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Late Dx, GI keen on Biologics this week (skipping vax)

I had a lot of early warnings (fatigue, pains, brain fog) for decades but only confirmed fistulizing Crohns Colitis recently. (Lots or allergies, then a shrug and a loose diagnosis of IBS 15 years ago). A relief to know but annoying that many indicators they were relying upon to not dive deeper are not useful. Now seemingly on my own navigating vaccines and method of treatment, as specialist is angling for Infliximab biosimilar ASAP without regard to immunities, and is unavailable for months on end. Vaccine specialists are slow going and having a hard time charting a clear course, again me trying to angle for the coverage recommended by IBD societies and medical journals. Fun!

I have a couple burning questions with some urgency below (talking to GI at the end of the week), but if you want more context:

I had a bad abscess a few years ago, requiring several days in hospital, plus a month of near daily visits to deal with dressings etc. It recurred last fall, with what turned out was my worst flare. I was “fast tracked” for a scope in January. Out of the gate barely coming to after scope, GI said we’ll race thru a number of meds, but more than likely land on a biologic. First 5ASA did nothing, 2nd Steroid could have killed me, 3rd I believe nearly did (after about a week of GP’s scrambling and GI MIA, I stopped meds and came back to reasonable life. A fill-in GI actually noted that some immunities were lower than desired, which caused me to look closer into that whole line. They started me on a high dose of Prednisone for a “short span” until I could start biologics - was great until I started tapering (a friend tells me I should have had a complimentary chill drug and been off work - lucky I still have a job and relationship, but both have been tenuous). I’ve stabilized on 10mg Prednisone to undertake vaccines while hopefully keeping IBD in check. Thinking of dosing down further and trying some herbs as I see long term prednisone effects can be nasty, mood is better but still far from ideal, and it looks like it will a while until I can actually start biologics. I like the occasional beverage, which everyone from pharmacists to docs say is fine in moderation (I skipped entirely until 10mg to be safer), but is it?

Questions:

1. Vaccines: Does anyone know with certainty if measles immunity marker simply means you’re covered? Or in the age of antivaxxers and outbreaks does it make sense to get another dose? I have come across info which suggests it does deteriorate, but have not really found titre level recommendations - or even blood work beyond “(non)reactive”.

2. Vaccines: I’m one dose into Live Varicella (chickenpox), and vaccine people are recommending I complete a second dose Varicella, plus 2 inactivated Shingrix series prior to biologics (or other immune suppressants). If you have any info pertaining to my IBD (fistulizing Crohn’s Colitis) and the balance of racing to treatment vs immunizing first, I would love to hear it.

3. Treatment: They’re “recommending” (telling) me for Inflectra (Infliximab Remicade biosimilar)... and I’m wondering if I could really start with a less invasive biologic first? A few doc friends are pretty shocked they’re not really discussing options and repercussions, which I think is just this GI’s style of “being in charge”. (I received a fuzzy 2pg handout with half of the web links which were dead). I can appreciate that Infliximab actually has a touch of medical evidence of being applicable and useful for the fistulizing variant, however I see many posts here which refute that, plus I see anecdotal notes that other biologics such as Humera and Stelara may be useful in that regard. As I have had more time to look into (and stumble upon) info, I have found that people find the IV treatments such as Remicade fairly restrictive. I travel for work regularly plus like the idea of a less institutional treatment. I get phone calls from the drug company “nurse” most weeks, asking if I’m ready to start, if I really need vaccines, etc. So, is it just a coin toss here, or should I really go with something which will fit my preference?

4. Treatment: How likely are Anti-rejection/complimentary treatments? And what do you think of them? If you’ve made it this far (serious thank you), you’re probably getting the picture that this likely wouldn’t be presented as an option, just “matter of fact, this is what you need”. I’m already iffy on Infliximab, and more so if they want to pair it with MTX or something, which further suppresses immune system and increases chance of side effects. Aside from keeping me alive in the moment, I’m not a fan of being cornered into more iffy drugs than I signed up for. I understand that you only switch a biologic if you fail, not if you’re uncomfortable with side effects or procedures.

5. Ok to fly?: I haven’t really found useful info on how long to wait before regional or international travel. Mentioning that I travel for work to Infliximab drug company, they said I shouldn’t be going anywhere for ~ 3 weeks on starting. I see on forums like this that some people have a bad reaction -6mo into treatment. Should I postpone treatment until returning from upcoming international travel? Or just try to get a decent induction window ahead of it. How about regionally, which would typically involve being a flight or two away from home (mid-major centres), and occasionally a 1.5 days drive away from a health centre of substance.

6. Denial: Once they make a diagnosis, do they ever change their mind? It seems to fit with a good chunk of my life, but I am gobsmacked they didn’t find it in the last 20 years, including previous scopes.

I’m really happy I found this site, as I have been reading medical journals and society recommendations more nights than not, typically until 3am. Thank you for your time to read and comment!
 

Lisa

Adminstrator
Staff member
Location
New York, USA
Questions:

1. Vaccines: Does anyone know with certainty if measles immunity marker simply means you’re covered? Or in the age of antivaxxers and outbreaks does it make sense to get another dose? I have come across info which suggests it does deteriorate, but have not really found titre level recommendations - or even blood work beyond “(non)reactive”. Not sure on this one....

2. Vaccines: I’m one dose into Live Varicella (chickenpox), and vaccine people are recommending I complete a second dose Varicella, plus 2 inactivated Shingrix series prior to biologics (or other immune suppressants). If you have any info pertaining to my IBD (fistulizing Crohn’s Colitis) and the balance of racing to treatment vs immunizing first, I would love to hear it. Once you start on a biologic, live vaccines are NOT supposed to be given. Reading your post, I gather you were never vaccinated for these diseases as a child? Are you in the US or another country?

3. Treatment: They’re “recommending” (telling) me for Inflectra (Infliximab Remicade biosimilar)... and I’m wondering if I could really start with a less invasive biologic first? A few doc friends are pretty shocked they’re not really discussing options and repercussions, which I think is just this GI’s style of “being in charge”. (I received a fuzzy 2pg handout with half of the web links which were dead). I can appreciate that Infliximab actually has a touch of medical evidence of being applicable and useful for the fistulizing variant, however I see many posts here which refute that, plus I see anecdotal notes that other biologics such as Humera and Stelara may be useful in that regard. As I have had more time to look into (and stumble upon) info, I have found that people find the IV treatments such as Remicade fairly restrictive. I travel for work regularly plus like the idea of a less institutional treatment. I get phone calls from the drug company “nurse” most weeks, asking if I’m ready to start, if I really need vaccines, etc. So, is it just a coin toss here, or should I really go with something which will fit my preference? Not sure what you mean by a less invasive biologic? As for fistulizing disease, from what I have seen/read/own experience it can be VERY beneficial - with other biologics being LESS beneficial with regrds to healing fistulae. Personally, I find being on Remicade is less restrictive also, I only need to shcedule around 1 day every 8 weeks, vs. getting syringes delivered, storage, etc. if I were on Humira for example.

4. Treatment: How likely are Anti-rejection/complimentary treatments? And what do you think of them? If you’ve made it this far (serious thank you), you’re probably getting the picture that this likely wouldn’t be presented as an option, just “matter of fact, this is what you need”. I’m already iffy on Infliximab, and more so if they want to pair it with MTX or something, which further suppresses immune system and increases chance of side effects. Aside from keeping me alive in the moment, I’m not a fan of being cornered into more iffy drugs than I signed up for. I understand that you only switch a biologic if you fail, not if you’re uncomfortable with side effects or procedures. When I started Remicade, I was also on 6MP, but eventually stopped that, so I've been on only Remicade now for quite a few years. You do not want to be switching back and forth between biologics, if something works, it is usually better to stay on it as long as possible, which leaves a bigger window open usually for other medications to be used if one stops working effectively.

5. Ok to fly?: I haven’t really found useful info on how long to wait before regional or international travel. Mentioning that I travel for work to Infliximab drug company, they said I shouldn’t be going anywhere for ~ 3 weeks on starting. I see on forums like this that some people have a bad reaction -6mo into treatment. Should I postpone treatment until returning from upcoming international travel? Or just try to get a decent induction window ahead of it. How about regionally, which would typically involve being a flight or two away from home (mid-major centres), and occasionally a 1.5 days drive away from a health centre of substance. Are you asking about when you have your loading doses? With Remicade, there are loading doses that are given initially, then 1 at 2 weeks then a 3rd 4 weeks later. Then the initial schedule is routinely every 8 weeks. This can be shortened if necessary. Once on a routine schedule, flying should not be an issue. Reactions usually occur during or within a day or two of getting an infusion, I've been on it long enough that I don't plan andything special around my infusion day. In fact, I usually work a half day, get my infusion then go home. Back to work the next day. I've also gotten an infusion and gone TO work if that's what my schedule allowed. I've flown almost every year, so far flights haven't fallen too close to infusion days, but I've traveled within the US and also outside with no issues. I also travel for work fairly often, being on the road for days at a time, 2-3 hours from home. In fact, I hit the road on the 24th, (have my infusion on the 23rd) and will be gone for 5 days. No worries on my end about it.

6. Denial: Once they make a diagnosis, do they ever change their mind? It seems to fit with a good chunk of my life, but I am gobsmacked they didn’t find it in the last 20 years, including previous scopes. Diagnosis can be a tricky thing, especially since people present quite differently. Diagnoses can go between Crohns/Ulcerative Colitis, but usually once the Crohns' diagnosis is made that is kept, as there are specific pathological changes that are noted with that.

I’m really happy I found this site, as I have been reading medical journals and society recommendations more nights than not, typically until 3am. Thank you for your time to read and comment!
 

Scipio

Well-known member
Location
San Diego
I'll take a shot:

1. How old are you? Are you "covered" with a prior immunization? Or if you are older you may be covered because you actually had the measles. If the former, a booster immunization might be a good idea. If the latter there is very little chance you will catch the measles a second time, so no vaccine necessary.

2. I'm already on a biologic, and the way I work it with vaccines is I get the immunization 1 to 2 weeks before the next infusion/injection of the biologic is due. That way the biologic is near its lowest levels in your blood and less likely to depress the immune response to the vaccine. You need to allow the vaccine a week or two to kick in before the suppressive biologic gets boosted, so that's why I don't get the immunization the day before the infusion. This isn't a validated medical protocol - It's just my own strategy based on what makes sense immunologically.

3. The doc probably wants to start with infliximab or similar because infliximab is the only biologic proven to be sometimes effective in closing fistulae. Some of the "less invasive" biologics might also help your fistula but they have less or no data to demonstrate that. Infliximab does have such data. If I had a fistula I definitely would start with infliximab.

4. I stay away from pretty much all unproven therapies. Some of them may help, but I'm going to wait until there is robust data proving that before I get on board. However, pairing a biologic with an immunsuppressive such as MTX or azathioprine has been proven to be beneficial in preventing the formation of anti-drug antibodies which can inactivate the drug. Using these drugs, especially with infliximab and Humira, is pretty routine practice these days. Newer drugs such as Entyvio and Stelara appear to be less immunogenic, so the need for an accompanying immunosuppressant is less. They are more commonly given alone as monotherapy.

5. I would not plan any travel for the first few days after your first infliximab treatment, just in case there is some adverse reaction to the infusion. But after that I'd base it more on how you feel than on any arbitrary dates. If you feel well enough, and your Crohn's is controlled well enough that you can travel okay, then IMO it's probably okay to travel.

6. I don't think docs "change their minds" about a diagnosis so much as they get new information that leads them to a different conclusion. Sometimes it's very difficult to tell the difference between IBS and IBD. Sometimes it's very hard to tell the difference between Crohn's and UC. So depending on how strong the evidence for Crohn's is in your particular case, there may or may not be any chance that they might arrive at a different diagnosis when given new information.
 
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Thanks very much Lisa and Scipio.

I’m 42 and in Canada. Never had chickenpox, or the vaccine (until now). I had 1x MMR as a kid. Tests indicate I have “normal person” immunity to measles, today. But I’m not normal, and what about a year or two from now?

By less invasive biologic, I largely am referring to the whole process: extra regular tests, going to a medical center for treatment, getting an IV so frequently, mouse protein...


2. Makes sense. Do you find that you get sick more frequently, on a biologic?

3. I am leaning that way, but wanted to see if anyone has had luck with fistulas and a different biologic.

4. Are u on a combo?

5. Travel: I suppose I could bail if I feel like crap, but my trips are generally lined up weeks in advance.

6. Is there a known role of poor water contributing to contracting or worsening disease? Or again mistaking disease? Our water is terrible.... often tastes like chemical.

I'll take a shot:

1. How old are you? Are you "covered" with a prior immunization? Or if you are older you may be covered because you actually had the measles. If the former, a booster immunization might be a good idea. If the latter there is very little chance you will catch the measles a second time, so no vaccine necessary.

2. I'm already on a biologic, and the way I work it with vaccines is I get the immunization 1 to 2 weeks before the next infusion/injection of the biologic is due. That way the biologic is near its lowest levels in your blood and less likely to depress the immune response to the vaccine. You need to allow the vaccine a week or two to kick in before the suppressive biologic gets boosted, so that's why I don't get the immunization the day before the infusion. This isn't a validated medical protocol - It's just my own strategy based on what makes sense immunologically.

3. The doc probably wants to start with infliximab or similar because infliximab is the only biologic proven to be sometimes effective in closing fistulae. Some of the "less invasive" biologics might also help your fistula but they have less or no data to demonstrate that. Infliximab does have such data. If I had a fistula I definitely would start with infliximab.

4. I stay away from pretty much all unproven therapies. Some of them may help, but I'm going to wait until there is robust data proving that before I get on board. However, pairing a biologic with an immunsuppressive such as MTX or azathioprine has been proven to be beneficial in preventing the formation of anti-drug antibodies which can inactivate the drug. Using these drugs, especially with infliximab and Humira, is pretty routine practice these days. Newer drugs such as Entyvio and Stelara appear to be less immunogenic, so the need for an accompanying immunosuppressant is less. They are more commonly given alone as monotherapy.

5. I would not plan any travel for the first few days after your first infliximab treatment, just in case there is some adverse reaction to the infusion. But after that I'd base it more on how you feel than on any arbitrary dates. If you feel well enough, and your Crohn's is controlled well enough that you can travel okay, then IMO it's probably okay to travel.

6. I don't think docs "change their minds" about a diagnosis so much as they get new information that leads them to a different conclusion. Sometimes it's very difficult to tell the difference between IBS and IBD. Sometimes it's very hard to tell the difference between Crohn's and UC. So depending on how strong the evidence for Crohn's is in your particular case, there may or may not be any chance that they might arrive at a different diagnosis when given new information.
 
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Scipio

Well-known member
Location
San Diego
2. Makes sense. Do you find that you get sick more frequently, on a biologic?
No, I get the same one or two colds a year, but I do think they last longer than they did before. What used to be a 1-week cold now takes two weeks to clear up, and what used to be a harsh 2-week cold can now drag on for a whole month.

4. Are u on a combo?
No, but if I were on Remicade or Humira I probably would be. I'm on Stelara without an immunosuppressant combo. The newer biologics like Entyvio and Stelara are turning out out be a lot less immunogenic than the Remicade and Humira and thus are less likely to need a combo drug to prevent antibody formation. On the downside, Stelara and Entyvio both take a lot longer to work than the anti-TNFs and do not (yet) have proven fistula-closing abilities.


6. Is there a known role of poor water contributing to contracting or worsening disease? Or again mistaking disease? Our water is terrible.... often tastes like chemical.
I've never heard of Crohns' diagnosis or misdiagnosis being linked to bad water, but it's probably not been studied much either. Like anything else it would depend on what is in the water to make it "bad."
 
I'm so sorry it took them so long to make a diagnosis, and it sounds like they're not given much information on the medicine. I can relate to being up in the middle of the night reading medical journals.

I also relate to not know if one can travel, as I fly for work.

For the measles shot, my husband and I recently got another shot because we weren't sure if our parents had gotten us 2 shots as kids. Anyways, nurse told us it doesn't hurt to get more measles shots. With international travel these days, and the resurgence of measles, you'd be sure you were covered if you've already had 1 shot. If there's any question about the first shot, I think it's 30 days between both shots.

I'm going to get the shingles shot. I had chickenpox as a kid, so I need the shingles shot. But if you never had chicken pox, and you get vaccinated for Chickenpox, would you need the shingles shot? I have no idea, but you might ask your GP that question. Shingles is horrible and so scary about possible blindness issues if it goes into the eyes. Seems worth it to get immunized if at all possible before starting meds.

Good luck with everything!
 
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I'm meeting with the specialist next week, and have been thinking about questions I have regarding various medicines.

You may want to get a second opinion if your GI is not detailing pros and cons of different biologics. I'd want the GI to explain why the biosimilar was recommended vs. another medicine like, say, Entyvio. I follow some GIs on twitter, and at one of their conferences this year, lots of promising research about Entyvio. (Not that it's appropriate for everyone.) But I'd want to know why Entyvio, Humira, and other biologics were ruled out by the doc.

I've read the first biologic is an important choice. (fyi - not knowledgable in this area. I am confused about which biologics works directly on TNF and which have other mechanisms. But I've gotten the impression the first choice of biologic med is important.)

Good luck with your meeting with the GI this week!
 

my little penguin

Moderator
Staff member
Remicade has the most success with fistulas that is known
Does have the pain of infusion but most insurances want it infused at home with home health
You can schedule out way in advance once every 6-8 weeks and it can be a few days either way.
Takes 6 weeks to be effective and dose can be adjusted (5 mg/kg up to 10 mg/kg) and timing of infusions from every 4weeks to every 8 weeks if needed


Humira is a shot but must be given every two weeks sometimes every week .
Insurance only sends one month at a time (typically) and must be stored cold but not frozen (or used within 14 days so travel would need to be planned around shipments with less ahead of time notice
Takes 3-5 months to work
Dose can NOT be adjusted only one dose
40 mg
Schedule can be adjust to every 5 days to every 14 days
Both are anti tnf

Entyvio has the most success with ulcerative colitis limited success with crohns
Takes 6 months minimum for crohns (only 27% success rate )


Introduction
Inflammatory bowel disease (IBD) is a chronic idiopathic inflammatory condition of the intestines of a relapsing and remitting nature. IBD is often associated with high morbidity due to both disease‐ and treatment‐related complications. Up to 50% of patients with Crohn's disease (CD) and 30% of patients with ulcerative colitis (UC) may require surgery in their life time.1 The addition of anti‐TNF therapies to the treatment armamentarium since 1997 was a paradigm shift, especially in the setting of fistulizing CD and acute severe colitis.2 This is the first medication class that changes natural history by decreasing the risk of surgery and hospitalization, especially when used early in the treatment course.3
However, up to one‐third of patients do not respond to anti‐TNF agents.2 For patients who respond initially, approximately 40% ultimately stop responding due to subtherapeutic drug levels, the development of antidrug antibodies, or because of mechanistic escape where another cytokine may become more important in disease pathogenesis.4 Furthermore, a small minority of patients may require change in treatment class due to adverse effects, for example, drug‐induced lupus, psoriasis, or demyelinating disease.
Vedolizumab, an anti‐integrin α4β7 antibody, and ustekinumab, an anti IL12/23 p40 antibody, now offer alternatives to patients in whom a change in treatment class is needed. In this article, we review the efficacy and safety data of vedolizumab and ustekinumab, as well as their limitations in guiding clinical decision on choices of biologics.
Vedolizumab
Efficacy
Registration trials and postmarketing reports
Vedolizumab is the first gut‐selective biological agent. It inhibits integrin α4β7, thus inhibiting lymphocyte trafficking from the blood vessel to the intestine. Its efficacy in induction and maintenance of remission for CD and UC, both in anti‐TNF‐naïve and anti‐TNF‐experienced patients, is well documented in registration trials and postmarketing cohort studies (Table 1). The efficacy of vedolizumab in CD at the induction phase was, however, modest in GEMINI 2. Although the vedolizumab group achieved a modest but significantly higher remission rate than the placebo, (14.5% vs 6.8%, respectively, P = 0.02), the CDAI‐100 response rate was not significant.5 This is likely because of CD being a transmural disease and the slow inductive effect of vedolizumab. Rather than having an end‐point at week 6, an end‐point at week 14 may be more appropriate, where a peak effect would be expected.6 Furthermore, up to 50% of the study cohort did not receive concomitant corticosteroids, which could have improved the response rate.7 Although there appears to be a lower percentage point difference with the placebo in CD than in UC during the induction phase, the percentage point difference with the placebo at week 52 appears to be comparable for both diseases.8, 9
Table 1. Efficacy data of vedolizumab in registration trials and postmarketing cohort studies
StudyDesignPatientsAnti‐TNF experiencedEfficacy
Registration trials
Feagan et al.9(GEMINI 1)Randomized controlled trial, phase 3UC: 895TNF failure: 48%At W6:
Clinical response: 47.1% (VDZ) vs25.5% (PBO), P < 0.001
At W52:
Clinical remission: 41.8% (VDZ q8w) vs44.8% (VDZ q4w) vs24.8% (PBO), P < 0.001
Sandborn et al.5(GEMINI 2)Randomized controlled trial, phase 3CD: 1115TNF failure: 63.8%At W6:
Clinical remission: 14.5% (VDZ) vs 6.8% (PBO), P = 0.02
CDAI‐100 response: 31.4% (VDZ) vs25.7% (PBO), P = 0.23
Sands et al.80(GEMINI 3)Randomized controlled trial, phase 3CD: 416TNF failure: 75.7%At W6:
Clinical remission: 15.2% (VDZ) vs12.1% (PBO), P = NS
At W10:
Clinical remission: 26.6% (VDZ) vs12.1%, P = 0.001
Sands et al.8GEMINI 2 and 3 trials (post hocanalysis)CD: 1476TNF naïve: 35%Clinical remission at W52:
TNF naïve: 48.9% (vs26.8% PBO)
TNF failure: 65%
TNF failure: 27.7% (vs 12.8% PBO)
Noman et al.81(GEMINI LTS)Single arm, open label, phase 3CD: 24TNF failure: 100%Mucosal healing:
UC: 34
CD: 29% (median 33 months)
UC: 50% (median 31 months)
Postmarketing cohort studies
Allegretti et al.17Retrospective multicenterCD: 96
UC: 40
Not clearAt W54:
CD:
Clinical response/remission: 52%
UC:
Clinical response/remission: 65%
Amiot et al.82Retrospective multicenterCD: 173
UC: 121
TNF failure: 99%At W14:
CD:
SFCR: 31%
Clinical response: 51%
UC:
SFCR: 36%
Clinical response: 50%
Amiot et al.83Prospective multicenterCD: 161
UC: 111
TNF failure: 99%At W54 (SFCR):
CD: 27.2%
UC: 40.5%
Baumgart et al.84Prospective multicenterCD: 97
UC: 115
TNF failure:At W14 (clinical remission):
CD: 94.8%
UC: 75.7%
CD: 23.7%
UC: 23.5%
Dulai et al.12 (US VICTORY)Retrospective multicenterCD: 212TNF failure: 90%At W52:
Clinical remission: 35%
Mucosal healing: 63%
Deep remission: 26%
Eriksson et al.85(SWIBREG)Prospective multicenter national registryCD: 147
UC: 92
IBD‐U: 7
TNF failure: 86%At median follow up of 17 (IQR: 14–20) months:
CD: 54% (clinical remission)
UC: 64% (clinical remission)
Kopylov et al.86Prospective multicenterCD: 130
UC: 69
TNF failure: 92.6%At W14:
CD: Clinical remission: 34.6%
SFCR: 29.2%
UC: Clinical remission 28.4%
SFCR: 24.3%
Shelton et al.87Prospective multicenterCD: 107
UC: 59
IBD‐U: 6
TNF failure: 97.1%At W14:
CD: Clinical response: 48.9%
Clinical remission: 23.9%
UC: Clinical response: 53.9%
Clinical remission: 29.3%
Singh et al.88Retrospective multicenterCD: 30
UC: 22
TNF failure: 90%At W14:
CD: Clinical remission:42%
UC: Clinical remission: 76%
Stallmach et al.89Prospective multicenterCD: 67
UC: 60
TNF failure:At W54 (clinical remission):
CD: 91%
UC: 81.7%
CD: 21%
UC: 25%
Vivio et al.90Prospective single centerCD: 30
UC: 21
TNF failure:At W14:
CD: 96.7%
UC: 76.2%
CD: improvement in CDAI score (mean 35 points, P = 0.04)
UC: clinical remission (55%)
  • † Deep remission: clinical remission + mucosal healing.
  • MH, mucosal healing; PBO, placebo; SFCR, steroid‐free clinical remission.

Long‐term efficacy data of patients in the GEMINI 1 and two studies who received 152 weeks of continuous vedolizumab were reported in GEMINI LTS. These included patients who responded at week 6 of the GEMINI study and completed 1 year of maintenance vedolizumab (either every 8 weeks or every 4 weeks) before receiving open‐label vedolizumab every 4 weeks in GEMINI LTS. When data were analyzed conservatively, with incomplete data considered to represent treatment failures, the clinical remission for CD (GEMINI 2) was 71, 69, and 43% at weeks 52, 104, and 152, respectively.10For UC (GEMINI 1), clinical remission was 74, 78, and 46% at week 52, 104, and 152, respectively.11Anti‐TNF‐naïve patients responded better to vedolizumab compared with anti‐TNF‐experienced CD patients.8, 10 For UC, however, both groups appeared to have responded equally well.11 For patients where vedolizumab treatment was interrupted for medical or nonmedical reasons, retreatment was successful for both CD and UC patients with no increase in anti‐vedolizumab antibody regardless of the duration of time from last vedolizumab dose.10 Similar to anti‐TNF agents, a relatively lower vedolizumab level was noted in the secondary nonresponders in the GEMINI 2 cohort. Shortening the dosing interval to every 4 weeks could be considered salvage therapy, with up to 45% of the treatment response recaptured in the GEMINI LTS cohort.10
Mucosal healing
Significant mucosal healing in UC with vedolizumab was reported in the GEMINI 1 trial at week 6 [40.9% (vedolizumab) vs 24.8% with placebo, P = 0.001] and week 52 (56% [vedolizumab Q4W] vs 51.6% [vedolizumab Q8W] vs 19.8% [placebo], P < 0.001).9While endoscopy data were not reported in the GEMINI 2 and 3 trials, GEMINI LTS has observed mucosal healing in 29% patients at a median of 33 months for CD.8 A postmarketing report observed mucosal healing in 63% of patients at week 52 for CD.12
Immunogenicity
Overall immunogenicity for vedolizumab appears to be low in comparison with conventional anti‐TNF agents. When patients who received/had not received concomitant immunosuppressant at baseline were compared, the risk of developing anti‐vedolizumab antibody was only marginally lower, 3% versus 4%.13
Combination therapy with immunomodulator
The superiority of combination therapy with an immunomodulator over monotherapy with use of biologics was first reported in SONIC (infliximab and azathioprine in CD) and UC SUCCESS (infliximab and azathioprine in UC).14, 15 The benefit of its use with vedolizumab is, however, less clear. Post hoc analyses from GEMINI 1 and 2 trials did not reveal any additional clinical benefit with combination therapy, both at week 6 and week 52.7, 16 A separate retrospective study of 136 patients observed higher clinical response or remission at week 54 for CD patients who received combination therapy but not patients with UC.17Prospective data will be required to confirm any synergistic effect with combination therapy or whether the long‐term benefit is only a result of the reduced immunogenicity. With the coadministration of an immunomodulator, it should be considered that the benefit of gut‐selective immunosuppression with vedolizumab will be negated.
Role of therapeutic drug monitoring (TDM)
Based on the premise of the drug exposure–clinical efficacy relationship, the measurement of an active drug level and antidrug antibodies has been increasingly used, especially for anti‐TNF therapies. However, the utility of TDM for vedolizumab is unclear. To achieve clinical remission at week 6, post hoc analysis from GEMINI trials observed that a minimum serum vedolizumab trough of 17.1 μg/mL is required for UC and 16.0 μg/mL for CD.6 A separate prospective study observed that a median trough level of >18 μg/mL at week 6 is less likely to be associated with the need for further vedolizumab dose optimization within the first 6 months.18 This echoes the observation of further response recapturing when the vedolizumab administration interval is shortened from every 8 to every 4 weeks.10 While a higher vedolizumab trough level is beneficial, its relationship with clinical remission is not linear, especially for CD, as observed from the GEMINI trials.6 As little as 2 mg/kg of vedolizumab is sufficient to saturate most α4β7 integrin receptors. Furthermore, receptor occupancy does not correlate with treatment response.13, 19 It is unclear if this may be related to other unknown mechanisms of action that may benefit from a higher level of vedolizumab.19
Perianal CD
Prospective data on the efficacy of vedolizumab in perianal CD is currently limited. Post hoc analysis from the GEMINI 2 trial reported higher sustained perianal fistula closure at week 52 for patients who received vedolizumab Q8W versus placebo, 41.2% (95% CI: 18.4–67.1) versus 11.1% (95% CI: 1.4–34.7), respectively.20 A separate retrospective cohort study observed 34.3% complete remission of perianal disease at week 54.21 A specifically designed trial on the efficacy of vedolizumab on perianal fistulizing CD is currently in progress (ClinicalTrials.gov Identifier: NCT02630966).
Primary sclerosing cholangitis
Due to the expression of MadCAM‐1 receptors in the liver, it was thought that the inhibition of α4β7 by vedolizumab may have a potential therapeutic role in patients with primary sclerosing cholangitis (PSC). However, evidence of clinical efficacy is lacking. Two abstracts were presented recently, with one reporting no change in liver chemistry, whereas the second abstract observed an increasing trend of serum alkaline phosphatase at the 30‐week follow up.22, 23
Safety
A recent systematic review of vedolizumab‐exposed patients from six registration trials (2830 patients) and six postmarketing cohort studies (1049 patients) demonstrated no increase in adverse events (AE) or serious adverse events (SAE) in the vedolizumab‐exposed group.24 Follow up ranged from 10 weeks to 46 months for the registration trials and 14 to 53 weeks for the cohort studies. Risk of SAE for the vedolizumab‐exposed group was 20.0/100 patient years (95% CI, 18.5–21.5) versus 28.3/100 patient years (95% CI, 20.6–35.9) for the placebo group.
Infection
Nasopharyngitis was the most common AE reported. This is, however, not higher as compared with placebo, 13.5/100 PY (95% CI, 12.3–14.7) versus 14.1/100 PY (95% CI, 8.8–19.3), respectively.24 All other infections were comparable between both cohorts. When assessed using the Cox proportional hazards model, independent risk factors of serious infection for UC included prior anti‐TNF therapy and narcotics use. For CD, younger age, concomitant steroid and narcotic use were predictors of serious infection.25
Unlike natalizumab, an anti‐α4 integrin antibody, patients administered vedolizumab do not develop progressive multifocal leukoencephalopathy (PML) from JC virus reactivation in the central nervous system (CNS). In addition to inhibiting the trafficking of gut‐specific lymphocytes, it is believed that natalizumab inhibits lymphocyte trafficking to the CNS by targeting integrin α4β1‐positive cells. A single dose of natalizumab has been observed to reverse the CD4/CD8 ratio in the cerebrospinal fluid.26 This has not been observed in patients who received vedolizumab.27 To date, there is no reported case of vedolizumab‐related PML.25
Malignancy
There has been a theoretical concern for GI malignancies due to reduced immunosurveillance in the gut. From the registration trials of 2830 patients, there were 18 malignancies reported, 6 of which were gastrointestinal. However, the risk of malignancies were not significantly higher when compared with anti‐TNF agents using placebos as common comparators (OR: 0.87; 95% CI, 0.26–2.88).28 In a postmarketing surveillance study, 25 malignancies were reported, half of which were gastrointestinal. Of note, this was not higher when compared with the background risk. Furthermore, most of the malignancies reported in the cohorts were patients with short vedolizumab exposure of less than 6 months, tobacco users, or those who had a previous history of malignancy prior to vedolizumab treatment.25 While vedolizumab is not thought to be associated with increased risk of malignancy, more long‐term data is required.
Safety of vedolizumab in special populations
Children
Children <18 years old were excluded from the registration trials. Postmarketing case series demonstrate that vedolizumab is safe in children.29 ESPGHAN recently published the largest multicenter case series of 64 children, mean 14.5 (range 2–18) years old and treated with vedolizumab. No serious drug‐related AEs were reported at a median follow up of 24 weeks (IQR 14–38, range 6–116).30
Elderly
Post hoc analysis of the GEMINI 1 and 2 trials was performed, with patients stratified by age into <35, 35–54, and > 55 years old.31 Of the entire cohort, 11% (220/2010) were > 55 years old. Safety profile was similar across all age groups for vedolizumab and placebo. A separate, single‐center, retrospective study showed that vedolizumab is safe and efficacious in 29 patients (10 UC and 19 CD) who were more than 60 years old.32 A total of 41% achieved clinical remission at week 52, while four patients (13.8%) developed pneumonia, clostridium difficile infection, and flu‐like symptoms.
Pregnancy and lactation
Animal studies using supratherapeutic doses of vedolizumab did not report an increased risk of teratogenicity, still birth, impaired intrauterine growth, or postnatal physical development up to 6 months of age.33 Data from vedolizumab trials (pregnancies in 27 female participants, 19 with male partners exposed to vedolizumab) and postmarketing reports (81 pregnancies) were published recently.34 The exposure of female trial participants to vedolizumab was limited as vedolizumab was terminated once pregnancy was confirmed. In postmarketing reports, pregnancy outcomes were only available in 15 pregnancies (4 live birth and 11 spontaneous miscarriages), while remaining 66 had either ongoing pregnancies or undocumented outcomes.34
Vedolizumab was detected in the milk of lactating monkeys, but there is currently no human data available.33 A human lactation study on vedolizumab is currently in progress (ClinicalTrials.gov identifier NCT02559713).
Perioperative setting
Safety data of vedolizumab in the perioperative setting have so far been conflicting. While vedolizumab's gut selectivity does not result in systemic immunosuppression, there are theoretical concerns that the inhibition of lymphocyte trafficking may impede intestinal healing (Table 2). Lightner et al. observed that perioperative vedolizumab use was associated with higher surgical site infection. However, their vedolizumab cohort was sicker, had higher median platelet levels, was more likely to be on a concomitant immunomodulator, and had less primary anastomosis and more ostomy. It is uncertain if these could have confounded the findings.35 A more recent study by Yamada et al. and a pediatric study from the Mayo Clinic, however, did not show an increased risk of infection with preoperative vedolizumab exposure.36, 37
Table 2. Perioperative safety outcomes with vedolizumab
StudyDesignPatient numbersTypes of IBDDurationPredictors of postop complicationConclusion
Lightner et al.35Retrospective, single center (VDZ vs anti‐TNF/nonbiologics)VDZ: 94
Anti‐TNF: 126
Nonbiologics: 172
CD and UC30 daysVDZ useVDZ group has higher rates of postoperative infection: 53% vs 33% anti‐TNF, 28% non‐biologics, P < 0.001
Lightner et al.(2)37Retrospective single center (VDZ vs anti TNF agents)
*pediatric cohorts (≤18 years)
VDZ: 13
Anti‐TNF: 36
CD and UC30 daysAge > 50 yearsNo increased risk with vedolizumab use
Yamada et al.36Retrospective single center (VDZ vs anti‐TNF/nonbiologics)VDZ: 64
anti‐TNF: 129
Nonbiologics: 250
CD and UC30 daysAge > 65, low albuminNo increased risk with vedolizumab use
  • VDZ, vedolizumab.

Pitfalls with vedolizumab
Slow onset of action
The clinical response with vedolizumab is slow in comparison with anti‐TNF therapies. While the clinical response in relation to placebo is reported to be significantly different at week 6, the peak effect may not be expected till weeks 10–14.6 This is not unexpected given vedolizumab's unique mechanism in inhibiting lymphocyte trafficking rather than directly inhibiting cytokine activity.
Post hoc analysis of the GEMINI 2 trial observed synergistic efficacy at week 6 for CD when corticosteroid was used in addition to vedolizumab. Patients who received corticosteroid with vedolizumab or a combination of corticosteroid, immunomodulator, and vedolizumab at baseline were more likely to be in clinical remission at week 6 in comparison with patients who received vedolizumab alone or vedolizumab in combination with immunomodulator.7 While this additional benefit was not observed in UC from the GEMINI 1 post hoc analysis, a prospective study will be required as GEMINI trials were not specifically designed to assess outcomes with combination therapy.16
Use of combination treatment with anti‐TNF therapy or tacrolimus (in the setting of acute severe UC) to overcome the delayed efficacy of vedolizumab has been reported.38, 39 Favorable long‐term efficacy and safety outcomes of up to 21 months of combination therapy with certolizumab (used off label) have been reported in UC.40 To confirm its utility, dedicated clinical trials are currently in progress. This includes the use of vedolizumab monotherapy versus combination therapy with tacrolimus for moderate‐to‐severe UC (ClinicalTrials.gov Identifier: NCT02954159) and triple therapy with anti‐TNF therapy and methotrexate for CD (ClinicalTrials.gov Identifier: NCT02764762).
Ustekinumab
Efficacy
Ustekinumab is a fully human monoclonal antibody targeting the common p40 subunit of IL‐12 and IL‐23. Through the inhibition of IL‐23, ustekinumab limits the differentiation of naïve T cells to TH17 cells. While clinical efficacy was well documented in the CERTIFI and UNITI trials, a more rapid clinical response at induction was observed when ustekinumab is administered intravenously (in comparison with subcutaneous administration) and at higher doses. Patients are then maintained subcutaneously at a lower dose, which offers the benefit of convenience to the patients.
There is as yet no direct head‐to‐head comparison with anti‐TNF therapies. However, a significant clinical response has been observed both for biologic naïve and experienced patients, as summarized in Table 3.
Table 3. Efficacy data of ustekinumab for Crohn's disease in registration trials and postmarketing cohort studies
StudyDesignPatientsAnti‐TNF experiencedEfficacy
Registration trials
Sandborn et al. (CERTIFI)91RCT (phase 2b)
Induction: IV UST 1 mg/kg vs 3 mg/kg vs6 mg/kg vsplacebo
Maintenance: SC UST 90 mg at week 8 and 16
CD: 526TNF failure: 99.7%Clinical response at week 6:
1 mg/kg: 36.6% (P = 0.02)
3 mg/kg: 34.1% (P = 0.06)
6 mg/kg: 39.7% (P = 0.005)
Placebo: 23.5%
Clinical response at week 22:
69.4% vs 42.5% (placebo)
Clinical remission at week 22:
41.7% vs 27.4% (placebo)
Feagan et al. (UNITI‐1, UNITI‐2, and IM‐UNITI)43RCT (phase 3)
Induction
UNITI‐1
(patients failing anti‐TNF therapy)
IV UST 130 mg vs 6 mg/kg
vs placebo
CD: 741TNF failure: 99.2%Clinical response at week 6:
IV UST 130 mg/kg: 34.4%
IV UST 6 mg/kg: 33.7%
Placebo: 21.5%
UNITI‐2
(patients failing conventional therapy)
IV UST 130 mg vs 6 mg/kg
vs placebo
CD: 628TNF failure: 32%Clinical response at week 6:
IV UST 130 mg/kg: 51.7%
IV UST 6 mg/kg: 55.5%
Placebo: 28.7%
Maintenance (IM‐UNITI)
SC UST 90 mg Q8W vsQ12W vsplacebo
CD: 397TNF failure: 60.5%Clinical remission at week 44:
SC UST Q8W: 53.1% (P = 0.005)
SC UST Q12W: 48.8% (P = 0.04)
Placebo: 35.9%
Postmarketing cohort studies
Harris et al.92Retrospective multicenter (US)CD: 45TNF failure: 100%At 3 months:
Clinical response:46%
Clinical remission: 35%
Khorrami et al.44Retrospective multicenter (Spain)CD: 116TNF failure: 100%Clinical response:
After induction: 83.6%
At 6 months: 76.4%
At 12 months: 63.6%
Kopylov et al.93Retrospective multicenter (Montreal, Canada)CD: 38TNF failure: 100%Clinical response:
At 3 months: 73.7%
At 6 months: 64.5%
At 12 months: 47.4%
Ma et al.42Retrospective multicenter (Alberta, Canada)CD: 167TNF failure: 95.2%Steroid‐free clinical response/remission:
At 3 months: 38.9%, 15.0%
At 6 months: 60.3%, 25.2%
At 12 months: 59.5%, 27.9%
Endoscopic/radiographic response:
At 6 months: 54.5%
At 12 months: 55.8%
Wils et al.63Retrospective multicenter (GETAID, France/Swiss)CD: 122TNF failure: 100%Clinical benefits:
At 3 months: 65%
  • † Defined as reductions in symptoms, biochemical markers, steroid free, and without surgery or immunosuppressant therapies.
  • UST, ustekinumab.

Mucosal healing
Endoscopic healing was reported in a post hocanalysis of UNITI trials.41 Colonoscopy was performed at baseline (week 0), week 8, and week 52 (IM‐UNITI week 44). At week 8, the endoscopic response, defined by ≥3 points reduction of SES‐CD, was significantly higher in the ustekinumab group compared with the placebo group, 47.7% versus 29.9%, P < 0.01. A sustained response in the ustekinumab group was observed at week 52, with 50% reduction in SES‐CD in 33.3% (q8w group) versus 17.0% (q12w group) versus 13.7% (placebo group), P = 0.01. A postmarketing cohort study from Canada reported an endoscopic response and remission of 55.4 and 27.2%, respectively, at median follow up of 46 weeks.42
Role in perianal CD
While up to 43% of patients in UNITI‐1 and 30% of patients in UNITI‐2 trials had perianal disease, the efficacy of ustekinumab in patients with perianal CD was not specifically addressed.43 Limited real‐world data have reported favorable efficacy, with a clinical improvement rate of 61–100%.44, 45 It is possible that this cohort of patients may benefit from a higher ustekinumab trough level, but more data will be required.42, 45
Safety
Ustekinumab is approved for use in CD in North America and Europe since 2016. While long‐term safety data are limited in CD, safety data are available on its use in psoriasis/psoriatic arthritis.46 Ustekinumab, which is used at a lower dose in psoriasis, appears to be safe, with no increased risk of AEs, SAEs, infection, and malignancy. Data from clinical trials (phase 2 CERTIFI, phase 3 UNITI) demonstrated a similarly favorable safety profile with no increased risk in comparison with placebo‐treated participants.
Infection
Four cases of opportunistic infections were reported during the UNITI trials: one case of listeria meningitis (patient received concomitant ustekinumab and oral prednisone 30 mg daily), two cases of esophageal candidiasis (one patient who received ustekinumab 90 mg every 8 weeks and one patient who received placebo and concomitant prednisone), and a case of pulmonary tuberculosis occurring 10 months after the administration of a single dose of ustekinumab 130 mg intravenously.43
Using phases 2 and 3 clinical trials data for ustekinumab across all indications (CD, psoriasis, and psoriatic arthritis), the overall incidence rates of active tuberculosis was low compared with patients treated with anti‐TNF agents—0.02 per 100 patient years; (95% CI: 0.00, 0.06) versus 0.28 (95% CI: 0.21, 0.37), respectively.47 With isoniazid prophylaxis, ustekinumab treatment appeared to be safe with no latent TB reactivation in a systematic review of five clinical trials (3177 patients).48
Malignancy
The 5‐year safety data of 3117 ustekinumab‐treated psoriasis patients reported 47 cases of non‐melanoma skin cancer (NMSC).46 The risk of NMSC with ustekinumab is, however, not increased in comparison with the placebo‐treated cohort, 0.48 versus 0.52 per 100 patient years, respectively. Furthermore, there is no reversal of the BCC and SCC ratio (4:1), as expected in the general population.49 Over the 5‐year follow up, there was no time‐ or dose‐dependent (45 mg vs 90 mg) difference observed.46 Despite the use of higher doses for the CD cohort, no increased risk of NMSC was noted in comparison with the placebo cohort in the registration trials.43 No concern for other malignancies (excluding NMSC) was raised.46
Major adverse cardiovascular events
Concern regarding the association of ustekinumab with major adverse cardiovascular events was first raised in psoriasis trials. This included briakinumab, which has a similar mode of action. Meta‐analyses of RCTs in the psoriasis cohorts have so far reported conflicting conclusions.50Nonetheless, 5‐year safety data of ustekinumab in psoriasis did not show any dose‐ or duration‐dependent relationship.46 As psoriasis is independently related to adverse cardiovascular events, it is unclear if this could be a concern for CD.51 No association has so far been reported.
Safety of ustekinumab in special populations
Children
Use of ustekinumab in pediatric patients with CD was only limited to case reports.52 Larger cohort studies will be required to validate the efficacy and side effect profile in the pediatric population.
Elderly
Use of ustekinumab in elderly patients (65 years and above), a total 46 patients, with psoriasis was reported in two retrospective studies.53, 54 No increased risk of AE was reported at the end of 1 year. No data for the CD cohort are yet available.
Pregnancy
Prior to the implementation of the Pregnancy and Lactation Labelling Rule (PLLR), ustekinumab was labeled as FDA pregnancy category B. Human data have so far been restricted to the patient registry, case reports, and observational studies. Animal studies with cynomolgus macaques receiving doses of up to 45 mg/kg twice weekly did not report an increased risk of teratogenicity or developmental delay up to 6 months of age.55 The current dermatology literature has not reported an increased risk of miscarriage or congenital malformation.56 Case reports for its use in CD have observed conflicting pregnancy outcomes.57-59 As most of the patients had active disease during pregnancy, it is unclear if the adverse outcomes were related to the active disease state rather than the medication. More data from prospective pregnancy registry will be needed.
Perioperative settings
Perioperative safety outcomes of patients exposed to ustekinumab were assessed in two retrospective multicenter cohort studies.60, 61 Ustekinumab use was not observed, in both studies, to be associated with the increased risk of postoperative surgical site infection when compared with anti‐TNF‐treated patients. This is in spite of a higher use of concomitant immunosuppressants in the ustekinumab group in the study by Shim et al. The study by Lightner et al., however, noted an increased risk of reoperation in the ustekinumab cohort. It is unclear if the observations were limited by the small sample number. While perioperative ustekinumab exposure appears to be safe, more studies are required. This will hopefully guide the decision on the role of an elective drug holiday prior to elective operation.
Other challenges
Immunogenicity

Immunogenicity with ustekinumab is remarkably low. Antibodies to ustekinumab were reported in 0.7% of patients by week 36 in the CERTIFI trial and in 2.3% by 1 year in the maintenance IM‐UNITI trial.43 This is much lower compared with anti‐TNF agents, such as infliximab (0–83%), adalimumab (0–54%), and golimumab (0–19%).62 Long‐term immunogenicity data for ustekinumab are eagerly awaited.
Combination therapy
In comparison with anti‐TNF therapies, the benefit of combination therapy in ustekinumab is less clear. The synergistic effect of a concomitant immunomodulator was observed in the GETAID cohort but not in others.42, 44, 63 In a prospective study of 62 patients, there was no significant difference in the ustekinumab trough level between those with and without concomitant immunomodulator use.64 Given this observation and the overall low immunogenicity associated with ustekinumab, it is likely that the use of a concomitant immunomodulator is less important.
The use of ustekinumab in combination with another biologics (anti‐TNF agent or vedolizumab) in refractory CD has been described with favorable outcomes.65, 66 Evidence to date is, however, very limited, particularly for long‐term safety.
Choice of biologics
For more than a decade, the only biologics licensed for use in IBD patients were the anti‐TNF agents. It was not possible for patients to be switched out of class even when they are obviously not responding to anti‐TNF agents. This has changed dramatically since 2014, with vedolizumab and ustekinumab joining the ranks of biologics approved for use in IBD.
These new agents appear to be associated with a lower risk of patients developing cancers and a lower risk of infective complications. They also appear to be less immunogenic than the older anti‐TNF agents. However, we have less real‐world data on how different subsets of IBD patients will respond, for example, pregnant patients, patients with pouchitis, patients with perianal CD, and patients with the extraintestinal manifestations. With the advent of biosimilars, the newer agents are also more expensive than the anti‐TNF agents.
To date, there are no published data on the direct head‐to‐head comparison between various biologics therapies. Clinical trials of UC comparing vedolizumab and adalimumab (NCT02497469) and etrolizumab and infliximab (NCT02136069) are currently under way. Currently, available comparative safety and efficacy data between various biologics therapies in both UC and CD are derived solely from network meta‐analyses. The overall safety profile appears to be comparable, although vedolizumab may theoretically be the safest. For treatment of UC, there was no significant difference in mucosal healing between vedolizumab and anti‐TNF agents.67 For infliximab‐experienced UC, vedolizumab was found to be superior to adalimumab in achieving mucosal healing during maintenance, OR 6.72, (95% CI 1.36–41.0), although no difference was found during induction.68 For treatment of CD, adalimumab and combination infliximab with azathioprine are more effective than vedolizumab in achieving clinical remission, OR 2.4 (95% CrI, 1.2–4.6).69
Rather than one‐size‐fits‐all, the choice of biologics should be tailored to the individual patient profile. The strength and limitation of each agent, given the inherent differences in the pharmacokinetics and pharmacodynamics properties should be considered in conjunction with the heterogeneous disease profile in each patient (Figs 1, 2, 1, 2). A patient with CD with concomitant extraintestinal manifestation or psoriasis, for example, may benefit from anti‐TNF therapies or ustekinumab rather than vedolizumab. On the other hand, vedolizumab may be preferable in a patient with a history of non‐GI malignancy or other comorbidities, such as hepatitis B or C or pulmonary tuberculosis infection. Vedolizumab and ustekinumab have lower immunogenicity than anti‐TNF agents and could be a better option if monotherapy is considered.62
image
Figure 1
Open in figure viewerPowerPoint
Strength of various agents in Crohn's disease (CD).
image
Figure 2
Open in figure viewerPowerPoint
Strength of various agents in ulcerative colitis (UC).
Data to guide subsequent choices of biologics, especially in CD, are currently limited. While registration data observed a relatively inferior response with vedolizumab in comparison with ustekinumab in anti‐TNF‐experienced patients, no definite conclusion could be drawn given the heterogeneity in study design. Clear evidence from direct head‐to‐head comparisons is currently lacking. Indirect comparisons by separate groups did not observe any significant difference between ustekinumab and vedolizumab in achieving clinical remission in anti‐TNF‐experienced CD.70-72 The efficacy of ustekinumab and vedolizumab in patients with fistulizing CD was reported in a recent meta‐analysis, with pooled RR 1.77 (95% CI, 0.93–3.37; P = 0.08) and RR 2.54 (95% CI, 0.63–10.29; P = 0.19), respectively.73 Interestingly, while treatment response is known to be poorer in biologic‐experienced patients, there may be a potential role of using the etiology of withdrawal to guide subsequent choices of biologic. In a recent meta‐analysis, treatment response of a second biologic, particularly with ustekinumab, is poorer in anti‐TNF therapy primary nonresponder, in comparison with secondary nonresponder (RR, 0.64 [0.52–0.80]). There was no difference in treatment response to vedolizumab for both anti‐TNF primary nonresponder and secondary nonresponder (RR, 1.16 [0.85–1.58]).74
Predictor of response
Clinicians have tried to predict which patients will respond to biologics since the advent of biologics. Clinical characteristics, drug factors, biochemical markers, endoscopic factors, and genetic and serological markers have been proposed as predictors of response. These have recently been reviewed by Ding et al. with regard to anti‐TNF agents.75
Clinical predictors of response to vedolizumab and ustekinumab have also been studied. Patients with severe, complicated disease phenotype (in CD) or previous anti‐TNF therapy exposure were less likely to respond. Other poor prognostic factors in CD include smoking, history of intestinal resection, ileocolonic disease, and low trough level of both biologics.76 Genetic polymorphism contributes to the variation in clinical presentation and the response to ustekinumab.75, 77 HLA‐cw6 (C*06:02) expression, a major psoriasis‐susceptible gene, was found to be useful in predicting response to ustekinumab in the psoriasis cohort.77 In a phase 2a study, CD patients who received MEDI2070, a selective IL 23/p19 inhibitor, and who responded had a greater reduction in IL 22. In particular, the benefit was greater for those with a higher baseline IL 22 level.78 For vedolizumab, molecular imaging of mucosal α4β7 integrin expression with FITC‐labeled vedolizumab was useful in predicting response to vedolizumab in CD in a small case series.79 While validation with more data is required, these exploratory observations are encouraging and may allow personalized treatment in the future.
Conclusions
The availability of novel therapeutics modalities for IBD is encouraging. Vedolizumab and ustekinumab complement anti‐TNF agents and provide us with alternatives for patients who have failed anti‐TNFs. While more real‐world data is awaited, the safety and efficacy profiles of these two novel agents in the registration trials have been encouraging. In selected patient subsets, they could be considered first‐line biologics over anti‐TNF agents.


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Thx for you help @Kate123 @my little penguin @Scipio - very informative!

Update: Vax are underway, but boy either the last MMR or Chickenpox either did a number on me or I’m just going through a ton of stress about the whole situation. Wonder if I’m toying with a flare. GI and health unit both significantly warned about who we bring in our house when on biologics, suggesting my wife do something else for work - she typically brings in groups of ~8 a few times a week for classes. She also rents out a few of our rooms as medium term rentals (1-4mo) to students etc. So a career and income she has been building may be shot. Pretty challenging to ask these people for vax records, and even then there are other bugs. I’m also in the beginning stages of asking for accommodations at work... plus other stressors too.

I have a new question in the main Remicade thread- Allergies better or worse on Infliximab?
I would love to hear your take, as I can’t imagine living with even worse food allergies. And considering these and environmental allergies (which have sent me to the hospital many times), I worry about my body’s acceptance of biologics.

You may have the gist, I’m getting scared. Sometimes I feel so crummy mentally and physically. I’m sure I mostly come across bad stories about allergies, but it is still concerning as I already have so many. Can’t wait to get off Prednisone though!
 
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