Introduction
Endoscopic ultrasound (EUS) is routinely used for patients undergoing surveillance
for presumed cystic neoplasms (PCN), especially presumed mucinous cysts including
mucinous cystic neoplasms (MCN) and intraductal papillary mucinous neoplasm (IPMN).
Although there has been a move away from routine EUS examinations for surveillance
in favor of using noninvasive imaging with computed tomography (CT) or magnetic resonance
imaging (MRI) instead, recent guidelines including the American Gastroenterological
Association (AGA), [1 ] the Fukuoka, [2 ] more recently the revised Fukuoka, [3 ] and American College of Gastroenterology (ACG) [4 ] guidelines, published in 2015, 2012, 2017, and 2018, respectively, recommend EUS
with fine-needle aspiration (FNA) for patients who on CT or MRI have a morphologic
change (e. g. dilated main pancreas duct, cyst size ≥ 30 mm, solid cystic component,
and more recently increasing cyst growth rate in the revised Fukuoka guidelines).
Although visualization and characterization of PCNs may be better achieved with EUS,
the quality of existing noninvasive imaging such as CT or MRI scans may be sufficiently
good that the true impact on diagnosis and management of EUS performed during surveillance
of presumed mucinous cysts for the indication of new morphological change seen on
noninvasive imaging remains unclear.
This matter is further complicated by interoperator variability in cyst characterization,
measurement, and classification amongst different radiologists. One retrospective
evaluation of PCNs (with pathologic confirmation) by two radiologists, using well-established
morphologic features, agreed on correct diagnosis in only 60 % of cases [5 ]. An additional study assessing interobserver variability in measurement of PCNs
with MRI and the impact of measurement standards showed that the within-subject standard
deviation measurement variability only changed from 4.0 mm prior to standardization
to 3.3 mm after introduction of measurement standards. In the same study, inter-observer
agreement, kappa, improved from 0.59 to 0.65 (P = 0.04), suggesting that there is significant and frequent interobserver variability
in measurement of pancreatic cystic lesions with MRI, which could affect clinical
management [6 ]. Additional studies have supported this real discrepancy in measurement of pancreatic
cyst size between CT and MRI imaging, which becomes relevant in cases where imaging
modality may be switched during follow-up either because of timing, availability,
or patient characteristics which may preclude them from undergoing one particular
type of study [7 ].
The primary aim of this study was to detect changes in diagnosis and/or management
decisions based on addition of EUS results compared with noninvasive imaging alone.
Furthermore, we aimed to determine which subgroup(s) of patients, if any, truly benefit
from EUS when performed after a routine surveillance CT or MRI shows a morphologic
change.
Patients and methods
A single-institution pancreatic cyst database was queried for all patients who underwent
esophagogastroduodenoscopy with EUS for evaluation of a PCN during surveillance after
a noninvasive imaging study (CT or MRI) suggested a morphologic change such as cyst
size increase, a cyst ≥ 30 mm, change in main pancreatic duct (PD) caliber, or a cyst
with a solid component during a defined period of time (January 1, 2013 – October,
2016).
Using available clinical and imaging data, diagnoses were classified both before and
after EUS as: presumed mucinous without worrisome features (WF) or high-risk stigmata
(HRS), with WF or with HRS, or non-mucinous lesions, using previously published guidelines
[2 ]. Worrisome features were defined as clinical pancreatitis, cyst ≥ 3 cm, thickened/enhancing
cyst walls, main PD size 5 mm to 9 mm, non-enhancing mural nodule, and/or abrupt change
in caliber of pancreatic duct with distal pancreatic atrophy. High-risk stigmata were
defined as obstructive jaundice in a patient with cystic lesion of the head of the
pancreas, enhancing solid component within cyst, and/or main PD ≥ 10 mm. Non-mucinous lesions were categorized as either serous cystadenomas (SCA) or pseudocysts.
Presumed mucinous cysts were defined as unilocular or multifocal cysts with elevated
carcinoembryonic antigen (CEA) levels (> 192 ng/UL), positive mucinous cytology of
any grade, communication of the cyst with the main PD, with lack of convincing evidence
supporting a non-mucinous lesion such as a SCA or a pseudocyst. SCA were defined as
microcystic lesions with or without a central calcification, as well as a low CEA
(< 2 ng/UL) [8 ]. Pseudocysts were defined as lesions with pancreatic fluid collections arising in
the setting of pancreatitis (without prior evidence of a pancreatic cyst), with or
without confirmation of resolution of the pancreatic fluid collection with time or
after drainage.
Management decisions were defined a priori as either surgical evaluation for all patients
diagnosed with presumed mucinous lesions with HRS or for those with positive cytology
or a mural nodule, or continued surveillance for all others. Both pre- and post-EUS
diagnoses and management decisions were made separately in a blinded fashion to avoid
bias.
We collected baseline characteristics such as size and location as reported by CT
or MRI. Imaging reports reviewed included initial noninvasive imaging that first described
presence of a PCN, the “baseline image”; the imaging that triggered the indication
for EUS based on a change in pancreatic cyst morphology, the “trigger image”; and
the noninvasive imaging report that immediately preceded the trigger image, the “comparison
image.” By comparing data gathered during these imaging studies, we extrapolated changes
in morphologic characteristics including overall size of the cyst during surveillance
period as well as the rate of change, “cyst change rate.” We calculated and recorded
“cyst change rate” by first calculating the overall growth, in millimeters, and then
dividing by the number of months that had elapsed between imaging studies. Thus, “cyst
change rate” represents the rate of change in size of the PCN. We also recorded any
changes in caliber of the main PD. Furthermore, we evaluated the “cyst change rate”
of each case that triggered the EUS in order to determine if there were factors which
were predictive of a change in diagnosis or management.
Both diagnoses and management decisions were determined based on the clinical and
radiologic imaging available at the time of the “trigger image” and again after the
subsequent EUS was performed. Management decisions included continued surveillance
with CT or MRI imaging with the same or increased or decreased frequency, or referring
the patient for surgical evaluation.
Results are presented as mean ± standard deviation or median with interquartile range
when data are skewed. Categorical variables (e. g. presence of change in cyst size,
cyst size ≥ 30 mm, change in main PD caliber, presence of a solid cystic component)
were analyzed using chi-square testing. A P value < 0.05 was considered statistically significant. Using logistic regressions
analysis, we examined variables that could be used as predictors for a change in diagnosis
or management post-EUS compared to diagnosis and management pre-EUS. IRB approval
was sought and obtained prior to the initiation of this study.
Results
Between January 2013 and October 2016, a total of 709 EUS examinations for evaluation
of a PCN were completed at our institution. A total of 89 examinations were performed
(M:F – 34:55, average 65.36 ± 13 years, range 15 – 82 years) for the indication of
cyst morphology change, including a change in cyst size (87 examinations), a cyst ≥ 30 mm
(27 examinations), a change in PD caliber (8 examinations), and a cyst with a solid
component (1 examination). Total surveillance time amongst these 89 cases was on average
3.58 ± 2.57 years.
Presumed mucinous neoplasms
A total of 70 pancreatic cyst EUS examinations were performed in 59 patients for presumed
mucinous cyst of the pancreas (M:F – 21:38, average 66.9 ± 12 years, range 28 – 82
years) who had been under surveillance for 3.5 ± 2.25 years. Indications for EUS examinations
included change in cyst size (68 examinations), a cyst ≥ 30 mm (10 examinations),
a change in PD caliber (7 examinations), and a cyst with a solid component (1 examination).
Preceding EUS, patients were imaged with CT or MRI at least twice, an earlier “comparison
image” and a second, “trigger image”, leading to the EUS. These two noninvasive imaging
studies were done 2 ± 1.9 years apart during which time the lesion being surveyed
grew 6.57 ± 7 mm for a “cyst change rate ” of 0.64 ± 1 mm. The time elapsed between
the “trigger image” and the resulting EUS occurred at an average 3 ± 4 months after
the “trigger image.”
Impact of EUS on diagnosis and management
Prior to EUS, patients with presumed mucinous cysts of the pancreas were categorized
as follows: without WF or HRS – 52 cases (cyst size 18.6 ± 6 mm), with WF – 17 cases
(cyst size 28.8 ± 18 mm), and with HRS – 1 case (cyst size, 22 mm). Accordingly, the
management plan was to continue surveillance with CT/MRI imaging in all cases with
the exception of the one case with HRS, which would be referred for surgical evaluation.
Following EUS done for indication of morphologic change, the distribution of diagnosis
changed ([Fig. 1 ]). Of the 52 cases classified as presumed mucinous neoplasm without WF or HRS, 47
cases remained classified as the same after EUS. Of the remaining five cases, one
case was changed to SCA, and four cases (7 %) were upgraded to a worse diagnosis –
one neuroendocrine tumor (NET), one adenocarcinoma, one presumed mucinous neoplastic
cyst with WF, and one presumed mucinous neoplastic cyst with high-grade dysplasia
(HGD) considered to be malignant. Management decisions changed as well, with 3 cases
(NET, adenocarcinoma, and HGD) all being referred for surgical evaluation (instead
of ongoing surveillance) ([Fig. 2 ]).
Fig. 1 Changes in diagnosis in patients undergoing surveillance following EUS.
Fig. 2 Changes in management in patients undergoing surveillance following EUS.
Of the 17 cases classified as presumed mucinous with WF prior to EUS, three were downgraded
to presumed mucinous without WF, two were upgraded to a worse diagnosis – one malignancy
and one presumed mucinous with HRS, and 12 remained presumed mucinous with WF of which
nodules were detected in four cases ([Fig. 3 ]). Management decisions were impacted; six cases were referred for surgical evaluation
(1 malignancy detected on FNA, 1 HRS, and 4 cases with nodules).
Fig. 3 Mural nodule detected on EUS not detected on prior cross-sectional imaging.
The single case classified as presumed mucinous with HRS prior to EUS was in fact
detected to be a malignant lesion following EUS. Management did not change as the
patient was referred for surgical evaluation regardless.
In total, EUS done for morphologic change resulted in a change in diagnosis in 11
cases (16 %), with 7 cases (64 %) being a worse diagnosis. In addition, mural nodules
were detected using EUS in four cases not detected on cross-sectional imaging, ranging
from 2.4 mm to 11 mm × 8 mm in size. In total, management decisions were changed in
9 cases (13 %) leading to surgical evaluation.
Using logistic regressions analysis, we examined variables that could be used as predictors
for a change in diagnosis or management after EUS was done for morphologic change.
Among our cohort, 47 cases demonstrated a “cyst change rate” ≥ 2 mm/year, of which
9 (19 %) had a change in diagnosis. This did not represent a significant correlation
(P = 0.318). However, overall growth of ≥ 10 mm was found to be a significant predictor
of change in diagnosis P = 0.01, with 11 cases having ≥ 10 mm of growth and 5 (45.5 %) having a change to
a worse diagnosis (P = 0.01). The indication of cyst size ≥ 30 mm and presence of any growth of a cyst,
and presence of both features had significant correlation with changes in diagnosis
(P = 0.015, 0.004, and 0.009, respectively). ([Table 1 ]). There were no significant predictors of changes in management following EUS.
Table 1
Changes in diagnosis pre- vs. post-EUS.
Total # of EUS procedures
Change in Diagnosis post EUS/FNA
P value
Indication
Cyst Growth
68
10
0.004
Cyst ≥ 30 mm
10
3
0.015
Growth + Cyst ≥ 30 mm
10
3
0.009
Cyst Growth ≥ 10 mm
11
5
0.01
Cyst Change rate ≥ 2 mm/year
47
9
0.318
Discussion
The ability to accurately preoperatively classify pancreatic cysts in surveillance
studies remains challenging, as no reliable method exists to consistently predict
whether a PCN will degenerate to advanced malignancy. Identifying high- and low-risk
lesions reliably could lead to early referral and intervention in patients whose lesions
would eventually progress to malignancy and allow for periodic imaging in those cases
where progression to malignancy is unlikely (but still possible) [9 ]. For example, whereas the rates of progression to malignancy for SCA are negligible,
those for IPMNs carry a wide range of malignant potential (5 % – 62.2 %) [2 ]
[10 ]
[11 ].
Several studies report poor accuracy rates for classifying pancreatic cysts preoperatively,
however, most of these are either out of date or focused on the inaccuracies of separating
main duct from branch duct IPMN [5 ]
[12 ]. With increasing interest in pancreatic cyst surveillance, there are growing guidelines
for more accurate preoperative diagnoses and management of pancreatic cysts, however,
they may be understating the modest but significant role of EUS [1 ]
[2 ].
This becomes problematic for practitioners who are deciding between referring patients
for aggressive surgical intervention or conservative surveillance. Patients who undergo
aggressive pancreatic surgical intervention, according to a longitudinal study including
851 patients who underwent resection for a cystic neoplasm of the pancreas, are at
considerable risk for postoperative complications and mortality [13 ]. These risks of malignant degeneration must be balanced with risks and benefits
associated with definitive surgical management, patient comorbidities, and life expectancy.
Recent guidelines have favored less invasive imaging both during initial evaluation
and management during surveillance, as well as even making recommendations about stopping
surveillance in certain subgroups (e. g. those without positive features on cross-sectional
imaging over 5-year surveillance and those who lack positive cytology and positive
features on initial EUS followed by stable cross-sectional imaging during 5-year surveillance)
[1 ].
Our data suggest that use of selective EUS impacts both diagnosis and management of
pancreas cystic neoplasms during surveillance. Overall, EUS performed during routine
surveillance of presumed mucinous neoplasms done for a change in morphology resulted
in a change in diagnosis and management in 11 (16 %) and 9 cases (13 %), respectively.
This is not surprising based on existing data on the impact of EUS on diagnosis and
management [14 ]
[15 ]
[16 ]
[17 ]. When comparing noninvasive cross-sectional imaging with EUS in terms of diagnostic
accuracy, one retrospective review noted that diagnostic accuracy for neoplastic cysts
(defined as cystic pancreatic ductal adenocarcinoma, cystic pancreatic neuroendocrine
tumor, MCN, IPMN, and solid pseudopapillary neoplasm) improved by 36 % with the addition
of EUS compared to CT or MRI alone [18 ]. When noninvasive imaging alone is used to make preoperative diagnosis in patients
undergoing surgical intervention, accurate diagnosis are made in 30 % and 29 % of
cases of mucinous cystadenoma and mucinous cystadenocarcinoma as demonstrated in a
large multicenter study [5 ]. This is due in large part to the superior imaging with EUS and its ability to detect
cystic features such as nodules ([Fig. 4a ], [Fig. 4b ], and [Fig. 4c ]). Among our cohort of patients, 4 (6 %) were found to have a nodule using EUS not
detected with cross-sectional imaging. It has been suggested that significant proportion
of echogenic nodules identified on EUS are in fact mucus, however, experienced endosonographers
are able to perform maneuvers during EUS examinations, and thereby increase diagnostic
sensitivity and specificity. These maneuvers include changing patient body position
and attempting to dislodge echogenic materials from needle tip prior to performing
fine-needle aspiration (FNA) [19 ]. Among mural nodules detected in our series, all would have qualified for surgical
evaluation per Fukuoka guideline, as presence of mural nodule regardless of size represents
indication for surgical evaluation. Newer European guidelines include a size cut-off
of > 5 mm, above which surgical evaluation is absolutely indicated [20 ]. Adding FNA resulted in a change in diagnosis in an additional 5 cases (7 %) due
to the added benefit of cytology and tumor marker data, making supplementation of
noninvasive imaging with EUS examinations valuable in evaluation of patients with
cystic lesions. In a prospective study looking at 302 patients with pancreatic cysts
including 110 measuring < 30 mm, the overall impact of EUS on management was calculated
to be 72 % of cases [21 ]. In our cohort, diagnosis was upgraded to a worse diagnosis or the same diagnosis
with higher-risk features in 11 patients (16 %), with 9 (13 %) additional patients
necessitating surgical evaluation.
Fig. 4 Image series demonstrating a the same pancreas cyst as seen on initial cross-sectional imaging, b follow-up trigger cross-sectional imaging, and c subsequent EUS imaging.
Overall growth rate of cystic neoplasms, and not just the actual size should also
be taken in to consideration when making management decisions. It has been suggested
that a growth rate of ≥ 2 mm/year and total growth ≥ 10 mm are predictive of BD-IPMN
malignant degeneration and should be considered worrisome features [20 ]
[22 ]
[23 ]. In fact the most recent revision of the Fukuoka guidelines does include a rate
of cyst size change of > 5 mm within 2 years as a worrisome feature necessitating
EUS evaluation for further evaluation [3 ]. This conclusion was drawn from following a cohort of 284 patients with presumed
BD-IPMN without WF or HRS for an average of 56 months [22 ]. On closer examination of the 9 patients who developed malignant lesions amongst
this cohort, it was found that their growth rate was 18.6 mm/year compared with 0.8 mm/year
in patients who did not develop malignant lesions. In our cohort of patients with
presumed mucinous cysts, the average pancreatic cyst growth rate was 7.68 mm/year.
Among patients whose post-EUS diagnosis was worse than pre-EUS, a pancreatic cyst
growth rate of 12.48 mm/year was measured and was higher still in patients who developed
malignant lesions, 14.58 mm/year, compared with 5.76 mm/year in patients with no change
in diagnosis. From our cohort, the pancreatic cyst growth rate of ≥ 2 mm/year could
be used as a predictor for a worse diagnosis following EUS, however, the sample size
may not be large enough to draw a significant conclusion (P = 0.318). Similarly, considering overall growth in cyst size with various cutoffs
can also serve as a reliable predictor for changes in diagnosis, thereby supporting
use of EUS in patients who demonstrate significant growth during surveillance. In
our cohort, patients with presumed mucinous neoplasms of the pancreas that grew by
≥ 10 mm, regardless of the rate of growth, were more likely to have a change in diagnosis
following EUS (P = 0.01).
There are several limitations of this study. A limitation of surveillance studies
in general, including our own, is that the majority of pancreatic cysts are not operated
on and do not have a definitive diagnosis. By virtue of limitation in diagnostic accuracy
of both imaging and cyst fluid biomarkers, diagnoses remain presumed based on available
imaging and clinical data. In addition, our study is retrospective and thus is open
to biases in terms of defining diagnosis and management decisions. To overcome these
inherent biases, both diagnoses and management decisions were defined a priori and
were applied to both the pre- and post-EUS scenarios in a blinded fashion. In addition,
relying on imaging reports to document changes in cyst size is concerning due to the
lack of standardization of measurement. CT or MRI, rather than EUS, are appropriate
for surveillance in many cases of PCNs, especially those ≤ 30 mm, without thickened
or enhancing walls, main PD size < 5 mm, non-enhancing nodule, and without abrupt
change in main PD caliber [2 ]. However, the problem arises when considering cases where these characterizations
cannot be reliably made and the fact that interobserver agreement in classifying pancreatic
cysts using MRI is moderate at best, with variability in cyst size characterization
amongst radiologists measured to be 4 mm, and agreement in characterization in just
51 % of cases [6 ]
[24 ]. Discrepancies are also described between radiologists assessing patients for pancreatic
cystic neoplasms on CT compared to MRI, with a median difference in cyst measurement
of 1.5 mm between the two modalities, which led to an inappropriate change in surveillance
regimen in 6 % of cases [7 ]. EUS, like CT and MRI, is also prone to interobserver discrepancy in interpretation
[25 ]
[26 ]. It is to be noted that our evaluation and recording of presumed mucinous lesions
on noninvasive imaging did not include reevaluation of actual films. While reviewing
films would allow us to ensure consistent and accurate measurements of presumed mucinous
lesions, it is unlikely that this is what actually happens consistently in clinical
practice. This draws attention to the importance of consistent and standardized techniques
for measuring and reporting presumed mucinous lesions by radiologists. However, use
of the imaging reports rather than formally documenting and remeasuring all the imaging
reflects the “real-world” scenario of how patients with pancreatic cysts are managed.
Prospectively, standardization of how pancreatic cysts are documented and reported,
in addition to formal multidisciplinary imaging review, will improve this issue. Furthermore,
our study was also limited by the fact that CEA measurements were not available in
several patients.
Currently pancreatic cyst fluid biomarkers (e. g. CEA, Kras, GNAS) may have a role
in differentiating mucinous from non-mucinous cysts, however, not with sufficient
accuracy to ignore other clinical and radiologic data when making decisions regarding
surgical or surveillance management [27 ]
[28 ]
[29 ]
[30 ]. Pancreatic cyst fluid biomarkers are currently inaccurate for making the diagnosis
of advanced malignancy including HGD and cancer [31 ]. However, it is possible that with development of next-generation DNA sequencing
markers and methylation markers, this may improve. It is also therefore possible that
in the future these newer cyst fluid biomarkers may be incorporated into clinical
guidelines about surveillance and surgical management.
Finally, although this study focused on the impact of EUS on diagnosis and/or management,
we were unable to calculate the impact of EUS on overall outcome in this patient subgroup. A
future direction of our research will be to inquire as to the final outcomes of patients
who were referred for surgical evaluation (if an intervention was undertaken that
changed their overall outcome), as there are very few studies looking at the role
of EUS in overall outcome in patients with pancreatic cysts [32 ].
Conclusion
In evaluating the role of EUS and whether there is added benefit in diagnosis and
management of patients who are enrolled in surveillance programs for presumed mucinous
lesions, EUS carries a modest but clinically significant role in changing diagnosis
and management when performed for the indication of morphologic change. Furthermore,
predictors such as interval growth between noninvasive imaging studies as well as
the rate of growth may also be valuable clinical predictors of worsening clinical
diagnosis after EUS.