Karen Titus
July 2016—Time was running out for Yuri Nikiforov, MD, PhD, vice chair for molecular pathology and division director of molecular and genomic pathology, University of Pittsburgh Medical Center.
For nearly a year he had been working to assemble an international group of experts—pathologists, endocrinologists, a surgeon, and, unusually, a psychiatrist and a patient advocate—to discuss that most vexing of thyroid tumors, encapsulated follicular variant of papillary thyroid carcinoma, or EFVPTC.
“Way overdue” is how many see the nomenclature revision for noninvasive encapsulated follicular variant of papillary thyroid carcinoma, says Dr. Yuri Nikiforov (right), with Dr. Sally Carty and Dr. Raja Seethala at UPMC.
Their goals were less ambiguous than the tumor: to evaluate clinical outcomes, refine diagnostic criteria, and develop a new nomenclature. No detail was too small, and nothing was left to chance. Prior to the meeting, “We had collected a large number of EFVPTC pathological samples”—265 patients with noninvasive or invasive tumors—“and the cases were distributed and reviewed by 24 pathologists,” Dr. Nikiforov says. This was followed by eight weekly, one-hour teleconferences to review the difficult cases and discuss opinions and consensus criteria, all prior to the day-and-a-half, face-to-face meeting in Boston in March 2015.
At the conference, participants learned the blinded results of the follow-up. All 109 cases that were called noninvasive were highly indolent. The invasive EFVPTCs, on the other hand, were quite aggressive. That review took most of the day. “And at the end of the day, we started to discuss a new name for the tumor,” Dr. Nikiforov says. Carcinoma in situ? Follicular adenoma? Noninvasive follicular thyroid neoplasm?
Round after round went the discussion and voting, like an Iowa caucus, into the evening. “We could not decide,” says Dr. Nikiforov.
Work resumed the next day. The clock was ticking. “We had to end the conference at noon,” he remembers. Finally, “At 11:30, we reached a consensus.”
Behold noninvasive follicular thyroid neoplasm with papillary-like nuclear features, or NIFTP (Nikiforov YE, et al. JAMA Oncol. Published online April 14, 2016). Though it’s not part of any official guideline, it’s likely here to stay, for better (say many), possibly for worse (fret a few detractors), or to little effect at all (shrug some).
The name is notable for what it lacks: the words “carcinoma” and “cancer.” The presentation by Guy Maytal, MD, medical director, ambulatory psychiatry, Massachusetts General Hospital, and assistant professor, psychiatry, Harvard Medical School, influenced many to steer clear of these words, given their impact on, among other things, patients’ psyches. As a medical-geometry truism, in patients’ minds the shortest distance between diagnosis and death is “cancer.”
But the change began several years before the Boston meeting, as a notion, a whisper of sorts, at the end of a prior research effort. The Cancer Genome Atlas project mapped the somatic mutational landscape of the most common types of papillary thyroid carcinomas and showed that PTC fundamentally consists of two types of tumors, those that are driven by RAS and those driven by BRAF. (See “Thyroid cancer: In a flourish of subtypes, genes, and drivers,” CAP TODAY, January 2015.) “That laid the foundation for us thinking about these follicular tumors,” says TCGA project co-chair Thomas Giordano, MD, PhD, who was also part of the most recent effort. Some pathologists even suggested the encapsulated type might be given a new name, and noted that FCIS was already being used by some.
Dr. Nikiforov predicted at the time that a name change could indeed happen—but only after much time and wrangling. Thus he’s pleased the wait turned out to be relatively short, at least in medical years. Looking at this most recent conference and paper, he says, “It’s remarkable. I can tell you honestly, the task was humongous.”
Adds Virginia LiVolsi, MD, who participated in both studies: “‘Quick’ can be defined in various ways. In medicine, two years is not that bad.” Dr. LiVolsi is a professor of pathology and laboratory medicine, University of Pennsylvania Perelman School of Medicine.
Their work has drawn praise from nonparticipants as well. Sally Carty, MD, says she was impressed the task was accomplished “so rapidly and so elegantly. It’s a brilliant idea,” says Dr. Carty, a professor of surgery and chief, Division of Endocrine Surgery, University of Pittsburgh, and past president, American Association of Endocrine Surgeons.
The study even caught the attention of The New York Times, whose April 15 article stirred interest among patients and physicians in revisiting EFVPTC diagnoses.
The group’s accomplishment was not completely unexpected. Interest in these tumors is considerable, as evidenced by the response to the paper. Dr. Nikiforov reports that in the first three weeks after the study’s publication, 67,000 people looked at the article online. By way of comparison, he says, other, similarly consequential studies might draw 5,000 hits. “The number of emails, questions, and comments I get every day is enormous,” he says. “I’ve received hundreds of emails since the paper came out. Many people say, ‘This is way overdue.’”
Pathologists who see these lesions routinely are all too familiar with the dilemma they pose. Though there is no invasion, they have the nuclear features of papillary carcinoma. So is it benign or malignant?
Not all tumor types pose similar dilemmas. In colorectal cancer, for instance, the spectrum has been well delineated: polyp, dysplasia low-grade, dysplasia high-grade, carcinoma in situ, invasive carcinoma. “In thyroid, we ignored this for many years,” Dr. Nikiforov says. (He could be speaking about Illinois’ state budget.) Though several previous studies had shown prognosis was excellent if these lesions were noninvasive, they were based on smaller series of cases. Consensus diagnostic criteria were lacking, as was methodical, lengthy follow-up. And so it went, “for many years, without resolution,” Dr. Nikiforov says.
It was time for a solid study.
An important part of the study design, he says, is that “we didn’t simply have 24 pathology experts meet and say, ‘In our expert opinion, this should now be benign.’” In the era of evidence-driven medicine, “You cannot do this.”
Among the patients with noninvasive disease, who were followed for 10 to 26 years (median, 13 years), all were alive and had no recurrences or other signs of disease at final follow-up. “None of these tumors was ever heard from again,” as Dr. LiVolsi puts it. In this group, 67 received lobectomy alone, and none received radioactive iodine ablation. The findings correspond with previous studies of noninvasive EFVPTCs. Among 352 such tumors, the authors note, only two recurred. In one case, the tumor had been incompletely excised; in the other, the noninvasive status was questionable.
In the second group, 85 of the 101 patients with invasive disease were treated with radioactive iodine ablation. In one- to 18-year follow-up, 12 had an adverse event, including distant metastases (two of these five patients died of their disease), lymph node recurrence, persistent disease, and detectable serum thyroglobulin, indicating either indeterminate or incomplete response to therapy.
The upshot, the authors say, is that an absence of invasion entails a very low risk and should not be termed “cancer.” Pathologists are no longer forced to decide between malignant and benign—it can be a borderline, pre-cancer lesion, says Dr. Nikiforov. “If the tumor is removed, progression is stopped.” These patients don’t need to be labeled with cancer, and they can avoid completion of thyroidectomy, radioactive iodine therapy, and the cycle of six- or 12-month follow-ups.
The study offered a set of diagnostic criteria for identifying NIFTP, including lack of invasion, follicular growth pattern, and PTC nuclear features. Since the JAMA Oncology article targets a more general audience—the better to reach clinicians, says Dr. Nikiforov—the authors had limited space to describe pathology-related details in depth. A subsequent article, containing a detailed review of morphology features, is nearly complete. Dr. Nikiforov calls it “a step-by-step guide to making this diagnosis.”
Identifying NIFTP demands scrutiny of the lesion to look for invasion, says Dr. LiVolsi. “The definition of the lesion has to really be perfect for the pathologist to apply this terminology.”
Pathologists need to examine the entire lesion. “I think expert pathologists have been examining the entire capsule for some time. That’s not to say it’s been universally done,” says Gerard Doherty, MD, the Utley professor and chair of surgery, Boston University, and surgeon-in-chief, Boston Medical Center.
If pathologists have not been submitting the entire lesional capsule for histologic interpretation, they need to do so, says Raja R. Seethala, MD, pathologist and director, Head and Neck/Endocrine Pathology Center of Excellence, UPMC. Dr. Seethala says this has been a matter of debate in the past, with practice patterns differing along academic/community lines. “It’s no longer optional to submit the entire capsule,” he says.
For pathologists, “If the lesion is 1.5 cm, that’s not so bad. If the lesion is 4.5 cm, that’s a lot more work,” Dr. LiVolsi acknowledges. Moreover, she adds, some of these lesions might have only one lone focus of invasion. The risk associated with such lesions is still low—but not as low as the risks of lesions now known as NIFTPs, which have no invasion and thus better clinical implications. “So if you do not train pathologists in the importance of examining the entire capsule of the lesion—and if there’s no capsule, the entire perimeter—then we’ve failed,” Dr. LiVolsi says.
Though this is one paper, already it’s making waves. The WHO has accepted the new entity and included it in its new classification of tumors of endocrine organs that will appear in print next spring. “This is a big step,” Dr. Nikiforov says. “It ensures the acceptance of this terminology around the world.”
Closer to home, individual pathologists are feeling reverberations as well.
Dr. Giordano, the Henry Clay Bryant professor of pathology, University of Michigan, says he was recently asked to re-review a case of a thyroid nodule that was called PTC. “The surgeon was looking for any reason not to be all that aggressive with the patient.” Dr. Giordano sent the paper, in prepublication form, to U-M’s head endocrine surgeon, who “read it, liked it, and discussed it with the patient, then wrote back and said the patient was thrilled to have a justifiable reason not to have a total thyroidectomy and undergo radioactive iodine treatment,” says Dr. Giordano, who is also director of both the Division of Molecular and Genomic Pathology and the UMCCC Tissue and Molecular Pathology Core, Department of Pathology.
In another recent case, the head thyroid endocrinologist at Michigan asked for review of a case involving a patient who’d already undergone a total thyroidectomy, based on a diagnosis of papillary carcinoma and the presence of bilateral nodules. No invasion was noted. The case will be revised to NIFTP, Dr. Giordano says. “That will be a clear signal not to give the patient radioactive iodine” and to regularly check the patient’s thyroglobulin levels.
Dr.Giordano
Revisiting cases presents technical challenges, Dr. Giordano concedes. “If you can’t be confident there isn’t invasion, based on a thorough examination of the entire tumor capsule, you’ll still have to use the old nomenclature.” Not every case can be reviewed, but moving forward, he says, he hopes this will mandate that pathologists sample these nodules more thoroughly.
Using the NIFTP nomenclature could eventually have wide clinical impact, Dr. Giordano predicts, though “It all depends on the clinical group.” While Michigan seems poised to adopt it, “I can imagine other places where people are more comfortable with the more aggressive treatment.” Just as there is interobserver variability among pathologists, so, too, is there variability in surgeons’ practices. “Some like to do total thyroidectomies more than others, even for a traditional papillary carcinoma. There’s a lot of regional variation,” Dr. Giordano says.
Regardless, he’s joined the chorus of physicians who call the move “long overdue.” Over the years, he says, “Pathologists have gotten a little too aggressive with these tumors. We focused more on the nuclear features, and less on whether the tumor was invasive. And I think the true malignant potential resides in whether the tumor’s invasive.”
In the first case he mentioned, Dr. Giordano notes, the likelihood of the patient’s tumor becoming a metastatic cancer “is not zero, but it is really close to zero. So what we’re trying to do is balance all that extra surgery, all that radioactive iodine, for tens of thousands of patients—maybe more, globally—versus the rare patient who may still develop a clinically significant cancer.” It can be a tough decision, he concedes. “Because people want to be absolutely certain.” While noninvasive tumors only rarely behave like cancers, he says, there are examples of follicular adenomas that metastasize.
When this occurs, it’s not unusual for these to be considered a mistake on the part of the pathologist. The fact is, “There is always some built-in sampling error.” As a result, “Every endocrinologist will tell you about their one or two patients” who had what turned out to be follicular carcinoma, rather than, as thought, a follicular adenoma.
“Is that going to happen with NIFTP? Probably,” says Dr. Giordano, launching into a mini-Q&A. “Does that mean it’s not the right thing to do? Absolutely not. Is pathology black and white? No. Do people want it to be? Yes.”
He’s also heard positive response from his clinical colleagues. “One endocrinologist looked at me and said, ‘Oh, thank God you’re doing this.’” So far, he says, he’s encountered very little confusion among his endocrine surgeons or endocrinologists. “They all recognize what we are trying to do and have supported it.” It’s likely more confusing to patients, he says. “This is about as granular as you can get.” It’s a papillary carcinoma, now without the carcinoma label, and a follicular variant, and it’s noninvasive. But for physicians, “It’s a pretty simple concept.”
Some clinicians take it a step further. Not only is NIFTP simple to understand, they say, but it’s also somewhat simplistic. “It’s a tempest in a teapot,” says Dr. Doherty, who was not involved in the study. Assuming the entity is treated with lobectomy—which it has been for decades, he says—nothing much has changed. While he calls it a well-done study, one that helpfully confirms earlier data, it doesn’t necessarily solve a long-standing problem he and his colleagues have been grappling with. NIFTP may be causing ripples, but it’s hardly threatening to break the levees.
The change might even create a new (if temporary) problem.
Clinical colleagues have raised few questions, says Dr. LiVolsi, but when they do it’s been at the prompting of patients who’ve read The New York Times article. “They want their tumor from two years ago to be reviewed, which is totally inappropriate,” says Dr. LiVolsi, who points to the obvious: Two years ago, the entity and the name did not exist. Patients were treated at the time according to the standards of the time, she says. “I feel strongly that research results—that’s what these are—do not belong in a patient’s medical record. To go back on the basis of somebody reading something in The New York Times? That’s wrong.”
Dr. LiVolsi
As of early May, Dr. LiVolsi had received one request. “I have refused to revise the diagnosis, and I have refused to look back at the slides. That case was signed out in 2012. In 2012, that was the diagnosis.”
Dr. Doherty is equally emphatic. He and his colleagues at Boston have heard from several patients wondering if the “new” tumor applied to them. “It hasn’t,” he says.
“We don’t see any clinical reason to go back and tell patients that a group of people has suggested we change the name of a low-risk disease they already knew they had. It doesn’t change clinical management at all. Changing the name doesn’t change the follow-up,” says Dr. Doherty.
Four years ago, Dr. LiVolsi notes, it was not the standard to examine the entire capsule. Older literature called for examining 10 sections of a nodule. “So you can’t apply current criteria or terminology to [a case from] two, four, six, 10 years ago and expect to bless it with this term.” It would, she agrees, be a bit like judging America’s founding fathers by today’s current moral standards.
Dr. Maytal, the MGH psychiatrist, also argues against such historical revisionism. “You operate with the knowledge that you had. At the time, they were given a diagnosis of cancer, and that’s what they had. That doesn’t negate or diminish anything they’ve experienced or however they were treated.”
These aren’t idle concerns. One pathologist has already heard from patients who are convinced their past lesions were misdiagnoses, and that they were overtreated as a result. But, says Dr. Nikiforov, “It’s important to stress that this was not an error before. This is a change in criteria; it’s not fixing an error.” The criteria, he reiterates, include examining the entire capsule, which might not be possible with archival cases.
Dr. Nikiforov mused on the possibility of revisiting old cases at the end of The New York Times piece. While he doesn’t say he misspoke to the reporter, he notes that when he and his colleagues then looked into doing it at UPMC, it quickly became clear how difficult the task would be. Not only might samples be insufficient for review, but would it be possible to contact former patients and their physicians? Rather than inviting such confusion, he and his UPMC colleagues are revisiting cases only at patient and/or clinician request, with results reported as an addendum rather than an amendment to the case.
Pointing the car in the other direction, so to speak, clinicians want firm answers about future cases. “They want to know how sure we are of the diagnosis,” Dr. Nikiforov says.
A NIFTP diagnosis is, in essence, a red traffic light. “They will stop completion thyroidectomy, they will stop radioactive iodine, they will stop very close follow-up,” Dr. Nikiforov says. “So they want to make sure pathologists are familiar with and understand how to make this diagnosis.”
Toward that end, in addition to reviewing cases as part of the study, Dr. Seethala, along with Dr. Nikiforov, oversaw development of the nuclear scoring scheme for including tumors into the NIFTP category.
“The scheme itself is not rocket science,” Dr. Seethala says. The basic nuclear features of PTC still form the basis for NIFTP, though the criteria have been restructured, Dr. Seethala says—the equivalent of moving furniture around rather than building a new house.
In the study, the scheme was used on still images of slides that were digitized in their entirety, to specifically focus on nuclear scores and increase reproducibility. In clinical practice, of course, pathologists will still need to find the relevant features themselves. “That’s going to be a challenge,” Dr. Seethala says.
There was some disagreement over the scores assigned to classify the nuclear features, Dr. Seethala continues. But collectively, within the test set and validation set, the accuracy was surprisingly high, based on prior review of the literature and given that reproducibility for nuclear features historically has been mediocre to poor, he says.
The scoring scheme should be useful in standardizing the NIFTP diagnosis, Dr. Seethala says, adding that its strength lies in how it was developed: The nine broad parameters used were assigned points, and a statistician reviewed the pathologists’ performances on both sets. “That type of thing is not typically done in pathology, despite its value,” he says. “It should be done more commonly,” he adds, though he admits it’s logistically difficult.
Though the published scheme should answer many questions, Dr. Seethala wants to make one point clear now: The grading scheme is not the only component of a NIFTP diagnosis. Its sole purpose is to help pathologists decide whether a tumor contains enough nuclear features to consider this entity.
Anticipating other misperceptions, Dr. Seethala pulls a few other potential weeds. “The general assumption is that this new category basically encompasses everything that we used to call encapsulated, well-demarcated or noninvasive follicular variant papillary thyroid carcinoma,” he says. “That’s true, to some extent.
“The difference is now we have a lot of criteria to ensure that we don’t keep in more aggressive tumors,” he continues. “As a result, you’re going to have to be stricter in terms of other growth patterns.” While they may have been a somewhat acceptable part of this category before, that’s no longer the case. This would include a true papillary component, solid component, and mitoses, which are now considered exclusionary criteria.
The goal, says Dr. Seethala, is to recognize that NIFTP is a neoplasm with a very low malignant potential based on the literature to date—nearly 500 cases. “But to ensure that, we have to keep this category fairly clean. That’s why the exclusionary criteria also come into play.”
At UPMC, Dr. Seethala says, the term NIFTP has already come into use. Because of the exclusionary criteria, “We’re finding we’re not using it as often as we anticipated.”
Reporting will continue to evolve, Dr. Seethala says. “If this is no longer equated at the same level as other carcinomas, AJCC staging is no longer relevant to this entity.” The relevant parameters are somewhat limited. “The name [NIFTP] implies the absence of a lot of things that we would normally report in a thyroid cancer in the CAP synoptic,” hence the current discussion about how/whether the synoptic should change. “Because it’s not entirely benign; it’s provisionally categorized into a very low malignant potential grouping. But it’s no longer ‘cancer.’” The CAP Cancer Committee’s head, neck, and endocrine panel is mulling it over, says Dr. Seethala, who is part of that group. “There may be room for a limited, optional data set,” he says. “The advantage of reporting these in synoptic form is that you can still capture these data points.”
Dr. Nikiforov sees two other long-term impacts, both of which he calls “quite interesting to think about.”
By way of background, thyroid cancer has been one of the fastest growing types of cancer in the United States as well as other countries, with rates tripling in the past 30 years. A significant portion, says Dr. Nikiforov, are what would now be called NIFTPs. Should this new category gain acceptance, it seems reasonable that the rate would drop, Dr. Nikiforov says.
More exciting, he says, is the possibility that this paper will point researchers in a similar direction for other indolent cancers, something the NCI has long been concerned about. The study could easily provide a blueprint for other groups that want to explore the possibility of reclassifying other types of indolent tumors. Indeed, he says he’s already been contacted by physicians who are interested in such work. “I hope this can have a profound effect, not only on pathology, but on the field of oncology.”
At its core, NIFTP is a surgical disease,but preoperative factors can predict its presence. The most potent are molecular markers.
The TCGA study (to simplify matters greatly) essentially identified two classes of tumors. It turns out, Dr. LiVolsi says, that the follicular variant of papillary carcinoma that is encapsulated—whether or not it’s invasive—tends to have molecular signatures closer to follicular adenoma than to classic papillary carcinoma. Although they share similar nuclei, from the molecular standpoint they really are not papillary carcinomas, says Dr. LiVolsi. “So these tumors not only appear to behave clinically very well, but also, at a deep level, they are different from papillary carcinomas.”
Dr. Nikiforov says he’s often asked if molecular testing is required to make a NIFTP diagnosis. His answer is simple: No.
Can the disease be predicted on molecular markers? His answer is just as succinct: Yes.
“The landscape of the molecular profile of NIFTP is pretty well defined,” Dr. Nikiforov says, as shown in the recent study and previous studies. “And now we are preparing another study to confirm it,” he says.
Four events—RAS mutations, PPARγ and THADA gene fusions, and (less commonly) BRAF K601E mutations (as opposed to the better-known BRAF V600E mutations)—are responsible for almost 90 percent of NIFTP. This gives rise to an interesting idea, Dr. Nikiforov says: Perhaps molecular testing on preoperative fine-needle aspiration biopsy can be used to make recommendations for lobectomy versus total thyroidectomy. UPMC routinely does such testing to reduce the extent of thyroidectomy, Dr. Carty says.
Another intriguing molecular development, says Dr. Nikiforov, is evidence that the more aggressive thyroid lesions have multiple mutations. If an examination of the nodule reveals only, say, a RAS mutation, there is a very good chance the tumor is a NIFTP, says Dr. Nikiforov. But finding RAS and, say, a TERT or TP53 mutation, “We know this is a really aggressive cancer and have to treat with total thyroidectomy.”
His UPMC colleague N. Paul Ohori, MD, professor of pathology, puts it in terms Ansel Adams would have appreciated: Molecular testing adds a layer of information to help sort out gray-zone diagnoses. “It’s adding or subtracting shades of gray,” says Dr. Ohori, medical director of cytopathology, UPMC Presbyterian.
Dr. Ohori’s main interest in NIFTP, not surprisingly, lies in implications for cytology.
Dr. Ohori
The diagnostic criteria for those categories may or may not change, says Dr. Ohori, who was not involved in the study. But there have been recent pilot studies looking at the influence of NIFTP diagnosis on the rate of malignant outcome. “As you would imagine, there is a drop in each of the diagnostic categories,” he says, with the “suspicious” diagnostic category showing the biggest decline—just over 40 percent.
Notes Dr. Ohori: “Each institution has a somewhat different threshold as to what they call NIFTP in surgical pathology, and where they draw the line for each diagnostic category in cytology.” Given such variations, “I would advocate each institution do its homework, if you will, in calculating out the risk of malignancy, based on the change in this categorization,” by doing the cyto-histo correlation for each of the Bethesda categories.
“I know that is a lot of work,” acknowledges Dr. Ohori, who adds that he and his colleagues were in the midst of doing this themselves. But the need is clear, he says. “It’s a matter of communicating the risk of a particular nodule to a clinician and patient. And in my opinion, nothing is better than your own personal data.”
Every change includes growing pains, Dr. Carty says. “When you remove the word ‘cancer,’ you reassure the patient and you reduce the health care cost burden. But you complicate the cytology reporting.”
There are also adjustments to be made on the clinical end, she says. The American Thyroid Association (she’s a board member) is responding to the JAMA Oncology study with a letter that will include concrete suggestions for implementing NIFTP. “This is groundbreaking,” she says. “But just like any enzyme, it requires some activation energy to get working.”
For the group Dr. Nikiforov assembled, the work continued right up until the meeting was adjourned. Once the group reviewed the clinical outcomes and refined the diagnostic criteria, one crucial task remained: What should they call these less-threatening lesions?
Enter MGH’s Dr. Maytal. “I have to give him credit for doing a lot to convince people,” says Dr. Nikiforov, who asked the psychiatrist to talk about the impact of the word “cancer.” “When patients hear that word, it’s a huge, huge change in how you see life, and this is a very, very big stress. And yet we know these tumors are indolent.”
Are psychiatrists typically part of the mix?
“I can tell you, this was not a usual meeting,” Dr. Nikiforov says. Conferences involving a pathological reclassification typically include only pathologists, he says. In this case, including a thyroid surgeon and two endocrinologists raised the level of discussion. So, he says, did the patient advocate. “She said, ‘Look, I am not a physician—I cannot tell you how to name this tumor. But you need to know that what you do is important for us,’” Dr. Nikiforov says. “I can tell you, it was very important for all of us in the room to hear that.”
Dr. LiVolsi called Dr. Maytal’s talk “absolutely amazing.” She recalls being particularly struck by one example. If a patient is told he has congestive heart failure and has a 50 percent risk of dying within five years without a transplant, he is likely to by buoyed by the idea he can be treated and will accept the diagnosis. Ditto for a patient who’s told he has chronic renal failure—he will accept the need for dialysis, understand he might be put on a transplant list, and, again, accept the diagnosis.
“But if you tell a patient they have basal cell carcinoma of the earlobe . . . ,” Dr. LiVolsi says.
Regardless of prognosis, says Dr. Giordano, “‘Carcinoma’ gives the message you’re a cancer patient. So FCIS, like DCIS, sent the wrong message.” It’s an idea he says he’s struggled with for years in his own practice. When he makes a cancer diagnosis but doesn’t think the entity will behave like a true cancer, he includes in his path report a comment to the effect that the likelihood of a clinically significant cancer occurring is exceptionally low, the implication being to refrain from drastic treatment.
Listening to Dr. Maytal speak about the impact on patients, Dr. Giordano says, was powerful. “As pathologists, we’re sort of removed from that. And it drove home the point that what we do is profoundly significant for people. ‘I’ve got a NIFTP in my thyroid’ doesn’t carry the same connotation as, ‘I have thyroid cancer.’”
Dr. Maytal’s clinical work involves caring for patients along the cancer spectrum, from diagnosis to end of life, through remission or relapse. “I think quite a bit about what the diagnosis means to people, and how they make sense of it.” Not surprisingly, he sees conversations, and creating the opportunity for conversations, as crucial.
Dr. Maytal
Once people hear the word “cancer” in their diagnosis, Dr. Maytal says, “they’re down that rabbit hole. The word destroys space for inquiry, no matter how well a clinician explains the word and why it may not be worrisome.” Patients simply stop listening when they hear it. On the other hand, “If I say you have a noninvasive follicular thyroid neoplasm with papillary-like nuclear features, you’re probably going to say, ‘What is that?’ And then you and your doctor can actually have a conversation.” These talks require more time, and physicians will have to answer more questions, he says. But it avoids trapping patients in the metaphor of cancer.
Naming these lesions would fluster even the slickest marketer. Neither encapsulated follicular variant of papillary thyroid cancer nor EFVPTC rolls off the tongue. Even as pathologists recognized, informally, that a new name might be useful, their efforts fell short. “A raft of names have been applied,” Dr. LiVolsi says. Follicular tumor of uncertain malignant potential? Follicular tumor borderline type?
“Noninvasive follicular tumor” worked for many, but it also describes follicular adenoma, which doesn’t have nuclear features. Hence the addition of the phrase “papillary-like nuclei.” Asks Dr. LiVolsi: “Do we like the term? Not really.” She says it sounds “stilted and a little strange.” But, like a cast-iron skillet, it’s useful, if not elegant. “It serves the purpose.”
Dr. Seethala says many have told him the name is awkward (bringing to mind the old saw that a camel is a horse planned by a committee). “I can’t disagree,” he says. “Luckily, the acronym is nice.” When you can’t say cancer or carcinoma, he says, “your options change quite a bit. How do you describe these nuclei if you’re not going to call this papillary carcinoma?”
As he considers the name, Dr. Giordano’s sympathies lie with his cytopathologist colleagues. Because they can’t assess invasion on FNA, they have to focus on nuclear features. Say they make a diagnosis of suspicious for papillary alterations based on nuclear alterations, which are recognized as papillary carcinoma, Dr. Giordano says. At surgery, “If we call it a noninvasive follicular thyroid neoplasm, we’re not closing that loop. We’re leaving cytologists out to dry.” Adding the phrase “with papillary-like features” ties things together and renders a diagnosis consistent with what cytopathologists see. “But as a consequence, the name got really long.” NIFTP, by comparison, seems positively elegant.
But even the acronym has sent people stumbling. Says one observer, “We’re not really sure how to pronounce it.” Some call it nift-P. Others recite the letters, N-I-F-T-P, and some are suggesting that despite its spelling, “Nifty” might be appropriate. Dr. Ohori is fond of using “Nift shift” to describe the transition.
Some question whether the name needed to change at all.
Dr. Doherty
“I think the nomenclature change is a bad thing,” Boston University’s Dr. Doherty says. The impact on treatment is nil, he says, since these patients have been seen, and treated, as low risk for years.
He’s not insensitive to the impact of the words “cancer” and “carcinoma.” They might be important from a personal point of view, he says. Likewise, not being labeled with a cancer diagnosis might make it easier to obtain, say, life insurance. And for a patient needing a kidney transplant, for example, a diagnosis of a benign neoplasm doesn’t have the same implication as a malignant neoplasm. But even in that latter scenario, says Dr. Doherty, the fix is relatively simple. “It has involved someone with molecular knowledge writing a letter saying there’s no risk of recurrence.” It’s an extra step, not a prohibitive problem, in other words.
Given the choice, Dr. Carty says she prefers “carcinoma in situ.”
Are her patients okay with the word “carcinoma”? It depends, she says, on who they it hear it from. “What I really dread is when someone has shared the pathology report with the patient before I do.”
“When my patients hear the words ‘thyroid cancer,’ they’re unsettled until I talk to them,” she says. “I immediately explain to them that most forms of thyroid cancer have a wonderful prognosis, and the odds are excellent they’re going to live to be 99 and die of something else.”
Dr. Doherty agrees. In his experience, it’s the clinicians’ job to recognize how the word “cancer” might affect patients. “We have to manage their expectations of what the diagnosis means, whether it’s cancer or not.” While the psychological implications are real, and important, he says, “It’s not as simple as saying, ‘This isn’t cancer; this is cancer.’ We need a deeper conversation with our patients.”
While the study has generally garnered high praise, more work needs to be done.
The study looked at and validated the nuclear features in isolation. Now “it would be good to validate that across different practice patterns,” Dr. Seethala says. It works among experts and specialists, but what about those who practice in a more general setting? And though the study addressed nuclear features in a methodical fashion, it would be nice to do the same for the other inclusion/exclusion criteria as well, he says. The group decided on the latter by consensus, so they’re not as well vetted.
The follow-up is impressive, Dr. Seethala says, but thyroid cancer itself is somewhat indolent. “So is 13 years enough? Possibly not. Some people talk about much longer follow-up.”
Most agree that the variant papillary lesions are diagnostically challenging. “Pathologists have had trouble with these lesions for a long time,” Dr. Doherty says. “In fact, we all know we can send the same slides to different pathologists and get different results. Whether they’re encapsulated or not, some pathologists will call most of them benign; some pathologists will call most of them cancer. And that has more to do with individual bias and criteria than the biology of the lesion.”
Ideally, he adds, “We would like to see a more definitive way to make a consistent diagnosis on the part of the pathologist,” perhaps through different criteria for light microscopy or more definitive molecular characterization. But even if this category can be tidied up, so to speak, “That might make the other categories adjacent to this one more fuzzy,” he says with a rueful laugh.
It would also be good to look at NIFTP prospectively, on a population-level scale, Dr. Seethala says. “That’s where its role in terms of being reported in the registry becomes important. It’s better to know that there’s a half a percent recurrence for these tumors based on thousands of cases, rather than hundreds.”
As he continues to talk about additional studies he would like to see, including scoring schemes for oncocytic lesions and multifocal, small tumors, Dr. Seethala suddenly stops. He applauds the multidisciplinary, systematic approach to reclassification, but contrary to what optimists might think, he says, the NIFTP entity “doesn’t solve all the thyroid problems we have, even pertaining to these indolent entities.” Rather, he says, “It’s a shift in the right direction.”
[hr]
Karen Titus is CAP TODAY contributing editor and co-managing editor.