Profuse Diarrhea Research Articles

Alterations in oxidative stress parameters and its associated correlation with clinical disease on experimental Cryptosporidium parvum infection in Swiss albino mice.

The present study was conducted to evaluate the changes in oxidative stress parameters on experimental infection with Cryptosporidium parvum in Swiss albino mice. The mice were divided into four groups viz., group I-IV, each group comprising of 15 mice. Group I mice served as healthy control. In Group II mice, C. parvum oocysts @ 104/os were administered, mice of group III were given dexamethasone @ 30µg/ml in drinking water whereas group IV mice were given dexamethasone @ 30µg/ml along with C. parvum oocysts @ 104/os. Significant changes were seen in oxidative stress parameters which included significant increase in LPO and decrease in levels of SOD, CAT and GSH in liver and intestine in group IV mice at 10th DPI when compared to others indicating an important role played by free radical induced oxidative stress in the development of C. parvum infection in mice which was clinically characterized by loss of body condition, profuse bloody diarrhoea and peak oocyst shedding intensity occurring at 10th DPI.

Undiagnosed Amoebic Colitis Presenting as Anemia

Amoebic colitis is caused by Entamoeba histolytica, a parasitic protozoan which is found in areas with poor sanitation and contaminated water. Infection is spread via the fecal-oral, oral-anal or oral-genital route. Infected patients may experience abdominal pain, profuse diarrhea and weight loss. We describe a patient with amoebic colitis who presents with exertional dyspnea and profound anemia. A seventytwo year old male presented to the emergency department with exertional shortness of breath for the past three months. On further questioning, he endorsed frequent loose stools and a ten pound weight loss over the past two months. Patient had traveled to India three months prior and recalled having several bouts of diarrhea which self-resolved. On exam, patient was tachycardic with pale conjunctiva and normal rectal exam, revealing brown stool. Labs were significant for hemoglobin of 4.4 g/dL with MCV of 57fL and a ferritin of 8 ng/dL. Patient was transfused 3 units packed red blood cells and started on intravenous iron. Stool specimens were obtained and colonoscopy was performed for further evaluation. On colonoscopy patient was noted to have discontinuous ulcerated mucosa in the cecum and ascending colon. Histological examination of the biopsy revealed trophozoites of Entamoeba histolytica. Patient was started on metronidazole for 10 days and discharged with appropriate follow-up. Amoebiasis is the second leading parasitic cause of death in the world. Intestinal amoebiasis is normally localized to the ascending colon or cecum. Most infected patients are asymptomatic and can shed amoebic cysts in the stool. Although gastrointestinal symptoms may be present, the onset is usually insidious, making the diagnosis difficult. If left untreated complications such as massive hemorrhage, colonic perforation, strictures and liver abscesses can develop. Thus, it is important to have a high clinical suspicion, specifically if patients visit endemic areas and return with gastrointestinal symptoms. In this particular case, our patient experienced symptoms for several months but remained undiagnosed. The significant anemia, which was likely from the bleeding ulcerations, led to a colonoscopy and the diagnosis of amoebic colitis.Figure 1

Emergency therapy for liver metastases from advanced VIPoma: surgery or transarterial chemoembolization?

VIPoma is a rare neuroendocrine tumor (NET) with a high potential to develop hepatic metastases and poor prognosis. The primitive tumor is nonsymptomatic and usually localized within the pancreas. Liver metastasis drives the prognosis and induces profuse watery diarrhea or renal failure. We herein present severe renal failure or diarrhea in two patients hospitalized in intensive care justifying emergency treatment of liver metastasis. The two patients experienced severe diarrhea due to a hypersecretion of vasoactive intestinal peptide (VIP) from liver metastasis released into the blood circulation. Therapeutic management was discussed and liver transarterial chemoembolization (TACE) was performed with chemotherapy-loaded embospheres, which cause necrosis of tumor lesions. TACE controlled the hormonal syndrome and made patients eligible for curative surgery. Tumor necrosis occurred and VIP levels collapsed. Surgery was performed in one of the two cases after TACE and the patient was considered in remission. Both patients were still alive after 3 years of follow up. Thus, TACE is feasible and appears to be an effective emergency treatment in patients with a VIP-hormonal syndrome due to liver metastases. Despite the biological disorder due to the hormonal secretion, an aggressive approach is warranted in VIP liver metastasis.

Prise en charge du gastrinome

Gastrinoma is a very rare tumor leading to gastrin hypersecretion and characterised by Zollinger-Ellisson syndrome (ZES) i.e. severe gastric and duodenal ulceration and profuse diarrhea. This disease can be sporadic or familial within a multiple endocrine neoplasia type1 (MEN-1) syndrome. Diagnosis is based on hypergastrinemia/hypercholrhydria. Tumors are usually located in the duodeno-pancreas. Preoperative tumor location by CT, echoendoscopy and fibroscopy is not always possible because of the small size of the lesion that are frequently multiple. The aim of gastrinoma treatment is 1/to control the hormonal hypersecretion 2/to remove the neoplasm when it is possible. Surgery is the only chance to cure. Gastrinoma is a slow-growing tumor, and overall survival is good with a median survival above 10years and a 5-year survival above 80% in surgically resected patients. Recurrence is frequent, a biochemical recurrence is observed in 65% of cases and morphological recurrence in 40% of patients at 2years. Metastases are associated with a dismal prognosis.

First description of an in vitro culture system for Eimeria ovinoidalis macromeront formation in primary host endothelial cells

The apicomplexan parasite Eimeria ovinoidalis is distributed worldwide and causes clinical ovine coccidiosis. As one of the most pathogenic species in sheep, the principal clinical sign is profuse diarrhoea in young animals, which leads to important economic losses in the ovine industry. We here aimed to establish an in vitro culture system for the development of E. ovinoidalis macromeronts, as no suitable systems are currently available for any ovine Eimeria species. Faecal samples containing more than 90% of E. ovinoidalis oocysts were collected from naturally infected lambs and ewes in Murcia Region (Spain). E. ovinoidalis oocysts were collected, left to sporulate in potassium dichromate and stored at 4°C until further studies were conducted. Moreover, a suitable excystation protocol was effectively established, resulting in the release of viable sporozoites, which were allowed to infect primary bovine umbilical vein endothelial cells (BUVEC) and permanent bovine colonic epithelial cells (BCEC). In vitro first merogony was successfully accomplished exclusively in BUVEC leading to macromeront formation (up to 100μm) and the release of fully developed and viable merozoites I stages. Given that we were able to establish a suitable in vitro system for the first merogony of such pathogenic Eimeria species in sheep, advances might be further made not only on studies regarding the control of ovine coccidiosis, such as drug screenings, but also on the better understanding of molecular parasite–host cell interactions as already demonstrated for other ruminant Eimeria species.

Supporting patients to manage faecal incontinence.

British Journal of NursingVol. 25, No. 7 RegularsSupporting patients to manage faecal incontinenceSue WoodwardSue WoodwardSearch for more papers by this authorSue WoodwardPublished Online:15 Apr 2016https://doi.org/10.12968/bjon.2016.25.7.370AboutSectionsView articleView Full TextPDF/EPUB ToolsAdd to favoritesDownload CitationsTrack CitationsPermissions ShareShare onFacebookTwitterLinked InEmail View article References Beeckman D, Woodward S, Rajpaul K, Vanderwee K (2011) Clinical challenges of preventing incontinence-associated dermatitis. Br J Nurs 20(13): 784–6,788,790. doi: https://doi.org/10.12968/bjon.2011.20.13.784 Link, Google ScholarBritish Society of Gastroenterologists (2016) Clinical Commissioning Report: Faecal Incontinence. http://tinyurl.com/gpp8es9 (accessed 5 April 2016) Google ScholarBurch J, Collins B (2010) Using biofeedback to treat constipation, faecal incontinence and other bowel disorders. Nurs Times 106(37): 18–21 Medline, Google ScholarCotterill N, Norton C, Avery KN, Abrams P, Donovan JL (2008) A patient-centered approach to developing a comprehensive symptom and quality of life assessment of anal incontinence. Dis Colon Rectum 51(1):82–7 Crossref, Medline, Google ScholarNational Institute for Health and Care Excellence (2007) Faecal incontinence in adults: management. [CG49]. http://tinyurl.com/zyvoey4 (accessed 5 April 2016) Google ScholarNorton C, Chelvanayagum S, eds (2004) Bowel Continence Nursing. Beaconsfield Publishers, Beaconsfield Google ScholarTariq SH (2007) Constipation in long-term care. J Am Med Dir Assoc 8(4):209–18 Crossref, Medline, Google ScholarWoodward S (2012) Management options for faecal incontinence. Nursing and Residential Care 14(5): 224–229 Link, Google Scholar FiguresReferencesRelatedDetails 14 April 2016Volume 25Issue 7ISSN (print): 0966-0461ISSN (online): 2052-2819 Metrics History Published online 15 April 2016 Published in print 14 April 2016 Information© MA Healthcare LimitedPDF download

Significant weight loss related to Briquet syndrome: A case report

IntroductionSomatization Disorder is more prevalent in females and is historically known as Briquet Syndrome. It is characterized by complaints in several systems, has early onset and chronic fluctuating course, but without organic substrate. When the duration of symptoms is less than two years or they are less obvious, it is called Undifferentiated Somatoform Disorder.ObjectivesThis study reports the case of a female patient, previously healthy and with no psychiatric history, which abruptly presented lush somatic symptoms without organic origin.Case PresentationCase report of a previously healthy woman of 32 years, followed up for 14 months, by a sudden onset frame of profuse diarrhea, tenesmus, fecal incontinence, vomiting, anorexia and weight loss (18 kilos in 2 months), associated with headache and autonomic signs of anxious origin, without clear physical and/or psychogenic trigger. She had only a mild response to drug therapy and excellent improvement in symptoms after psychotherapy.ResultsUnconscious triggers came to light only after psychotherapy starts, justifying that the magnitude of autonomic somatoform symptoms surpasses the time period established by ICD-10 for Somatization Disorder. Therefore, the rapid resolution did not allow a diagnosis of Somatization Disorder, according to ICD-10. So, it was diagnosed as Undifferentiated Somatoform Disorder.ConclusionIt is suggested that the grandeur of clinical symptoms in this case is caused by psychogenic factors.Disclosure of interestThe authors have not supplied their declaration of competing interest.

When Symptomatic Treatment Becomes Antitumor Treatment for Vipoma: Opportunity for Frail Elderly Adults

To the Editor: An 82-year-old woman was admitted to the emergency department because of a fall with head injury and loss of consciousness. Her hospital record revealed a history of untreated urinary incontinence, dyslipidemia, and hypertension. During the previous 6 weeks, she had had untreated profuse diarrhea (>10 watery stools per day), a 10-kg loss of weight, and severe asthenia. On examination, she showed evidence of delirium with fluctuating level of consciousness and disorientation, ophthalmic zoster lesions, and severe dehydration. Laboratory tests showed hypokalemia 1.5 mmol/L (normal range 3.5–5.0 mmol/L), hypercalcemia 3.2 mmol/L (normal range 2.2–2.6 mmol/L), and acute renal failure. Her electrocardiogram showed inverted T waves and ST depression. Fluid and electrolyte replacement urgently performed under cardiac monitoring led to partial improvement of her condition. Thoracoabdominal computed tomography was performed to investigate the profuse diarrhea and showed a 7-cm hypervascularized tumor in the tail of the pancreas, with nodes of peritoneal carcinomatosis and lesions in the liver and lungs, and a bilateral pulmonary embolism. Emergency physicians consulted the mobile geriatric team, and she was admitted to the geriatric ward, because it was best suited to provide the comprehensive care required. Anticoagulant therapy was initiated, and in consultation with gastroenterologists, short-acting octreotide (somatostatin analogue) 100 μg twice a day for symptomatic diarrhea was initiated, leading to dramatic improvement. To implement the best care plan, comprehensive geriatric assessment was performed 3 weeks after admission.1, 2 Of the 10 standard domains assessed, six were impaired: mild cognitive impairment, mobility and balance disturbance, activity of daily living impairment, malnutrition, and social isolation. It was decided to investigate further her pancreatic tumor to determine the best treatment. Computed tomography–guided needle biopsy of the pancreatic mass diagnosed a well-differentiated neuroendocrine tumor. Chromogranin A was 143 ng/mL (normal <85 ng/mL) and vasoactive intestinal peptide (VIP) was 157 ng/L (normal 23–63 ng/L). Indium-111-octreotide scintigraphy showed an isolated strong uptake in the tail of the pancreas. A potential diagnosis of metastatic VIPoma was reached. The institutional tumor board chose palliative care for this frail 82-year-old woman and decided to switch to a long-acting somatostatin analogue for its antisecretory and antitumor effects. She died 5 months later, before progression of the tumor could be assessed. VIPoma is a rare functional neuroendocrine tumor of the pancreas (pNET) that secretes VIP. Although VIPoma is rare (estimated incidence 0.05–0.2/1,000,000 individuals), the incidence of NET is rising and could be more common in elderly adults.3-5 The typical clinical features of VIPoma result from excessive secretion of VIP and include large-volume secretory diarrhea, hypokalemia, and dehydration.3 Somatostatin analogues, which inhibit the release of neuroendocrine hormones, control hormone-related symptoms in up to 70% to 90% of symptomatic pNETs.6 Forty percent to 95% of VIPomas are metastatic at presentation, and the symptoms related to excessive secretion of VIP are more likely to shorten life expectancy than tumor growth.7 Thus, management of these tumors in frail elderly adults requires collaboration between endocrinologists and geriatricians to weigh the pros and cons of each therapeutic option. Two new therapeutic options are worth mentioning. First, two targeted therapies everolimus and sunitinib, have recently been approved for treatment of progressive metastatic pNET, although no evidence of efficacy in older adults is available.8 Second, somatostatin analogues, which have an excellent tolerance profile, have been shown to have an antitumor effect: in retrospective studies, stabilizing up to 50% of 60% of NET, and in two randomized controlled trials of octreotide long-acting release in metastatic midgut NET and nonfunctioning gastroenteropancreatic NET.6, 9, 10 Somatostatin analogues are thus recommended for antiproliferative purposes in nonresectable, slowly progressive, low proliferative NET.6, 8 Even though there is no evidence of efficacy in older adults, somatostatin analogues have been used in elderly adults for their antisecretory effects and could be a nonaggressive alternative treatment for frail elderly adults. In conclusion, this case illustrates that multidisciplinary collaboration enabled the choice of adequate treatment for this frail elderly woman. Moreover, a well-known symptomatic treatment has been proven to have an antitumor effect, increasing the spectrum of treatment options in this population. Conflict of Interest: All the authors declare no conflict of interest. Author Contributions: All the authors met the ICMJE criteria to be considered as authors. Sponsor's Role: No sponsor.

Epidemiological study of drug resistant cholera in and around Miraj, India

Background: Cholera is an intestinal infection caused by Vibrio cholerae . The hallmark of the disease is profuse secretory diarrhea. Cholera can be endemic, epidemic, or pandemic. Despite all the major advances in research, the condition still remains a challenge to the modern medical world. Objectives: This study was conducted to observe various epidemiological profile of cholera outbreak and to determine the antibiotic sensitivity pattern of isolates . Methods: A descriptive study was conducted from 18th January 2010 to 31st July 2010. All confirmed cases of cholera were included in the present study during the study period. Antibiotic sensitivity testing was performed by disc diffusion method. Results: Total 63 patients of cholera caused by Vibrio cholerae O1 were admitted in the hospital during the present study; majorities (60.32%) of cases were males and cases were more (79.36%) amongst adults (>15 years). All strains were El Tor. The outbreak started on 18th January 2010, peaked in February and lasted till 24 th July 2010. Detection of V. cholera O1 biotype El Tor serotype Ogawa was 81.25% and rests (18.75%) were serotype Inaba. Clinically all cases (100%) presented with profuse watery diarrhea, 28.57% had vomiting, 20.63% had abdominal cramps while fever was present in 9.53% of cases. Majority of isolates were sensitive to amikacin and cephalexin but resistant to ampicillin and chloramphenicol . Conclusions: Provision of safe drinking water, improving sanitation and strengthening of disease surveillance especially in coordination with local health authorities across the border is necessary to avoid recurrences of cholera.

Oral Proton Pump Inhibitor for Treatment of Congenital Chloride Diarrhea

Congenital chloride diarrhea (CCD) is a rare autosomal recessive disease, which is characterized by electrolyte absorption defect due to impaired function of the Cl-/ HCO3exchanger in the ileum and the colon. Its main features are profuse watery diarrhea, high fecal chloride concentration, and failure to thrive. Profuse watery diarrhea characterized by a high concentration of chloride in stools results in hypochloremia, hyponatremia, and dehydration with metabolic alkalosis. Early detection and therapeutic intervention can prevent life-threatening symptoms of CCD and growth failure. Recently, several therapies, such as proton pump inhibitors and butyrate, have been suggested for amelioration of diarrhea. Here, we report a case of CCD in a preterm male infant who was successfully treated with an oral proton pump inhibitor.

A Case Study: Cholera

The bacterium named Vibrio cholerae is known to be the microorganism causing the deadly disease called as cholera. The first successful isolation of the V. cholerae bacterium occurs as an important instance in the history of medicine on the whole. New, more virulent and drug-resistant strains of V. cholerae continue to emerge, and the frequency of large protracted outbreaks with high case fatality ratios has increased, reflecting the lack of early detection, prevention and access to timely health care. The primary symptoms of cholera are profuse diarrhea (Looseness of bowl movement) and vomiting of clear fluid. Cholera is only one of many types of diarrhoeal disease, but its global importance is underlined by its inclusion in the WHO Communicable Disease Surveillance and Response (CSR) list. A patient who is infected with bacteria V. cholerae (Cholera is caused by the bacterium V. cholera, this bacterium is Gram stain-negative), by eating contaminated food and water and by drink water after watermelon. In most cases cholera can be successfully treated with oral rehydration therapy which is highly effective.

Immunostaining of Cryptosporidiosis with Human Immunodeficiency Virus Infection.

A 33-year-old man with human immunodeficiency virus (HIV) infection was referred to our hospital because of profuse diarrhea and weight loss (Body mass index 14.5). The HIV-RNA and CD4 counts were 640,000 copies/mL and 22 /μL, respectively. Hematoxylin and Eosin stained colonic biopsy specimens showed Cryptosporidium oocysts attached to the epithelial cells (Picture 1). On immunostained tissue specimens with anti-Cryptosporidium antibodies, parasites were found to be penetrating the mucosal epithelium and they were also observed in the lamina propria (Picture ​(Picture2,2, ​,3).3). Notably, the parasites were more abundant right under the damaged mucosal surface (Picture 3). His diarrhea improved 2 weeks after the initiation of antiretroviral therapy. These findings may indicate that HIV-associated mucosal immune dysfunction can sometimes lead to the onset of invasive cryptosporidiosis (1). Although immunological diagnostic stool tests are well documented (2), histological examinations in such cases are rarely performed. Immunostaining may therefore be a powerful tool to elucidate the mechanisms by which Cryptosporidium cause life-threatening diarrhea in HIV-infected patients.

Blastocystis sp. Infection Mimicking Clostridium Difficile Colitis.

We report an unusual case of severe diarrhea related to Blastocystis sp. infection in a patient with end stage renal disease on hemodialysis. The patient was admitted due to profuse diarrhea associated with fever and leukocytosis. Pertinent stool work-up such as leukocytes in stool, stool culture, clostridium difficile toxin B PCR, and serology for hepatitis A, hepatitis B, and hepatitis C and cytomegalovirus screening were all negative. Ova and parasite stool examination revealed Blastocystis sp. The patient was given intravenous metronidazole with clinical improvement by day three and total resolution of symptoms by day ten.

Fecal Microbiota Transplantation in Refractory Clostridium difficile Infection in Children: Case Report and Review of the Literature

The human gastrointestinal tract evolves gradually from being sterile as neonates to being populated with trillions of bacterial species existing symbiotically for proper colonic function [1]. Disruption of homeostasis predisposes the gastrointestinal tract to increased incidence of enteric infections. Antibiotic use and immunocompromised states have been associated with an increased incidence of Clostridium difficile infection (CDI). Although approximately 35% of children's guts are colonized with CDI, it rarely causes symptoms [5]. Antibiotic therapy is considered first line for CDI; however, fecal microbiota transplantation (FMT) has recently gained favorable results for refractory and recurrent cases [6]. This involves reintroducing typical microbiota to reestablish balance of the gut flora [6,7]. We report a case of refractory CDI affecting half of an immunocompromised child's life that was cured with single FMT treatment. A 4-year-old male born via cesarean section at 37 weeks was diagnosed with a genetic disorder, Kabuki syndrome. His early life was complicated by recurrent infections, requiring several courses of antibiotics. As a result, he developed refractory CDI that lasted for 30 months, affecting his growth. His parents sought alternative options in which he was evaluated for FMT. He underwent FMT with his father as the stool donor. A 250mL aliquot of stool slurry was infused into the terminal ileum via colonoscopy, according to our institution's protocol. The child recovered from CDI with decreased bowel movements within 24 hours. He remained CDI negative and asymptomatic at 8 weeks after the procedure. Antibiotic use and immunocompromised states have been associated with an increased incidence of CDI [6]. CDI causes profuse diarrhea and may progress to colitis or complications including multi-organ failure and sepsis [6]. Recurrence after initial treatment course with antibiotics is noted to be as high as 20% [8]. In this case, Kabuki syndrome predisposed this patient to multiple infections requiring several courses of antibiotics. Each course of antibiotics caused an additional insult to the homeostasis of the gut microbiome, leading to refractory CDI. FMT has been reported to successfully treat patients with recurrent CDI in immunocompetent patients; however, there have been no reported cases of FMT in the immunocompromised pediatric population with Kabuki syndrome and CDI. The success in this case should prompt consideration of FMT in he pediatric population.

A Rare Presentation of Cecal Plasmablastic Lymphoma in an HIV Positive Patient

A 35 year old man with a history of HIV/AIDS (CD4: 39, Viral Load: 1.4 million) noncompliant with HAART and untreated hepatitis C presented with acute on chronic shortness of breath and abdominal pain associated with nausea and vomiting for one week. On admission, he was afebrile and hemodynamically stable. He appeared cachectic and tachypneic, with right upper quadrant tenderness, without rebound or guarding. Skin was notable for scattered non-pigmented nodules over his abdomen and groin. Labs were significant for a microcytic anemia (9.3 mg/dL) with a normal white blood cell count. Chest and abdominal CT showed right middle and lingual lobe collapse with calcified lymph nodes, as well as a heterogeneous mass in the cecum with peripheral air, but without obstruction or perforation. The patient was started on empiric antibiotics for pneumonia. He underwent an IR-guided biopsy of the mass, as well as a skin biopsy. Pathology was consistent with Epstein Barr Virus positive B-cell lymphoma with plasmacytoid features. PET-CT scan showed FDG avid lymph nodes in the head and neck with pulmonary nodules and skull based lesions. CSF was suspicious for lymphoma involvement. He received rituximab, etoposide, prednisone, vincristine, cyclophosphamide, doxorubicin (R-EPOCH) with intrathecal methotrexate. He subsequently developed profuse diarrhea and E. coli septic shock in the setting of neutropenia. Given his overall poor prognosis, the patient's family chose to pursue comfort measures and he expired shortly thereafter. Plasmablastic lymphoma (PBL) is a mature B-cell lymphoma. The majority of cases have occurred in patients who are immunocompromised, specifically HIV patients. Most cases are associated with EBV infection [1]. Pathogenesis of this relationship is still unclear, however. PBL is classically described as a lesion in the oral cavity in HIV positive patients but is rare to find in the GI tract, especially the cecum [2, 3]. It is an aggressive cancer without a definitive treatment protocol. Current literature suggests chemotherapy and radiotherapy, such as EPOCH [3, 4]. However, there have been improved regimens based on HAART therapy along with chemotherapy. [5]. Prognosis is poor in patients with PBL in the GI tract and literature reports an average survival time of 6 months [6]. This case highlights the importance of early diagnosis and treatment of this rare and aggressive form of cancer.Figure 1

Local and systemic inflammatory and immunologic reactions to cyathostomin larvicidal therapy in horses

Encysted cyathostomin larvae are ubiquitous in grazing horses. Arrested development occurs in this population and can lead to an accumulation of encysted larvae. Large numbers of tissue larvae place the horse at risk for developing larval cyathostominosis. This disease complex is caused by mass emergence of these larvae and is characterized by a generalized acute typhlocolitis and manifests itself as a profuse protein-losing watery diarrhea with a reported case-fatality rate of about 50%. Two anthelmintic formulations have a label claim for larvicidal therapy of these encysted stages; moxidectin and a five-day regimen of fenbendazole. There is limited knowledge about inflammatory and immunologic reactions to larvicidal therapy. This study was designed to evaluate blood acute phase reactants as well as gene expression of pro-inflammatory cytokines, both locally in the large intestinal walls and systemically. Further, mucosal tissue samples were evaluated histopathologically as well as analyzed for gene expression of pro- and anti-inflammatory cytokines, cluster of differentiation (CD) cell surface proteins, and select transcription factors. Eighteen juvenile horses with naturally acquired cyathostomin infections were randomly assigned to three treatment groups; one group served as untreated controls (Group 1), one received a five-day regimen of fenbendazole (10mg/kg) (Group 2), and one group received moxidectin (0.4mg/kg) (Group 3). Horses were treated on day 0 and euthanatized on days 18–20. Serum and whole blood samples were collected on days 0, 5, and 18. All horses underwent necropsy with collection of tissue samples from the ventral colon and cecum. Acute phase reactants measured included serum amyloid A, iron and fibrinogen, and the cytokines evaluated included interferon γ, tumor necrosis factor α, transforming growth factor (TGF)-β, and interleukins 1β, 4, 5, 6, and 10. Transcription factors evaluated were FoxP3, GATA3 and tBet, and CD markers included CD163, CD3z, CD4, CD40, and CD8b. Histopathology revealed an inflammatory reaction with higher levels of lymphocytes, T cells, B cells, eosinophils and fibrous tissue in the moxidectin-treated group compared to controls or horses treated with fenbendazole. No apparent systemic reactions were observed. Expression of IL-5 and TGF-β in intestinal tissues was significantly lower in Group 3 compared to Group 1. This study revealed a subtle inflammatory reaction to moxidectin, which is unlikely to cause clinical issues.

Self-assessment questions: paediatric cardiology

A 2-month-old baby with known hypoplastic left heart syndrome presents to the paediatric emergency department from home with a history of poor oral feeds and lethargy. The parents describe the baby having had profuse watery diarrhoea and non-bilious vomiting over the last 24 hours. Urine output has been reduced to about half the usual amount according to the family. The patient is on 12 hourly furosemide and spironolactone (each at 1 mg/kg/dose), 8 hourly captopril (0.3 mg/kg/dose) and aspirin (5 mg/kg/daily). On examination, the baby is clubbed and cyanosed with a sternotomy scar and a loud continuous murmur at the right upper sternal border radiating to the back. The anterior fontanel is slightly sunken. The abdomen is soft and non-tender with active but normal pitched bowel sounds.

Origin, evolution, and virulence of porcine deltacoronaviruses in the United States.

ABSTRACTA novel porcine deltacoronavirus (PdCV) was first discovered in Ohio and Indiana in February 2014, rapidly spread to other states in the United States and Canada, and caused significant economic loss in the swine industry. The origin and virulence of this novel porcine coronavirus are not known. Here, we characterized U.S. PdCV isolates and determined their virulence in gnotobiotic and conventional piglets. Genome analyses revealed that U.S. PdCV isolates possess unique genetic characteristics and share a close relationship with Hong Kong and South Korean PdCV strains and coronaviruses (CoVs) of Asian leopard cats and Chinese ferret-badgers. The PdCV-positive intestinal content (Ohio CVM1) and the cell culture-adapted PdCV Michigan (MI) strain were orally inoculated into gnotobiotic and/or conventional piglets. Within 1 to 3 days postinfection, profuse watery diarrhea, vomiting, and dehydration were observed. Clinical signs were associated with epithelial necrosis in the gastric pits and small intestine, the latter resulting in severe villous atrophy. Mild interstitial pneumonia was identified in the lungs of PdCV-infected piglets. High levels of viral RNA (8 to 11 log RNA copies/g) were detected in intestinal tissues/luminal contents and feces of infected piglets, whereas moderate RNA levels (2 to 5 log RNA copies/g) were detected in blood, lung, liver, and kidney, indicating multisystemic dissemination of the virus. Polyclonal immune serum against PdCV but not immune serum against porcine epidemic diarrhea virus (PEDV) reacted with PdCV-infected small-intestinal epithelial cells, indicating that PdCV is antigenically distinct from PEDV. Collectively, we demonstrate for the first time that PdCV caused severe gastrointestinal diseases in swine.

A case of Protracted Diarrhea in a Newborn: a Diagnostic Challenge.

Congenital diarrhea comprises a broad range of pathologies and often requires a thorough workup and immediate treatment. Although rare, microvillous inclusion disease (MVID) should be included in differential diagnosis of this presentation in the neonate. We report the case of a 36-week newborn who developed signs of severe dehydration and lethargy, requiring fluid resuscitation and total parenteral nutrition. MVID was diagnosed by recognition of profuse secretory diarrhea after an exhaustive etiological investigation, confirmed by DNA analysis.

Immunizing adult female mice with a TcpA-A2-CTB chimera provides a high level of protection for their pups in the infant mouse model of cholera.

Vibrio cholerae expresses two primary virulence factors, cholera toxin (CT) and the toxin-coregulated pilus (TCP). CT causes profuse watery diarrhea, and TCP (composed of repeating copies of the major pilin TcpA) is required for intestinal colonization by V. cholerae. Antibodies to CT or TcpA can protect against cholera in animal models. We developed a TcpA holotoxin-like chimera (TcpA-A2-CTB) to elicit both anti-TcpA and anti-CTB antibodies and evaluated its immunogenicity and protective efficacy in the infant mouse model of cholera. Adult female CD-1 mice were immunized intraperitoneally three times with the TcpA-A2-CTB chimera and compared with similar groups immunized with a TcpA+CTB mixture, TcpA alone, TcpA with Salmonella typhimurium flagellin subunit FliC as adjuvant, or CTB alone. Blood and fecal samples were analyzed for antigen-specific IgG or IgA, respectively, using quantitative ELISA. Immunized females were mated; their reared offspring were challenged orogastrically with 10 or 20 LD50 of V. cholerae El Tor N16961; and vaccine efficacy was assessed by survival of the challenged pups at 48 hrs. All pups from dams immunized with the TcpA-A2-CTB chimera or the TcpA+CTB mixture survived at both challenge doses. In contrast, no pups from dams immunized with TcpA+FliC or CTB alone survived at the 20 LD50 challenge dose, although the anti-TcpA or anti-CTB antibody level elicited by these immunizations was comparable to the corresponding antibody level achieved by immunization with TcpA-A2-CTB or TcpA+CTB. Taken together, these findings comprise strong preliminary evidence for synergistic action between anti-TcpA and anti-CTB antibodies in protecting mice against cholera. Weight loss analysis showed that only immunization of dams with TcpA-A2-CTB chimera or TcpA+CTB mixture protected their pups against excess weight loss from severe diarrhea. These data support the concept of including both TcpA and CTB as immunogens in development of an effective multivalent subunit vaccine against V. cholerae.