The COVID-19 pandemic may cause psychological distress, changes in numbers and distributions of patients in spine surgery patients, which all affect the strategies of spine surgery treatment. These changes may be related to the number of new COVID-19 cases per day since they are visual indicators of the changes in the epidemic and are of interest to the public. This descriptive research took the spine surgery department as an example in a Grade-A tertiary hospital in Anhui province, China. The number and distribution of patients from January 24 to April 2, 2020 was collected and compared with the past 5 years. A psychological scale was constructed to assess the psychological distress of patients and the number of new COVID-19 cases per day in Anhui, China was collected each day from January 24 to April 2, 2020. Also, this research compared these variables with the emergency response or the number of new COVID-19 cases per day. All distributions dropped dramatically during first-level emergency response and then back to normal. The psychological distress of patients was relatively higher at the beginning of the outbreak and then gradually returned to normal. The trends between the psychological distress of patients and the number of new COVID-19 cases per day were similar. The number of new COVID-19 cases per day could be used to predict psychological distress, changes in patient numbers and distributions, which was beneficial for the department of spine surgery to adjust its treatment strategy during the epidemic.

The 75-year-old male patient had been diagnosed with CML 25 years ago. Over 3 years after starting bosutinib, he was diagnosed with a HGBCL. A total of six courses of DA-EPOCH-R therapy brought complete remission of the lymphoma. Eight months after stopping bosutinib, BCR-ABL1 transcript copies remained undetectable by RT-PCR.

Background. Coronavirus disease 2019 (COVID-19) is expected to continue to cause worldwide fatalities until the World population develops ‘herd immunity’, or until a vaccine is developed and used as a prevention. However, the vaccine may prove ineffective due to rapid changes in viral antigenic determinants. Bacillus Calmette–Guérin (BCG) vaccine has been recognized for its beneficial effects on the immune system, and it is currently in being tested in clinical trials for COVID-19. However, BCG shortages may affect clinical decisions regarding the prioritization of BCG to protect from viral infections, hence, small-molecule BCG-mimics will be valuable alternatives. Methods. We developed and applied a systems biology workflow capable of identifying antiviral drugs and vaccines that can boast immunity and impact viral disease pathways to prevent the fatal consequences of COVID-19. Results. Our results indicate that BCG and small-molecule BCG-mimics affect the production and maturation of naïve T cells, which results in enhanced long-lasting innate immune responses to tackle novel viruses. Our workflow identified several antiviral drugs including raltegravir and lopinavir as high confidence BCG mimics. Top hits including emetine and lopinavir were validated to inhibit the growth of novel coronavirus SARS-CoV-2 in vitro. Conclusions. Herein, we provide systems biology support for using BCG as a protection measure from the lethal consequences of emergent viruses including SARS-CoV-2. We also provide systems biology evidence that certain small molecule drugs could mimic the effects of BCG and serve as alternatives to BCG.

Since the beginning of the 21st century, three coronaviruses have crossed the species barrier and caused serious human disease: severe acute respiratory syndrome coronavirus (SARS-CoV) in November 2002 [1, 2], Middle-East respiratory syndrome coronavirus (MERS-CoV) in 2012 [3, 4], and SARS-CoV-2 in 2019 [5, 6]. SARS-CoV-2 [7], initially called 2019-nCoV, is the etiological agent of COVID-19, a highly contagious infectious illness that was first reported in December 2019 in Wuhan, China and subsequently spread globally [8]. As of May 24, 2020, COVID-19 has caused >5,370,000 infections and >343,000 deaths worldwide [9].Unfortunately, nearly 20 years after the SARS outbreak, and despite many attempts for vaccines and therapeutic agents directed against SARS and MERS, no approved prophylactics or therapeutics exist. As a result, the management of COVID-19 largely relies on supportive care [10, 11] and on hopes surrounding compounds that appeared promising against previous coronaviruses [12, 13]. This lost opportunity, in itself, offers a valuable lesson for current and future outbreaks, and the need for new experimental rationales to accelerate discovery.The cellular entry of coronaviruses is fairly conserved across members of the Coronaviridae family and is mediated by the transmembrane spike (S) glycoprotein [14], a homotrimer [15, 16] that is often heavily glycosylated [17] and protrudes from the viral surface. Each of the three monomers of the spike glycoprotein consists of two functional subunits, S1, involved in membrane attachment, and S2, required for membrane fusion [15, 18]. In many coronaviruses, the spike glycoprotein is cleaved at the S1/S2 interface by host cell proteases [19]. Within the S1 domain, the receptor binding domain (RBD) attaches to the cellular receptor, which in the case of both SARS-CoV and SARS-CoV-2 is the angiotensin-converting enzyme 2 (ACE2) [19-21]. Another cleavage site, S2’, is located within S2 [17, 19]. The spike glycoproteins of SARS-CoV and SARS-CoV-2 share 76% identity at the amino acid level [22, 23], although biophysical assays indicate that SARS-CoV-2 binds their common receptor, ACE2, with a 10-20 fold higher affinity than SARS–CoV [14].As we contemplate the dynamics of COVID-19 and the development of prophylactic and therapeutic interventions, one of the key considerations is the emergence and potential relevance of viral mutations. In the short time since the pandemic started, several missense mutations have been observed in various SARS-CoV-2 isolates [24]. One of these, the 23403A>G variant, substitutes the aspartic acid at position 614 of the viral spike glycoprotein with glycine (D614G), and is frequently documented in European countries but rarely observed in China [25].In the current issue of the IJCP , Becerra-Flores and Cardozo interrogate the impact of this mutation on pathogenicity and offer a structural correlate for their findings [26]. Their analysis includes confirmed COVID-19 cases and deaths as reported by the European CDC during the first week of April 2020 and examines the viral spike genomic sequences deposited in the GISAID database over that period, correlating the prevalence of the D614G mutation with fatality rates in the same regions. The authors then use cryo-electron microscopy data andin silico mutagenesis of this key residue to predict conformational preferences of the two variants of the spike protein.The analysis indicates that viruses isolated from European patients predominantly expressed a glycine at position 614 of the spike glycoprotein, while a high percentage of the isolates collected from Far East patients favored aspartic acid at the same position. The proportion of viral isolates having a glycine at this position significantly correlated with higher average and median case fatality rates across geographic areas. Interestingly, their data also imply a rationale for divergence in the behavior of the disease between the East and West coasts of the United States, based upon the provenance of the viral ‘founders’ in these regions, from the European and Asian variants, respectively.Surprisingly, the authors’ molecular modeling indicates that the presence of a glycine at position 614 diminishes binding to the cellular receptor when replacing the aspartic acid at that residue, mainly by reducing the spike protein’s occupancy of the “up” or liganded state, when it is most amenable to receptor interaction. While seemingly counterintuitive, this finding opens at least two fascinating scenarios. As the authors hypothesize, a spike glycoprotein that harbors glycine at this position might be better protected from immune recognition, elicit the production of harmful antibodies, flood the host with ineffective antibodies, or some combination of all three. A delay in immune recognition may impact viral transmission by delaying symptomatic presentation or allowing unfettered infection without effective immune response. An aberrant response, suited to the viral conformation at large but not the infective conformation, could equally allow for an increased—but poorly targeted—inflammatory cascade. The possibility of a harmful immune response is particularly thought provoking, as antibody-dependent enhancement, the phenomenon by which antibodies facilitate viral entry into host cells that do not necessarily have viral receptors [27, 28], has been reported for many viruses, including coronaviruses [27, 29], dengue virus [30, 31], feline infectious peritonitis virus [32] , Ebola virus [33], and HIV [34]. Another possibility, not mutually exclusive, is that the D614G mutation creates or exposes a novel cleavage site in the spike glycoprotein.Delving into these molecular mechanisms with confirmatory in vitro studies will hopefully reap the benefits of decades of scientific strides while simultaneously highlighting deficiencies in key areas that can guide our approach to the current pandemic. One of the immediate questions involves the impact of this and other mutations on vaccine efficiency and the potential need to develop multiple candidate vaccines that cover a range of epitopes and their variants. In all likelihood, there is a lengthy and tortuous road ahead, but characterizing significant variants will allow us to better understand many elusive aspects of this virus’ success – the latent/incubation period, immune evasion and hyper-response, variable receptor binding, replication dynamics, and organ-specific pathogenesis—and discover host vulnerabilities that mutations such as D614G seem to exploit.The D614G mutation appears to become more common as the pandemic unfolds [35]. That this phenomenon is simply the result of a founder effect is possible but unlikely, and rather may be explained by this variant’s selective advantage allowing more efficient spread. Whether this advantage is conferred by infectivity, immune evasion, or pathogenicity—or some combination of these—is yet to be understood. Interestingly, this mutation is now known to travel simultaneously with other mutations, including one that affects the RNA-dependent RNA polymerase, with implications for proofreading, replication efficiency (and thus viral titer), and the emergence of drug-resistant viral phenotypes [36].Addressing these molecular questions relies heavily on widespread efforts to assemble accurate and comprehensive data on population infection rates and mortality, and frequent sampling of the genotypes of circulating isolates on a global basis. So far, this feat has been challenging and continued deficiencies will translate into missed singular opportunities to link molecular findings with population-level consequences, ultimately leaving us less prepared to address both this and future pandemics.The valuable and timely experimental strategy used by Becerra-Flores and Cardozo serves as an important analytic model that should be employed routinely to understand the ‘molecular strategy’ of this virus in the context of the evolving pandemic. This approach will also prove to be an indispensable instrument if also employed routinely at the onset of future outbreaks, which are all but guaranteed in the coming years, given the only recently appreciated ease of global spread of viruses in the modern world. In summary, this set of tools allows us to perform active surveillance, monitor the emergence of deleterious mutations prior to their widespread distribution, and use informed in silico and structural data to make informed decisions guiding molecular research and epidemic preparedness.

Objective: To deepen the understanding of clinical characteristics of pediatric patients with COVID-19. Methods: Retrospective analysis was executed among 21 children and their 38 families with laboratory-conformed novel coronavirus disease in five designated hospitals. Results: In total of 21 children (10 males and 11 females) aged from 1 to 17 years, 90.5% were from 18 family clusters and admitted to designated hospitals 2 days after illness onset, shorter than the adults. Besides 5 asymptomatic cases, pediatric patients mainly performed as fever (66.7%), cough (19.0%) and expectoration (14.3%). Among the 38 adult patients, the major symptoms included fever (63.2%), cough (63.2%), expectoration (44.7%), fatigue (6.8%), chill (15.8%) and dizziness (15.8%). Most cases had normal (76.2%, 68.4%) or decreased (19.0%, 26.3%) leucocytes, nearly half of children showed decreased neutrophils. 15 children and 32 adults had pulmonary involvement, consisted of ground-glass opacity (57.1%, 60.5%), spots (14.3%, 23.7%), stripes (14.3%, 7.9%) and patchy shadow (9.5%, 36.8%). All adults received antiviral therapy: lopinavir/ritonavir (92.1%), interferon (76.3%), arbidol (71.1%), chloroquine (18.4%) and ribavirin (10.5%). 16 children used interferon; 12 took lopinavir/ritonavir; 7 were given arbidol; two received ribavirin. All patients had been recovered and discharged with duration of admission 4-47 days (median 17 days). Conclusions: Pediatric patients with COVID-19 presented as milder symptoms and limited lung lesions than adults. Laboratory abnormalities were atypical in mild patients, neutropenia may be a potential characteristic of children. Efficiency of antiviral therapy need to be further investigated.

Functional and structural changes in atrial muscle constitute a substrate for atrial fibrillation. The pathological changes in the left atrium decrease conduction velocity and result in prolongation of the P wave duration. The aim of the study was to assess the duration of the P wave in patients with paroxysmal and persistent atrial fibrillation. The study group consisted of 119 patients diagnosed with atrial fibrillation, 57 women and 62 men, aged 65.3+/-9.4 years. There were 65 patients with paroxysmal AF and 54 with persistent AF. In this group the electrical cardioversion was performed. The P wave duration, was measured using electrophysiological system in all leads at paper speed of 200 mm/s. The studied patients did not differ in term of age, gender and comorbidities. The patients with persistent AF had longer P wave duration (159.9+/-22.3 vs 144.6+/-17.2 ms, p<0.001), higher glucose concentration (119.4+/-33.4 vs 108.0+/-24.6 mg/dL, p=0.015). Those results were not influenced by the anti-arrhythmic treatment. The persistent atrial fibrillation shows prolongation of the P wave duration over the paroxysmal form of the arrhythmia, independently to age, gender and anti-arrhythmic medication. The prolongation of the P wave related to persistent arrhythmia should force the physicians to earlier restoration of the sinus rhythm in order to its more successful long term maintenance. Key words: P wave duration, atrial fibrillation, diabetes mellitus, chronic kidney disease

Incisional atrial tachycardia (AT) with multiple penetrating points on one surgical incision has not been reported. We present a case of incisional AT following mitral annuloplasty with a superior transseptal approach, in which two reconduction sites were part of the reentrant circuit. Radiofrequency ablation at the reconduction site successfully terminated the tachycardia. A total of four penetrating points were found on the incision line, and radiofrequency ablation at these sites was completed. Detailed mapping with consideration of possible reconduction sites along the incision line should be performed to avoid further instances of AT following open heart surgery.

An adolescent female with ventilator-dependent spinal muscular atrophy type 1 (SMA-1) and megalencephaly-capillary malformation-polymicrogyria (MCAP) syndrome had been struggling with recurrent small to large volume hemoptysis for years secondary to complex arteriovenous malformations (AVMs) in her lungs. Despite numerous embolizations, she continued to experience hemoptysis from new AVMs. She was then started on sirolimus (rapamycin) and remains hemoptysis-free for over 12 months. To our knowledge, there are no known cases of SMA-1 with MCAP syndrome and related complex vascular malformations successfully treated with sirolimus.

The COVID-19 pandemic has necessitated rapid implementation of innovative strategies to manage patients remotely, in order to reduce the risk of community and nosocomial transmission. This case demonstrates the use of an Apple Watch to monitor for arrhythmias and QT prolongation in a patient with COVID-19 infection during home isolation.

Introduction: Sudden Cardiac Death (SCD) risk assessment is limited, particularly in patients with non-ischemic cardiomyopathies. This is the first application, in patients with non-ischemic cardiomyopathies, of two novel risk markers, Regional Restitution Instability Index (R2I2) and Peak Electrocardiogram Restitution Slope (PERS), which have been shown to be predictive of ventricular arrhythmias (VA) or death in ischemic cardiomyopathy patients. Methods and Results: Blinded retrospective study of 50 patients: 33 dilated cardiomyopathy and 17 other; undergoing electrophysiological study (EPS) for SCD risk stratification, and 29 controls with structurally normal hearts undergoing EPS. R2I2 was calculated from an EPS using ECG surrogates for action potential duration and diastolic interval. Cut-offs for high and low R2I2/PERS were predefined. R2I2 was significantly higher in study than control patients (0.99±0.05 vs. 0.63±0.04, <0.001). PERS showed a trend to higher values in the study group (1.18[0.63] vs. 1.09[0.54], p=0.07). During median follow up of 5.6 years [IQR 1.9 years] 9 study patients reached the endpoint of ventricular arrhythmia(VA)/death. Patients who experienced VA/death showed trends to higher mean R2I2 (1.14±0.07vs.0.95±0.05, p=0.12) and PERS (1.46[0.49] vs. 1.13[0.62], p=0.22). A Cox proportional hazards model using grouped markers: R2I2<1.03+PERS<1.21 / either R2I2≥1.03 or PERS≥1.21 / R2I2≥1.03+PERS≥1.21; significantly predicted VA/death (p=0.02) with a hazard ratio per positive component of 3.2 (95% confidence interval 1.2 to 8.8). Conclusion: R2I2≥1.03+PERS≥1.21 predict VA/death in patients with non-ischemic cardiomyopathies. R2I2≥1.03+PERS≥1.21 have the potential to play an important role in SCD risk stratification in non-ischemic cardiomyopathies but their validity should be confirmed in a larger study.

Background: Currently, no effective treatment method is available for neutrophilic asthma. Th17 play an important role in the promotion of asthma inflammation. And IDO-dependent tryptophan metabolism has been shown to act as a molecular “switch” for the conversion of Th17 cells into Tregs under certain conditions. Objective: Therefore this study aimed to regulate IDO expression in vivo and in vitro in a neutrophilic asthma animal model and investigate whether IDO could reduce Th17 cells and the secretion of related factors to ameliorate airway hyperreactivity and inflammation in neutrophilic asthma. Methods: A neutrophilic asthma model was established using ovalbumin（OVA）and lipopolysaccharide. IDO expression in the model mice was regulated using an IDO inducer and an IDO inhibitor. Th17 cells and the secretion of related factors were examined, and changes in airway hyperreactivity and inflammation were observed. Plasmacytoid dendritic cells and naïve CD4+ T cells were cocultured in vitro. After OVA stimulation and IDO inhibitor treatment, changes in Th17 cells and the secretion of related factors were examined. Results: Airway hyperreactivity and inflammation were ameliorated in the neutrophilic asthma model mice in the IDO induction group. IDO reduced Th17 cells and inflammatory cytokine secretion (IL-17, IL-6, and TGF-β1). Conclusion: IDO ameliorated airway hyperreactivity and inflammation in neutrophilic asthma. The mechanisms may be associated with the influence of the differentiation direction of CD4+ T (Th0) cells and inhibition of Th17 cell production. These results will provide new bases for potential therapeutic targets for the prevention and treatment of neutrophilic asthma using IDO.

The article  "Studying Physics, getting to know Python: RC circuit, simple experiments and coding with Raspberry Pi" introduces a hands-on, integrative studies approach to teaching electronics, physics, and computer science.  I believe it provides all of the steps (and code) needed to reproduce the basic exercises in  the classroom and there is room to add on new ideas.  The course is designed to use Raspberry Pis; because of the affordable nature of the equipment (less than a textbook). I could see proposing to use this setup as an online lab where students purchase the equipment and run the lab while they are quarantined at home.  Unfortunately, as written the article is over 8,0000 words when counting figures which is significantly over the 3000 word limit given in the  CISE guidelines for department papers: Up to 3000 words in length, including the abstract, references, bios, figures (see below), and all other text in the article.  When counting words, note that tables and figures should be counted as 250 words each. The article is over 8,000 words when counting the figures and I would be concerned that cutting it to 3000 words would  take away from one of the article's strengths.  A compromise would be to provide the examples in an online git repository and reference the repository in the article. 

Background and purpose KCNQ-encoded KV7 channels are expressed within vascular smooth muscle cells (VSMCs) and are key regulators of vascular reactivity, regulating resting tone and as functional targets of endogenous responses. Endothelial cells (ECs) form a paracrine signaling platform that line all blood vessels and regulate tone, but little is known of KV7 channels in vascular ECs. This study aims to characterize the expression and function of KV7 channels within rat mesenteric artery ECs. Experimental approach In rat mesenteric artery, KCNQ transcript and KV7 channel protein expression were determined via RT-qPCR, immunocytochemistry, immunohistochemistry and immunoelectron microscopy. Wire myography was used to determine vascular reactivity. Key results KCNQ transcript was identified in EC marker expressing cells using a reductive approach. KV7.4 and KV7.5 protein expression was determined in both isolated EC and VSMC and in whole vessels. Removal of ECs attenuated vasorelaxation to two structurally different KV7.2-5 activators S-1 and ML213. KIR2 blockers ML133 and BaCl also attenuated S-1 or ML213-mediated vasorelaxation in an endothelium-dependent process. KV7 inhibition attenuated receptor-dependent nitric oxide (NO)-mediated vasorelaxation to carbachol, but had no impact on relaxation to the NO donor, SNP. Conclusions and implications In rat mesenteric artery ECs, KV7.4 and KV7.5 channels are expressed, functionally interact with endothelial KIR2.x channels and contribute to endogenous eNOS-mediated relaxation. This study identifies KV7 channels as novel functional channels within rat mesenteric ECs and suggests that these channels are involved in NO release from the endothelium.

Background and Purpose: Cancer resistance to chemotherapy is a clinical dilemma that eventually leads to increased mortality. It is widely accepted that cancer stem cells (CSCs) have a pivotal role in the development of resistance. Nonsteroidal anti-inflammatory drugs (NSAIDs) have shown a promise to combat CSCs, thus, we addressed for the first time the effect of indomethacin on cisplatin (CDDP)-resistant murine breast cancer along with the relevant mechanisms. Experimental Approach: The murine mammary adenocarcinoma, Ehrlich ascites carcinoma (EAC) cells, were made resistant by exposure to CDDP and the surviving cells were then analyzed by flow cytometry for the breast CSCs markers (CD44+CD24-). CDDP heavily enriched the CSCs population which was subsequently injected into mice. After induction of tumors, mice were treated with CDDP, or indomethacin, or co-treatment with both drugs, or left untreated. Upon termination of the treatment period, blood samples were collected to measure the percentage of CSCs markers (CD44, CD24, SCa-1) and the immune cells (CD4+, CD62L+, and CD117+). The tumors were excised and analyzed for the relative expression of drug resistance-mediating miRNAs (miR-7, miR-21, miR-22, and miR-145) in addition to histopathological examination. Key Results: Indomethacin drastically diminished the tumorigenicity of CDDP-resistant cells along with enhancing its sensitivity to CDDP which were correlated with its suppressing ability of CD44+CD24- cells and manipulating effect on miRNAs expression. Besides, indomethacin expanded the pool of immune cells that impart antitumor response. Conclusion and Implications: Indomethacin through targeting CSCs may confer better outcome than conventional chemotherapeutics in the treatment of resistant breast cancer.

Background and Purpose: Selective negative allosteric modulators (NAMs), targeting α5 subunit-containing GABAA receptors (GABAARs) as potential therapeutic targets for disorders associated with cognitive deficits, including Alzheimer’s disease (AD), continually fail clinical trials. We investigated whether this was due to the alteration of synaptic mechanisms associated with α5 GABAARs in AD. Experimental approach: Using medicinal chemistry and computational modelling, we developed aqueous soluble hybrids of 6,6-dimethyl-3-(2-hydroxyethyl)thio-1-(thiazol-2-yl)-6,7-dihydro-2-benzothiophen-4(5H)-one, that demonstrated selective binding and high negative allosteric modulation, specifically for the α5 GABAAR subtype in constructed HEK293 stable cell-lines. Using a knock-in mouse model of AD (APPNL-F/NL-F), which expresses a mutant form of human amyloid-β (Aβ), we performed immunofluorescence studies combined with electrophysiological whole-cell recordings to investigate the effects of our key molecule, α5-SOP002 in the hippocampal CA1 region. Key Results: In aged APPNL-F/NL-F mice, a selective preservation of α5 GABAARs was observed in: dis-inhibitory, calretinin- (CR), cholecystokinin- (CCK), somatostatin- (SST) expressing interneurons, and pyramidal cells. Synaptic inhibition recorded from CR interneurons in APPNL-F/NL-F mice, was abnormally excessive, but was “normalised” with bath-applied α5-SOP002 (1 μM). However, α5-SOP002, further impaired inhibition onto CCK and pyramidal cells that were already largely compromised by exhibiting a deficit of inhibition in the AD model. Conclusions and Implications: Using a multi-disciplinary approach, we show that exposure to α5 GABAAR NAMs may further compromise aberrant synapses in AD. We therefore suggest that the α5 GABAAR is not a suitable therapeutic target for the treatment of AD or other cognitive deficits due to the widespread neuronal-networks that use α5 GABAARs.

River network extraction is the basis of hydrological analysis and related issues. The accuracy of river extraction directly affects the accuracy of watershed related research. The key to extracting the river network by using hydrological analysis method is to determine the drainage area threshold. At present, there are existing methods for determining the drainage area threshold, which have problems such as inaccurate extraction with a single threshold and difficulty in obtaining data with multi-threshold. In view of this, based on DEM data of Jiuyuangou watershed in the Loess Plateau, combined hydrological analysis and digital terrain analysis methods, based on the principle of river network extraction from slope runoff, and taking into full consideration the hydrological characteristics of the terrain of the watershed, this paper proposes a threshold determination method based on multi-threshold constraints of local characteristics of the water system and compares the river network accuracy between the river network extracted by the threshold determined by this method and the single t value determination method and the river network extracted by the threshold determined by the river network density method. The results show that among the two river network quantitative indicators including average branch ratio and average length ratio, the corresponding values of the extracted river network by the threshold determined by the multi-threshold constraint method are 4.94 and 9.90, which are the least different from the real river network (4.36 and 9.60), and the other two methods are quite different. The research results show that the river network extracted by the threshold determined by the multi-threshold constraint method can more realistically express the characteristics of the water system, and requires less data, which provides a new idea for determining the optimal the drainage area threshold for the DEM water system.

Title pageFull Title of Manuscript: Neonatal goat’s milk protein allergy – a rare cause for food protein allergyAuthors’ full names: Yee Ian Yik (MBBS, MS, MRCS Ed, Ph.D.)1, Ann Kee How (MBBS, MRCP)2Authors’ Institutional Affiliations: 1Division of Paediatric & Neonatal Surgery, Department of Surgery, Faculty of Medicine, University of Malaya, 50603 Kuala Lumpur, Malaysia2Cardiology Department, Hospital Serdang, Jalan Puchong, 43000 Kajang, Selangor, Malaysia.Running title: Neonatal goat’s milk protein allergyCorresponding author: Prof. Dr. Yee Ian Yik (MBBS, MS, MRCSEd, Ph.D.)Postal address:Division of Paediatric & Neonatal Surgery, Department of Surgery, Faculty of Medicine, University of Malaya, 50603 Kuala Lumpur, MalaysiaFax: +603-79586360Phone: +603-79492441Email:yiyik2003@gmail.comWord count: 905 words; number of figures : 3

Objectives To clarify the clinical features of cured patients with coronavirus disease (COVID-19) and the relevance of IgM and IgG testing. Methods A total of 187 cured COVID-19 patients with antibody test were followed up every two weeks. Assessment for general condition, symptoms, epidemiological contact history, polymerase chain reaction (PCR) assay, and antibody tests were performed and recorded. Information from Guangzhou CDC was also screened. Results The mean follow-up time was 45.7 days. There were 33 (17.6%) patients with negative results for IgG and 35 (18.7%) patients with positive results for IgM. PCR assay was positive in 10 (5.3%) patients during the follow-up. Neither IgG nor IgM results showed a relationship with PCR test results (all P > 0.05). Neither re-infection nor person-to-person transmission was found in the cured patients. Factors associated with appearance of antibody comprised hospitalization days (OR: 1.07, 95%CI: 1.02-1.13, P = 0.004) and antibiotics treatment (OR: 2.78, 95%CI: 1.10-7.01, P = 0.031) . Conclusions In our study, neither re-infection nor person-to-person transmission was found in cured patients with COVID-19. Additionally, neither IgG nor IgM can be used to replace the PCR test in cured patients.

Introduction: The diagnosis of acute viral bronchiolitis (AVB) is primarily based on the findings in pulmonary auscultation. There is no consensus on which auscultatory finding is the most frequent in AVB. This study aims to describe the pulmonary auscultation in a series of patients with AVB and verify its association with age, sex, viral agent, and duration of oxygen therapy. Method: Pulmonary auscultation was recorded in patients hospitalized for AVB between October 2018 and October 2019 using an electronic stethoscope and then parallelly analyzed by two examiners. The effect of other factors such as sex, age, duration of oxygen therapy and etiological agent was analyzed for any possible associations. Results: Of 114 patients, 67 (58.8%) produced wheeze, 43 (37.7%) produced crackles, and 4 (3.5%) had normal auscultation. Wheezing was predominant in male patients while crackling in female patients (67.1% and 52.3%, respectively; p = 0.039). Age had no significant influence on the auscultation pattern (p = 0.054), etiological agent (p = 0.053) and the duration of oxygen therapy (p = 0.877). The median age was higher in patients with parainfluenza compared to those with RSV (6.5 and 4.4 months, respectively; p = 0.044). The duration of oxygen therapy was higher in patients with RSV compared to those with no identified virus (median 5.2 and 2.68 days, respectively; p = 0.018). Conclusions: Wheezing was recorded as the predominant auscultation finding among hospitalized patients with AVB. The type of virus associated with AVB had no influence on the changes in pulmonary auscultation.

Introduction: Tachycardia-induced cardiomyopathy (TCM) has been known for decades as a reversible form of non-ischemic cardiomyopathy. However, its mechanism and properties remain poorly understood. Methods: This retrospective study investigated endomyocardial biopsy samples from 18 patients with TCM and compared them with samples from 170 patients with dilated cardiomyopathy (DCM), and 496 patients with inflammatory cardiomyopathy (ICM). Results: 684 patients with recent-onset heart failure and reduced ejection fraction not caused by valvular or ischemic heart disease were analyzed. In the TCM group, 81% were male, mean age was 60±13 years, and 94% had heart failure symptoms ≥2 NYHA class. At baseline (BL), 78% had atrial fibrillation/flutter, and 11% inappropriate sinus tachycardia, heart rate was higher compared to DCM and ICM patients (122±25 versus 78±21; p<0.001). Mean ejection fraction at BL was lower compared to DCM and ICM (27±12% versus 39.0±14.6%; p=0.001), but improved significantly more during follow-up (FU) (20% versus 6%; p<0.001). At FU, heart rate and presence of sinus rhythm were similar in all groups. 69% of TCM patients underwent electrical cardioversion or ablation. Compared with DCM patients, TCM patients had a stronger myocardial expression of MHC class II and an equal amount of infiltration with T-cells/macrophages. Compared with ICM patients, the presence of T-cells/macrophages was significantly lower in TCM. The marker of apoptosis (caspase 3) was comparably elevated in TCM/ICM patients. Conclusion: TCM is characterized by immuno-histological changes comparable to DCM except for caspase 3 levels, which were similar to those in ICM.

Objectives: Squamous cell carcinoma(SCC) is the most common laryngeal neoplasm. Squamous cell carcinoma variants (vSCC), on the other hand, show different clinical and pathological features than conventional type. The purpose of this study is to analyze the clinical and pathological findings of vSCC of the larynx. Methods: This retrospective study evaluates 110 patients diagnosed with vSCC in our institution between 2006-2017. Treatment of primary and recurrent diseases was evaluated. Overall survival, disease-specific survival and follow-up times were calculated as months. Difference between preoperative and postoperative pathology reports of surgically treated patients were compared. Results: There were 1497 patients diagnosed with laryngeal malignancy and 110 (7,34%) of these patients were diagnosed with vSCC. The most common pathological subgroup was verrucous carcinoma. The best prognosis was found in verrucous carcinoma and the worst was in spindle cell carcinoma. Overall survival rates was 90% and 54.7%, respectively. A group of patients had a preoperative pathological diagnosis, not vSCC, but conventional SCC with the incidence of 38.5-100% according to the histological subtype. This was most common in acantholytic carcinoma, followed by adenosquamous, basaloid and spindle cell carcinoma, respectively. Conclusions: Spindle cell carcinoma and basaloid type squamous cell carcinoma have the worst prognosis and the highest metastatic potential. Patients diagnosed with these two variants should be followed up more cautiously. It should also be kept in mind that the diagnosis of vSCC can be missed in patients diagnosed only with a small tissue biopsy sample.

Objectives: To evaluate the upper airway changes before and after the use of Mandibular Advancement Device (OAm) of the patients with mild to moderate obstructive sleep apnoea hypopnea syndrome (OSAHS) using Cone Beam Computed Tomography (CBCT). Design: Prospective study recruiting patients from February 2015 to January 2017 Settings: Department of Stomatology at Yan’an Hospital Affiliated to Kunming Medical University, China. Participants: PSG confirmed Chinese OSAHS patients. Main outcomes measures: CBCT scans were done before and after the use of OAm to assess the change in the sagittal and coronal diameter, volumetric changes and the change in Minimal Cross-sectional Area (MCA) of different segments of upper airway. Results: A total of 30 patients were included with an average age of 49.53 ± 6.62 years. A significant increase in sagittal and coronal diameter of the lower margin of soft palate and the upper epiglottis was observed except the hard palate plane after OAm (P>0.05). MCA and volume of the posterior soft palate, lingual, epiglottis area and total airway were significantly increased with the use of OAm (P<0.001). Conclusion: OAm is a beneficial device in OSAHS patients as it increases the upper airway area and the volumetric changes thereby reducing the effects of OSAHS.

“TWEETABLE” ABSTRACT: Extramammary Paget’s treatment with imiquimod and photodynamic therapy in combination can be easily tolerated and used safely and effectively.

Objective: To assess the risk of vulvar cancer and precursors in a cohort of women with vulvar lichen planus (LP) and the clinical and therapeutic features of these patients. Design: retrospective case series review Setting: Lower genital tract Unit of a tertiary hospital in Porto, Portugal Participants: 127 women with the diagnosis of vulvar LP, followed in one institution during a period of eleven years - January 2008 until December 2018. Main outcome measures: Demographic and clinical data were evaluated, as well as treatment, follow-up and histology results. Results: A total of 127 women were diagnosed with vulvar LP. The mean follow-up time was 3.90.5 years (range 1-11 years). Ultra-potent topical corticosteroids were first line treatment in 91.8% (n=112), with 32 cases (25.2%) needing an alternative treatment. An overall of 30 biopsies were performed, in 19 women (15%). Vulvar HSIL was diagnosed in 3 (2.4%) women, 2 (1.6%) of which were later diagnosed with vulvar squamous cell carcinoma. No cases of differentiated vulvar intraepithelial neoplasia were observed. Conclusion: Pre-malignant/malignant transformation in women with vulvar LP under surveillance and compliant with treatment is low. A close follow-up appears to be crucial to prevent future malignancy. Biopsies should be performed whenever a suspicious lesion appears during the follow-up.