Tungo za Mzee Kimbunga: Haji Gora Haji

Haji Gora Haji (1933) is a Swahili poet from Tumbatu. Some people in Zanzibar call him `The Old Hurricane´ after the title and the first poem of his anthology Kimbunga (1994 Dar es Salaam: Taasisi ya Uchunguzi wa Kiswahili) that made him well-known all over Taniania. While making a living from the sea, as a fisherman, porter in the harbour, sailor and transporter of cloves, he has been composing, since 1955, a large amount of ngoma and taarab songs, riddles, tenzi and mashairi, short stories and, recently, a short novel. This paper discusses metaphors and images that are characteristic of Haji Gora`s work, the way in which they reveal his identity and how they have been put in terms of contradictions and oppositions

‘Hammatbihi wahammabiha’: fasihi ya Kiswahili na kisa cha Yusuf

The story of Joseph (in the Bible), Yusuf (in the Quran), has inspired literatures in many languages. This paper explores how some Swahili writers and translators have dealt with this inspiration, the implications for their language use and the way they have interpreted Yusuf as a theme for their writings. After a brief introduction on the importance of the story itself and putting the focus on a major theme of the plot, the following works are discussed: the new Quran translation by Sh Ali Muhsin (1995), a short novel by Mzee Salim A. Kibao (1975), two short stories by Amur bin Nasur il-Omeiri (1894), the utenzi Qissat-il Yusuf (l913) and Abdulrazak Gurnah\''s English written novel Paradise (1995). The paper concludes with the observation that in analyzing how these Swahili writers have integrated the story of Yusuf in their writings, prose as well as poetry, it becomes clear that attempts in defining what is ‘foreign’ (or ‘Oriental’) and what is ‘indigenous’ (or ‘African’) are bound to fail

Characterization of Recombinant Human PRG4 as an Ocular Surface Boundary Lubricant

Introduction: Dry-eye disease involves tear film instability that can result in surface-to-surface contact between the cornea and eyelid or contact lens, where boundary lubrication can be dominant1. Motivated by the recent discovery that proteoglycan 4 (PRG4, a mucin-like glycoprotein originally discovered in synovial fluid as a boundary lubricant2), functions as an ocular surface boundary lubricant3, advances in recombinant protein expression technology4, and PRG4’s potential use as a friction-reducing contact lens coating, the objectives of this study were to: 1) biochemically characterize recombinant human PRG4 (rh- PRG4); and 2) assess the boundary lubricating properties of rh-PRG4, both before and after autoclave sterilization, at a cornea-contact lens material (PDMS) biointerface. Methods: SDS-PAGE western blot analysis using a variety of anti-PRG4 antibodies and lectins was performed on native PRG4 (nPRG4) and rh-PRG4 samples, both nonreduced and reduced, with and without enzymatic removal of O-linked glycosylations. Human corneas and PDMS were articulated against each other, subject to physiological loads of 8-25 kPa, at effective sliding velocities of 0.3-30 mm/s. Test lubricant sequences were A) saline, rh-PRG4 @300μg/mL, nPRG4 @300μg/mL, and saline; and B) saline, autoclaved rh-PRG4 @300μg/mL, rh-PRG4 @300μg/mL, and saline. Static and kinetic coefficients of friction were calculated. Results: rh-PRG4 demonstrated similar immunoreactivity to nPRG4, and effectively lowered friction at the cornea-PDMS biointerface. Western blotting indicated immunoreactive rh-PRG4 bands had a similar apparent molecular weight (MW) to nPRG4, and decreased appropriately upon reduction as well as enzymatic removal of glycosylations. Kinetic friction coefficients, which were highest in saline (0.31±0.06 to 0.40±0.06, mean±SEM), were similar in rh-PRG4 (0.12±0.01 to 0.25±0.03) and nPRG4 (0.19±0.02 to 0.28±0.03) across all velocities. Autoclaved rh-PRG4 had similar values to rh-PRG4 as well (0.19±0.02 to 0.26±0.04, 0.16±0.02 to 0.26±0.02, respectively). Conclusions: rh-PRG4 demonstrates similar biochemical and ocular surface lubricating properties to nPRG4, and may function as an effective friction-reducing contact lens coating

Faecalibacterium prausnitzii Strain HTF-F and Its Extracellular Polymeric Matrix Attenuate Clinical Parameters in DSS-Induced Colitis

Date of Acceptance: 26/02/2015 Funding: The authors received no specific funding for this work.Peer reviewedPublisher PD

Local immune regulation of mucosal inflammation by tacrolimus

Purpose: Tacrolimus is a potent immunomodulator that is effective in the treatment of inflammatory bowel disease (IBD). However, potential toxicity and systemic effects with oral intake limit its use. Local tacrolimus treatment is effective in a subgrou

Faecalibacterium prausnitzii A2-165 has a high capacity to induce IL-10 in human and murine dendritic cells and modulates T cell responses

Acknowledgements This work was financially supported by the EC FP7 Cross-talk project (PITN-GA-2008-215553). The authors thank the Histology Platform from GABI research unit and especially Abdelhak Boukadiri for their technical support in the histology sample preparation and Marlène Héry, Charline Pontlevoy, Jerome Pottier and André Tiffoche (UE0907 IERP, Jouy en Josas) for their help during animal experiments. The authors thank Rafael Muñoz-Tamayo (INRA) for his help in performing the PCA.Peer reviewedPublisher PD

Developmental pathways to autism: a review of prospective studies of infants at risk

Autism Spectrum Disorders (ASDs) are neurodevelopmental disorders characterized by impairments in social interaction and communication, and the presence of restrictive and repetitive behaviors. Symptoms of ASD likely emerge from a complex interaction between pre-existing neurodevelopmental vulnerabilities and the child's environment, modified by compensatory skills and protective factors. Prospective studies of infants at high familial risk for ASD (who have an older sibling with a diagnosis) are beginning to characterize these developmental pathways to the emergence of clinical symptoms. Here, we review the range of behavioral and neurocognitive markers for later ASD that have been identified in high-risk infants in the first years of life. We discuss theoretical implications of emerging patterns, and identify key directions for future work, including potential resolutions to several methodological challenges for the field. Mapping how ASD unfolds from birth is critical to our understanding of the developmental mechanisms underlying this disorder. A more nuanced understanding of developmental pathways to ASD will help us not only to identify children who need early intervention, but also to improve the range of interventions available to them

Development and Function of Immune Cells in an Adolescent Patient with a Deficiency in the Interleukin-10 Receptor

OBJECTIVE:: Monogenic defects in the interleukin-10 (IL-10) pathway are extremely rare and cause infantile-onset inflammatory bowel disease (IBD)-like pathology. Understanding how immune responses are dysregulated in monogenic IBD-like diseases can provide valuable insight in “classical” IBD pathogenesis. Here, we studied long-term immune cell development and function in an adolescent IL-10 receptor (IL10RA)-deficient patient who presented in infancy with severe colitis and fistulizing perianal disease and is currently treated with immune suppressants. METHODS:: Biomaterial was collected from the IL10RA-deficient patient, pediatric IBD patients and healthy controls. The frequency and phenotype of immune cells were determined in peripheral blood and intestinal biopsies by flow cytometry and immunohistochemistry. Functional changes in monocyte-derived dendritic cells and T cells were assessed by in vitro activation assays. RESULTS:: The IL10RA-deficient immune system developed normally with respect to numbers and phenotype of circulating immune cells. Despite normal co-stimulatory molecule expression, bacterial lipopolysaccharide-stimulated monocyte-derived dendritic cells from the IL10RA-deficient patient released increased amounts of TNFα compared to healthy controls. Upon T-cell receptor ligation, IL10RA-deficient peripheral blood mononuclear cells released increased amounts of T cell cytokines IFNγ and IL-17 agreeing with high numbers of T-bet and IL-17 cells in intestinal biopsies taken at disease onset. In vitro, the immunosuppressive drug thalidomide used to treat the patient decreased peripheral blood mononuclear cell-derived TNFα production. CONCLUSIONS:: With time and during immunosuppressive treatment the IL10RA- deficient immune system develops relatively normally. Upon activation, IL-10 is crucial for controlling excessive inflammatory cytokine release by dendritic cells and preventing IFNγ and IL-17-mediated T-cell responses

Impaired Hyperglycemia-Induced Delay in Gastric Emptying in Patients With Type 1 Diabetes Deficient for Islet Amyloid Polypeptide

OBJECTIVE—Slowing of gastric emptying by hyperglycemia, a physiological response to minimize postprandial hyperglycemia, may be impaired in patients with type 1 diabetes. The causes and consequences on glucose homeostasis are unknown