Why is endosonography insufficient for residual diagnosis after neoadjuvant therapy for esophageal cancer? Solutions using muscle layer evaluation.

BACKGROUND: The diagnosis of residual tumors using endoscopic ultrasound (EUS) after neoadjuvant therapy for esophageal cancer is considered challenging. However, the reasons for this difficulty are not well understood. AIM: To investigate the ultrasound imaging features of residual tumors and identify the limitations and potential of EUS.
METHODS: This exploratory prospective observational study enrolled 23 esophageal squamous cell carcinoma patients receiving esophagectomy after neoadjuvant therapy [15 patients after neoadjuvant chemotherapy (NAC) and 8 patients after chemoradiotherapy (CRT)] at the Department of Surgery, Chiba University Hospital, between May 2020 and October 2021. We diagnosed the T stage for specimens using ultrasound just after surgery and compared ultrasound images with the cut surface of the fixed specimens of the same level of residual tumor. The ratio of esophageal muscle layer defect measured by ultrasound was compared with clinicopathological factors. Furthermore, the rate of reduction for the muscle layer defect was evaluated using EUS images obtained before and after neoadjuvant therapy.
RESULTS: The accuracy of T stage rate was 61% (n = 14/23), which worsened after CRT (38%, n = 3/8) than after NAC (73%, n = 11/15) because of overstaging. Moreover, pT0 could not be diagnosed in all cases. The detection rate of residual tumor for specimens using ultrasound retrospectively was 75% (n = 15/20). There was no correlation between after-NAC (79%, n = 11/14) and after-CRT (67%, n = 4/6) detection rate. The detection of superficial and submucosal types was poor. The pathologic tumor size and pathological response were correlated. Tumor borders were irregular and echogenicity was mixed type after CRT. There was a correlation between the pT stage (pT0/1 vs pT2/3) and the length of muscle layer circumference (P = 0.025), the length of muscle layer defect (P < 0.001), and the ratio of muscle layer defect (P < 0.001). There was also a correlation between the pT stage and the rate of muscle layer defect reduction measured by EUS (P = 0.001).
CONCLUSION: Compared to pathological images, some tumors are undetectable by ultrasound. Focusing on the esophageal muscle layer might help diagnose the depth of the residual tumor. ©The Author(s) 2022. Published by Baishideng Publishing Group Inc. All rights reserved.

Core Tip: This exploratory prospective observational study evaluated the effectiveness of endoscopic ultrasound (EUS) in diagnosing residual tumors after neoadjuvant therapy for esophageal squamous cell carcinoma. It is well known that the diagnosis using EUS after neoadjuvant therapy is inaccurate. The results of ultrasound for surgical specimens are not satisfactory as well. Our study found that the inability to distinguish scar tissue from the tumor made detection and diagnosis impossible in some residual tumors. Esophageal muscle layer defect as an indirect finding correlated with the depth of the residual tumor. These insights could help improve the diagnosis of residual tumors.

INTRODUCTION

Esophageal cancer is the seventh most common cancer worldwide in terms of incidence and the sixth most common in terms of mortality. Especially in Asia, esophageal squamous cell carcinoma (ESCC) accounts for more than 90% of all esophageal cancers[1]. There is strong evidence supporting the superiority of neoadjuvant chemoradiotherapy (CRT) and neoadjuvant chemotherapy (NAC) plus surgery over surgery alone for locally advanced esophageal cancer[2]. In ESCC patients, pathological complete response (pCR) was 62% after CRT and 2%-7% after NAC[3-5]. While patients with pCR may have avoided unnecessary esophagectomy, the residual tumor must be accurately identified to justify not performing a surgical resection.

In contrast, residual tumors after CRT and NAC are often present only at a depth of the esophageal wall, without any exposure to the superficial mucosa[6,7]. Although Endoscopic ultrasound (EUS) has a well-established role in the initial staging of esophageal cancer[8], the diagnosis of esophageal cancer after neoadjuvant therapy has been controversial. EUS sensitivity for residual tumors at the primary site after neoadjuvant CRT is as high as 0.96; however, the specificity is as low as 0.08, and thus it does not seem to be sufficiently accurate to detect residual tumor[9]. In addition, the accuracy of staging after NAC is not sufficient[10]. Several studies have correlated EUS measurements with tumor regression grade and survival. However, it is unclear whether the echogenic lesions detected using EUS are indeed residual tumors and how they appear on ultrasound. The purpose of this study was to characterize the ultrasound images of residual tumors, explore the limitations of EUS, and assess its potential in residual diagnosis.

MATERIALS AND METHODS

Patient population

This exploratory prospective observational study was conducted in two steps. The first step (study 1) aimed to investigate the limitations and characteristics of residual tumor diagnosis using ultrasound. Based on study 1, the second step (study 2) aimed to implement EUS to detect remanent tumors deep in the muscle layer. Study 1 enrolled 23 ESCC patients undergoing esophagectomy after neoadjuvant therapy, including NAC or CRT in the Department of Surgery, Chiba University Hospital, between May 2020 and October 2021. All patients were histologically proven to have ESCC based on biopsy specimens. The clinical stage was determined by endoscopy, barium esophagography, chest and abdominal computed tomography (CT) scans, and 18F-fluorodeoxyglucose positron emission tomography, based on the 11th Edition of the Japanese Classification of Esophageal Cancer[11]. Study 2 enrolled 20 out of the initial 23 participants in the first study who underwent EUS for staging and were diagnosed with cT2 or deeper. Our Institutional Review Board (IRB No. 3550) approved this study. We obtained written informed consent from patients for all examinations and treatments.

Preoperative and surgical treatment

As recommended by the Japanese Clinical Oncology Group (JCOG) 9907 Study, we performed preoperative chemotherapy postoperatively for patients with clinically UICC stage II/III resectable ESCC in our department's criteria[5]. NAC was composed of two cycles of 5-fluorouracil (800 mg/m2 infusion for five consecutive days) and cisplatin (80 mg/m2 on day 1). Some patients received three cycles of docetaxel (70 mg/m2 on day 1), cisplatin (70 mg/m2 on day 1) and 5-fluorouracil (750 mg/m2 infusion for five consecutive days) based on the JCOG 1109 study[12]. After NAC, all patients were evaluated by CT, PET, and endoscopy, and underwent radical esophagectomy with three-field lymphadenectomy, including cervical, mediastinal, and abdominal lymph node dissection. CRT was composed of 2 Gy/fraction at a total dose of 40 Gy with a long-T radiation field from the cricoid cartilage to the upper abdomen, including the gross tumor volume. Concurrent chemotherapy was performed with 5-fluorouracil (500 mg/m2 infusion on day 0-4) and cisplatin (15 mg/m2 on day 1-5). After receiving a 40 Gy dose, all patients were evaluated by CT, PET, and endoscopy. An additional 20 Gy dose was delivered to patients with potentially resectable tumors, making the total irradiation dose 60 Gy (definitive CRT), and concurrent chemotherapy with the same regimen was also provided. After CRT, patients with resectable tumors underwent radical esophagectomy with three-field lymphadenectomy four weeks after CRT. The criteria for the pathological response of primary tumor were categorized as ineffective (Grade 0); viable cancer cells accounted for 1/3 or more of tumor tissue (Grade 1); viable cancer cells accounted for less than 1/3 of tumor tissue (Grade 2); no viable cancer cells (Grade 3).

Procedure of ultrasound for surgical specimens

In study 1, the surgical specimens of all patients were collected from the operation room, and an ultrasound was performed immediately. The unfixed specimens immersed in saline solution were scanned vertically and horizontally using 15 MHz electronic linear ultrasound. The imaging procedure was recorded on video. We used LOGIQ S8 (GE Healthcare Japan Corporation, Tokyo, Japan) ultrasound platform in all studies. The ultrasound for specimens showed the mucosal layer, submucosal layer, inner muscle layer, intermuscular connective tissue layer, and outer muscle layer, as shown in EUS. We diagnosed the presence and depth of the tumor on the day of surgery before pathology results were known. We assessed the accuracy of diagnosing residual tumor depth using ultrasound. The prefix “u” indicates ultrasound diagnosis. Furthermore, to clarify the characteristic features of residual tumor, we compared ultrasound images with the cut surface of the fixed specimens at the same level of tumor site in the esophageal wall.

Measurements of muscle layer defect

In study 1, in addition to the direct finding of the tumor, we focused on the esophageal muscle layer as an indirect finding, which is the most visible on ultrasound. We set up a cross-sectional image vertical to the esophagus at the center of the tumor. We measured the length of muscle layer circumference and the length of muscle layer defect. We calculated the ratio of muscle layer defect and compared each pathological factor.

Muscle layer defect angle

Study 2 aimed to evaluate the muscle layer defect using EUS. However, the EUS and ultrasound findings for specimens were different since the specimens were fully stretched. Keeping the esophageal wall stretched in vivo and measuring the circumference of the muscle layer by EUS would be challenging. Therefore we substituted the ratio of muscle layer defect with the total circumference of the muscle layer by the angle and named it as muscle layer defect angle (MDA). MDA was defined as the angle between the center of the lumen and the two points where EUS could not help visualize the inner muscle and intermuscular connective tissue layer. Using MDA, we measured the percentage of improvement in muscle layer defect caused by neoadjuvant therapy using the still images as well as video images of EUS. EUS was performed before and after neoadjuvant therapy by three or more skilled endoscopists. We calculated the MDA reduction rate using Pre-MDA and Post-MDA. MDA reduction rate was expressed using the following equation:

MDA reduction rate (%) = {[PreMDA(°) - PostMDA(°)] / PreMDA(°)} × 100

We compared each MDA factor with the pathological T stage. The echo images were analyzed using ImageJ software (National Institutes of Health, available at http://rsb.info.nih.gov/ij) specialized for morphological evaluation.

Statistical analysis

This study compared the results of prospectively collected data after confirming pathology. All statistical analyses were conducted with the JMP® Pro software program, version 13.2 (SAS Institute Inc., Cary, NC, United States). Continuous variables were expressed as median (min–max) or mean (± SD). Fisher’s exact test was used to compare and analyze categorical variables. Continuous variables were analyzed using Wilcoxon’s signed-rank sum test. P values of < 0.05 were considered statistically significant. Receiver operating characteristics (ROC) analysis was performed to assess the highest diagnostic values to determine the optimal cut-off points.

RESULTS

Patients’ characteristics

From May 2020 to October 2021, 61 patients underwent esophagectomy for esophageal cancer, and 37 patients underwent neoadjuvant therapy in our department. Of these, we excluded 5 patients with adenocarcinoma, 2 patients with neuroendocrine carcinoma, and 7 patients whose surgical specimens could not be analyzed using ultrasound. The clinical characteristics and pathological examination are summarized in Table 1. Fifteen patients received NAC, of which 13 patients received cisplatin plus 5-fluorouracil (CF), and 2 patients received docetaxel plus cisplatin plus 5-fluorouracil (DCF). Eight patients received CRT, of which 6 patients received 38-40 Gy irradiation, and 2 patients received additional irradiation to the total of 60 Gy as their tumors were considered unresectable by the end of 40 Gy irradiation. These two patients underwent salvage surgery after the additional irradiation. Three patients achieved pathological pCR (pathological grade 3); of these, 2 patients received CRT, and 1 patient received NAC only.

Table 1

Patients’ characteristics

	All population (n = 23)	NAC (n = 15)	CRT (n = 8)
Age (yr)
Median (range)	72 (43-81)	72 (43-78)	72 (49-81)
Sex
Male	19	12	7
Female	4	3	1
Tumor location
Ut	2	2	0
Mt	15	8	7
Lt	4	4	0
Ae	2	1	1
Clinical T stage
cT1b	1	1	0
cT2	3	3	0
cT3	11	11	0
cT4a	1	0	1
cT4b	7	0	7
Chemotherapy regimen
CF	21	13	8
DCF	2	2
Total irradiation dose
38-40Gy	6		6
60Gy	2		2
Time of surgery after therapy (d)
Median (range)	37 (31-61)	36 (31-61)	40 (35-57)
Pathological T stage
pT0	3	1	2
pT1a	3	1	2
pT1b	6	6	0
pT2	3	1	2
pT3	8	6	2
Pathological response
Grade1	13	11	2
Grade2	7	3	4
Grade3	3	1	2

Ut: Upper thoracic esophagus; Mt: Middle thoracic esophagus; Lt: Lower thoracic esophagus; Ae: Abdominal esophagus; CF: Cisplatin plus 5-fluorouracil; DCF: Docetaxel plus cisplatin plus 5-fluorouracil; NAC: Neoadjuvant chemotherapy; CRT: Chemoradiotherapy.

The diagnosis of uT stage with ultrasound for specimens

We diagnosed uT stage by ultrasound for specimens just after surgery (Table 2). There was poor agreement between uT and pT stages. The overall accuracy uT stage rate was 61% (n = 14/23). The respective accuracy uT stage rate was 0% (n = 0/3) for pT0, 0% (n = 0/3) for pT1a, 67% (n = 4/6) for pT1b, 67% (n = 2/3) for pT2, and 100% (n = 8/8) for pT3. All pT0 and pT1a patients could not be diagnosed. Regarding comparison with NAC and CRT, the overall accuracy of uT stage rates were 73% (n = 11/15) and 38% (n = 3/8), respectively. The overall accuracy of overstaging uT stage rates was 13% (n = 2/15) and 62% (n = 5/8), respectively.

Table 2

Comparison Ultrasound for specimens uT stage to histological pT stage

Ultrasound T stages	pT0	pT1a	pT1b	pT2	pT3	Total
	Pathological T stages after NAC and CRT
uT0	0	1	1	0	0	2
uT1a	0	0	0	0	0	0
uT1b	0	0	4	0	0	4
uT2	1	1	1	2	0	5
uT3	2	1	0	1	8	12
Total	3	3	6	3	8	23
Accuracy (%)	0	0	67	67	100	61
Overstaging (%)	100	67	17	33	0	30
Understaging (%)		33	16	0	0	9
	Pathological T stages after NAC
uT0	0	1	1	0	0	2
uT1a	0	0	0	0	0	0
uT1b	0	0	4	0	0	4
uT2	1	0	1	1	0	3
uT3	0	0	0	0	6	6
Total	1	1	6	1	6	15
Accuracy (%)	0	0	67	100	100	73
Overstaging (%)	100	0	17	0	0	13
Understaging (%)		100	17	0	0	13
	Pathological T stages after CRT
uT0	0	0	0	0	0	0
uT1a	0	0	0	0	0	0
uT1b	0	0	0	0	0	0
uT2	0	1	0	1	0	2
uT3	2	1	0	1	2	6
Total	2	2	0	2	2	8
Accuracy (%)	0	0	0	50	100	38
Overstaging (%)	100	100	0	50	0	62
Understaging (%)		0	0	0	0	0

NAC: Neoadjuvant chemotherapy; CRT: Chemoradiotherapy.

Detect for residual tumor retrospectively

Among 20 patients, excluding 3 patients who achieved complete response, we compared ultrasound images with the cut surface of the fixed specimens of the same level of residual tumor site in the esophageal wall to examine whether the residual tumor itself could be detected (Table 3). The overall detection rate for residual tumors was 75% (n = 15/20), with no correlation between after NAC (79%, n = 11/14) and after CRT (67%, n = 4/6). The macroscopic types after neoadjuvant therapy were classified into two groups; 11 patients had ulcerative and protruding tumor types, while 9 patients had superficial and submucosal tumors. The superficial and submucosal types were poorly detected (P = 0.008). In addition, pathologic tumor size and the pathological response showed a significant correlation (P = 0.008, 0.127). Echoic characteristics of the residual tumor are shown in Table 4.

Table 3

Relationship between detection of residual tumor and clinicopathological factors

	Detection of residual tumor
	Possible	Impossible	P
All, n (%)	15 (75)	5 (25)
Preoperative treatment, n (%)
NAC	11 (79)	3 (21)
CRT	4 (67)	2 (33)	0.613
Macroscopic type after neoadjuvant therapy, n (%)
Ulcerative and protruding type	11 (100)	0 (0)
Superficial and SMT type	4 (44)	5 (56)	0.008
Pathologic tumor size (mm)
Median (range)	42 (5-65)	4 (2-34)	0.008
Pathological T stage, n (%)
pT1a/1b	5 (56)	4 (44)
pT2/3	10 (91)	1 (9)	0.127
Pathological response, n (%)
Grade1	12 (92)	1 (8)
Grade2	3 (43)	4 (57)	0.031

NAC: Neoadjuvant chemotherapy; CRT: Chemoradiotherapy.

Table 4

Echoic characteristics of the detected residual tumor

	All population (n = 15)	NAC (n = 11)	CRT (n = 4)	P
Border
Regular	10	10	0
Irregular	5	1	4	0.004
Echogenicity
Hypoechoic	5	5	0
Hypo and isoechoic (mixed)	10	6	4	0.231

NAC: Neoadjuvant chemotherapy; CRT: Chemoradiotherapy.

The tumor borders were relatively regular, and echogenicity was hypoechoic after NAC. In contrast, tumor borders were irregular, and echogenicity was hypo and iso (mixed) echoic type in all patients after CRT (Figure 1).

Figure 1

Ultrasound for specimens. A: In the after neoadjuvant chemotherapy cases, the residual tumor was SMT type with no exposure to the mucosal surface; B: Ultrasound showed the tumor as hypoechoic with regular borders (arrowhead); C: Pathology showed 18 mm × 18 mm, pT1b-SM3 (arrowhead). The pathological response was Grade1; D: After chemoradiotherapy, the residual tumor was ulcerative type; E: Ultrasound showed the tumor as mixed echoic with irregular borders; F: Pathology showed 45 mm × 20 mm, pT3 (arrowhead). The pathological response was Grade1.

Relationship between muscle layer measurements and pathological characteristics

We measured the muscle layer using ultrasound images (Figure 2). Ultrasound showed a clearly defined disruption of the muscle layer. We compared muscle layer factors with pathological characteristics (Figure 3). There was a significant correlation between pT stage (pT0/1, n = 12 vs pT2/3, n = 11) and length of muscle layer circumference (36.2 ± 5.9 mm vs 44.3 ± 8.9 mm, P = 0.025), length of muscle layer defect (22.5 ± 8.0 mm vs 7.1 ± 7.2 mm, P < 0.001), and the ratio of muscle layer defect (63.0 ± 22.8% vs 16.1 ± 16.0%, P < 0.001).

Figure 2

Measurements of muscle layer defect. A: In this case of cT4b to pT1a after chemoradiotherapy, most of the primary tumors were replaced by degenerative tissue (arrowhead), and the muscle layer was taking over; B: Ultrasound for specimens showed a clearly defined disruption of the muscle layer; C: Length of muscle layer circumference (X) was 45 mm. The length of the muscle layer defect (Y) was 12 mm. In this case, the ratio of muscle layer defect was 27%.

Figure 3

Relationship between muscle layer measurements and pathological characteristics. A: Length of muscle layer circumference correlated with pT (pT0/1 vs pT2/3); B: Length of muscle layer defect correlated with pT; C: Ratio of muscle layer defect correlated with pT.

There was no correlation between pathological response (Grade 1/2, n = 20 vs Grade 3, n = 3) and length of muscle layer circumference (40.0 ± 9.0 mm vs 42.6 ± 4.9 mm, P = 0.438), length of muscle layer defect (14.5 ± 11.5 mm vs 14.6 ± 4.5 mm, P = 1.00), and the ratio of muscle layer defect (39.2 ± 32.9% vs 33.8 ± 6.8%, P = 0.927).

Relationship between MDA and pathological T stage

In study 2, we measured MDA using EUS images (Figure 4). To confirm the reduction of muscle layer defect after adjuvant therapy compared to before, we excluded 3 patients (EUS before therapy did not show muscle layer invasion in 2 patients, and 1 patient did not undergo EUS before therapy). The clinical characteristics and pathological examination results are summarized in Table 5. There was no significant difference between pT0/1 and pT2/3 in terms of clinical characteristics. MDA factors were compared with pathological T stage (Figure 5). There was no correlation between preoperative treatment (NAC, n = 12 vs CRT, n = 8), pre-MDA (50.0 ± 35.3° vs 70.0 ± 27.9°, P = 0.137), post-MDA (30.5 ± 33.6° vs 43.2 ± 28.4°, P = 0.279), and MDA reduction rate (51.4 ± 34.9% vs 40.4 ± 25.7%, P = 0.589). There was a significant correlation between pT stage (pT0/1, n = 10 vs pT2/3, n = 10), pre-MDA (142.5 ± 110.6° vs 274.0 ± 91.7°, P = 0.039), post-MDA (45.9 ± 49.3° vs 210.0 ± 98.7°, P < 0.001), and MDA reduction rate (68.9 ± 24.4% vs 25.1 ± 20.3%, P = 0.001).

Figure 4

Measurements of muscle layer defect angle. A: Endoscopic ultrasound showed the normal muscle layer as hypoechoic inner muscle layer, hyperechoic intermuscular connective tissue layer, and hypoechoic outer muscle layer (arrowhead). In this case of cT3 before neoadjuvant chemotherapy (NAC), pre-muscle layer defect angle (MDA) was 125°; B: After NAC, post-MDA was 39°, and thus MDA reduction rate was 34.8%. This case achieved pCR.

Table 5

Patients’ characteristics in study 2

	pT0/1 (n = 10)	pT2/3 (n = 10)	P
Age (yr)
Median (range)	73 (52-79)	72 (43-81)	0.94
Sex
Male/Female	9/1	7/3	0.582
Tumor location
Ut, Mt, Lt/Ae	10/0	8/2	0.473
Clinical T stage
cT2, 3/cT4a, b	6/4	6/4	1
Preoperative treatment
NAC/CRT	6/4	6/4	1
Chemo regimen
CF/DCF	9/1	9/1	1
Total irradiation dose
38-40Gy/60Gy	2/2	4/0	0.429
Time of EUS after therapy (d)
Median (range)	37 (21-49)	29 (14-50)	0.172
Time of surgery after therapy (d)
Median (range)	41 (34-57)	37 (31-61)	0.471

Ut: Upper thoracic esophagus; Mt: Middle thoracic esophagus; Lt: Lower thoracic esophagus; Ae: Abdominal esophagus; CF: Cisplatin plus 5-fluorouracil; DCF: Docetaxel plus cisplatin plus 5-fluorouracil; NAC: Neoadjuvant chemotherapy; CRT: Chemoradiotherapy.

Figure 5

Relationship between muscle layer defect angle measurements and clinicopathological factors. A: Pre-muscle layer defect angle (MDA) not correlated with preoperative treatment [neoadjuvant chemotherapy (NAC) vs chemoradiotherapy (CRT)]; B: Post-MDA not correlated with preoperative treatment (NAC vs CRT); C: MDA reduction rate not correlated with preoperative treatment (NAC vs CRT); D: Pre-MDA correlated with pT (pT0/1 vs pT2/3); E: Post-MDA correlated with pT (pT0/1 vs pT2/3); F: MDA reduction rate correlated with pT (pT0/1 vs pT2/3).

We conducted ROC analysis to determine the optimal MDA reduction rate cut-off points that could yield the maximum difference between the two groups (Figure 6). From this ROC curve analysis, 57.0% was determined as the best cut-off rate to detect the patients in the pT0/1 group with the highest accuracy. Based on the optimal cut-off values of the MDA reduction rate, that could distinguish the pT0/1 group with a sensitivity of 0.80, specificity of 0.90, and accuracy of 0.93.

Figure 6

Receiver operating characteristics curve of the muscle layer defect angle reduction rate. The AUS was 0.93, and 57% was the optimal cut-off value to detect the patients in the pT0/1 group with the highest accuracy.

DISCUSSION

We conducted two studies; study 1 was performed to investigate the limitations and characteristics of residual tumor diagnosis using ultrasound and study 2 aimed to implement EUS to detect remanent tumors deep in the muscle layer. The first study revealed the limitations and potential of ultrasound for residual tumors. After cross-referencing ultrasound images with the correct pathological diagnosis, some residual tumors were found to be undetectable on ultrasound. In contrast, the ratio of the esophageal muscle layer defect, which was not focused upon so far, was considered helpful in diagnosing the depth of the residual tumor. In the second study, muscle layer defect was measured using EUS. The results showed that the rate of muscle layer defect reduction in neoadjuvant therapy correlated with the pathological depth of the tumor. Our findings can help improve EUS diagnosis and provide more treatment options for ESCC patients after neoadjuvant therapy.

We considered comparing pathological and ultrasound images. However, using only EUS was considered unreliable for the following reasons. First, it was difficult to compare the measured level of tumor site in the esophagus with the level of the fixed specimens. Second, EUS was good for evaluating targeted areas but not for scanning large areas. In contrast, ultrasound for surgical specimens allowed us to compare pathological and ultrasound images with the same level of ultrasound images and scans of the entire lesion. This could help clarify whether the modality of echo itself contributes to the residual diagnosis after neoadjuvant therapy.

According to several meta-analyses examining the accuracy of detecting residual tumors for esophageal cancer after CRT, the consensus was that EUS had high sensitivity but low specificity[10,13]. Even after NAC, the concordance rate between EUS and pathological T-stage was reportedly as low as 29%, and the depth was overstaged in more than half of the cases (51%)[14]. It is well known that tumor invasion might be overestimated due to inflammation within and surrounding the tumor[15]. Our study showed 61% accuracy and 30% overstaging of uT, which was better than previous studies. Even though the ultrasound on surgical specimens was performed in a stable environment, these results are not sufficiently accurate. A previous study analyzing the accuracy of EUS in patients with esophageal cancer after NAC or CRT showed that accuracy of uT was significantly worse after CRT (16%) than after NAC (43%)[16]. In line with this previous study, our results showed that the accuracy of uT worsened after CRT (38%) than after NAC (73%). Our study showed that CRT downstaged tumors more effectively than NAC. As a result, there were more tumors with pT0 and pT1a, which were difficult to detect using ultrasound. All pT0 and pT1a patients could not be diagnosed because the scar tissue associated with tumor disappearance was misidentified as a residual tumor, causing overstaging. Diagnosing T3 was easy because the esophageal muscle layer was destroyed or replaced by fibrosis. However, distinguishing between a residual tumor and a fibrosis tissue seemed impossible.

We also examined the retrospective detection rate for residual tumor and the echoic characteristics of the residual tumor by comparing ultrasound images with the cut surface of the fixed specimens of the same level of the esophageal wall. Our results showed no difference in the detection rate after CRT and after NAC; however, the after CRT specimens appeared to have an irregular border and mixed echogenicity. According to a study that classified the echogenicity of gastrointestinal tumors, most esophageal cancers expressed echo levels between the muscularis propria and the deep mucosa[17]. However, our study showed that the residual tumors lost heterogeneity and higher echogenicity after CRT compared to deep mucosa. This result indicated that the preoperative treatment increased the brightness of echogenicity. In a previous pathological study, chemotherapy was found to generally decrease tumor cellularity and cause fragmentation of cell nuclei. Additionally, in squamous cell carcinoma, chemotherapy is known to increase keratinization with the formation of keratin pearls, acellular keratin with islands of nonviable tumor cells, histiocytic giant cells, and lymphocytes surrounding tumor cells in squamous cell carcinoma[18]. Our pathological findings after neoadjuvant therapy, particularly after CRT, showed that the density of collagen fibers increased as the cancer cells disappeared. Consequently, the ratio of cancer cells to stromal components also changed, which might have led to a difference in echo level, such as mixed echogenicity. The increase in the echogenicity of tumors is reportedly related to the positive response to NAC in breast tumors[19]. Although such phenomena correlating echogenicity and treatment effect are not reported for esophageal cancers, and our study could not prove the relationship, some changes in echogenicity of ESCC could be attributed to treatment.

When predicting patient prognosis after CRT or NAC, it is reasonable to measure the reduction in tumor volume using EUS. However, the conventional measurement method involving direct identification and measurement of the tumor is not accurate. Several studies have assessed the predictive value of tumor thickness and area using EUS to determine patient prognosis and tumor regression in patients with esophageal cancer undergoing NAC or CRT[20-23]. Although these studies focused on lesions identified on EUS, our results showed that EUS could not detect the residual tumor. Tumors were either scattered on the esophageal wall, had unclear borders, or were scar tissue that appeared like a tumor.

For this reason, we considered it inappropriate to include EUS-confirmed echo lesions as residual tumors. In our clinical experience, we have observed that the esophageal muscle layer can be clearly visualized using EUS in patients with a good response to neoadjuvant therapy. Therefore, we focused on the esophageal muscle layer as indirect findings instead of the tumor. In the first study, ultrasound findings for specimens in the group with pT0 and pT1 showed that the muscle layer circumference was longer, the length of muscle layer defect was shorter, and the rate of muscle layer defect was lower than in the group with pT2 and pT3. Tissue heterogeneity was noted if residual cancer cells remained in the muscle layer or deeper; in such cases, we could not explore the muscle layer using ultrasound findings. In addition, it was improbable that the muscle layer destroyed by tumor invasion could be regenerated, at least during the observation period. We considered that the reduction in the muscle layer defect in the specimens with stages pT0 and pT1 was because of scar contraction caused by the disappearance of the tumor due to neoadjuvant therapy. In the second study, findings of EUS performed before and after neoadjuvant therapy in the group with pT0 and pT1 showed that pre-MDA was smaller, post-MDA was smaller, and MDA reduction rate was larger in the groups with pT2 and pT3 staging. The improvement of the muscle layer defect was considered useful in EUS depth diagnosis.

If EUS helps diagnose pCR or superficial residual tumors and deep remanent tumors in patients after neoadjuvant therapy by focusing on the muscle layer, the clinical treatment options can be expanded significantly. In recent years, endoscopic salvage resection has been preferred over esophagectomy for patients with superficial localized residual tumors after CRT[24,25]. In addition, it was reported that overall, 29% of patients with esophageal cancer achieved pCR after neoadjuvant CRT[26], and 62% of patients with ESCC achieved pCR according to the JCOG9906 study in Japan[3]. A study reported that 2%-7% of patients with ESCC achieved pCR after NAC; however, they included only a small number of cases[4,5]. Because of such response rates, recent studies have focused on assessing the efficacy of active surveillance to help avoid highly invasive esophagectomy[27]. In addition to the usual endoscopic diagnosis, which mainly involves biopsy, subsequent MDA reduction rate may allow the selection of endoscopic salvage resection instead of esophagectomy.

Our study had some limitations. First, it was a single-center study with a small sample size. The usefulness of EUS must be evaluated in the future by conducting larger prospective studies. Second, it was difficult to seamlessly match the sites measured before and after preoperative treatment with EUS. We attempted to match the measurement sites by recording the scope length from the mouth and comparing it to the surrounding vessels and structures. Third, the value of post-MDA could be different depending on the time since preoperative treatment. We assessed MDA 4 to 6 wk after the last preoperative treatment. However, to determine the effectiveness of neoadjuvant therapy and for active surveillance, it is necessary to examine the differences in MDA according to the time since treatment.

CONCLUSION

This study showed that ultrasound could not detect some residual tumors after neoadjuvant therapy. Meanwhile, focusing on the esophageal muscle layer as indirect findings rather than the residual tumor as direct findings could help diagnose the depth of the tumor. Applying these results in clinical practice may help clinicians provide more treatment options for patients with ESCC after neoadjuvant therapy.

ARTICLE HIGHLIGHTS

Research background

The diagnosis of endoscopic ultrasound (EUS) for esophageal cancer after neoadjuvant therapy is controversial. In addition, it is unclear whether the echogenic lesions detected using EUS are indeed residual tumors and how they appear on ultrasound.

Research motivation

There are few studies that contrast echographic and pathologic images of esophageal cancer after neoadjuvant therapy. In our clinical experience, we have observed that the esophageal muscle layer can be clearly visualized using EUS in patients with a good response to neoadjuvant therapy.

Research objectives

To investigate the ultrasound imaging features of residual tumors and identify the limitations and potential of EUS.

Research methods

Twenty-three patients receiving esophagectomy after neoadjuvant therapy [15 patients after neoadjuvant chemotherapy (NAC) and 8 patients after chemoradiotherapy (CRT)] were studied. We diagnosed the T stage and compared ultrasound images with pathological findings using ultrasound for surgical specimens. Furthermore, the rate of reduction for the muscle layer defect was evaluated using EUS images obtained before and after neoadjuvant therapy.

Research results

The accuracy of T stage rate was 61%, which worsened after CRT (38%) than after NAC (73%). Moreover, pT0 could not be diagnosed in all cases. The detection rate of residual tumor for specimens using ultrasound retrospectively was 75%. Tumor borders were irregular and echogenicity was mixed type after CRT. There was a correlation between the pT stage and the rate of muscle layer defect reduction measured by EUS.

Research conclusions

Some tumors are undetectable on ultrasound when compared to pathological images. However, focusing on the esophageal muscle layer may improve the accuracy of T stage diagnosis of residual tumors.

Research perspectives

If EUS helps diagnose T stage of residual tumors in patients after neoadjuvant therapy by focusing on the muscle layer, the clinical treatment options can be expanded significantly.

ACKNOWLEDGEMENTS

We are deeply grateful to Ishimura R, Department of Photo Center, Chiba University Hospital, Japan, who provided great illustrations.