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1. Chemosensitivity of Patient-Derived Cancer Stem Cells Identifies Colorectal Cancer Patients with Potential Benefit from FGFR Inhibitor Therapy

Author

00609076, 50884326, 90980178, 90322651, Yamamoto, Takehito, Miyoshi, Hiroyuki, Kakizaki, Fumihiko, Maekawa, Hisatsugu, Yamaura, Tadayoshi, Morimoto, Tomonori, Katayama, Toshiro, Kawada, Kenji, Sakai, Yoshiharu, Taketo, M. Mark, 00609076, 50884326, 90980178, 90322651, Yamamoto, Takehito, Miyoshi, Hiroyuki, Kakizaki, Fumihiko, Maekawa, Hisatsugu, Yamaura, Tadayoshi, Morimoto, Tomonori, Katayama, Toshiro, Kawada, Kenji, Sakai, Yoshiharu, and Taketo, M. Mark

Abstract

Some colorectal cancer patients harboring FGFR (fibroblast growth factor receptor) genetic alterations, such as copy number gain, mutation, and/or mRNA overexpression, were selected for enrollment in several recent clinical trials of FGFR inhibitor, because these genetic alterations were preclinically reported to be associated with FGFR inhibitor sensitivity as well as poor prognosis, invasiveness, and/or metastatic potential. However, few enrolled patients were responsive to FGFR inhibitors. Thus, practical strategies are eagerly awaited that can stratify patients for the subset that potentially responds to FGFR inhibitor chemotherapy. In the present study, we evaluated the sensitivity to FGFR inhibitor erdafitinib on 25 patient-derived tumor-initiating cell (TIC) spheroid lines carrying wild-type RAS and RAF genes, both in vitro and in vivo. Then, we assessed possible correlations between the sensitivity and the genetic/genomic data of the spheroid lines tested. Upon their exposure to erdafitinib, seven lines (7/25, 28%) responded significantly. Normal colonic epithelial stem cells were unaffected by the inhibitors. Moreover, the combination of erdafitinib with EGFR inhibitor erlotinib showed stronger growth inhibition than either drug alone, as efficacy was observed in 21 lines (84%) including 14 (56%) that were insensitive to erdafitinib alone. The in vitro erdafitinib response was accurately reflected on mouse xenografts of TIC spheroid lines. However, we found little correlation between their genetic/genomic alterations of TIC spheroids and the sensitivity to the FGFR inhibitor. Accordingly, we propose that direct testing of the patient-derived spheroids in vitro is one of the most reliable personalized methods in FGFR-inhibitor therapy of colorectal cancer patients.

Published
2020

2. Disruption of CCR1-mediated myeloid cell accumulation suppresses colorectal cancer progression in mice

Author

90322651, 50315933, 80814029, Kiyasu, Yoshiyuki, Kawada, Kenji, Hirai, Hideyo, Ogawa, Ryotaro, Hanada, Keita, Masui, Hideyuki, Nishikawa, Gen, Yamamoto, Takamasa, Mizuno, Rei, Itatani, Yoshiro, Kai, Masayuki, Taketo, Mark Makoto, Sakai, Yoshiharu, 90322651, 50315933, 80814029, Kiyasu, Yoshiyuki, Kawada, Kenji, Hirai, Hideyo, Ogawa, Ryotaro, Hanada, Keita, Masui, Hideyuki, Nishikawa, Gen, Yamamoto, Takamasa, Mizuno, Rei, Itatani, Yoshiro, Kai, Masayuki, Taketo, Mark Makoto, and Sakai, Yoshiharu

Abstract

Tumor-stromal interaction is implicated in tumor progression. Although CCR1 expression in myeloid cells could be associated with pro-tumor activity, it remains elusive whether disruption of CCR1-mediated myeloid cell accumulation can suppress tumor progression. Here, we investigated the role of CCR1 depletion in myeloid cells in two syngeneic colorectal cancer mouse models: MC38, a transplanted tumor model and CMT93, a liver metastasis model. Both cells induced tumor accumulation of CCR1+ myeloid cells that express MMP2, MMP9, iNOS, and VEGF. Lack of the Ccr1 gene in host mice dramatically reduced MC38 tumor growth as well as CMT93 liver metastasis. To delineate the contribution of CCR1+ myeloid cells, we performed bone marrow (BM) transfer experiments in which sub-lethally irradiated wild-type mice were reconstituted with BM from either wild-type or Ccr1-/- mice. Mice reconstituted with Ccr1-/- BM exhibited marked suppression of MC38 tumor growth and CMT93 liver metastasis, compared with control mice. Consistent with these results, administration of a neutralizing anti-CCR1 monoclonal antibody, KM5908, significantly suppressed MC38 tumor growth and CMT93 liver metastases. Our findings highlight the importance of the application of CCR1 blockade as a therapeutic strategy.

Published
2020

3. Frequent mutations that converge on the NFKBIZ pathway in ulcerative colitis

Author

90839721, 90322651, 20515514, 00789638, 40511829, 80646373, 40883707, 20772403, 70335454, 40402127, 10252462, 10379092, 90335266, Kakiuchi, Nobuyuki, Yoshida, Kenichi, Uchino, Motoi, Kihara, Takako, Akaki, Kotaro, Inoue, Yoshikage, Kawada, Kenji, Nagayama, Satoshi, Yokoyama, Akira, Yamamoto, Shuji, Matsuura, Minoru, Horimatsu, Takahiro, Hirano, Tomonori, Goto, Norihiro, Takeuchi, Yasuhide, Ochi, Yotaro, Shiozawa, Yusuke, Kogure, Yasunori, Watatani, Yosaku, Fujii, Yoichi, Kim, Soo Ki, Kon, Ayana, Kataoka, Keisuke, Yoshizato, Tetsuichi, Nakagawa, Masahiro M., Yoda, Akinori, Nanya, Yasuhito, Makishima, Hideki, Shiraishi, Yuichi, Chiba, Kenichi, Tanaka, Hiroko, Sanada, Masashi, Sugihara, Eiji, Sato, Taka-aki, Maruyama, Takashi, Miyoshi, Hiroyuki, Taketo, Makoto Mark, Oishi, Jun, Inagaki, Ryosaku, Ueda, Yutaka, Okamoto, Shinya, Okajima, Hideaki, Sakai, Yoshiharu, Sakurai, Takaki, Haga, Hironori, Hirota, Seiichi, Ikeuchi, Hiroki, Nakase, Hiroshi, Marusawa, Hiroyuki, Chiba, Tsutomu, Takeuchi, Osamu, Miyano, Satoru, Seno, Hiroshi, Ogawa, Seishi, 90839721, 90322651, 20515514, 00789638, 40511829, 80646373, 40883707, 20772403, 70335454, 40402127, 10252462, 10379092, 90335266, Kakiuchi, Nobuyuki, Yoshida, Kenichi, Uchino, Motoi, Kihara, Takako, Akaki, Kotaro, Inoue, Yoshikage, Kawada, Kenji, Nagayama, Satoshi, Yokoyama, Akira, Yamamoto, Shuji, Matsuura, Minoru, Horimatsu, Takahiro, Hirano, Tomonori, Goto, Norihiro, Takeuchi, Yasuhide, Ochi, Yotaro, Shiozawa, Yusuke, Kogure, Yasunori, Watatani, Yosaku, Fujii, Yoichi, Kim, Soo Ki, Kon, Ayana, Kataoka, Keisuke, Yoshizato, Tetsuichi, Nakagawa, Masahiro M., Yoda, Akinori, Nanya, Yasuhito, Makishima, Hideki, Shiraishi, Yuichi, Chiba, Kenichi, Tanaka, Hiroko, Sanada, Masashi, Sugihara, Eiji, Sato, Taka-aki, Maruyama, Takashi, Miyoshi, Hiroyuki, Taketo, Makoto Mark, Oishi, Jun, Inagaki, Ryosaku, Ueda, Yutaka, Okamoto, Shinya, Okajima, Hideaki, Sakai, Yoshiharu, Sakurai, Takaki, Haga, Hironori, Hirota, Seiichi, Ikeuchi, Hiroki, Nakase, Hiroshi, Marusawa, Hiroyuki, Chiba, Tsutomu, Takeuchi, Osamu, Miyano, Satoru, Seno, Hiroshi, and Ogawa, Seishi

Abstract

Chronic inflammation is accompanied by recurring cycles of tissue destruction and repair and is associated with an increased risk of cancer1, 2, 3. However, how such cycles affect the clonal composition of tissues, particularly in terms of cancer development, remains unknown. Here we show that in patients with ulcerative colitis, the inflamed intestine undergoes widespread remodelling by pervasive clones, many of which are positively selected by acquiring mutations that commonly involve the NFKBIZ, TRAF3IP2, ZC3H12A, PIGR and HNRNPF genes and are implicated in the downregulation of IL-17 and other pro-inflammatory signals. Mutational profiles vary substantially between colitis-associated cancer and non-dysplastic tissues in ulcerative colitis, which indicates that there are distinct mechanisms of positive selection in both tissues. In particular, mutations in NFKBIZ are highly prevalent in the epithelium of patients with ulcerative colitis but rarely found in both sporadic and colitis-associated cancer, indicating that NFKBIZ-mutant cells are selected against during colorectal carcinogenesis. In further support of this negative selection, we found that tumour formation was significantly attenuated in Nfkbiz-mutant mice and cell competition was compromised by disruption of NFKBIZ in human colorectal cancer cells. Our results highlight common and discrete mechanisms of clonal selection in inflammatory tissues, which reveal unexpected cancer vulnerabilities that could potentially be exploited for therapeutics in colorectal cancer.

Published
2020

4. Precise Three-Dimensional Morphology of the Male Anterior Anorectum Reconstructed From Large Serial Histologic Sections: A Cadaveric Study

Author

40848206, 40447983, 90322651, Okada, Tomoaki, Hasegawa, Suguru, Nakamura, Tatsuro, Hida, Koya, Kawada, Kenji, Takai, Akihiro, Shimokawa, Tetsuya, Matsuda, Seiji, Shinohara, Hisashi, Sakai, Yoshiharu, 40848206, 40447983, 90322651, Okada, Tomoaki, Hasegawa, Suguru, Nakamura, Tatsuro, Hida, Koya, Kawada, Kenji, Takai, Akihiro, Shimokawa, Tetsuya, Matsuda, Seiji, Shinohara, Hisashi, and Sakai, Yoshiharu

Published
2019

5. Robot-assisted low anterior resection after aluminum potassium sulfate and tannic acid sclerosing therapy for internal hemorrhoids

Author

80814029, 40848206, 90322651, 40447983, 70571454, Itatani, Yoshiro, Okada, Tomoaki, Kawada, Kenji, Hida, Koya, Oshima, Nobu, Inamoto, Susumu, Mizuno, Rei, Okuchi, Yoshihisa, Sakai, Yoshiharu, 80814029, 40848206, 90322651, 40447983, 70571454, Itatani, Yoshiro, Okada, Tomoaki, Kawada, Kenji, Hida, Koya, Oshima, Nobu, Inamoto, Susumu, Mizuno, Rei, Okuchi, Yoshihisa, and Sakai, Yoshiharu

Abstract

Background: Internal hemorrhoids are the most common anal diseases. Aluminum potassium sulfate and tannic acid (ALTA) injection is a new sclerosing therapy for the treatment of internal hemorrhoids. Although ALTA injection has been widely used, there are no previous reports of rectal cancer patients who underwent robot-assisted low anterior resection (Rob-LAR) after ALTA injection to treat internal hemorrhoids. Case presentation: A 70-year-old man with rectal cancer was presented to our hospital. He had an ALTA injection 2 months before presentation at a clinic due to hematochezia with internal hemorrhoids. The rectal tumor was located 7 cm above the anal verge, and Rob-LAR with the da Vinci Xi system was performed. The patient had sclerosis on the stump of the anal side, which made it difficult to transect the rectum with linear staplers. This required multiple repeats of compression through the SmartClamp feedback. After anastomosis with the double-stapling technique, we constructed a diverting ileostomy. Conclusion: Although ALTA injection is a promising strategy for internal hemorrhoids, rectal cancer should be excluded before the sclerosing therapy.

Published
2019

6. Laparoscopic distal gastrectomy for gastric cancer patient with intestinal malrotation: report of a case

Author

50322649, 30829487, 80814029, 50534351, 60597300, 40447983, 90322651, Inamoto, Susumu, Obama, Kazutaka, Asai, Satsuki, Mizuno, Rei, Itatani, Yoshiro, Hashimoto, Kyoichi, Hisamori, Shigeo, Tsunoda, Shigeru, Hida, Koya, Kawada, Kenji, Sakai, Yoshiharu, 50322649, 30829487, 80814029, 50534351, 60597300, 40447983, 90322651, Inamoto, Susumu, Obama, Kazutaka, Asai, Satsuki, Mizuno, Rei, Itatani, Yoshiro, Hashimoto, Kyoichi, Hisamori, Shigeo, Tsunoda, Shigeru, Hida, Koya, Kawada, Kenji, and Sakai, Yoshiharu

Abstract

Background: Intestinal malrotation, which arises from incomplete rotation of the embryonic midgut, is one of the congenital anomalies usually diagnosed in infancy. On the other hand, intestinal malrotation detected in asymptomatic adults is very rare. It is frequently diagnosed incidentally during abdominal surgery. We report a case of asymptomatic intestinal malrotation diagnosed during laparoscopic distal gastrectomy for gastric cancer. Case presentation: A 59-year-old female was diagnosed with early-stage gastric cancer during health screening and admitted to our hospital for radical surgical treatment. Physical examinations and blood tests revealed nothing of note. The type 0-IIc gastric cancer was located in the posterior wall of the mid-body of the stomach. The histological type was poorly differentiated adenocarcinoma. Esophagogastroduodenoscopy and computed tomography (CT) suggested that the depth of tumor invasion was the submucosal layer without regional lymph node swelling. The clinical stage according to the TNM 7th edition was cT1b N0 M0, cStage I. Laparoscopic distal gastrectomy with D1+ lymph node dissection and Billroth-I method reconstruction was planned. During the infrapyloric lymph node dissection, a part of the pancreatic head showed unusual adherence to the first part of the duodenal wall. For safe and accurate lymphadenectomy while avoiding pancreatic injury, we deliberately focused on tracing the dissectible layer between the pancreatic parenchyma and fatty tissues including lymph nodes. Also, we changed the reconstruction procedure from Billroth-I to Roux-en-Y. After distal gastrostomy, we could not find the ligament of Treitz or jejunum on the left side below the transverse colon. Based on a review of the CT image, this patient was diagnosed with intestinal malrotation. Although the detection of malrotation during the operation was incidental, we could complete radical surgery and Roux-en-Y reconstruction safely. The type of malrotation was

Published
2019

7. Bone marrow-derived mesenchymal stem cells promote colorectal cancer progression via CCR5

Author

90322651, 30829487, 80814029, Nishikawa, Gen, Kawada, Kenji, Nakagawa, Jun, Toda, Kosuke, Ogawa, Ryotaro, Inamoto, Susumu, Mizuno, Rei, Itatani, Yoshiro, Sakai, Yoshiharu, 90322651, 30829487, 80814029, Nishikawa, Gen, Kawada, Kenji, Nakagawa, Jun, Toda, Kosuke, Ogawa, Ryotaro, Inamoto, Susumu, Mizuno, Rei, Itatani, Yoshiro, and Sakai, Yoshiharu

Abstract

Mesenchymal stem cells (MSCs) are recruited from BM to the stroma of developing tumors, where they serve as critical components of the tumor microenvironment by secreting growth factors, cytokines, and chemokines. The role of MSCs in colorectal cancer (CRC) progression was controversial. In this study, we found that C-C chemokine receptor type 5 (CCR5) ligands (i.e., C-C motif chemokine ligand 3 (CCL3), CCL4, and CCL5) were highly produced from MSCs using a chemokine array screening with conditioned media from the cultured human MSCs. A relatively strong CCR5 expression could be detected within the cytoplasm of several CRC cell lines. Regarding the effect of MSC, we found that the xenografts in which CCR5-overexpressing HCT116 cells were inoculated into immunocompromised mice were highly promoted in vivo by a mixture with MSCs. Notably, the CCR5 inhibitor, maraviroc, significantly abolished the MSC-induced tumor growth in vivo. In human clinical specimens (n = 89), 20 cases (29%) were high for CCR5, whereas 69 cases (71%) were low. Statistical analyses indicated that CCR5 expression in primary CRC was associated with CRC patients’ prognosis. Especially, stage III/IV patients with CCR5-high CRCs exhibited a significantly poorer prognosis than those with CCR5-low CRCs. Furthermore, we investigated the effects of preoperative serum CCR5 ligands on patients’ prognosis (n = 114), and found that CRC patients with high serum levels of CCL3 and CCL4 exhibited a poorer prognosis compared to those with low levels of CCL3 and CCL4, while there was no association between CCL5 and prognosis. These results suggest that the inhibition of MSC–CRC interaction by a CCR5 inhibitor could provide the possibility of a novel therapeutic strategy for CRC, and that serum levels of CCL3 and CCL4 could be predictive biomarkers for the prognosis of CRC patients.

Published
2019

8. The Role of Tumor-Associated Neutrophils in Colorectal Cancer

Author

30829487, 90322651, 80814029, Mizuno, Rei, Kawada, Kenji, Itatani, Yoshiro, Ogawa, Ryotaro, Kiyasu, Yoshiyuki, Sakai, Yoshiharu, 30829487, 90322651, 80814029, Mizuno, Rei, Kawada, Kenji, Itatani, Yoshiro, Ogawa, Ryotaro, Kiyasu, Yoshiyuki, and Sakai, Yoshiharu

Published
2019

9. Accurate diagnosis of mismatch repair deficiency in colorectal cancer using high-quality DNA samples from cultured stem cells

Author

50884326, 90980178, 00609076, 90322651, 50212220, Yamaura, Tadayoshi, Miyoshi, Hiroyuki, Maekawa, Hisatsugu, Morimoto, Tomonori, Yamamoto, Takehito, Kakizaki, Fumihiko, Higasa, Koichiro, Kawada, Kenji, Matsuda, Fumihiko, Sakai, Yoshiharu, Taketo, M. Mark, 50884326, 90980178, 00609076, 90322651, 50212220, Yamaura, Tadayoshi, Miyoshi, Hiroyuki, Maekawa, Hisatsugu, Morimoto, Tomonori, Yamamoto, Takehito, Kakizaki, Fumihiko, Higasa, Koichiro, Kawada, Kenji, Matsuda, Fumihiko, Sakai, Yoshiharu, and Taketo, M. Mark

Abstract

Mismatch repair (MMR)-deficient or microsatellite instability (MSI) colorectal cancer includes two subtypes; Lynch syndrome and sporadic MSI cancer, both of which generate multiple neoantigens due to unrepaired mutations. Although such patients respond very well to immune checkpoint therapy, their diagnosis can be confused by low quality DNA samples owing to formalin fixation and/or low cancer cell content. Here we prepared high-quality DNA samples from in vitro-cultured cancer spheroids that consisted of the pure cell population. We evaluated their diagnostic power by on-chip electrophoresis, mutational burden assessment, and direct sequencing. Because formalin-fixed paraffin-embedded (FFPE) tissues are widely used as the DNA source, we compared such samples with spheroid DNA. Additionally, we performed immunohistochemistry (IHC) for MMR proteins on spheroids as well as primary tumor sections. Of 111 cases of colorectal cancer patients, we found seven MSI-high cases in which all diagnostic results agreed on spheroid-based assays, whereas the results with the FFPE DNA were less reliable though analyzable. Importantly, there was an MSS case that appeared as MSI by IHC on primary tumor sections. Based on these results, we propose to employ cultured cancer spheroids as the source of both DNA and IHC specimens for more reliable clinical diagnosis.

Published
2018

10. An improved method for culturing patient-derived colorectal cancer spheroids

Author

50884326, 00609076, 90322651, Miyoshi, Hiroyuki, Maekawa, Hisatsugu, Kakizaki, Fumihiko, Yamaura, Tadayoshi, Kawada, Kenji, Sakai, Yoshiharu, Taketo, M. Mark, 50884326, 00609076, 90322651, Miyoshi, Hiroyuki, Maekawa, Hisatsugu, Kakizaki, Fumihiko, Yamaura, Tadayoshi, Kawada, Kenji, Sakai, Yoshiharu, and Taketo, M. Mark

Abstract

Recent advances allowed culturing and examination of patient-derived colorectal cancer (PD-CRC) cells as organoids or spheroids. To be applied to practical personalized medicine, however, current methods still need to be strengthened for higher efficiency. Here we report an improved method to propagate PD-CRC tumor initiating cells (TICs) in spheroid culture. We established > 100 cancer spheroid lines derived from independent colorectal cancer patients employing a serum-containing medium with additional inhibitors, Y27632 and SB431542. Because colorectal cancer spheroids showed wide-range growth rates depending on the patient tumors, we searched for supplementary factors that accelerated proliferation of slow-growing CRC-TIC spheroids. To this end, we introduced a convenient growth-monitoring method using a luciferase reporter. We found that epidermal growth factor (EGF) and/or basic fibroblast growth factor (bFGF) were critical for steady propagation of a subset of CRC-TIC spheroids carrying the wild-type RAS and RAF genes. We also identified 5′-(N-ethyl-carboxamido)-adenosine (NECA), an adenosine receptor agonist, as an essential supplement for another subset of spheroids. Based on these results, we propose to optimize culture conditions for CRC-TIC spheroids by adjusting to the respective tumor samples. Our method provides a versatile tool that can be applied to personalized chemotherapy evaluation in prospective clinical studies.

Published
2018

11. Resistance to Anti-Angiogenic Therapy in Cancer—Alterations to Anti-VEGF Pathway

Author

80814029, 90322651, Itatani, Yoshiro, Kawada, Kenji, Yamamoto, Takamasa, Sakai, Yoshiharu, 80814029, 90322651, Itatani, Yoshiro, Kawada, Kenji, Yamamoto, Takamasa, and Sakai, Yoshiharu

Abstract

Anti-angiogenic therapy is one of the promising strategies for many types of solid cancers. Bevacizumab (Avastin), a recombinant humanized monoclonal antibody of vascular endothelial growth factor (VEGF) A, was approved for the first time as an anti-angiogenic drug for the treatment of metastatic colorectal cancer (CRC) by the Food and Drug Administration (FDA) in 2004. In addition, the other VEGF pathway inhibitors including small molecule tyrosine kinase inhibitors (sunitinib, sorafenib, and pazopanib), a soluble VEGF decoy receptor (aflibercept), and a humanized monoclonal antibody of VEGF receptor 2 (VEGFR2) (ramucirumab) have been approved for cancer therapy. Although many types of VEGF pathway inhibitors can improve survival in most cancer patients, some patients have little or no beneficial effect from them. The primary or acquired resistance towards many oncological drugs, including anti-VEGF inhibitors, is a common problem in cancer treatment. This review summarizes the proposed alternative mechanisms of angiogenesis other than the VEGF pathway. These mechanisms are involved in the development of resistance to anti-VEGF therapies in cancer patients.

Published
2018

12. Enhanced anastomotic healing by Daikenchuto (TJ-100) in rats

Author

90322651, Wada, Toshiaki, Kawada, Kenji, Hirai, Kenjiro, Toda, Kosuke, Iwamoto, Masayoshi, Hasegawa, Suguru, Sakai, Yoshiharu, 90322651, Wada, Toshiaki, Kawada, Kenji, Hirai, Kenjiro, Toda, Kosuke, Iwamoto, Masayoshi, Hasegawa, Suguru, and Sakai, Yoshiharu

Published
2018

13. Delayed anastomotic leakage following laparoscopic intersphincteric resection for lower rectal cancer: report of four cases and literature review

Author

90322651, 40447983, Iwamoto, Masayoshi, Kawada, Kenji, Hida, Koya, Hasegawa, Suguru, Sakai, Yoshiharu, 90322651, 40447983, Iwamoto, Masayoshi, Kawada, Kenji, Hida, Koya, Hasegawa, Suguru, and Sakai, Yoshiharu

Abstract

Background: Anastomotic leakage (AL) is one of the most dreadful postoperative complications because it can result in increased morbidity and mortality as well as poorer long-term prognosis. Although most studies of AL limited their investigation time to a period of 30 days postoperatively, only a few studies have shown that AL can occur after that period. Here, we report four patients of rectal cancer with delayed AL following laparoscopic intersphincteric resection (ISR) and conduct a literature review on delayed AL. Case presentation: Case 1 was a 67-year-old male who underwent laparoscopic partial ISR in July 2009. Although the patient was asymptomatic, an anastomotic-urethral fistula was observed 57 months after ISR. Case 2 was a 44-year-old female who underwent laparoscopic partial ISR in July 2008. She presented with discharge of gas and feces from her vagina, and an anastomotic-vaginal fistula was observed 14 months after ISR. Case 3 was a 74-year-old man who underwent laparoscopic partial ISR in August 2007. He presented with pneumaturia and fecaluria, and an anastomotic-urethral fistula was observed 4 months after ISR. Case 4 was a 68-year-old woman who underwent laparoscopic subtotal ISR for rectal cancer in February 2013 and partial hepatic resection for liver metastases in March 2013. She presented with anal pain and purulent perineal discharge, and an anastomotic-perineal fistula was observed 9 months after ISR. All four cases presented with fistula formation and required reoperation (establishment of a diverting ileostomy). Conclusions: Since delayed AL is not a rare postoperative complication, surgeons need to provide long-term follow-up and remain alert to the possible development of delayed AL.

Published
2017

14. In vivo and ex vivo cetuximab sensitivity assay using three-dimensional primary culture system to stratify KRAS mutant colorectal cancer

Author

90322651, 10342990, Tashiro, Takahiro, Okuyama, Hiroaki, Endo, Hiroko, Kawada, Kenji, Ashida, Yasuko, Ohue, Masayuki, Sakai, Yoshiharu, Inoue, Masahiro, 90322651, 10342990, Tashiro, Takahiro, Okuyama, Hiroaki, Endo, Hiroko, Kawada, Kenji, Ashida, Yasuko, Ohue, Masayuki, Sakai, Yoshiharu, and Inoue, Masahiro

Abstract

In clinic, cetuximab, an anti-EGFR antibody, improves treatment outcomes in colorectal cancer (CRC). KRAS-mutant CRC is generally resistant to cetuximab, although difference of the sensitivity among KRAS-mutants has not been studied in detail. We previously developed the cancer tissue-originated spheroid (CTOS) method, a primary culture method for cancer cells. We applied CTOS method to investigate whether ex vivo cetuximab sensitivity assays reflect the difference in sensitivity in the xenografts. Firstly, in vivo cetuximab treatment was performed with xenografts derived from 10 CTOS lines (3 KRAS-wildtype and 7 KRAS mutants). All two CTOS lines which exhibited tumor regression were KRAS-wildtype, meanwhile all KRAS-mutant CTOS lines grew more than the initial size: were resistant to cetuximab according to the clinical evaluation criteria, although the sensitivity was quite diverse. We divided KRAS-mutants into two groups; partially responsive group in which cetuximab had a substantial growth inhibitory effect, and resistant group which exhibited no effect. The ex vivo signaling assay with EGF stimulation revealed that the partially responsive group, but not the resistant group, exhibited suppressed ERK phosphorylation ex vivo. Furthermore, two lines from the partially responsive group, but none of the lines in the resistant group, exhibited a combinatory effect of cetuximab and trametinib, a MEK inhibitor, ex vivo and in vivo. Taken together, the results indicate that ex vivo signaling assay reflects the difference in sensitivity in vivo and stratifies KRAS mutant CTOS lines by sensitivity. Therefore, coupling the in vivo and ex vivo assays with CTOS can be a useful platform for understanding the mechanism of diversity in drug sensitivity.

Published
2017

15. Clinical role of ASCT2 (SLC1A5) in KRAS-mutated colorectal cancer

Author

80814029, 90322651, Toda, Kosuke, Nishikawa, Gen, Iwamoto, Masayoshi, Itatani, Yoshiro, Takahashi, Ryo, Sakai, Yoshiharu, Kawada, Kenji, 80814029, 90322651, Toda, Kosuke, Nishikawa, Gen, Iwamoto, Masayoshi, Itatani, Yoshiro, Takahashi, Ryo, Sakai, Yoshiharu, and Kawada, Kenji

Abstract

Mutation in the KRAS gene induces prominent metabolic changes. We have recently reported that KRAS mutations in colorectal cancer (CRC) cause alterations in amino acid metabolism. However, it remains to be investigated which amino acid transporter can be regulated by mutated KRAS in CRC. Here, we performed a screening of amino acid transporters using quantitative reverse-transcription polymerase chain reaction (RT-PCR) and then identified that ASCT2 (SLC1A5) was up-regulated through KRAS signaling. Next, immunohistochemical analysis of 93 primary CRC specimens revealed that there was a significant correlation between KRAS mutational status and ASCT2 expression. In addition, the expression level of ASCT2 was significantly associated with tumor depth and vascular invasion in KRAS-mutant CRC. Notably, significant growth suppression and elevated apoptosis were observed in KRAS-mutant CRC cells upon SLC1A5-knockdown. ASCT2 is generally known to be a glutamine transporter. Interestingly, SLC1A5-knockdown exhibited a more suppressive effect on cell growth than glutamine depletion. Furthermore, SLC1A5-knockdown also resulted in the suppression of cell migration. These results indicated that ASCT2 (SLC1A5) could be a novel therapeutic target against KRAS-mutant CRC.

Published
2017

17. Metabolic Alterations Caused by KRAS Mutations in Colorectal Cancer Contribute to Cell Adaptation to Glutamine Depletion by Upregulation of Asparagine Synthetase

Author

90322651, Toda, Kosuke, Kawada, Kenji, Iwamoto, Masayoshi, Inamoto, Susumu, Sasazuki, Takehiko, Shirasawa, Senji, Hasegawa, Suguru, Sakai, Yoshiharu, 90322651, Toda, Kosuke, Kawada, Kenji, Iwamoto, Masayoshi, Inamoto, Susumu, Sasazuki, Takehiko, Shirasawa, Senji, Hasegawa, Suguru, and Sakai, Yoshiharu

Abstract

A number of clinical trials have shown that KRAS mutations of colorectal cancer (CRC) can predict a lack of responses to anti-epidermal growth factor receptor–based therapy. Recently, there have been several studies to elucidate metabolism reprogramming in cancer. However, it remains to be investigated how mutated KRAS can coordinate the metabolic shift to sustain CRC tumor growth. In this study, we found that KRAS mutation in CRC caused alteration in amino acid metabolism. KRAS mutation causes a marked decrease in aspartate level and an increase in asparagine level in CRC. Using several human CRC cell lines and clinical specimens of primary CRC, we demonstrated that the expression of asparagine synthetase (ASNS), an enzyme that synthesizes asparagine from aspartate, was upregulated by mutated KRAS and that ASNS expression was induced by KRAS-activated signaling pathway, in particular PI3K-AKT-mTOR pathway. Importantly, we demonstrated that KRAS-mutant CRC cells could become adaptive to glutamine depletion through asparagine biosynthesis by ASNS and that asparagine addition could rescue the inhibited growth and viability of cells grown under the glutamine-free condition in vitro. Notably, a pronounced growth suppression of KRAS-mutant CRC was observed upon ASNS knockdown in vivo. Furthermore, combination of L-asparaginase plus rapamycin markedly suppressed the growth of KRAS-mutant CRC xenografts in vivo, whereas either L-asparaginase or rapamycin alone was not effective. These results indicate ASNS might be a novel therapeutic target against CRCs with mutated KRAS.

Published
2016

18. Laparoscopic repair for recurrent parastomal hernia of an end stoma using the sandwich technique while preserving an ileal conduit: A case report

Author

90322651, Wada, Toshiaki, Kawada, Kenji, Hasegawa, Suguru, Sakai, Yoshiharu, 90322651, Wada, Toshiaki, Kawada, Kenji, Hasegawa, Suguru, and Sakai, Yoshiharu

Abstract

Introduction: Parastomal hernia is a common complication following stoma creation. The surgical approaches included local repair by suture, stoma relocation and mesh-based techniques; but none has been able to provide satisfactory results. Presentation of case: A 60-year-old asian female was referred complaining of abdominal pain and constipation caused by recurrent parastomal hernia of an end stoma. She had undergone total cystectomy with creation of an ileal conduit at the age of 53 years, and laparoscopic sigmoid colostomy at the age of 55 years. Parastomal hernia of an end stoma had developed postoperatively, and she had undergone recreation of colostomy at the same place with fasciorrhaphy at the age of 59 years, but parastomal hernia recurred 6 months later because of split fascia sutures. Laparoscopic repair for recurrent parastomal hernia was conducted using the sandwich technique while preserving an ileal conduit. The patient has been followed postoperatively for more than 3 years without any sign of recurrence. Discussion: Although further cases are required to get definitive conclusions, we suppose that the laparoscopic sandwich technique can be useful for parastomal hernia. Conclusion: We herein report a case of recurrent parastomal hernia treated laparoscopically while preserving an ileal conduit using the sandwich technique which combines the keyhole and Sugarbaker techniques. This is a quite rare case report of laparoscopic repair for recurrent parastomal hernia in a patient with an ileal conduit.

Published
2016

19. Right hemicolectomy for mesenteric phlebosclerosis potentially caused by long-term use of herbal medicine: A case report and literature review

Author

40447983, 90322651, Hoshino, Nobuaki, Hasegawa, Suguru, Hida, Koya, Kawada, Kenji, Sakai, Yoshiharu, 40447983, 90322651, Hoshino, Nobuaki, Hasegawa, Suguru, Hida, Koya, Kawada, Kenji, and Sakai, Yoshiharu

Abstract

Introduction:Mesenteric phlebosclerosis is a rare ischemic disease affecting the colon. Systemic disease and herbal medicine have been pointed out as possible causes, and the disease is characterized by calcifications involved the mesocolic veins. Patients who do not respond to conservative therapy require surgical treatment. In surgical intervention, an adequate extent of colonic resection is important. Presentation of case We present a case of an 87-year-old woman with mesenteric phlebosclerosis who had consumed herbal medicine for 40 years. She suffered from ileus caused by mesenteric phlebosclerosis, and the symptoms did not improve with conservative therapy. Right hemicolectomy was performed since the disease was localized in the right colon. Long-term use of herbal medicine was considered the potential cause of mesenteric phlebosclerosis. The postoperative course was mostly uneventful. The patient stopped using herbal medicine and had no signs of recurrence 2 years after surgery. Discussion and conclusion The greatest concern in surgery for mesenteric phleboscrerosis is to detect the affected area, which should be removed. Characteristic findings in computed tomography and intraoperative findings can help to determine the optimal extent of colonic resection. Mesenteric phlebosclerosis caused by herbal medicines occurs as localized disease in the right colon compared with mesenteric phlebosclerosis caused by other pathogenesis. Limited colonic resection is usually indicated for mesenteric phlebosclerosis caused by herbal medicine.

Published
2016

20. Preoperative, intraoperative and postoperative risk factors for anastomotic leakage after laparoscopic low anterior resection with double stapling technique anastomosis

Author

90322651, Kawada, Kenji, Sakai, Yoshiharu, 90322651, Kawada, Kenji, and Sakai, Yoshiharu

Abstract

Anastomotic leakage (AL) is one of the most devastating complications after rectal cancer surgery. The double stapling technique has greatly facilitated intestinal reconstruction especially for anastomosis after low anterior resection (LAR). Risk factor analyses for AL after open LAR have been widely reported. However, a few studies have analyzed the risk factors for AL after laparoscopic LAR. Laparoscopic rectal surgery provides an excellent operative field in a narrow pelvic space, and enables total mesorectal excision surgery and preservation of the autonomic nervous system with greater precision. However, rectal transection using a laparoscopic linear stapler is relatively difficult compared with open surgery because of the width and limited performance of the linear stapler. Moreover, laparoscopic LAR exhibits a different postoperative course compared with open LAR, which suggests that the risk factors for AL after laparoscopic LAR may also differ from those after open LAR. In this review, we will discuss the risk factors for AL after laparoscopic LAR.

Published
2016

21. The role of chemokines in promoting colorectal cancer invasion/metastasis

Author

80814029, 90322651, Itatani, Yoshiro, Kawada, Kenji, Inamoto, Susumu, Yamamoto, Takamasa, Ogawa, Ryotaro, Taketo, Makoto Mark, Sakai, Yoshiharu, 80814029, 90322651, Itatani, Yoshiro, Kawada, Kenji, Inamoto, Susumu, Yamamoto, Takamasa, Ogawa, Ryotaro, Taketo, Makoto Mark, and Sakai, Yoshiharu

Abstract

Colorectal cancer (CRC) is one of the leading causes of cancer-related death worldwide. Although most of the primary CRC can be removed by surgical resection, advanced tumors sometimes show recurrences in distant organs such as the liver, lung, lymph node, bone or peritoneum even after complete resection of the primary tumors. In these advanced and metastatic CRC, it is the tumor-stroma interaction in the tumor microenvironment that often promotes cancer invasion and/or metastasis through chemokine signaling. The tumor microenvironment contains numerous host cells that may suppress or promote cancer aggressiveness. Several types of host-derived myeloid cells reside in the tumor microenvironment, and the recruitment of them is under the control of chemokine signaling. In this review, we focus on the functions of chemokine signaling that may affect tumor immunity by recruiting several types of bone marrow-derived cells (BMDC) to the tumor microenvironment of CRC.

Published
2016

23. EP4 Receptor–Associated Protein in Macrophages Ameliorates Colitis and Colitis-Associated Tumorigenesis

Author

90511907, 90335266, 40838679, 70644897, 90322651, 20252447, Nakatsuji, Masato, Minami, Manabu, Seno, Hiroshi, Yasui, Mika, Komekado, Hideyuki, Higuchi, Sei, Fujikawa, Risako, Nakanishi, Yuki, Fukuda, Akihisa, Kawada, Kenji, Sakai, Yoshiharu, Kita, Toru, Libby, Peter, Ikeuchi, Hiroki, Yokode, Masayuki, Chiba, Tsutomu, 90511907, 90335266, 40838679, 70644897, 90322651, 20252447, Nakatsuji, Masato, Minami, Manabu, Seno, Hiroshi, Yasui, Mika, Komekado, Hideyuki, Higuchi, Sei, Fujikawa, Risako, Nakanishi, Yuki, Fukuda, Akihisa, Kawada, Kenji, Sakai, Yoshiharu, Kita, Toru, Libby, Peter, Ikeuchi, Hiroki, Yokode, Masayuki, and Chiba, Tsutomu

Abstract

Prostaglandin E2 plays important roles in the maintenance of colonic homeostasis. The recently identified prostaglandin E receptor (EP) 4–associated protein (EPRAP) is essential for an anti-inflammatory function of EP4 signaling in macrophages in vitro. To investigate the in vivo roles of EPRAP, we examined the effects of EPRAP on colitis and colitis-associated tumorigenesis. In mice, EPRAP deficiency exacerbated colitis induced by dextran sodium sulfate (DSS) treatment. Wild-type (WT) or EPRAP-deficient recipients transplanted with EPRAP-deficient bone marrow developed more severe DSS-induced colitis than WT or EPRAP-deficient recipients of WT bone marrow. In the context of colitis-associated tumorigenesis, both systemic EPRAP null mutation and EPRAP-deficiency in the bone marrow enhanced intestinal polyp formation induced by azoxymethane (AOM)/DSS treatment. Administration of an EP4-selective agonist, ONO-AE1-329, ameliorated DSS-induced colitis in WT, but not in EPRAP-deficient mice. EPRAP deficiency increased the levels of the phosphorylated forms of p105, MEK, and ERK, resulting in activation of stromal macrophages in DSS-induced colitis. Macrophages of DSS-treated EPRAP-deficient mice exhibited a marked increase in the expression of pro-inflammatory genes, relative to WT mice. By contrast, forced expression of EPRAP in macrophages ameliorated DSS-induced colitis and AOM/DSS-induced intestinal polyp formation. These data suggest that EPRAP in macrophages functions crucially in suppressing colonic inflammation. Consistently, EPRAP-positive macrophages were also accumulated in the colonic stroma of ulcerative colitis patients. Thus, EPRAP may be a potential therapeutic target for inflammatory bowel disease and associated intestinal tumorigenesis.

Published
2015

24. Intramural metastasis of T1 rectal cancer: Report of a case report

Author

90322651, Toda, Kosuke, Kawada, Kenji, Hasegawa, Suguru, Yamada, Masahiro, Kawamura, Junichiro, Sakai, Yoshiharu, 90322651, Toda, Kosuke, Kawada, Kenji, Hasegawa, Suguru, Yamada, Masahiro, Kawamura, Junichiro, and Sakai, Yoshiharu

Abstract

Background: Intramural metastasis (IM) is extremely rare in colorectal cancer, although it often occurred in esophageal cancer. Case Presentation: We report a rare case of T1 rectal cancer with IM which was successfully resected by laparoscopic surgery. A 62-year-old man was admitted to our institution for the treatment of rectal cancer detected by medical examination. Colonoscopy revealed two tumors in the rectum: a type II rectal cancer of 2 cm in diameter located 5 cm proximal to the anal verge and a submucosal tumor of 1 cm in diameter located approximately 1.5 cm proximal to the rectal cancer. Abdominal computed tomography (CT), magnetic resonance imaging (MRI), and transrectal ultrasonography indicated the rectal cancer invaded into the submucosal layer with no metastasis to regional lymph nodes or distant organs. The patient underwent laparoscopic intersphincteric resection.Histopathological analysis revealed that the rectal cancer was moderately differentiated adenocarcinoma (stage I; pT1N0M0 according to the 7th edition of UICC) with severe lymphovascular invasion (ly1, v3) and that the submucosal tumor was composed of moderately differentiated adenocarcinoma proliferating within the muscularis propria. A number of features of the submucosal tumor indicated that this was an IM of the rectal cancer: clearly distinct location from the rectal cancer, growth predominantly within the muscularis propria, similar structural and cellular heterogeneity, and the presence of tumor emboli within vascular vessels. The patient was postoperatively followed for more than 4 years without any sign of recurrence. Conclusions: To the best of our knowledge, this is the first report of the T1 rectal cancer with IM.

Published
2015

25. Obtaining secure stapling of a double stapling anastomosis.

Author

40447983, 90322651, Nakayama, Shinya, Hasegawa, Suguru, Hida, Koya, Kawada, Kenji, Sakai, Yoshiharu, 40447983, 90322651, Nakayama, Shinya, Hasegawa, Suguru, Hida, Koya, Kawada, Kenji, and Sakai, Yoshiharu

Abstract

[Background]Anastomotic leakage is a serious complication after rectal surgery. The aim of this study was to assess the effect of waiting time during firing of stapling devices on optimal staple formation. [Methods]An endoscopic linear stapler (Echelon Flex 60 Endopath) with either a 60 mm blue or gold cartridge was applied to the cardiac and pyloric portions of 27 fresh porcine stomachs. Three different waiting times were used for the precompression and interstroke periods (0/0, 2/0, and 2/2 min). The staple line was divided into four portions (oral, anal and top, base), and the shape of each staple was evaluated. Optimal staple formation was also assessed using the circular stapler (CDH 29). [Results]Mean thickness of the cardiac and pyloric portions was 2.4 ± 0.35 mm and 4.0 ± 0.4 mm, respectively. The waiting time improved optimal staple formation for the blue cartridge, especially when it was used for the pyloric portion. Staple malformation was observed more commonly in the top portion than in the base portion; however, the former was improved by an interstroke waiting time. Staple formation using the circular stapler was satisfactory and not influenced by the prefiring waiting time or tissue thickness. [Conclusions]Employment of a waiting time improves optimal staple formation when the endoscopic linear stapler is used for challenging tissue.

Published
2015

26. Adenocarcinoma arising at a colostomy site with inguinal lymph node metastasis: report of a case.

Author

90322651, 40447983, Iwamoto, Masayoshi, Kawada, Kenji, Hida, Koya, Hasegawa, Suguru, Sakai, Yoshiharu, 90322651, 40447983, Iwamoto, Masayoshi, Kawada, Kenji, Hida, Koya, Hasegawa, Suguru, and Sakai, Yoshiharu

Abstract

Inguinal lymph node metastasis from adenocarcinoma arising at a colostomy site is extremely rare, and the significance of surgical resection for metastatic inguinal lymph nodes has not been established. An 82-year-old woman who had undergone abdominoperineal resection 27 years earlier was admitted to our hospital complaining of bleeding from a colostomy. Physical examination revealed that a tumor at the colostomy site directly invaded into the peristomal skin, and that a left inguinal lymph node was firm and swollen. Positron emission tomography/computed tomography scan demonstrated accumulation of (18)F-fluorodeoxy glucose into both the colostomy tumor and the left swollen inguinal lymph node, while there was no evidence of metastasis to liver or lungs. She underwent open left hemicolectomy with wide local resection of the colostomy, and dissection of left inguinal lymph nodes. Histological diagnosis was a moderately differentiated adenocarcinoma that directly invaded into the surrounding skin and metastasized to the left inguinal lymph node. The patient has been followed up for >5 years without any sign of recurrence. In general, inguinal lymph node metastasis from colorectal cancers is regarded as a systemic disease with a poor prognosis, and so systemic chemotherapy and radiotherapy, but not surgical lymph node dissection, are recommended. Considering the lymphatic drainage route in the present case, inguinal lymph node metastasis does not represent a systemic disease but rather a sentinel nodal metastasis from adenocarcinoma at a colostomy site. Surgical dissection of metastatic inguinal lymph nodes should be considered to enable a favorable prognosis in the absence of distant metastasis to other organs.

Published
2014

27. Inhibitory role of Gas6 in intestinal tumorigenesis.

Author

90335266, 40838679, 90322651, 60273455, Akitake-Kawano, Reiko, Seno, Hiroshi, Nakatsuji, Masato, Kimura, Yuto, Nakanishi, Yuki, Yoshioka, Takuto, Kanda, Keitaro, Kawada, Mayumi, Kawada, Kenji, Sakai, Yoshiharu, Chiba, Tsutomu, 90335266, 40838679, 90322651, 60273455, Akitake-Kawano, Reiko, Seno, Hiroshi, Nakatsuji, Masato, Kimura, Yuto, Nakanishi, Yuki, Yoshioka, Takuto, Kanda, Keitaro, Kawada, Mayumi, Kawada, Kenji, Sakai, Yoshiharu, and Chiba, Tsutomu

Published
2013

28. Loss of SMAD4 From Colorectal Cancer Cells Promotes CCL15 Expression to Recruit CCR1(+) Myeloid Cells and Facilitate Liver Metastasis.

Author

80814029, 90322651, 00609076, 50315933, 10362500, 80229286, 40252449, 60273455, 70281714, Itatani, Yoshiro, Kawada, Kenji, Fujishita, Teruaki, Kakizaki, Fumihiko, Hirai, Hideyo, Matsumoto, Takuya, Iwamoto, Masayoshi, Inamoto, Susumu, Hatano, Etsuro, Hasegawa, Suguru, Maekawa, Taira, Uemoto, Shinji, Sakai, Yoshiharu, Taketo, Makoto Mark, 80814029, 90322651, 00609076, 50315933, 10362500, 80229286, 40252449, 60273455, 70281714, Itatani, Yoshiro, Kawada, Kenji, Fujishita, Teruaki, Kakizaki, Fumihiko, Hirai, Hideyo, Matsumoto, Takuya, Iwamoto, Masayoshi, Inamoto, Susumu, Hatano, Etsuro, Hasegawa, Suguru, Maekawa, Taira, Uemoto, Shinji, Sakai, Yoshiharu, and Taketo, Makoto Mark

Published
2013

30. Fluorescence diagnosis of metastatic lymph nodes using 5-aminolevulinic acid (5-ALA) in a mouse model of colon cancer.

Author

90322651, 10362500, 60273455, Kato, Shigeru, Kawamura, Junichiro, Kawada, Kenji, Hasegawa, Suguru, Sakai, Yoshiharu, 90322651, 10362500, 60273455, Kato, Shigeru, Kawamura, Junichiro, Kawada, Kenji, Hasegawa, Suguru, and Sakai, Yoshiharu

Abstract

[Background]Lymph node metastasis is one of the most critical prognostic factors in patients with colorectal cancer. Although regional lymph nodes should be surgically resected and pathologically examined, techniques for the intraoperative diagnosis of lymph node metastasis remain to be well established. Fluorescence diagnosis using 5-aminolevulinic acid (5-ALA) is a promising technique for evaluating various malignancies. After exogenous administration of 5-ALA, protoporphyrin IX (PPIX) accumulates in malignant cells and can be detected as red fluorescence. In this study, we investigated the usefulness of fluorescence diagnosis using 5-ALA for the detection of lymph node metastasis in a mouse model of colon cancer. [Materials and Methods]An orthotopic colon cancer model was prepared by inoculating the cecal wall of nude mice with HCA7, a human colon adenocarcinoma cell line. After 3 wk, 40 mg/kg of 5-ALA was administered intraperitoneally (IP) or orally (PO). Fluorescence diagnosis with a D-Light System (Karl Storz) was then performed after 3 or 6 h. [Results]In the IP group, PPIX fluorescence was detected in metastatic lymph nodes as well as in other malignant lesions, including primary tumors and abdominal implantations, while non-metastatic nodes were fluorescence-negative. In contrast, no obvious fluorescence was detected in cancerous tissues in the PO group. [Conclusions]PPIX fluorescence induced by intraperitoneal injection of 5-ALA allows metastatic lymph nodes to be accurately diagnosed in this mouse model. This technique may facilitate the intraoperative diagnosis of lymph node metastases from colon cancer in a clinical setting.

Published
2012

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