3:1 to a single intravenous injection of BI 655066 at various doses ranging from 0.01 mg/kg to 5 mg/kg or to placebo in order to get an initial sense of the agent’s safety and tolerability.
In the second part of the study, 15 other participants received a single subcutaneous injection: two got placebo and the rest were randomized to BI 655066 at either 0.25 mg/kg or 1.0 mg/kg. Safety and efficacy were assessed at weeks 0, 2, 4, 12, and 24. In addition, skin biopsies were obtained at weeks 0 and 8 for immunohistochemistry studies and RNA sequencing analysis.

By week 12, the PASI 75 response rate in subcutaneous BI 655066 recipients was 87% and the PASI 90 rate was 58%. At week 24, nine patients elected to continue structured prospective follow-up while remaining off treatment, including six PASI 100 responders. Those six PASI 100 responders remained PASI 100 at ongoing follow-up 48-66 weeks after receiving their single dose of the agent.

Biopsy specimens obtained at week 8 showed normalization of the epidermal psoriasiform hyperplasia which had been present at baseline. A normal-looking granular layer had been reestablished. “This looks essentially like the pattern of normal or nonlesional skin,” according to the dermatologist.

RNA sequencing analysis and gene profiling showed normalized production of the IL-23/IL-17-induced proteins that had been strongly overexpressed at baseline, including lipocalin, beta-defensin, and psoriasin.

“The immune axis is turned down. The number of immune cells is way down, although they’re not completely eliminated. With placebo, you still see a psoriasislike pattern of the disease. With blockade of IL-23, most cases have a gene profile like nonlesional skin. This represents a profound cellular and disease modulation,” Dr. Krueger said.

Among all 39 participants, the only serious adverse event deemed possibly treatment related was a 5-minute transient ischemic attack (TIA) episode in a patient on BI 655066. This caught Dr. Krueger’s attention as a possible red flag; however, he noted that more than 200 patients have since received the biologic agent in the ongoing phase IIb trial, with no reported major adverse cardiovascular events.

“I think that TIA may just be bad luck with small numbers,” he added.

Asked what he thinks might explain the remarkably lengthy disease remission seen following a single dose of the biologic, Dr. Krueger offered two possibilities.

“It may be that IL-23 is necessary to sustain pathogenic clones of memory cells in the skin, and as we get rid of it those clones most likely apoptose. And if you’ve sufficiently removed the clones, then you don’t get the expansion. That’s guess one. Guess two would be that we’ve renormalized tolerance mechanisms in some way. Both of these hypotheses can be tested,” according to Dr. Krueger.

Source: skinandallergynews.com

*The study was funded by Boehringer Ingelheim.
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jiml Offline
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#2
Sat-01-11-2014, 18:32 PM
Wow that's a good one for the future . I will follow the progress of this with great interest It's a great drug from the sound of it with no real adverse side effects...... Things are moving very fast with the drug companies..... I am guessing it will be expensive when it does go to market as they aren't going to sell much a single shot every four to five years
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Fred Offline Author
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#3
Sat-01-11-2014, 22:13 PM
(Sat-01-11-2014, 18:32 PM)jiml Wrote: Wow that's a good one for the future .

It is Jim but the problem I have with it is 5 years between treatment although sounds good, what if things go wrong. ?

For example the other day I was saying to Sarah to miss her next shot of Humira as she may have a virus, now Humira is taken usually every two weeks, Enbrel is two shots per week, and Stelara is one shot every 3 months.

Now when I felt rough whilst on Enbrel I would just stop, and restart once I felt ok again. But if I feel rough just after my shot of Stelara I'm stuck and will just have to get on with it.

So five years between treatment is something I would have to consider very strongly before going on to it.
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Bill Offline
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#4
Sun-02-11-2014, 09:52 AM
Come on, Fred. A once in 5 1/2 year treatment with minimal side effects? I'd take it in a heartbeat, and hopefully my heart would keep beating. The memory cell hypothesis is interesting. DMF suppresses the expression of IL-23 from dendritic cells, so it may also reduce the number of memory cells. Fits with the way my disease has changed.

Cheers,

Bill
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Fred Offline Author
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#5
Sun-02-11-2014, 12:08 PM
(Sun-02-11-2014, 09:52 AM)Bill Wrote: Come on, Fred. A once in 5 1/2 year treatment with minimal side effects? I'd take it in a heartbeat, and hopefully my heart would keep beating.

Big Grin

At least it was only 1 case and lasted 5 minutes.
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Bill Offline
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#6
Sun-02-11-2014, 12:14 PM
True enough, Fred, and thanks for the info.

Cheers,

Bill
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Fred Offline Author
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#7
Sun-02-11-2014, 12:29 PM
(Sun-02-11-2014, 12:14 PM)Bill Wrote: True enough, Fred, and thanks for the info.

Cheers,

Bill

You're welcome Bill let us know if you make your own version. Rolleyes
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Kit Offline
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#8
Tue-08-03-2016, 14:10 PM
Having read through this thread I wondered if there was any more news on this trial

I found another online article on the "PMLIVE" website regarding BI 655066 which was dated 9th October 2015.   (I've removed as many links as I could locate)

/Quote:  

Boehringer says anti-IL-23 drug beats Stelara in psoriasis trial
Interleukin-23 inhibitor outperforms Johnson & Johnson's blockbuster
Boehringer HQ
New data from a phase II trial of Boehringer Ingelheim's psoriasis candidate BI 655066 back up earlier results showing it is more effective than a rival drug from Johnson & Johnson.
After nine months' treatment, 69% of moderate-to-severe plaque patients treated with the highest dose (180mg) of Boehringer's interleukin-23 inhibitor had clear or almost clear skin, compared to 30% of patients treated with J&J's Stelara (ustekinumab), which blocks both IL-12 and IL-23.
Patients on BI 855066 also achieved this level of skin clearance in around eight weeks - around half the time recorded for Stelara, and the response lasted for around two months longer (32 weeks versus 24 weeks), according to the company.
"Achieving clear skin quickly and maintaining clearance is an important goal for patients that have to deal with the daily impact of psoriasis," said the study's lead investigator, Kim Papp of Canada's Probity Medical Research.
Boehringer also reported updated phase II results - originally released in March which showed that after 12 weeks of treatment, BI 655066 achieved nearly-clear skin in 81% of patients, compared to 30% of the Stelara group. At the time, Papp said that the study suggested Stelara's IL-12 activity was making little or no contribution to the drug's efficacy.
Stelara achieved sales of $1.3bn last year as a better-tolerated alternative to tumour necrosis factor (TNF) inhibitors in psoriasis therapy, but looks set to come under significant pressure from new drugs which have shown superior efficacy in trials.
That list includes Novartis' IL-17 inhibitor Cosentyx (secukinumab), recently approved for psoriasis in US, Europe and Japan, and AstraZeneca's brodalumab which hits the same target. 
Meanwhile, the market for non-TNF-based therapies for psoriasis looks set to get increasingly crowded, with two other IL-23 inhibitors - J&J's guselkumab and Merck & Co/Sun Pharma tildrakizumab - both reporting phase II clinical data in the last few months, and Lilly's anti-IL-17 drug ixekizumab also progressing through late-stage testing.

/End Quote.

I'm a bit confused.  The original article which must have been written before November 2014, seemed to refer to a single dose which - at that time - had kept at least one triallists skin clear for 66 months (and counting?)

This article refers to several months or several weeks of treatment in different paragraphs   - perhaps indicating a course of treatments of some kind?  Dunno. More research on my part needed.    However it still looks very promising for those that could afford it.  I cant see this being cheap somehow.
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Fred Offline Author
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#9
Tue-08-03-2016, 14:13 PM
Pssssssssssssst New psoriasis treatment BI 655066 worked faster than Stelara  Whistle

EDIT: Put wrong link in.

But here his the latest: AbbVie and Boehringer Ingelheim to develop and commercialize BI 655066
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D Foster Offline
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#10
Tue-08-03-2016, 18:05 PM
This sounds really good, the cost will be high but how much would 5 years of Stelara cost !!
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