Considerations in the Development of Ovarian Cancer Pathways

In this journal section, we speak with cancer care practitioners about their clinical pathways and the pathways programs being used in their practice, how they are being applied in a particular disease state, and what challenges persist regarding treatment decision-making and personalized medicine integration.

In this “Pathways in Practice” installment, we speak with Robert M Wenham, MD, MS, FACOG, FACS, chair, department of gynecologic oncology, Moffitt Cancer Center (Tampa, FL) about the special challenges related to the creation of a clinical pathway for ovarian cancer. Driven and consistently guided by their own physicians and with input from across multiple services teams, Moffitt creates their own clinical pathways from start to finish in-house and updates them regularly. Dr Wenham has been involved in Moffitt’s clinical pathways program from its earliest stages. Dr Wenham has a strong interest in research and is a principal investigator for numerous clinical trials to improve cancer care for women. His research activities primarily include the use of novel drugs for the treatment of gynecologic cancers.

Please describe how clinical pathways are developed and used at Moffitt?

The development process I’m going to separate from the implementation process. Interestingly, I was appointed the original pathway lead here at Moffitt by our visionary physician-in-chief (and now current CEO), Alan F List, MD, about 9 years ago to try and figure out how to develop these pathways. The first pathway to be put down on paper actually was the ovarian cancer pathway, and it was on the back of a napkin at about 30,000 ft in an airplane. At that time, there were many different ideas that were circulating in the field about what a pathway should be and how our pathway might differ from other attempts to develop pathways. The big thing I found out when making the pathways is that it is one thing to write down what you do and make a little algorithm sheet, but it is a whole other thing to come to a consensus about what a pathway’s purpose is, the terminology that should be used, how it should be implemented, and the maintenance of pathways.

So we formed a group to ty to figure these issues out, and it became apparent that people thought everybody was on the same page but, in reality, there were some conflicting thoughts about the vision of the pathways program. One of the assumptions from some people on the business side was that pathways were going to be used as a way to homogenize practice, to decrease variability, to decrease costs, to inform payers of their potential risk, and to use as a negotiation thing. But from the clinical members, they primarily thought of using them to be a platform of discussion, of consensus, but also for understanding disagreement, and to being a research tool. For example, every time there is a branch in a pathway, it represents a divergence and means that there is a set of questions around why you go on one branch vs the other and that brings up opportunities for collecting information and doing specific research.

There were definitely some who thought that a pathway designed for improvement in quality may not decrease variability; it may actually increase variability and increase costs, so we had to figure out what our priorities were. So when our pathways were first designed, I and others went into it with more of an altruistic standpoint. We decided that we would establish how we deliver care, the reasons why we do that, and ignore certain things such as cost, etc, initially, so we can outline what we would consider ideal care for particular patients and try to make it as algorithmized as possible in medicine, understanding that there are going to be differences of opinion.

The other thing that I thought was important was annotating the pathways. Having a bunch of stick drawings is not sufficient. For someone to pick up a pathway and either understand the rationale or to modify the pathway at a later time, there had to be companion documents that explained the logic and had references to the literature that was appropriate and also would discuss why patients may or may not meet what a pathway shows.

Another item we thought was important was defining the terminology that would be used around the pathways. We tried to avoid words like “deviate” from pathways because “deviate” means, often, that there is deviance—and there is not really deviance in that sense, there is just disagreement. So rather than “adherence,” it was “alignment” or “agreement.” Those term choices are powerful because they send a signal or undertone that these are not punitive pathways; they are meant to help develop clinical practice.

Would you say that the pathways you have created and the idea of cost savings behind clinical pathways are less to do with consideration of the actual cost of therapy on the pathways and more to do with simply reducing variability of care, and as a result, reducing unwarranted costs?

Yeah. I think that’s right. We need to reduce unwarranted variability because when you have unwarranted variability in a system, that can also lead to things other than just cost; it can lead to error. For all those reasons, many people said that pathways may be useful. On the other hand, we aren’t oblivious to the fact that there may be times when cost may be a deciding factor. After we finish making the pathways and justifying it on an efficacy and tolerability standpoint, we then append—where there was division or controversy—some of the cost information. And certainly, I think they have been trying to track how one decision or another affects cost. But that’s a moving target, right? Cost is not a fixed thing. And a drug today may be expensive and tomorrow may be cheap, and it’s hard to plan an entire pathway with that being your primary motivator.

Shifting gears to focus our discussion more on ovarian pathways specifically, does Moffitt have a clinical pathway or a section in the ovarian clinical pathway for platinum-sensitive recurrent ovarian cancer, and if so, what is the approach to stratifying platinum-sensitive patients to guide therapeutic decision-making?

Yes, we have an ovarian cancer clinical pathway that has subsections/divergences based on platinum status. At Moffitt, we always select a physician to be the primary pathway author, and I am the ovarian primary author. This means I work with our clinical pathways development/revision team (non-physicians) on any new updates needed for the ovarian pathways. Karen K Fields, MD, medical director of the Moffitt Oncology Network, is the clinical overseer of this team. We typically meet quarterly and review the pathway to see if there are any changes to be made. Then the drafted changes are sent out to all members across the facility to get their multidisciplinary input, and then ultimately approved for inclusion.

So for initial presentation, we do have a platinum-sensitive path and a platinum-resistant path. I think if you had to divide the pathway into 4 major parts for ovary, it would be (1) initial diagnosis or suspicion of ovarian cancer, (2) primary therapy, (3) those who have the platinum-sensitive recurrence, and (4) platinum-resistant recurrence. And then built in there are these auxiliary things which I consider surveillance: genetic referral, clinical trials, etc. So, 4 different major areas.

The platinum-sensitive and platinum-resistant disease treatments were a fairly slow-moving and changing entity until the last 4 years or so. The approval now of both bevacizumab and of 3 different poly ADP ribose polymerase (PARP) inhibitors in those settings has quickly altered how we think about triaging these patients into various treatments. Even now we have to amend initial frontline therapy to include PARP inhibitors for maintenance of BRCA mutation cancers.

Probably the more difficult question for oncologists treating patients with ovarian cancer is what to do when a patient has their recurrence in a platinum-sensitive setting. Previously, it was trying to decide between a few different chemotherapy regimens, all of them having platinum because it was platinum-sensitive, so it was either platinum plus a second agent—most commonly paclitaxel, docetaxel, pegylated liposomal doxorubicin, or gemcitabine as pairing agents. To be honest, if you look across the literature, there really are not hugely significant differences between those chemotherapies. It was more schedule-based and toxicity-based and looking at what kind of chemotherapy the patient had before and what their tolerance was.

The approval of bevacizumab occurred at about the same time when we saw the approval of PARP inhibitors. The problem is, right now, that we don’t have approval of a combined bevacizumab and PARP inhibitor strategy for platinum-sensitive disease; if you’re going to make the decision to put somebody on bevacizumab, which was studied in basically a gene-agnostic population, you do that up front with the chemotherapy and then you continue the bevacizumab for a long duration after chemotherapy as maintenance. If you’re going to choose to do the PARP inhibitor route, then the PARP inhibitor is delivered after chemotherapy, and it’s for patients who have a response to chemotherapy. When bevacizumab is given before, you don’t know whether the patient is going to have a response or not. But for the PARP inhibitor, you give the chemotherapy, and then you look for a complete or partial response; and only then you can put them on maintenance.

To make it even more confusing, we know that there is some difference in the degree of response between patients who have certain mutations in their homologous re-combination repair genes, those who have assays that look like they’re homologous recombination repair-deficient, and then those patients who seem to have neither based on differences in responses. So the question is, do you start trying to guess ahead of time whether or not your patient is going to have a response and put them on a PARP inhibitor or do you put them on the bevacizumab agnostically? But then, if you did that and they respond and they happen to have, let’s say, a genetic mutation, do you then switch them over to a PARP inhibitor? Do you continue the bevacizumab and treat with a PARP inhibitor for recurrent disease?

This is what made creating the pathway complicated, and it partly can depend on what you were going to do in platinum-resistant disease later on. The two tie together somewhat in that many people were feeling like the real role of bevacizumab might be with platinum resistance because it had already been shown to significantly improve progression-free survival time in combination with chemotherapy in the platinum-resistant setting. But then, other data emerged about preserving the effect of bevacizumab throughout different settings like front-line to platinum- sensitive, then platinum-resistant.

Overall, it has become more confusing for the average oncologist deciding what to do with a patient with platinum-sensitive recurrence.

In the Moffitt ovarian pathway, what direction does the pathway guide you? Do you tend to go in the bevacizumab direction or do you tend to go in the PARP direction for platinum-sensitive recurrent disease? And what’s the next move within the pathways?

We’ve left a little bit of wiggle room in there because we realize the data are not complete and are evolving. For patients who have genetics that would indicate they’re a PARP inhibitor responder, we have a directive that maintenance should be given after a complete and partial response, regardless what they received before. Our justification for that is there were some patients who had received prior bevacizumab with their chemotherapy and then went on to a maintenance PARP inhibitor. So we leave it open for patients who’ve had a response to their platinum therapy, regardless of whether it contained bevacizumab, to at least have the option of going onto PARP inhibitor maintenance. We have left the decision open to physicians/patients realizing that this is a difficult decision and warrants a patient/physician discussion of the relative merits of that.

Earlier you said you meet with the pathway team quarterly and as new data comes out. How do you ensure that new approaches to therapy are incorporated into your pathway in a timely manner?

Well, as an example, something was recently approved and, interestingly, my pathway team was already aware of it and reached out to me to discuss. Our pathways team has become very in tune with new data that comes out. Dr Fields’ team will often get a hold of us (ie, primary authors on the pathways) and ask us if something is practice-changing or not. Or it goes the other way as well—if we find something that we feel is practice-changing, we get a hold of them. Meeting together quarterly is a reasonable enough time for the speed that things move in ovarian cancer research to where we can bring it up and put it into the pathways.

How do you balance the need for standardization of treatment decisions with the need to optimize care for individual patients?

Yes, what you have brought up is what I view as one of the greatest struggles between various factions that work around pathways. I alluded to this earlier—that there was a difference of opinion somewhat on what the primary purpose of a pathway is. If you treat a pathway as you would a clinical study, you’re only allowed to have so many primary aims, because if everything is of primary importance, then it pretty much comes to nothing. You wouldn’t be able to answer any question or actually address anything.

Everyone uses the word “quality.” “We want to have the highest quality patient care.” If that is true and you put that as your primary aim, then you have to accept that the other secondary things may not turn out the way you expect them to, ie, you may not save money by giving better quality care. It may turn out that the data points lead to doing the things that are more expensive or contrary to how things have been done prior, so these are the things you have to be prepared to handle. Pathways may not reduce costs and may even increase variability. Rather than having everybody get one or two major drugs, maybe the data will point to doing various genetic analyses and having many different subgroups and tailoring and individualizing it to where it becomes more difficult.

We should have perhaps expected it, but, again, it was a challenge to get everyone on the same page as far as what outcomes we expect the pathways to provide. Having said that, I think one of the things I like about working on the pathways here at Moffitt is that I truly feel like everybody came at this with an intention of trying to do the right thing for the patient, whether it is on an efficacy level, saving them from toxicities, or saving them money. I really feel like the primary aim and drive of why we made our own was we didn’t want to be stuck with one that may not have those same ideals behind it. There is a reasonable understanding at Moffitt that we are not using pathways primarily to discipline practice but to gather data to better inform our future. We do not use pathways as a punitive tool or to drive people to do things that they may not be comfortable with.

What are some of the challenges to optimizing decision making that you continue to see at your practice, and how do you see these challenges being overcome?

I think the biggest challenge is coming to some agreement where there’s controversy—that room for debate needs to be reflected on the pathway, or can you come to an agreement on the best practice? If there is no rule stating the best option, does the pathway become more of a guideline where you have many different options? And we didn’t really want something like the National Comprehensive Cancer Network guidelines that might have 30 different things you can do because so many possible options were put on there. We wanted to be a little bit more forceful with ourselves saying, what is it you do most of the time and where is it we can find agreement in that. We try to look at those gray areas where there are many options and decide whether the data are just not there to guide us yet.

Maintaining the pathways is the second challenge. It takes a lot of work to maintain our pathways. To ensure they are up to date and accurate, we sit down with the pathways team, go back through the data, do the mental exercise of going through all of the treatment steps. This mental exercise I find the hardest challenge, because when you try to put it into an algorithm, you can get trapped in these logical pitfalls; your brain may get to the answer quickly, but when you try to create arrows of those decisions, it doesn’t always make as much sense. Trying to figure out how you think and put it down into an algorithm is extremely challenging.