| Literature DB >> 27491544 |
Ruiqi Xue1, Huan Gu2,3, Yamei Qiu2, Yong Guo1, Christine Korteweg2, Jin Huang2, Jiang Gu1,2.
Abstract
CF is caused by mutations of the gene encoding the cystic fibrosis transmembrane conductance regulator (CFTR) which is an anion selective transmembrane ion channel that mainly regulates chloride transport, expressed in the epithelia of various organs. Recently, we have demonstrated CFTR expression in the brain, the spinal cord and the sympathetic ganglia. This study aims to investigate the expression and distribution of CFTR in the ganglia of the human gastrointestinal tract. Fresh tissue and formalin-fixed paraffin-embedded normal gastrointestinal tract samples were collected from eleven surgical patients and five autopsy cases. Immunohistochemistry, in situ hybridization, laser-assisted microdissection and nested reverse transcriptase polymerase chain reaction were performed. Expression of CFTR protein and mRNA was detected in neurons of the ganglia of all segments of the human gastrointestinal tract examined, including the stomach, duodenum, jejunum, ileum, cecum, appendix, colon and rectum. The extensive expression of CFTR in the enteric ganglia suggests that CFTR may play a role in the physiology of the innervation of the gastro-intestinal tract. The presence of dysfunctional CFTRs in enteric ganglia could, to a certain extent, explain the gastrointestinal symptoms frequently experienced by CF patients.Entities:
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Year: 2016 PMID: 27491544 PMCID: PMC4974654 DOI: 10.1038/srep30926
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379
Characteristics of the 16 subjects studied.
| Case No. | Sex/Age (y) | Pathological diagnosis | Segments investigated in the study | |||||||
|---|---|---|---|---|---|---|---|---|---|---|
| Stomach | Duodenum | Jejunum | Ileum | Cecum | Appendix | Colon | Rectum | |||
| 1 | M/41 | Ileum interstitialoma | √ | |||||||
| 2 | M/53 | Pancreatic head adenocarcinoma | √ | |||||||
| 3 | F/61 | Pancreatic head ductal adenocarcinoma | √ | |||||||
| 4 | F/36 | Colonic adenocarcinoma | √ | √ | ||||||
| 5 | F/60 | Colonic adenocarcinoma | √ | √ | ||||||
| 6 | M/77 | Rectal adenocarcinoma | √ | |||||||
| 7 | M/66 | Lesser curvature adenocarcinoma | √ | √ | ||||||
| 8 | M/50 | Duodenal adenocarcinoma | √ | √ | ||||||
| 9 | M/35 | Colonic adenocarcinoma | √ | √ | ||||||
| 10 | F/52 | Rectal adenocarcinoma | √ | √ | ||||||
| 11 | M/71 | Rectal adenocarcinoma | √ | √ | ||||||
| 12 | F/28 | Amniotic fluid embolism | √ | √ | √ | √ | ||||
| 13 | M/25 | Epidemic cerebrospinal meningitis | √ | √ | √ | |||||
| 14 | F/74 | Hypertensive heart disease | √ | √ | √ | √ | ||||
| 15 | M/81 | Dissecting aneurysm of the abdominal aorta | √ | √ | √ | √ | √ | |||
| 16 | F/78 | Acute pulmonary embolism | √ | √ | √ | √ | √ | √ | √ | |
Figure 1Cystic fibrosis transmembrane conductance regulator (CFTR) expression in the neurons of human enteric ganglia as detected by immunohistochemistry (IHC) and in situ hybridization (ISH).
(A–H): IHC results for CFTR in human gastrointestinal ganglia. (A–H) show segments of stomach (A), duodenum (B), jejunum (C), ileum (D), cecum (E), appendix (F), colon (G) and rectum (H). Lower right square insert in each figure shows the higher power image of indicated area of the lower power view. Each photograph shows cell groups of enteric ganglia between two layers of smooth muscle of different orientations. The brown positive signals developed with DAB show positive CFTR staining. CFTR-positive signals are localized to the cytoplasm of the neurons and to some dendrites, axons and nerve fibers. The nuclei and nucleoli lack positive signals. Smooth muscle cells and glial cells are also negative. (I–P): ISH results for CFTR in human enteric ganglia. (I–P) show segments of stomach (I), duodenum (J), jejunum (K), ileum (L), cecum (M), appendix (N), colon (O) and rectum (P). Lower right square insert in each figure shows the higher power image of indicated area of the lower power view. The purple-blue positive signals developed with NBT/BCIP show CFTR mRNA ISH staining. CFTR-positive signals are localized to the cytoplasm of the neurons, some of the nuclei and nucleoli, dendrites, axons and nerve fibers. Smooth muscle cells are negative. (Q–S): Higher power image for CFTR IHC and ISH results and consecutive sections of IHC with antibodies to neurofilament. (Q–S) consecutive sections show the CFTR IHC (Q), ISH (R) and the NF IHC (S) results of a same ganglion, and numbered arrows indicate the same cells. Positive NP signals are observed in CFTR IHC and CFTR mRNA ISH positive cells on consecutive sections, indicating that the CFTR positive cells are neurons. (T): Positive control of CFTR IHC: gastric epithelium. Lower right square insert shows the higher power image of a submucosal plexus. The brown positive signals developed with DAB show positive CFTR staining, same as the epithelium. (U): Positive control of CFTR mRNA ISH in gastric epithelium. Bar = 20 μm.
Figure 2Laser-assisted microdissection (LMD) and nested RT-PCR of CFTR in human enteric ganglia.
(A,B) show the location where the LMD dissected the collections of ganglion cells (A2) and smooth muscle cells (A1). (A) is photograph taken before, and (B) after LMD. Numbered arrows indicate the same collection of cells. (C) shows the expression of CFTR mRNA by nested RT-PCR. Lane 1, DNA marker; Lane 2, enteric ganglia; Lane 3, colon mucosa (positive control); Lane 4, smooth muscle; Lane 5, water (negative control); Lane 6, DNA marker; Lane 7, enteric ganglia; Lane 8, colon mucosa (positive control); Lane 9, smooth muscle; Lane 10, water (negative control). The CFTR product is 179 bp, and the 18S product is 155bp. Bar = 200 μm.