Traumatic ulcerative granuloma with stromal eosinophilia, an unusual clinical manifestation in the oral mucosa. Case report.

Introduction: Traumatic ulcerative granuloma with stromal eosinophilia is an uncommon condition of the oral mucosa with a chronic course, usually affecting the tongue. Case Report: Clinically it presents as a chronic ulcer, with raised and indurated borders, rarely presented as a tumor. Histologically it shows a diffuse mixed inflammatory infiltrate, rich in eosinophils. The etiology of this lesion is still unclear; however, chronic irritation from traumatic agents is considered a major initiating factor. In some cases, the presence of CD30+ mononuclear cells within the lesions suggest the possibility of a CD30+ lymphoproliferative disorder. This article presents a case of a traumatic ulcerative granuloma with stromal eosinophilia manifested in a 56-year-old female with a solitary ulcerated tumor inside the right cheek. Conclusion: It was diagnosed based on clinical data and histopathological features. In a brief literature review, the entity has been characterized, analyzing its etiology and nature.

Parotid salivary mucocele in a companion rabbit (Oryctolagus cuniculus): a report on the clinical and laboratory characteristics and surgical treatment ˗ case report

ABSTRACT The present report aimed to describe the main characteristics of the parotid salivary mucocele in an adult male rabbit, which presented with a painless fluctuating mass with fluid content. Owing to the need for repeated fluid drainage, surgical excision was the chosen mode of treatment. Preoperative evaluation included radiography and blood analysis. The patient underwent surgical excision of the affected gland. Inhalation anesthesia was maintained by means of isoflurane and the cardio-respiratory parameters were monitored throughout the surgery. A bipolar electrocautery was used to assist in the incision and polyglactin 910 and nylon were the suture materials used in the wound closure technique. Post-operative medications included analgesics, anti-inflammatory agents and antibiotics. Histopathology of the excised glandular tissue revealed a mixed inflammatory infiltrate, fibroblasts, hemorrhage and hyperemia. The observations in this case suggest that surgical excision of the affected gland is the treatment of choice for the management of mucocele in companion rabbits, which has already been identified for other animals. Periodic acid-reactive Schiff staining confirmed the diagnosis of salivary mucocele. The complementary investigations helped to rule out the differential diagnosis and indicated a favorable prognosis, in view of the fact that the case was successfully resolved without complications or recurrence.

A Rare Case of Angiolymphoid Hyperplasia without Eosinophils, with Review of the Literature

The epithelioid hemangioma, more commonly termed angiolymphoid hyperplasia with eosinophils, is a pathologic vascular proliferation characterized by a distinctive eosinophil-rich mixed inflammatory infiltrate. A nonspecific accompanying infiltrate has only rarely been reported, and may confound the diagnosis of this benign process with malignant mimics. We present such a case of angiolymphoid hyperplasia without eosinophils, and consider its diagnosis and pathogenesis within the spectrum of related entities.

Rosai-Dorfman Disease: A Less Common Cause of Leptomeningeal and Nerve Root Enhancement

A 46-year-old male experienced progressive neurocognitive decline, weight loss, intermittent headaches, and weakness over 6 months. Magnetic resonance imaging of the brain revealed hydrocephalus and the spinal cord imaging showed diffuse leptomeningeal enhancement with prominent nerve root involvement. Intradural biopsy of lumbar arachnoid tissue found mixed inflammatory infiltrate consisting predominantly of histiocytes, S100 and CD68 positivity, and lymphocytophagocytosis (emperipolesis) consistent with extranodal Rosai-Dorfman disease. Rosai-Dorfman disease, a non-Langerhans cell histocytic disorder, can mimic the appearance of neurosarcoidosis and leptomeningeal carcinomatosis and should remain on the differential of a patient presenting with diffuse leptomeningeal enhancement, a common occurrence on a neurohospitalist service.

Gastric Xanthomatous Hyperplastic Polyps – Just an Incidental Endoscopic Finding?

Background: Laparoscopic sleeve gastrectomy (LSG) progressively became the preferred procedure worldwide for the treatment of morbid obesity. Occasionally, unknown gastrointestinal diseases may be incidentally discovered during the procedure or on the histologic gastric specimen. Gastric xanthomas are uncommon lesions of the lamina propria, composed by foamy macrophages and mixed inflammatory infiltrate. Rarely, xanthoma cells develop within a gastric hyperplastic polyp. Although usually benign, they may be associated with pre-malignant conditions or even gastric cancer, making advisable an appropriate workup. Case Presentation: A hyperplastic polyp with xanthomatous proliferation was discovered in the gastric specimen of a young man, suffering from severe obesity and metabolic syndrome. The patient had been treated with proton pump inhibitors for gastric discomfort for years. After the surgical procedure, the gastric discomfort rapidly disappeared. Conclusion: Obesity is often complicated by gastrointestinal abnormalities discovered during ultrasound or endoscopic procedures. Incidental findings of unknown gastric lesions are common occurrences during sleeve gastrectomy. Although xanthelasmas per se are harmless, they might coexist with pre-malignant/ malignant lesions, especially when associated with gastric polyps. Thus, prompt intra-operative recognition and adequate work-up are mandatory. Although cases of gastric polyps or xanthomas are not a novelty, to our knowledge, this is the first case reporting about the discovery of a gastric hyperplastic polyp with xanthomatous proliferation on gastric histological piece. From the discussion of this case and of similar reports in the literature, we advocated for the importance of endoscopic screening in obese patients admitted for bariatric surgery to address the proper surgical approach and follow-up.

Three Cases of Pyogenic Granuloma of the Gastrointestinal Tract

Pyogenic granuloma also known as lobular capillary hemangioma occurs commonly in the skin and oral mucosa. This entity has been rarely reported in the gastrointestinal tract. We herein report three cases of pyogenic granuloma, located in the duodenum, ileum, and rectum, respectively. Case 1 is a 54-year-old female with a history of angioimmunoblastic T-cell lymphoma who underwent an esophagogastroduodenoscopy for severe heartburn. The endoscopy showed a 13-mm nonbleeding, pedunculated polyp in the second portion of duodenum, which was removed using a hot snare after injection of epinephrine. The patient had an episode of massive gastrointestinal bleeding postpolypectomy, with a significant drop of her hemoglobin, which was managed with blood transfusion. Case 2 is a 68-year-old male with a history of right hemicolectomy due to trauma who had a colonoscopy for chronic diarrhea. The colonoscopy revealed a 14-mm, nonbleeding, pedunculated polyp in the ileum, located 3 cm from the ileocolonic anastomosis. The polyp was removed with hot snare, without complications. Case 3 is a 44-year-old female with morbid obesity who underwent a colonoscopy for iron-deficiency anemia. The colonoscopy showed an 8-mm multilobulated sessile lesion in the distal rectum, which was completely removed using hot snare. No complications were seen postpolypectomy. Histological examination of all the three polyps showed a proliferation of capillary-sized blood vessels with a mixed inflammatory infiltrate, resembling granulation tissue. Additionally, the ileal polyp in our case had marked eosinophilic infiltrate, the etiology of which remains unknown. In conclusion, pyogenic granuloma, given its vascular nature, can be a cause of bleeding in the gastrointestinal tract. Awareness regarding this rare entity is important for its proper diagnosis and treatment.

25. Use of rituximab in refractory primary antiphospholipid syndrome with pulmonary and cerebral manifestations

Introduction We describe a 29-year-old gentleman with triple-antibody positive primary antiphospholipid syndrome (APS) who presented with recurrent cerebrovascular thrombotic events despite anticoagulation. He was escalated to rituximab. A pre-rituximab chest radiograph was abnormal resulting in a CT-chest which demonstrated bilateral widespread ground-glass opacities. Carbon monoxide transfer coefficient (KCO) was raised. Lung biopsy showed alveolar haemorrhage, alveolitis, capillaritis and a mixed inflammatory infiltrate consistent with APS. Alternative causes such as infection and malignancy were excluded. This case reflects a complex refractory APS with rare pulmonary manifestations. Management was multidisciplinary and included the use of rituximab to prevent further disease progression. Case description A previously well 29-year-old Asian gentleman presented in late 2015 with multiple right leg deep vein thromboses (DVTs). Rivaroxaban was commenced for six-months. A thrombophilia screen post-treatment demonstrated anti-cardiolipin IgG and IgM levels of > 420 kUnits/litre and 200 kUnits/litre respectively, anti-β2-glycoprotein-I IgG and IgM levels of 163 kUnits/litre and 50 kUnits/litre respectively, and a strongly positive lupus anticoagulant. A follow-up US-Doppler revealed chronic DVTs; apixaban was initiated. Secondary causes of APS were excluded clinically and serologically. Repeat APS antibodies remained strongly positive. In December 2016, he developed multiple APS-driven strokes affecting the occipital lobes, centrum semiovale and cerebellum. Other causes of stroke were excluded. Clopidogrel was commenced and apixaban was changed to warfarin with an INR target of 2.5-3.0. Despite consistently achieving this target he had an acute parietal lobe stroke in May 2017. Consequently, his INR target increased to 3.0-4.0. Hydroxychloroquine and high-dose atorvastatin were also added. In July 2018 he presented with recurrent transient ischaemic attacks. An MRI-head identified a previously unseen chronic temporal lobe infarct. Following a multidisciplinary discussion we changed warfarin to low molecular weight heparin and also planned to commence rituximab. Pre-biologic, his T-spot was positive and his chest radiograph was abnormal. He had no chest symptoms. A CT-chest demonstrated multiple bilateral ground-glass opacities. Pulmonary function tests (PFTs) revealed an elevated KCO (130% predicted). A lung biopsy revealed alveolar haemorrhage, alveolitis, capillaritis and a mixed inflammatory infiltrate consistent with APS. Infection (including tuberculosis), malignancy and granulomatous disease were all excluded. The patient was subsequently treated with high-dose corticosteroids and rituximab. His other treatment for APS remained unchanged. He was also treated for latent tuberculosis with isoniazid. Since this treatment regimen the patient has had no further thrombotic episodes. Moreover, repeat CT-chest and PFTs have both shown significant improvements. Discussion Primary APS is an autoimmune thrombophilic disorder characterised by recurrent arterial and venous thromboembolism, and obstetric morbidity. Deep vein thrombosis and stroke are the most common venous and arterial thrombotic manifestations respectively. Treatment includes the use of anticoagulation such as warfarin. Refractory APS is associated with recurrent thrombotic episodes despite anticoagulation therapy. Our patient developed recurrent cerebral thrombosis despite warfarin and clopidogrel. This continued to occur even after increasing the INR-target. Furthermore, prior to and during each thrombotic episode, our patient’s INR was always within the desired range. We also added secondary treatments for APS including atorvastatin and hydroxychloroquine and these also failed to prevent further cerebrovascular disease. We did not feel changing warfarin to low molecular weight heparin alone was sufficient to prevent further thromboses given the history of optimal INRs. We therefore opted to also add rituximab given its role in preventing further production of B-cell driven autoantibodies via CD20 binding. In addition, our patient had significant APS-driven pulmonary abnormalities which required addressing. Pulmonary embolism and pulmonary hypertension are the most common respiratory pathologies of APS. Rarely APS can also cause pulmonary artery thrombosis and fibrosing alveolitis. Moreover and particular to our patient, it can cause alveolar haemorrhage, alveolitis and pulmonary capillaritis. This occurs via neutrophilic infiltration of the alveolar septum and pulmonary capillary wall, and microthrombi which results in inflammation. Necrosis and loss of capillary integrity then causes disruption of the alveolar-capillary basement membrane resulting in haemorrhage. Remarkably despite the evident APS-driven lung disease in our patient, he was asymptomatic from a chest perspective. Our patient has responded positively to rituximab with improvement in PFTs and CT-chest appearance. Moreover he has had no further thrombotic events. We aim to repeat brain imaging and recheck APS antibody titres to observe the effect of rituximab. Key learning points Excluding pulmonary embolism and pulmonary hypertension, pulmonary disease is an under-recognised manifestation of APS. Rarer lung sequelae include pulmonary capillaritis, alveolitis and alveolar haemorrhage which our patient exhibited. These pathologies require a combination of investigations to diagnose including imaging, PFTs and histopathological biopsy. Most cases of APS respond to first-line treatment with anticoagulation such as warfarin provided INR targets are consistently achieved. Our patient continued to have recurrent thrombotic cerebrovascular events despite anticoagulation, antiplatelet therapy and other treatments. This case raises awareness of a complex refractory APS case which necessitated the introduction of biologic therapy in rituximab. Rituximab is already well-recognised in the treatment of catastrophic APS. We intend by this case to raise awareness of the effectiveness of rituximab in non-catastrophic APS, and its value in treating inflammatory APS-driven lung pathology. We await results for the effect of rituximab on APS-antibodies and whether this has any impact on prevention of disease progression. This case also highlights the importance of a multidisciplinary approach in managing complex cases. We worked alongside other specialities including neurology, stroke medicine, haematology and respiratory medicine to achieve optimal patient care. Conflicts of interest The authors have declared no conflicts of interest.

Hydrolytic degradation and in vivo resorption of poly-l-lactic acid-chitosan biomedical devices in the parietal bones of Wistar rats

Objectives This study sought to describe events related to the degradation/resorption of a device composed of polylactic acid (PLA) after implantation into Wistar rats. Methods Five-millimeter-diameter PLA rigid scaffolds and flexible analogs were elaborated, bioactivated through culture with osteoblasts, and implanted into the parietal bones of adult Wistar rats after 15 days. After 3 months, the samples were recovered and analyzed via optical microscopy (histochemical techniques) and scanning electron microscopy. This research was approved by the animal ethics review committee of Universidad of Valle in Cali, Colombia, according to the endorsement of the ethics committee CEAS 001-016. Results Initially, there was surface erosion and fragmentation of the device, inducing an inflammatory response compatible with the foreign body reaction, in addition to the presence of a pseudocapsule and a mixed inflammatory infiltrate that was responsible for phagocytosis of the material. Regeneration of the defect via the apposition of new bone occurred simultaneously with resorption of the material. Conclusions The results illustrated that the degradation/resorption of PLA occurs in a centripetal pattern.

Immunopathological findings in a cat with auricular chondritis

At clinical examination, a 5-year-old male domestic short-haired cat exhibited painful swelling and erythema of the pinnae of both ears. Microscopically, the lesions on both pinnae were composed of diffuse granulomatous chondritis with degeneration and necrosis of the pinnal cartilage. Numerous mast cells were also observed within and surrounding the inflammatory lesion. Immunohistochemistry showed a mixed inflammatory infiltrate characterised by the predominance of macrophages (CD68+, MAC 387+ and Lysozyme+), T lymphocytes (CD3+), some B lymphocytes (CD79α+) and neutrophils. Immunopathological characterisation of the lesion showed a granulomatous inflammation profile and suggests that the morphological changes and immunopathogenesis of auricular chondritis in cats presents a similarity with relapsing polychondritis in humans.

Rheumatoid arthritis presenting as rheumatoid meningitis

Rheumatoid meningitis (RM) is a rare extra-articular manifestation of rheumatoid arthritis (RA). A 59-year-old man presented with a 10-day history of right-sided frontal headache and a 7-day history of subacute left-sided weakness. He had no history of RA. He was febrile (38.2°C). Left ankle dorsiflexion and plantarflexion were graded at 4+/5. He developed focal onset motor seizures. He was intermittently febrile with minimal improvement despite intravenous antivirals and antimicrobials. Serology revealed elevated rheumatoid factor 88.2 IU/mL and anti-cyclic citrullinated peptide (anti-CCP) IgG >340 AU/mL. Initial cerebrospinal fluid (CSF) was predominantly lymphocytic 96%, with elevated protein 672 mg/L and normal glucose 3.4 mmol/L. Interval CSF revealed newly low glucose 2.6 mmol/L. Extensive CSF microbiology tests were negative. CSF cytology confirmed reactive lymphocytes. MRI brain revealed right frontoparietal leptomeningeal enhancement. Brain and leptomeningeal biopsy demonstrated florid leptomeningeal mixed inflammatory infiltrate without granulomas. The combination of elevated anti-CCP IgG, erosive arthropathy, CSF lymphocytosis, asymmetrical leptomeningeal enhancement and biopsy findings confirmed RM.