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61. Differences in plant cover and species composition of semiarid grassland communities of Central Mexico and its effects on net ecosystem exchange.

Author

Delgado-Balbuena, J., Arredondo, J. T., Loescher, H. W., Huber-Sannwald, E., Chavez-Aguilar, G., Luna-Luna, M., and Barretero-Hernandez, R.

Subjects
GROUND cover plants, ARID regions, CHEMICAL composition of plants, GRASSLANDS, PLANT species, BIOTIC communities
Abstract

Changes in land use across the semiarid grasslands of Northern Mexico have driven a decline of plant cover and alteration of plant species composition. A number of different plant communities have resulted from these changes, however, their implications on the carbon cycle and regional carbon balance are still poorly understood. Here, we examined the effects of plant cover loss and changes in species composition on net ecosystem CO2 exchange (NEE) and their biotic and abiotic controls. Five typical plant community types were examined in the semiarid grassland by encasing the entire above-ground ecosystem using the geodesic dome method. Sites included an oat crop (crop), a moderately grazed grassland (moderate grazing), a 28 yr-old grazing exclosure (exclosure), an overgrazed site with low perennial grass cover (overgrazed), and an overgrazed site presenting shrub encroachment (shrub encroachment). For natural vegetation, rates of daytime NEE for sites with a high plant cover (exclosure and moderate grazing) were similar (P > 0.05) as compared to sites with low plant cover (overgrazed and shrub encroachment). However, night time NEE (carbon loss) was more than double (P < 0.05) for sites with high plant cover compared to sites with low cover, resulting into slight C sinks for the low plant cover sites and neutral or sources for the high plant cover sites on an annual basis. Differences in plant cover and its associated biomass defined the sensitivity to environmental controls. Thus, daytime NEE in low plant cover sites reached light compensation points at lower PPFD values than those from high plant cover sites. Differences in species composition did not influence NEE rates even though there were transient or permanent changes in C3 vs. C4 functional groups. [ABSTRACT FROM AUTHOR]

Published
2012
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65. POPULATION STRUCTURE OF ANISAKIS SIMPLEX (NEMATODA) IN HARBOR PORPOISES PHOCOENA OFF DENMARK.

Author

Herreras, M. V., Balbuena, J. A., Aznar, F. J., Kaarstad, S. E., Fernández, M., and Raga, J. A.

Subjects
ANISAKIS, ANISAKIDAE, NEMATODES, PORPOISES, CETACEA, PHOCOENA
Abstract

Describes the population structure and habitat selection of Anisakis simplex in harbor porpoises off Denmark. Categorization of the nematodes into stages; Analysis on the suggestion that recruitment and duration of each stage were the main factors accounting for infrapopulation structure; Implication of discrepancies for the reflection of differences in categorization criteria and statistical methods.

Published
2004
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66. Redescription of Odhneriella subtila (Skrjabin, 1959) (Digenea: Campulidae) from the intestine of Globicephala melaena (Traill, 1809) (Cetacea: Delphinidae) off the Faroe Islands (North-East Atlantic).

Author

Balbuena, J., Raga, J., and Abril, E.

Abstract

During parasitological investigations of long-finned pilot whales, Globicephala melaena (Traill, 1809), in the Faroe Islands, the trematode species Odhneriella subtila (Digenea: Campulidae), parasitising the small intestine, was detected. Skrjabin's (1959) original description of this species was based on a single individual. The collection and availability for study of several thousands of specimens permitted the redescription of this campulid and the noting of some new morphological characters. This trematode is reported for the first time from the long-finned pilot whale, and the Atlantic Ocean is a new locality record. [ABSTRACT FROM AUTHOR]

Published
1989
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67. PARASITISME DE LA TORTUE LUTH,DERMOCHELYS CORIACEA (LINNAEUS, 1766)DANS LES EAUX EUROPEENNESPAR PYELOSOMUM RENICAPITE (LEIDY, 1856)Parasitism ofa Leatherback turtle, Dermochelys coriacea (Linnaeus, 1766)in the European waters by Pyelosomum renicapite (Leidy, 1856)

Author

Almor, P, Raga, J, Abril, E, Balbuena, J, Duguy, R, Observatoire océanologique de Banyuls (OOB), and Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)

Subjects
[SDV]Life Sciences [q-bio], ComputingMilieux_MISCELLANEOUS
Abstract

International audience

Published
1989

73. SiD Letter of Intent

Author

Aihara, H., Burrows, P., Oreglia, M., Berger, E. L., Guarino, V., Repond, J., Weerts, H., Xia, L., Zhang, J., Zhang, Q., Srivastava, A., Butler, J. M., Goldstein, Joel, Velthuis, J., Radeka, V., Zhu, R. -Y, Lutz, P., Roeck, A., Elsener, K., Gaddi, A., Gerwig, H., Grefe, C., Klempt, W., Linssen, L., Schlatter, D., Speckmayer, P., Thom, J., Yang, J., Christian, D. C., Cihangir, S., Cooper, W. E., Demarteau, M., Fisk, H. E., Garren, L. A., Krempetz, K., Kutschke, R. K., Lipton, R., Para, A., Tschirhart, R., Wenzel, H., Yarema, R., Grunewald, M., Pankov, A., Dutta, T., Dauncey, P. D., Balbuena, J. P., Fleta, C., Lozano, M., Ullan, M., Christian, G. B., Faus-Golfe, A., Fuster, J., Lacasta, C., Marinnas, C., Vos, M., Duarte, J., Fernandez, M., Gonzalez, J., Jaramillo, R., Lopez, Virto A., Martinez-Eivero, C., Moya, D., Ruiz-Mimeno, A., Vila, I., Colledani, C., Dorokhov, A., Hu-Guo, C., Winter, M., Moortgat-Pick, G., Onoprienko, D. V., Kim, G. N., Park, H., Adloff, C., Blaha, J., Blaising, J. -J, Cap, S., Chefdeville, M., Drancourt, C., Espargiliare, A., Gaglione, R., Geffroy, N., Jacquemier, J., Karyotakis, Y., Prast, J., Vouters, G., Gronberg, J., Walston, S., Wright, D., Sawyer, L., Laloum, M., Ciobanu, C., Chauveau, J., Savoy-Navarro, A., Andricek, L., Moser, H. -G, Cowan, R. F., Fisher, P., Yamamoto, R. K., Kenney, C. J., Boos, E. E., Merkin, M., Chen, S., Chakraborty, D., Dyshkant, A., Hedin, D., Zutshi, V., Galkin, V., D Ascenzo, N., Ossetski, D., Saveliev, V., Kapusta, F., Masi, R., Vrba, V., Lu, C., Mcdonald, K. T., Smith, A. J. S., Bortoletto, D., Coath, R., Crooks, J., Damerell, C., Gibson, M., Nichols, A., Stanitzki, M., Strube, J., Turchetta, R., Tyndel, M., Weber, M., Worm, S., Zhang, Z., Barklow, T. L., Belymam, A., Breidenbach, M., Cassell, R., Craddock, W., Deaconu, C., Dragone, A., Graf, N. A., Haller, G., Herbst, R., Hewett, J. L., Jaros, J. A., Johnson, A. S., Kim, P. C., Macfarlane, D. B., Markiewicz, T., Maruyama, T., Mccormick, J., Moffeit, K., Neal, H. A., Nelson, T. K., Oriunno, M., Partridge, R., Michael Peskin, Rizzo, T. G., Rowson, P., Su, D., Woods, M., Chakrabarti, S., Dieguez, A., Garrido, Ll, Kaminski, J., Conway, J. S., Chertok, M., Gunion, J., Holbrook, B., Lander, R. L., Tripathi, S. M., Fadeyev, V., Schumm, B. A., Gill, J., Nauenberg, U., Oleinik, G., Wagner, S. R., Ranjan, K., Shivpuri, R., Varner, G. S., Orava, R., Kooten, R., Bilki, B., Charles, M., Kim, T. J., Mallik, U., Norbeck, E., Onel, Y., Brau, B. P., Willocq, S., Taylor, G. N., Riles, Keith, Yang, H. -J, Kriske, R., Cremaldi, L., Rahmat, R., Lastovicka-Medin, G., Seidel, S., Hildreth, M. D., Wayne, M., Brau, J. E., Frey, R., Sinev, N., Strom, D. M., Torrence, E., Banda, Y., Burrows, P. N., Devetak, E., Foster, B., Lastovicka, T., Li, Y. -M, Nomerotski, A., Riera-Babures, J., Vilasis-Cardona, X., Manly, S., Adeva, B., Iglesias Escudero, C., Vazquez Regueiro, P., Saborido Silva, J. J., Gallas Torreira, A., Gao, D., Jie, W., Jungfeng, Y., Li, C., Liu, S., Liu, Y., Sun, Y., Wang, Q., Yi, J., Yonggang, W., Zhao, Z., De, K., Farbin, A., Park, S., Smith, J., White, A. P., Yu, J., Lou, X. C., Abe, T., Iwasaki, M., Lubatti, H. J., Band, H. R., Feyzi, F., Prepost, R., Karchin, P. E., Milstene, C., Baltay, C., Dhawan, S., and Kwon, Y. -J

Subjects
High Energy Physics - Experiment (hep-ex), Physics - Instrumentation and Detectors, Physics::Instrumentation and Detectors, FOS: Physical sciences, Physics::Accelerator Physics, High Energy Physics::Experiment, Instrumentation and Detectors (physics.ins-det), physics.ins-det, High Energy Physics - Experiment
Abstract

Letter of intent describing SiD (Silicon Detector) for consideration by the International Linear Collider IDAG panel. This detector concept is founded on the use of silicon detectors for vertexing, tracking, and electromagnetic calorimetry. The detector has been cost-optimized as a general-purpose detector for a 500 GeV electron-positron linear collider., Comment: Letter of Intent for SiD detector concept presented to ILC IDAG

74. Detector concepts

Author

Aarons, G., Abe, T., Abernathy, J., Ablikim, M., Abramowicz, H., Adey, D., Adloff, C., Adolphsen, C., Afanaciev, K., Agapov, I., Ahn, J. -K, Aihara, H., Akemoto, M., Del Carmenalabau, M., Albert, J., Albrecht, H., Albrecht, M., Alesini, D., Alexander, G., Alexander, J., Allison, W., Amann, J., Amirikas, R., An, Q., Anami, S., Ananthanarayan, B., Anderson, T., Andricek, L., Anduze, M., Anerella, M., Anfimov, N., Angal-Kalinin, D., Antipov, S., Antoine, C., Aoki, M., Aoza, A., Aplin, S., Appleby, R., Arai, Y., Araki, S., Arkan, T., Arnold, N., Arnold, R., Arnowitt, R., Artru, X., Arya, K., Aryshev, A., Asakawa, E., Asiri, F., Asner, D., Atac, M., Atoian, G., Attié, D., Augustin, J. -E, Augustine, D. B., Ayres, B., Aziz, T., Baars, D., Badaud, F., Baddams, N., Bagger, J., Bai, S., Bailey, D., Bailey, I. R., Baker, D., Balalykin, N. I., Balbuena, J. P., Baldy, J. -L, Ball, M., Ballestrero, A., Ballin, J., Baltay, C., Bambade, P., Ban, S., Band, H., Bane, K., Banerjee, B., Barbanotti, S., Barbareschi, D., Barbaro-Galtieri, A., Barber, D. P., Barbi, M., Bardin, D. Y., Barish, B., Barklow, T. L., Barlow, R., Barnes, V. E., Barone, M., Bartels, C., Bartsch, V., Basu, R., Battaglia, M., Batygin, Y., Baudot, J., Baur, U., Baynham, D. E., Beard, C., Bebek, C., Bechtle, P., Becker, U. J., Bedeschi, F., Bedjidian, M., Behera, P., Behnke, T., Bellantoni, L., Bellerive, A., Bellomo, P., Bentson, L. D., Benyamna, M., Bergauer, T., Berger, E., Bergholz, M., Beri, S., Berndt, M., Bernreuther, W., Bertolini, A., Besancon, M., Besson, A., Beteille, A., Bettoni, S., Beyer, M., Bhandari, R. K., Bharadwaj, V., Bhatnagar, V., Bhattacharya, S., Bhattacharyya, G., Bhattacherjee, B., Bhuyan, R., Bi, X. -J, Biagini, M., Bialowons, W., Biebel, O., Bieler, T., Bierwagen, J., Birch, A., Bisset, M., Biswal, S. S., Blackmore, V., Blair, G., Blanchard, G., Blazey, G., Blue, A., Blümlein, J., Boffo, C., Bohn, C., Boiko, V. I., Boisvert, V., Bondarchuk, E. N., Boni, R., Bonvicini, G., Boogert, S., Boonekamp, M., Boorman, G., Borras, K., Bortoletto, D., Bosco, A., Bosio, C., Bosland, P., Bosotti, A., Boudry, V., Boumediene, D. -E, Bouquet, B., Bourov, S., Bowden, G., Bower, G., Boyarski, A., Bozovic-Jelisavcic, I., Bozzi, C., Brachmann, A., Bradshaw, T. W., Brandt, A., Brasser, H. P., Brau, B., Brau, J. E., Breidenbach, M., Bricker, S., Brient, J. -C, Brock, I., Brodsky, S., Brooksby, C., Broome, T. A., Brown, D., Brownell, J. H., Bruchon, M., Brueck, H., Brummitt, A. J., Brun, N., Buchholz, P., Budagov, Y. A., Bulgheroni, A., Bulyak, E., Bungau, A., Bürger, J., Burke, D., Burkhart, C., Burrows, P., Burt, G., Burton, D., Büsser, K., Butler, J., Butterworth, J., Buzulutskov, A., Cabruja, E., Caccia, M., Cai, Y., Calcaterra, A., Caliier, S., Camporesi, T., Cao, J. -J, Cao, J. S., Capatina, O., Cappellini, C., Carcagno, R., Carena, M., Carloganu, C., Carosi, R., Carr, F. S., Carrion, F., Carter, H. F., Carter, J., Carwardine, J., Cassel, R., Cassell, R., Cavallari, G., Cavallo, E., Cembranos, J. A. R., Chakraborty, D., Chandez, F., Charles, M., Chase, B., Chattopadhyay, S., Chauveau, J., Chefdeville, M., Chehab, R., Chel, S., Chelkov, G., Chen, C., Chen, H. S., Chen, H. B., Chen, J. E., Chen, S. Y., Chen, S., Chen, X., Chen, Y. B., Cheng, J., Chevallier, M., Chi, Y. L., Chickering, W., Cho, G. -C, Cho, M. -H, Choi, J. -H, Choi, J. B., Choi, S. Y., Choi, Y. -I, Choudhary, B., Choudhury, D., Choudhury, S. R., Christian, D., Christian, G., Christophe, G., Chung, J. -H, Church, M., Ciborowski, J., Cihangir, S., Ciovati, G., Clarke, C., Clarke, D. G., Clarke, J. A., Clements, E., Coca, C., Coe, P., Cogan, J., Colas, P., Collard, C., Colledani, C., Combaret, C., Comerma, A., Compton, C., Constance, B., Conway, J., Cook, E., Cooke, P., Cooper, W., Corcoran, S., Cornat, R., Corner, L., Gil, E. C., Corvin, W. C., Ramusino, A. C., Cowan, R., Crawford, C., Cremaldi, L. M., Crittenden, J. A., Cussans, D., Cvach, J., Da Silva, W., Khah, H. D., Dabrowski, A., Dabrowski, W., Dadoun, O., Dai, J. P., Dainton, J., Daly, C., Damerell, C., Danilov, M., Daniluk, W., Daram, S., Datta, A., Dauncey, P., David, J., Davier, M., Davies, K. P., Dawson, S., Boer, W., Curtis, S., Groot, N., La Taille, C., Lira, A., Roeck, A., Sangro, R., Santis, S., Deacon, L., Deandrea, A., Klaus Dehmelt, Delagnes, E., Delahaye, J. -P, Delebecque, P., Delerue, N., Delferriere, O., Demarteau, M., Deng, Z., Denisov, Yu N., Densham, C. J., Desch, K., Deshpande, N., Devanz, G., Devetak, E., Dexter, A., Di Benedetto, V., Diéguez, Á, Diener, R., Dinh, N. D., Dixit, M., Dixit, S., Djouadi, A., Dolezal, Z., Dollan, R., Dong, D., Dong, H. Y., Dorfan, J., Dorokhov, A., Doucas, G., Downing, R., Doyle, E., Doziere, G., Drago, A., Dragt, A., Drake, G., Drásal, Z., Dreiner, H., Drell, P., Driouichi, C., Drozhdin, A., Drugakov, V., Du, S., Dugan, G., Duginov, V., Dulinski, W., Dulucq, F., Dutta, S., Dwivedi, J., Dychkant, A., Dzahini, D., Eckerlin, G., Edwards, H., Ehrenfeld, W., Ehrlichman, M., Ehrlichmann, H., Eigen, G., Elagin, A., Elementi, L., Eliasson, P., Ellis, J., Ellwood, G., Elsen, E., Emery, L., Enami, K., Endo, K., Enomoto, A., Eozénou, F., Erbacher, R., Erickson, R., Eyser, K. O., Fadeyev, V., Fang, S. X., Fant, K., Fasso, A., Giannelli, M. F., Fehlberg, J., Feld, L., Feng, J. L., Ferguson, J., Fernandez-Garcia, M., Fernandez-Hernando, J. L., Fiala, P., Fieguth, T., Finch, A., Finocchiaro, G., Fischer, P., Fisher, P., Fisk, H. E., Fitton, M. D., Fleck, I., Fleischer, M., Fleury, J., Flood, K., Foley, M., Ford, R., Fortin, D., Foster, B., Fourches, N., Francis, K., Frey, A., Frey, R., Friedsam, H., Frisch, J., Frishman, A., Fuerst, J., Fujii, K., Fujimoto, J., Fukuda, M., Fukuda, S., Funahashi, Y., Funk, W., Furletova, J., Furukawa, K., Furuta, F., Fusayasu, T., Fuster, J., Gadow, K., Gaede, F., Gaglione, R., Gai, W., Gajewski, J., Galik, R., Galkin, A., Galkin, V., Gallin-Martel, L., Gannaway, F., Gao, J. S., Gao, J., Gao, Y., Garbincius, P., Garcia-Tabares, L., Garren, L., Garrido, L., Garutti, E., Garvey, T., Garwin, E., Gascón, D., Gastal, M., Gatto, C., Gatto, R., Gay, P., Ge, L., Ge, M. Q., Ge, R., Geiser, A., Gellrich, A., Genat, J. -F, Geng, Z. Q., Gentile, S., Gerbick, S., Gerig, R., Ghosh, D. K., Ghosh, K., Gibbons, L., Giganon, A., Gillespie, A., Gillman, T., Ginzburg, I., Giomataris, I., Giunta, M., Gladkikh, P., Gluza, J., Godbole, R., Godfrey, S., Goldhaber, G., Goldstein, J., Gollin, G. D., Gonzalez-Sanchez, F. J., Goodrick, M., Gornushkin, Y., Gostkin, M., Gottschalk, E., Goudket, P., Eschrich, I. G., Gournaris, F., Graciani, R., Graf, N., Grah, C., Grancagnolo, F., Grandjean, D., Grannis, P., Grassellino, A., Graugés, E., Gray, S., Green, M., Greenhalgh, J., Greenshaw, T., Grefe, C., Gregor, I. -M, Grenier, G., Grimes, M., Grimm, T., Gris, P., Grivaz, J. -F, Groll, M., Gronberg, J., Grondin, D., Groom, D., Gross, E., Grunewald, M., Grupen, C., Grzelak, G., Gu, J., Gu, Y. -T, Guchait, M., Guiducci, S., Guler, A. M., Guler, H., Gulmez, E., Gunion, J., Guo, Z. Y., Gurtu, A., Ha, H. B., Haas, T., Haase, A., Haba, N., Haber, H., Haensel, S., Hagge, L., Hagura, H., Hajdu, C., Haller, G., Haller, J., Hallermann, L., Halyo, V., Hamaguchi, K., Hammond, L., Han, L., Han, T., Hand, L., Handu, V. K., Hano, H., Hansen, C., Hansen, J. D., Hansen, J. B., Hara, K., Harder, K., Hartin, A., Hartung, W., Hast, C., Hauptman, J., Hauschild, M., Hauviller, C., Havranek, M., Hawkes, C., Hawkings, R., Hayano, H., Hazumi, M., He, A., He, H. J., Hearty, C., Heath, H., Hebbeker, T., Hedberg, V., Hedin, D., Heifets, S., Heinemeyer, S., Heini, S., Helebrant, C., Helms, R., Heltsley, B., Henrot-Versille, S., Henschel, H., Hensel, C., Hermel, R., Herms, A., Herten, G., Hesselbach, S., Heuer, R. -D, Heusch, C. A., Hewett, J., Higashi, N., Higashi, T., Higashi, Y., Higo, T., Hildreth, M. D., Hiller, K., Hillert, S., Hillier, S. J., Himel, T., Himmi, A., Hinchliffe, I., Hioki, Z., Hirano, K., Hirose, T., Hisamatsu, H., Hisano, J., Hlaing, C. T., Hock, K. M., Hoeferkamp, M., Hohlfeld, M., Honda, Y., Hong, J., Hong, T. M., Honma, H., Horii, Y., Horvath, D., Hosoyama, K., Hostachy, J. -Y, Hou, M., Hou, W. -S, Howell, D., Hronek, M., Hsiung, Y. B., Hu, B., Hu, T., Huang, J. -Y, Huang, T. M., Huang, W. H., Huedem, E., Huggard, P., Hugonie, C., Hu-Guo, C., Huitu, K., Hwang, Y., Idzik, M., Ignatenko, A., Ignatov, F., Ikeda, H., Ikematsu, K., Ilicheva, T., Imbault, D., Imhof, A., Incagli, M., Ingbir, R., Inoue, H., Inoue, Y., Introzzi, G., Ioakeimidi, K., Ishihara, S., Ishikawa, A., Ishikawa, T., Issakov, V., Ito, K., Ivanov, V. V., Ivanov, V., Ivanyushenkov, Y., Iwasaki, M., Iwashita, Y., Jackson, D., Jackson, F., Jacobsen, B., Jaganathan, R., Jamison, S., Janssen, M. E., Jaramillo-Echeverria, R., Jaros, J., Jauffret, C., Jawale, S. B., Jeans, D., Jedziniak, R., Jeffery, B., Jehanno, D., Jenner, L. J., Jensen, C., Jensen, D. R., Jiang, H., Jiang, X. M., Jimbo, M., Jin, S., Jobe, R. K., Johnson, A., Johnson, E., Johnson, M., Johnston, M., Joireman, P., Jokic, S., Jones, J., Jones, R. M., Jongewaard, E., Jönsson, L., Joshi, G., Joshi, S. C., Jung, J. -Y, Junk, T., Juste, A., Kado, M., Kadyk, J., Käfer, D., Kako, E., Kalavase, P., Kalinin, A., Kalinowski, J., Kamitani, T., Kamiya, Y., Kamoshita, J. -I, Kananov, S., Kanaya, K., Kanazawa, K. -I, Kanemura, S., Kang, H. -S, Kang, W., Kanjial, D., Kapusta, F., Karataev, P., Karchin, P. E., Karlen, D., Karyotakis, Y., Kashikhin, V., Kashiwagi, S., Kasley, P., Katagiri, H., Kato, T., Kato, Y., Katzy, J., Kaukher, A., Kaur, M., Kawagoe, K., Kawamura, H., Kazakov, S., Kekelidze, V. D., Keller, L., Kelley, M., Kelly, M., Kennedy, K., Kephart, R., Keung, J., Khainovski, O., Khan, S. A., Khare, P., Khovansky, N., Kiesling, C., Kikuchi, M., Kilian, W., Killenberg, M., Kim, D., Kim, E. S., Kim, E. -J, Kim, G., Kim, H., Kim, H. -C, Kim, J., Kim, K. -J, Kim, K. S., Kim, P., Kim, S., Kim, S. -H, Kim, S. K., Kim, T. J., Kim, Y., Kim, Y. -K, Kimmitt, M., Kirby, R., Kircher, F., Kisielewska, D., Kittel, O., Klanner, R., Klebaner, A. L., Kleinwort, C., Klimkovich, T., Klinkby, E., Kluth, S., Knecht, M., Kneisel, P., Ko, I. S., Ko, K., Kobayashi, M., Kobayashi, N., Kobel, M., Koch, M., Kodys, P., Koetz, U., Kohrs, R., Kojima, Y., Kolanoski, H., Kolodziej, K., Kolomensky, Y. G., Komamiya, S., Kong, X. C., Konigsberg, J., Korbel, V., Koscielniak, S., Kostromin, S., Kowalewski, R., Kraml, S., Krammer, M., Krasnykh, A., Krautscheid, T., Krawczyk, M., Krebs, H. J., Krempetz, K., Kribs, G., Krishnagopal, S., Kriske, R., Kronfeld, A., Kroseberg, J., Kruchonak, U., Kruecker, D., Krüger, H., Krumpa, N. A., Krumshtein, Z., Kuang, Y. P., Kubo, K., Kuchler, V., Kudoh, N., Kulis, S., Kumada, M., Kumar, A., Kume, T., Kundu, A., Kurevlev, G., Kurihara, Y., Kuriki, M., Kuroda, S., Kuroiwa, H., Kurokawa, S. -I, Kusano, T., Kush, P. K., Kutschke, R., Kuznetsova, E., Kvasnicka, P., Kwon, Y., Labarga, L., Lacasta, C., Lackey, S., Lackowski, T. W., Lafaye, R., Lafferty, G., Lagorio, E., Laktineh, I., Lal, S., Laloum, M., Lam, B., Lancaster, M., Lander, R., Lange, W., Langenfeld, U., Langeveld, W., Larbalestier, D., Larsen, R., Lastovicka, T., Lastovicka-Medin, G., Latina, A., Latour, E., Laurent, L., Le, B. N., Le, D. N., Le Diberder, F., Le Dû, P., Lebbolo, H., Lebrun, P., Lecoq, J., Lee, S. -W, Lehner, F., Leibfritz, J., Lenkszus, F., Lesiak, T., Levy, A., Lewandowski, J., Leyh, G., Li, C., Li, C. S., Li, C. H., Li, D. Z., Li, G., Li, J., Li, S. P., Li, W. M., Li, W., Li, X. P., Li, X. -Q, Li, Y., Li, Z., Li, Z. Q., Liang, J. T., Liao, Y., Lilje, L., Lima, J. G., Lintern, A. J., Lipton, R., List, B., List, J., Liu, C., Liu, J. F., Liu, K. X., Liu, L. Q., Liu, S. Z., Liu, S. G., Liu, S., Liu, W., Liu, W. B., Liu, Y. P., Liu, Y. D., Lockyer, N., Logan, H. E., Logatchev, P. V., Lohmann, W., Lohse, T., Lola, S., Lopez-Virto, A., Loveridge, P., Lozano, M., Lu, C. -D, Lu, C., Lu, G. -L, Lu, W. H., Lubatti, H., Lucotte, A., Lundberg, B., Lundin, T., Luo, M., Luong, M., Luth, V., Lutz, B., Lutz, P., Lux, T., Luzniak, P., Lyapin, A., Lykken, J., Lynch, C., Ma, L., Ma, Q., Ma, W. -G, Macfarlane, D., Maciel, A., Macleod, A., Macnair, D., Mader, W., Magill, S., Magnan, A. -M, Maiheu, B., Maity, M., Majchrzak, M., Majumder, G., Makarov, R., Makowski, D., Malaescu, B., Mallik, C., Mallik, U., Malton, S., Malyshev, O. B., Malysheva, L. I., Mammosser, J., Mamta, Mamuzic, J., Manen, S., Manghisoni, M., Manly, S., Marcellini, F., Marcisovsky, M., Markiewicz, T. W., Marks, S., Marone, A., Marti, F., Martin, J. -P, Martin, V., Martin-Chassard, G., Martinez, M., Martinez-Rivero, C., Martsch, D., Martyn, H. -U, Maruyama, T., Masuzawa, M., Mathez, H., Matsuda, T., Matsumoto, H., Matsumoto, S., Matsumoto, T., Matsunaga, H., Mättig, P., Mattison, T., Mavromanolakis, G., Mawatari, K., Mazzacane, A., Mcbride, P., Mccormick, D., Mccormick, J., Mcdonald, K. T., Mcgee, M., Mcintosh, P., Mckee, B., Mcpherson, R. A., Meidlinger, M., Meier, K., Mele, B., Meller, B., Melzer-Pellmann, I. -A, Mendez, H., Mercer, A., Merkin, M., Meshkov, I. N., Messner, R., Metcalfe, J., Meyer, C., Meyer, H., Meyer, J., Meyer, N., Meyners, N., Michelato, P., Michizono, S., Mihalcea, D., Mihara, S., Mihara, T., Mikami, Y., Mikhailichenko, A. A., Milardi, C., Miller, D. J., Miller, O., Miller, R. J., Milstene, C., Mimashi, T., Minashvili, I., Miquel, R., Mishra, S., Mitaroff, W., Mitchell, C., Miura, T., Miyamoto, A., Miyata, H., Mjörnmark, U., Mnich, J., Moenig, K., Moffeit, K., Mokhov, N., Molloy, S., Monaco, L., Monasterio, P. R., Montanari, A., Moon, S. I., Moortgat-Pick, G. A., Freitas, P. M., Morel, F., Moretti, S., Morgunov, V., Mori, T., Morin, L., Morisseau, F., Morita, Y., Morozov, N., Morozumi, Y., Morse, W., Moser, H. -G, Moultaka, G., Mtingwa, S., Mudrinic, M., Mueller, A., Mueller, W., Muennich, A., Muhlleitner, M. M., Mukherjee, B., Mukhopadhyaya, B., Müller, T., Munro, M., Murayama, H., Muto, T., Myneni, G. R., Nabhiraj, P. Y., Nagaitsev, S., Nagamine, T., Nagano, A., Naito, T., Nakai, H., Nakajima, H., Nakamura, I., Nakamura, T., Nakanishi, T., Nakao, K., Nakao, N., Nakayoshi, K., Nam, S., Namito, Y., Namkung, W., Nantista, C., Napoly, O., Narain, M., Naroska, B., Nauenberg, U., Nayyar, R., Neal, H., Nelson, C., Nelson, J., Nelson, T., Nemecek, S., Neubauer, M., Neuffer, D., Newman, M. Q., Nezhevenko, O., Ng, C. -K, Nguyen, A. K., Nguyen, M., Thi, H. V. N., Niebuhr, C., Niehoff, J., Niezurawski, P., Nishitani, T., Nitoh, O., Noguchi, S., Nomerotski, A., Noonan, J., Norbeck, E., Nosochkov, Y., Notz, D., Nowak, G., Nowak, H., Noy, M., Nozaki, M., Nyffeler, A., Nygren, D., Oddone, P., O, J., Oh, J. -S, Oh, S. K., Ohkuma, K., Ohlerich, M., Ohmi, K., Ohnishi, Y., Ohsawa, S., Ohuchi, N., Oide, K., Okada, N., Okada, Y., Okamura, T., Okugi, T., Okumi, S., Okumura, K. -I, Olchevski, A., Oliver, W., Olivier, B., Olsen, J., Olsen, S., Olshevsky, A. G., Olsson, J., Omori, T., Onel, Y., Onengut, G., Ono, H., Onoprienko, D., Oreglia, M., Oren, W., Orimoto, T. J., Oriunno, M., Orlandea, M. C., Oroku, M., Orr, L. H., Orr, R. S., Oshea, V., Oskarsson, A., Osland, P., Ossetski, D., Österman, L., Ostiguy, F., Otono, H., Ottewell, B., Ouyang, Q., Padamsee, H., Padilla, C., Pagani, C., Palmer, M. A., Pam, W. M., Pande, M., Pande, R., Pandit, V. S., Pandita, P. N., Pandurovic, M., Pankov, A., Panzeri, N., Papandreou, Z., Paparella, R., Para, A., Park, H., Parker, B., Parkes, C., Parma, V., Parsa, Z., Parsons, J., Partridge, R., Pasquinelli, R., Pásztor, G., Paterson, E., Patrick, J., Patteri, P., Patterson, J. R., Pauletta, G., Paver, N., Pavlicek, V., Pawlik, B., Payet, J., Pchalek, N., Pedersen, J., Pei, G. X., Pei, S. L., Pelka, J., Pellegrini, G., Pellett, D., Peng, G. X., Penn, G., Penzo, A., Perry, C., Peskin, M., Peters, F., Petersen, T. C., Peterson, D., Peterson, T., Petterson, M., Pfeffer, H., Pfund, P., Phelps, A., Phi, Q., Phillips, J., Phinney, N., Piccolo, M., Piemontese, L., Pierini, P., Piggott, W. T., Pike, G., Pillet, N., Jayawardena, T. P., Piot, P., Pitts, K., Pivi, M., Plate, D., Pleier, M. -A, Poblaguev, A., Poehler, M., Poelker, M., Poffenberger, P., Pogorelsky, I., Poirier, F., Poling, R., Poole, M., Popescu, S., Popielarski, J., Pöschl, R., Postranecky, M., Potukochi, P. N., Prast, J., Prat, S., Preger, M., Prepost, R., Price, M., Proch, D., Puntambekar, A., Qin, Q., Qu, H. M., Quadt, A., Quesnel, J. -P, Radeka, V., Rahmat, R., Rai, S. K., Raimondi, P., Ramberg, E., Ranjan, K., Rao, S. V. L. S., Raspereza, A., Ratti, A., Ratti, L., Raubenheimer, T., Raux, L., Ravindran, V., Raychaudhuri, S., Re, V., Rease, B., Reece, C. E., Regler, M., Rehlich, K., Reichel, I., Reichold, A., Reid, J., Reid, R., Reidy, J., Reinhard, M., Renz, U., Repond, J., Resta-Lopez, J., Reuen, L., Ribnik, J., Rice, T., Richard, F., Riemann, S., Riemann, T., Riles, K., Riley, D., Rimbault, C., Rindani, S., Rinolfi, L., Risigo, F., Riu, I., Rizhikov, D., Rizzo, T., Rochford, J. H., Rodriguez, P., Roeben, M., Rolandi, G., Roodman, A., Rosenberg, E., Roser, R., Ross, M., Rossel, F., Rossmanith, R., Roth, S., Rougé, A., Rowe, A., Roy, A., Roy, S. B., Roy, S., Royer, L., Royole-Degieux, P., Royon, C., Ruan, M., Rubin, D., Ruehl, I., Jimeno, A. R., Ruland, R., Rusnak, B., Ryu, S. -Y, Sabbi, G. L., Sadeh, I., Sadygov, Z. Y., Saeki, T., Sagan, D., Sahni, V. C., Saini, A., Saito, K., Sajot, G., Sakanaka, S., Sakaue, K., Salata, Z., Salih, S., Salvatore, F., Samson, J., Sanami, T., Sanchez, A. L., Sands, W., Santic, J., Sanuki, T., Sapronov, A., Sarkar, U., Sasao, N., Satoh, K., Sauli, F., Saunders, C., Saveliev, V., Savoy-Navarro, A., Sawyer, L., Saxton, L., Schäfer, O., Schälicke, A., Schade, P., Schaetzel, S., Scheitrum, G., Schibler, É, Schindler, R., Schlösser, M., Schlueter, R. D., Schmid, P., Schmidt, R. S., Schneekloth, U., Schreiber, H. J., Schreiber, S., Schroeder, H., Schüler, K. P., Schulte, D., Schultz-Coulon, H. -C, Schumacher, M., Schumann, S., Schumm, B. A., Schwienhorst, R., Schwierz, R., Scott, D. J., Scuri, F., Sefkow, F., Sefri, R., Seguin-Moreau, N., Seidel, S., Seidman, D., Sekmen, S., Seletskiy, S., Senaha, E., Senanayake, R., Sendai, H., Sertore, D., Seryi, A., Settles, R., Sever, R., Shales, N., Shao, M., Shelkov, G. A., Shepard, K., Shepherd-Themistocleous, C., Sheppard, J. C., Shi, C. T., Shidara, T., Shim, Y. -J, Shimizu, H., Shimizu, Y., Shimogawa, T., Shin, S., Shioden, M., Shipsey, I., Shirkov, G., Shishido, T., Shivpuri, R. K., Shrivastava, P., Shulga, S., Shumeiko, N., Shuvalov, S., Si, Z., Siddiqui, A. M., Siegrist, J., Simon, C., Simrock, S., Sinev, N., Singh, B. K., Singh, J., Singh, P., Singh, R. K., Singh, S. K., Singini, M., Sinha, A. K., Sinha, N., Sinha, R., Sinram, K., Sissakian, A. N., Skachkov, N. B., Skrinsky, A., Slater, M., Slominski, W., Smiljanic, I., Smith, A. J. S., Smith, A., Smith, B. J., Smith, J., Smith, S., Smith, T., Snodgrass, W. N., Sobloher, B., Sohn, Y. -U, Solidum, R., Solyak, N., Son, D., Sonmez, N., Sopczak, A., Soskov, V., Spencer, C. M., Spentzouris, P., Speziali, V., Spira, M., Sprehn, D., Sridhar, K., Srivastava, A., St Lorant, S., Stahl, A., Stanek, R. P., Stanitzki, M., Stanley, J., Stefanov, K., Stein, W., Steiner, H., Stenlund, E., Stern, A., Sternberg, M., Stockinger, D., Stockton, M., Stoeck, H., Strachan, J., Strakhovenko, V., Strauss, M., Striganov, S. I., Strologas, J., Strom, D., Strube, J., Stupakov, G., Su, D., Sudo, Y., Suehara, T., Suehiro, T., Suetsugu, Y., Sugahara, R., Sugimoto, Y., Sugiyama, A., Suh, J. S., Sukovic, G., Sun, H., Sun, S., Sun, W., Sun, Y., Suszycki, L., Sutcliffe, P., Suthar, R. L., Suwada, T., Suzuki, A., Suzuki, C., Suzuki, S., Suzuki, T., Swent, R., Swientek, K., Swinson, C., Syresin, E., Szleper, M., Tadday, A., Takahashi, R., Takahashi, T., Takano, M., Takasaki, F., Takeda, S., Takenaka, T., Takeshita, T., Takubo, Y., Tanaka, M., Tang, C. X., Taniguchi, T., Tantawi, S., Tapprogge, S., Tartaglia, M. A., Tassielli, G. F., Tauchi, T., Tavian, L., Tawara, H., Taylor, G., Telnov, A. V., Telnov, V., Tenenbaum, P., Teodorescu, E., Terashima, A., Terracciano, G., Terunuma, N., Teubner, T., Teuscher, R., Theilacker, J., Thomson, M., Tice, J., Tigner, M., Timmermans, J., Titov, M., Toge, N., Tokareva, N. A., Tollefson, K., Tomasek, L., Tomovic, S., Tompkins, J., Tonutti, M., Topkar, A., Toprek, D., Toral, F., Torrence, E., Traversi, G., Trimpl, M., Tripathi, S. M., Trischuk, W., Trodden, M., Trubnikov, G. V., Tschirhart, R., Tskhadadze, E., Tsuchiya, K., Tsukamoto, T., Tsunemi, A., Tucker, R., Turchetta, R., Tyndel, M., Uekusa, N., Ueno, K., Umemori, K., Ummenhofer, M., Underwood, D., Uozumi, S., Urakawa, J., Urban, J., Uriot, D., Urner, D., Ushakov, A., Usher, T., Uzunyan, S., Vachon, B., Valerio, L., Valin, I., Valishev, A., Vamra, R., Graaf, H., Kooten, R., Zandbergen, G., Vanel, J. -C, Variola, A., Varner, G., Velasco, M., Velte, U., Velthuis, J., Vempati, S. K., Venturini, M., Vescovi, C., Videau, H., Vila, I., Vincent, P., Virey, J. -M, Visentin, B., Viti, M., Vo, T. C., Vogel, A., Vogt, H., Toerne, E., Vorozhtsov, S. B., Vos, M., Votava, M., Vrba, V., Wackeroth, D., Wagner, A., Wagner, C. E. M., Wagner, S., Wake, M., Walczak, R., Walker, N. J., Walkowiak, W., Wallon, S., Walsh, R., Walston, S., Waltenberger, W., Walz, D., Wang, C. E., Wang, C. H., Wang, D., Wang, F., Wang, G. W., Wang, H., Wang, J., Wang, J. Q., Wang, L., Wang, M. -Z, Wang, Q., Wang, S. H., Wang, X., Wang, X. -L, Wang, Y. F., Wang, Z., Wanzenberg, R., Ward, B., Ward, D., Warmbein, B., Warner, D. W., Warren, M., Washio, M., Watanabe, I., Watanabe, K., Watanabe, T., Watanabe, Y., Watson, N., Wattimena, N., Wayne, M., Weber, M., Weerts, H., Weiglein, G., Weiland, T., Weinzierl, S., Weise, H., Weisend, J., Wendt, M., Wendt, O., Wenzel, H., Wenzel, W. A., Wermes, N., Werthenbach, U., Wesseln, S., Wester, W., White, A., White, G. R., Wichmann, K., Wienemann, P., Wierba, W., Wilksen, T., Willis, W., Wilson, G. W., Wilson, J. A., Wilson, R., Wing, M., Winter, M., Wirth, B. D., Wolbers, S. A., Wolff, D., Wolski, A., Woodley, M. D., Woods, M., Woodward, M. L., Woolliscroft, T., Worm, S., Wormser, G., Wright, D., Wu, A., Wu, T., Wu, Y. L., Xella, S., Xia, G., Xia, L., Xiao, A., Xiao, L., Xie, J. L., Xing, Z. -Z, Xiong, L. Y., Xu, G., Xu, Q. J., Yajnik, U. A., Yakimenko, V., Yamada, R., Yamaguchi, H., Yamamoto, A., Yamamoto, H., Yamamoto, M., Yamamoto, N., Yamamoto, R., Yamamoto, Y., Yamanaka, T., Yamaoka, H., Yamashita, S., Yamazaki, H., Yan, W., Yang, H. -J, Yang, J. M., Yang, J., Yang, Z., Yano, Y., Yazgan, E., Yeh, G. P., Yilmaz, H., Yock, P., Yoda, H., Yoh, J., Yokoya, K., Yokoyama, H., York, R. C., Yoshida, M., Yoshida, T., Yoshioka, T., Young, A., Yu, C. H., Yu, J., Yu, X. M., Yuan, C., Yue, C. -X, Yue, J. H., Zacek, J., Zagorodnov, I., Zalesak, J., Zalikhanov, B., Zarnecki, A. F., Zawiejski, L., Zeitnitz, C., Zeller, M., Zerwas, D., Zerwas, P., Zeyrek, M., Zhai, J. Y., Zhang, B. C., Zhang, B., Zhang, C., Zhang, H., Zhang, J., Zhang, J. R., Zhang, L., Zhang, X., Zhang, Y., Zhang, Z., Zhao, H., Zhao, J. J., Zhao, J. X., Zhao, M. H., Zhao, S. C., Zhao, T., Zhao, T. X., Zhao, Z. T., Zhao, Z., Zhou, D. M., Zhou, F., Zhou, S., Zhu, S. H., Zhu, X. W., Zhukov, V., Zimmermann, F., Ziolkowski, M., Zisman, M. S., Zomer, F., Zong, Z. G., Zorba, O., and Zutshi, V.

77. Normalised similarity assessment to inform grouping of advanced multi-component nanomaterials by means of an Asymmetric Sigmoid function.

Author

Zabeo A, Tsiliki G, Brunelli A, Badetti E, Balbuena J, and Hristozov D

Subjects
Software, Nanocomposites chemistry, Zinc Oxide chemistry, Nanostructures chemistry, Silicon Dioxide chemistry
Abstract

This manuscript presents a procedure for similarity assessment as a basis for grouping of multi component nanomaterials (MCNMs). This methodology is an adaptation of the approach by Zabeo et al. (2022), which includes an impactful change: the calculated similarities are normalised in the [0,1] domain by means of asymmetric Logistic scaling to simplify comparisons among properties' distances. This novel approach allows for grouping of nanomaterials that is not affected by the dataset, so that group membership will not change when new candidates are included in the set of assessed materials. It can be applied to assess groups of MCNMs as well as mixed groups of multi and single component nanomaterials as well as chemicals. To facilitate the application of the proposed methodology, a software script was developed by using the Python programming language, which is currently undergoing migration to a user-friendly web-based tool. The presented approach was tested against a real industrial case study provided by the Andalusian Innovation Centre for Sustainable Solution (CIAC): SiO 2 -ZnO hybrid nanocomposite used in building coatings, which is designed to facilitate photocatalytic removal of NOx gases from the atmosphere. The results of applying the methodology in the case study demonstrated that ZnO is dissimilar from the other candidates mainly due to its different dissolution profiles., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published
2024
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78. Lightweight Mortar Incorporating Expanded Perlite, Vermiculite, and Aerogel: A Study on the Thermal Behavior.

Author

Balbuena J, Sánchez M, Sánchez L, and Cruz-Yusta M

Abstract

Climate change is compelling countries to alter their construction and urbanization policies to minimize their impact on the environment. The European Union has set a goal to reduce greenhouse gas emissions by 55%, recognizing that 50% of its emissions originate from maintaining thermal comfort within buildings. As a response, the EU has developed comprehensive legislation on energy efficiency. In this article, special mortars using aerogel, perlite, and vermiculite as lightweight aggregates were prepared and studied to enhance the thermal properties of the mortar. Their thermal properties were examined and, using a solar simulator for both hot and cold conditions, it was found that varying proportions of these lightweight aggregates resulted in a mortar that provided insulation from the exterior up to 7 °C more than the reference mortar in warm conditions and up to 4.5 °C in cold conditions.

Published
2024
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79. Disentangling the determinants of symbiotic species richness in native and invasive gammarids (Crustacea, Amphipoda) of the Baltic region.

Author

Sarabeev V, Balbuena JA, Jarosiewicz A, Voronova N, Sueiro RA, Leiro JM, and Ovcharenko M

Subjects
Animals, Ecosystem, Introduced Species, Host-Parasite Interactions, Crustacea, Amphipoda parasitology, Parasites, Microsporidia physiology, Platyhelminths
Abstract

Dispersal of alien species is a global problem threatening native biodiversity. Co-introduction of non-native parasites and pathogens adds to the severity of this threat, but this indirect impact has received less attention. To shed light on the key factors determining the richness of microorganisms in native and invasive host species, we compared symbiotic (parasitic and epibiotic) communities of gammarids across different habitats and localities along the Baltic coast of Poland. Seven gammarid species, two native and five invasive, were sampled from 16 freshwater and brackish localities. Sixty symbiotic species of microorganisms of nine phyla were identified. This taxonomically diverse species assemblage of symbionts allowed us to assess the effect of host translocation and regional ecological determinants driving assembly richness in the gammarid hosts. Our results revealed that (i) the current assemblages of symbionts of gammarid hosts in the Baltic region are formed by native and co-introduced species; (ii) species richness of the symbiotic community was higher in the native Gammarus pulex than in the invasive hosts, probably reflecting a process of species loss by invasive gammarids in the new area and the distinct habitat conditions occupied by G. pulex and invasive hosts; (iii) both host species and locality were key drivers shaping assembly composition of symbionts, whereas habitat condition (freshwater versus brackish) was a stronger determinant of communities than geographic distance; (iv) the dispersion patterns of the individual species richness of symbiotic communities were best described by Poisson distributions; in the case of an invasive host, the dispersion of the rich species diversity may switch to a right-skewed negative binomial distribution, suggesting a host-mediated regulation process. We believe this is the first analysis of the symbiotic species richness in native and invasive gammarid hosts in European waters based on original field data and a broad range of taxonomic groups including Microsporidia, Choanozoa, Ciliophora, Apicomplexa, Platyhelminthes, Nematoda, Nematomorha, Acanthocephala and Rotifera, to document the patterns of species composition and distribution., (Copyright © 2023 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published
2023
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80. Seasonal controlling factors of CO 2 exchange in a semiarid shrubland in the Chihuahuan Desert, Mexico.

Author

Flores-Rentería D, Delgado-Balbuena J, Campuzano EF, and Curiel Yuste J

Subjects
Mexico, Ecosystem, Carbon Dioxide
Abstract

The still significant uncertainties associated with the future capacity of terrestrial systems to mitigate climate change are linked to the lack of knowledge of the biotic and abiotic processes that regulate CO 2 net ecosystem exchange (NEE) in space/time. Mainly, rates and controls of CO 2 exchange from arid ecosystems, despite dominating the global trends in interannual variability of the terrestrial CO 2 sink capacity, are probably the most poorly understood of all. We present a study on rates and controls of CO 2 exchange measured with the eddy covariance (EC) technique in the Chihuahuan Desert in the Northeast of Mexico, to understand how the environmental controls of the NEE switch throughout the year using a multilevel approach. Since this is a water-limited ecosystem, the hydroecological year, based on the last precipitation and the decay of air temperature, was used to compare the wet (from May 16 to October 30, 2019) and dry (November 1, 2019 to May 15, 2020) seasons' controlling mechanisms, both at diurnal and nocturnal times. Annual NEE was -303.5 g C m -2 , with a cumulative R eco of 537.7 g C m -2 and GPP of 841.3 g C m -2 . NEE showed radiation, temperature, and soil moisture sensitivity along the day, however, shifts in these controls along the year and between seasons were identified. The winter precipitations during the dry season led to fast C release followed by lagged C uptake. Despite this flux pulse, the ecosystem was a net sink throughout most of the year because the local vegetation is well adapted to grow and uptake C under these arid conditions, even during the dry season. Understanding the controls of the sink-source shifts is relevant since the predictions for future climate include changes in the precipitation patterns., Competing Interests: Declaration of competing interest Not applicable., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published
2023
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81. Disseminated Intravascular Coagulation in Varying Age Groups Based on Clinical Conditions.

Author

Geyer-Roberts E, Akhand T, Blanco A, Jose R, Chowdhury N, Ea M, Gutierrez E, Balbuena J, Anagnostis S, Henderson C, Fazio A, Burpee A, and Jacobs RJ

Abstract

Disseminated intravascular coagulation (DIC) is a serious syndrome characterized by the systemic activation of blood coagulation resulting in the thrombosis of vessels leading to organ dysfunction and severe bleeding. When physicians try to treat DIC, it is imperative to diagnose and treat the underlying conditions. Anyone can be affected by DIC, but vulnerable groups such as pediatric populations, pregnant women and the elderly may be at higher risk. In this review, the current literature on DIC in pregnancy, the pediatric population, and the elderly is reported. This review also highlights the similarities and differences in the etiology, clinical presentation, diagnosis, and management of DIC in the aforementioned groups (i.e., pediatrics, pregnant women, and the elderly). Findings from this study may help increase awareness about various presentations of DIC in these groups to facilitate rapid recognition of symptoms leading to correct diagnoses., Competing Interests: The authors have declared that no competing interests exist., (Copyright © 2022, Geyer-Roberts et al.)

Published
2022
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82. Effective definition of low humoral response to Clostridioides difficile infection.

Author

Ramos-Martínez A, Serrano-Martínez F, Pintos I, Valencia-Alijo Á, Gutiérrez-Rojas Á, Cítores MJ, Ortiz-Balbuena J, Royuela A, Martínez-Ruiz R, Sánchez-Romero I, Asensio Á, Múñez E, and Plaza A

Subjects
Aged, Aged, 80 and over, Antibodies, Bacterial immunology, Antigens, Bacterial immunology, Bacterial Proteins immunology, Comorbidity, Female, Humans, Immunoglobulin A immunology, Immunoglobulin G immunology, Immunoglobulin M immunology, Male, Middle Aged, Recurrence, Spain, Clostridioides difficile immunology, Clostridium Infections immunology, Clostridium Infections microbiology, Host-Pathogen Interactions immunology, Immunity, Humoral
Abstract

Background: Determination of the humoral response to Clostridioides difficile (CD) toxins could be of great value in the management of patients with CD infection (CDI)., Methods: A prospective study was conducted on the clinical characteristics and humoral response in patients with CDI. Determination of ELISA IgG CD anti-toxin B (tgcBiomics, Germany) was performed. The following dilutions were planned for each patient, 1:100, 1: 200, 1: 400, 1: 800: 1: 1600. A significant concentration of antibody was considered to be present in each dilution if an optical density 0.2 units higher than the negative control of the technique was evident., Results: Eighty-five patients were included during the study period, November 2018-February 2020. The median age was 73 years (interquartile range: 62.5-85 years), with female predominance (45 patients, 52.9%). Thirty-nine patients (45.9%) had a severe infection. Seven patients (8.2%) had suffered an episode of CDI in the previous three months. Seventeen patients (20%) had one or more recurrent episodes during the three-month follow-up: No patient died during admission or required surgery for severe-complicated infection. The incidence of recurrence in patients with no antibody detected at 1:400 dilution was 25.4% (16 patients) while it was 4.3% (one patient) in patients with antibody present at that dilution (p = 0.03). Liver cirrhosis was associated with higher humoral response against CD., Conclusions: Antibodies IgG CD anti-toxin B detection at a dilution of 1:400, using a B ELISA technique, effectively identified patients at increased risk of recurrence. This information could help assist in the management of patients., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper. Antonio Ramos-Martínez has received honoraria for lecturing activities and funding for conference attendance from MSD, Astellas, ERN and Angelini., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published
2021
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83. Risk Factors for Clostridioides Difficile Diarrhea In Solid Organ Transplantation Recipients.

Author

Ortiz-Balbuena J, Royuela A, Calderón-Parra J, Martínez-Ruiz R, Asensio-Vegas Á, Múñez E, Valencia-Alijo Á, Gutiérrez-Rojas Á, Ussetti P, Cuervas-Mons V, Segovia-Cubero J, Portolés-Pérez J, and Ramos-Martínez A

Subjects
Adult, Aged, Case-Control Studies, Clostridioides, Diarrhea, Humans, Male, Middle Aged, Retrospective Studies, Risk Factors, Transplant Recipients, Clostridioides difficile, Clostridium Infections diagnosis, Clostridium Infections epidemiology, Organ Transplantation adverse effects
Abstract

Background: There is limited knowledge about risk factors for Clostridioides difficile infection (CDI) and recurrent CDI in solid organ transplant (SOT) recipients., Methods: A case-control study of CDI in SOT recipients compared with controls (SOT recipients who did not present CDI)., Results: Sixty-seven patients from 1089 SOT recipients (6.2%) suffered at least one episode of CDI. The mean age was 55 ± 12 years and 20 cases (69%) were men. The accumulated incidence was 8% in liver transplantation, 6.2% in lung transplantation, 5.4% in heart transplantation, and 4.7% in kidney transplantation. Twenty-nine cases (43.3%) were diagnosed during the first 3 months after SOT. Forty-one cases (61.2%) were hospital acquired. Thirty-one patients with CDI presented with mild-moderate infection (46.3%), 30 patients with severe infection (44.8%), and 6 patients with severe-complicated disease (9%). Independent variables found to be related with CDI were hospitalization in the previous 3 months (odds ratio: 2.99; [95% confidence interval 1.21-7.37]) and the use of quinolones in the previous month (odds ratio: 3.71 [95% confidence interval 1.16-11.8]). Eleven patients (16.4%) had at least one recurrence of CDI. Previous treatment with amoxicillin-clavulanate, severe-complicated index episode, and high serum creatinine were associated with recurrent CDI in the univariant analysis CONCLUSIONS: Liver transplant recipients presented the highest incidence of CDI among SOT recipients. Risk factors for CDI were hospitalization in the previous 3 months and the use of quinolones in the previous month., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2021
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84. Decrease in the prevalence of hepatitis B and D virus infections in an endemic area in Peru 23 years after the introduction of the first pilot vaccination program against hepatitis B.

Author

Cabezas C, Trujillo O, Balbuena J, Peceros FM, Terrazas M, Suárez M, Marin L, Apac J, and Ramírez-Soto MC

Subjects
Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Cross-Sectional Studies, Endemic Diseases, Female, Hepatitis Antibodies blood, Hepatitis B epidemiology, Hepatitis B immunology, Hepatitis B Antibodies blood, Hepatitis B Surface Antigens blood, Hepatitis B Vaccines pharmacology, Hepatitis B virus immunology, Hepatitis D immunology, Hepatitis Delta Virus immunology, History, 20th Century, History, 21st Century, Humans, Infant, Infant, Newborn, Male, Middle Aged, Peru epidemiology, Pilot Projects, Prevalence, Young Adult, Hepatitis B prevention & control, Hepatitis B Vaccines history, Hepatitis D epidemiology, Immunization Programs history
Abstract

In 1991, Peru launched the first vaccination program against hepatitis B in children aged under 5 years in the hyperendemic [hepatitis B virus (HBV) and hepatitis D virus (HDV)] province of Abancay. We conducted a cross-sectional study to determine the prevalence of HBV and HDV infections, 23 years after the launch of the vaccination program, as well as the post-vaccine response against hepatitis B in terms of prevalence of hepatitis B surface antibody (anti-HBs ≥10 mUI/ml). Among 3165 participants aged from 0 to 94 years, the prevalence rates of hepatitis B surface antigen (HBsAg), and hepatitis B core antibody (total anti-HBc) were 1.2% [95% confidence interval (CI) 0.85-1.64%], and 41.67% (95% CI 39.95-43.41%), respectively. The prevalence rate of anti-HBs at protective levels (≥10 mUI/ml) in individuals who HBsAg and anti-HBc negative was 66.36% (95% CI 64.15-68.51%). The prevalence rate of HBsAg in children aged <15 years was nil, and among adult HBsAg carriers, the prevalence of hepatitis D antibody (anti-HDV) was 5.26% (2/38; 95% CI 0.64-17.74). These findings showed that HBV prevalence has changed from high to low endemicity, 23 years following implementation of the vaccination program against hepatitis B, and HDV infection was not detected in those aged <30 years., Competing Interests: The authors have declared that no competing interests exist.

Published
2020
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85. Seroepidemiology of hepatitis A, B, C, D and E virus infections in the general population of Peru: A cross-sectional study.

Author

Cabezas C, Trujillo O, Gonzales-Vivanco Á, Benites Villafane CM, Balbuena J, Borda-Olivas AO, Suarez-Jara MA, Peceros FM, and Ramírez-Soto MC

Subjects
Adolescent, Adult, Aged, Antibodies, Viral immunology, Cross-Sectional Studies, Female, Hepatitis A epidemiology, Hepatitis B epidemiology, Hepatitis C epidemiology, Hepatitis D epidemiology, Hepatitis E epidemiology, Humans, Male, Middle Aged, Peru epidemiology, Prevalence, Young Adult, Hepatitis, Viral, Human epidemiology, Seroepidemiologic Studies
Abstract

Background: Viral hepatitis (hepatitis A, B, C, D and E) remains a public health problem in Peru, with a high disease burden. There are limited data on the prevalence of viral hepatitis at a national level, and none reported for over two decades. In this study, the prevalence rates of hepatitis A (HAV), B (HBV), C (HCV), D (HDV) and E virus (HEV) infections in the Peruvian population were determined to provide updated baseline data that would help guide the development of strategies aimed at reducing the transmission of viral hepatitis in Peru., Methods: We conducted a cross-sectional, population-based study in the 25 regions of Peru. The study included participants of both sexes, aged 15-69 years, who had lived for >6 months in a specific region of Peru. Serum samples were analyzed by ELISA for anti-HAV (IgG), anti-HBs ≥10 mUI/ml, anti-HCV, anti-HDV and anti-HEV (IgG) antibodies, and by chemiluminescence for the HBV surface antigen (HBsAg) and antibodies against the core HBV antigen (anti-HBc IgM and IgG)., Results: In a total of 5183 study participants, the prevalence rates of anti-HAV (IgG), HBsAg, total anti-HBc IgG, anti-HBs ≥10 mUI/ml, anti-HCV and anti-HEV (IgG) were 98.4% [95% confidence interval (CI) 98.0-98.7), 0.4% (95% CI 0.21-0.55), 10.1% (95% CI 9.4-11.0), 60% (95% CI 58.5-61.2), 0.1% (95% CI 0.02-0.25), and 14% (95% CI 13.1-15.0%), respectively. The prevalence of anti-HDV among HBsAg carriers was 15% (3/20)., Conclusions: The prevalence of HAV and HEV in the population aged 15-69 years in Peru is high, while the prevalence of HBV and HDV has changed from intermediate to low endemicity level and the prevalence of HCV is low. These findings would prove useful in the development of new strategies aimed at reducing the transmission of viral hepatitis in Peru, with a view to ultimately eliminating these infections in the future., Competing Interests: The authors have declared that no competing interests exist.

Published
2020
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86. [Reduction of HBV and HDV infection in two indigenousmpeoples of Peruvian Amazon after the vaccination against hepatitis B].

Author

Cabezas C, Trujillo O, Balbuena J, Terrazas M, Manrique-de Lara C, Marín L, and Ramírez-Soto MC

Subjects
Adolescent, Adult, Age Distribution, Child, Child, Preschool, Cross-Sectional Studies, Female, Hepatitis B immunology, Hepatitis B prevention & control, Hepatitis B Antibodies blood, Hepatitis B Surface Antigens blood, Hepatitis B e Antigens blood, Hepatitis B virus immunology, Hepatitis D immunology, Hepatitis D prevention & control, Hepatitis Delta Virus immunology, Humans, Immunoglobulin G blood, Immunoglobulin M blood, Indians, South American ethnology, Infant, Male, Middle Aged, Peru epidemiology, Prevalence, Sex Distribution, Young Adult, Hepatitis Antibodies blood, Hepatitis B epidemiology, Hepatitis B Vaccines administration & dosage, Hepatitis D epidemiology, Indians, South American statistics & numerical data
Abstract

Objective: To determine the outcome of the vaccination against hepatitis, we determined the prevalence of hepatitis B virus (HBV) and hepatitis D virus (HDV) infections, eight years after introduction of the vaccination., Materials and Methods: A cross-sectional study was performed in 2 944 participants of 67 Kandozi and Chapra indigenous peoples in April 2010. Serological screening for hepatitis B surface antigen (HBsAg), antibody anti-HBc IgM and IgG, antibody anti-HBs and anti-HDV were determined by ELISA tests., Results: The prevalence rates of HBsAg, anti-HBc total, anti- HBs ≥10 mlUI/ml and anti-HDV were 2.3, 39.13, 50.95 and 2.11%, respectively. The prevalence rate of HBsAg in children <11 years was 0%. Among carriers of HBsAg, the prevalence rates of HDV and acute HBV infections were 2.11% (all were >14 years) and 11.94%, respectively. HBsAg and anti-HBc total were associated with individuals ≥10 years (p<0.001)., Conclusions: These findings show the elimination of HBVmcarriers in children <11 years, eight years following introduction of the vaccination against HBV., Competing Interests: Declaration of conflict of interests. The authors declare that they have no conflict of interests.

Published
2020
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87. Prevalence of retrovirus, hepatitis B and D infection in the Matsés ethnic group in Loreto, Peru.

Author

Cabezas C, Trujillo O, Balbuena J, Marin L, Suárez M, Themme M, Rodriguez H, Valencia P, and Crispin-Huamani L

Subjects
Child, Cross-Sectional Studies, HIV Infections ethnology, HTLV-I Infections ethnology, HTLV-II Infections ethnology, Humans, Peru epidemiology, Prevalence, Ethnicity statistics & numerical data, Hepatitis B ethnology, Hepatitis D ethnology, Retroviridae Infections ethnology
Abstract

Observational, cross-sectional, populational study to determine the prevalence of infection by hepatitis B virus (HBV), hepatitis D virus (HDV), human immunodeficiency virus (HIV) and human T-lymphotropic virus type 1 and 2 (HTLV-1/2) in the Matsés ethnic group, after immunization against HBV. ELISA and qPCR tests were used in 963 residents. The prevalence of HBsAg, Anti-HBc and Anti-HBs was 3.32%, 36.03% and 58.67% respectively. In 3.1% of the population the viral load was greater than 2000 IU/mL. In children under 10 years, the prevalence of HBsAg and anti-HBc was 0.0% and 2.6%, respectively, while protective antibodies were found in 94.4%. The prevalence of HIV and HTLV-1/2 infection was 1.5% and 0.6%, respectively. It is therefore concluded that there are low rates of HBV and HDV infection in the Matsés child population. Likewise, the presence of HIV and HTLV-1/2 infection is confirmed.

Published
2020
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88. Photochemical emission and fixation of NO X gases in soils.

Author

Barrón V, Méndez JM, Balbuena J, Cruz-Yusta M, Sánchez L, Giménez C, Sacristán D, González-Guzmán A, Sánchez-Rodríguez AR, Skiba UM, Inda AV, Marques J Jr, Recio JM, Delgado A, Del Campillo MC, and Torrent J

Abstract

Gaseous nitrogen oxides (NOx), which result from the combustion of fossil fuels, volcanic eruptions, forest fires, and biological reactions in soils, not only affect air quality and the atmospheric concentration of ozone, but also contribute to global warming and acid rain. Soil NOx emissions have been largely ascribed to soil microbiological processes; but there is no proof of abiotic catalytic activity affecting soil NO emissions. We provide evidence of gas exchange in soils involving emissions of NOx by photochemical reactions, and their counterpart fixation through photocatalytic reactions under UV-visible irradiation. The catalytic activity promoting NOx capture as nitrate varied widely amongst different soil types, from low in quartzitic sandy soils to high in iron oxide and TiO 2 rich soils. Clay soils with significant amounts of smectite also exhibited high rates of NOx sequestration and fixed amounts of N comparable to that of NO (nitric oxide) losses through biotic reactions. In these soils, a flux of 100 µg N NO m -2  h -1 , as usually found in most ecosystems, could be reduced by these photochemical reactions by more than 60%. This mechanism of N fixation provides new insight into the nitrogen cycle and may inspire alternative strategies to reduce NO emissions from soils., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published
2020
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89. Use of Steel Industry Wastes for the Preparation of Self-Cleaning Mortars.

Author

Balbuena J, Sánchez L, and Cruz-Yusta M

Abstract

An important problem, which must be solved, is the accumulation of industrial waste in landfills. Science has an obligation to transform this waste into new products and, if possible, with high added value. In this sense, we propose the valorization of the waste which is generated in the steel lamination process (HSL) through its conversion into a new material with photocatalytic activity which is suitable for use as an additive to obtain a self-cleaning construction material. The valorization of steel husk lamination waste is achieved through a grinding process, which allows the sample to be homogenized, in size, without altering its phase composition, and a thermal treatment that turns it into iron oxide, which acts as a photocatalyst. These residues, before and after treatment, were characterized by different techniques such as PXRD (Powder X-Ray Diffraction), TGA (Thermogravimetric Analysis), SBET (Specific surface area, Brunauer-Emmett-Teller), SEM (Scanning Electron Microscopy) and Diffuse reflectance (DR). MB and RhB tests show that this material is capable of self-cleaning, both of the material itself and when it is incorporated into a construction material (mortar). In addition, the NO x gas elimination test shows that it is also capable of acting on greenhouse gases such as NO x .

Published
2019
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90. Mesocrystalline anatase nanoparticles synthesized using a simple hydrothermal approach with enhanced light harvesting for gas-phase reaction.

Author

Balbuena J, Calatayud JM, Cruz-Yusta M, Pardo P, Martín F, Alarcón J, and Sánchez L

Abstract

Mesocrystalline TiO2 nanoparticles were synthesized using a hydrothermal approach. A simple two-step procedure at low temperature (<140 °C) allowed the nucleation of primary particles sized 2-4 nm and their subsequent assembly as almost spherical aggregates sized ≈20 nm. X-ray powder diffraction (XRD), Raman and X-ray photoelectron spectroscopy (XPS) studies, and HRTEM studies confirmed anatase as the unique TiO2 crystalline phase. The mesocrystalline structure of the anatase aggregates was clearly evidenced by HRTEM and SAED results. The mesocrystalline nanopowders exhibit a mesoporous structure with a surface area and pore volume of 63.5 m2 g-1 and 0.22 cm3 g-1, respectively. Ultraviolet (UV) and visible light (Vis) absorption ability were recorded. The combined high effectiveness and selectivity for the NOx abatement of the new mesocrystalline photocatalyst are reported. It is worth remarking that the maximised selectivity values reached for the NOx process are reported for the first time and could be associated with the mesoporous nature of the anatase photocatalyst.

Published
2018
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91. Peritoneal tuberculosis in patients with rheumatoid arthritis undergoing adalimumab treatment.

Author

Ortiz Balbuena J, Muñez Rubio E, and Ramos Martínez A

Subjects
Adalimumab therapeutic use, Adult, Antirheumatic Agents therapeutic use, Arthritis, Rheumatoid complications, Female, Humans, Opportunistic Infections complications, Peritonitis, Tuberculous complications, Adalimumab adverse effects, Antirheumatic Agents adverse effects, Arthritis, Rheumatoid drug therapy, Opportunistic Infections diagnosis, Peritonitis, Tuberculous diagnosis
Published
2017
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92. Characteristics of Clostridium difficile infection in patients with discordant diagnostic test results.

Author

Ramos Martínez A, Ortiz Balbuena J, Asensio Vegas Á, Sánchez Romero I, Múñez Rubio E, Cantero Caballero M, Cózar Llistó A, Portero Azorín F, and Martínez Ruiz R

Subjects
Adult, Aged, Diagnostic Tests, Routine, Diarrhea etiology, Female, Glutamate Dehydrogenase blood, Humans, Immunoenzyme Techniques, Male, Middle Aged, Polymerase Chain Reaction, Retrospective Studies, Clostridioides difficile, Enterocolitis, Pseudomembranous diagnosis
Abstract

Background: Clinical features of Clostridium difficile infection (CDI) cases diagnosed by detection of polymerase chain reaction (PCR), with negative toxin enzyme immunoassay results (EIA) have not been fully elucidated. The purpose of this study was to determine the magnitude of CDI patients who had negative EIA toxin determinations but positive PCR tests, and their differences in clinical presentation., Methods: We performed a retrospective study comparing the clinical features of CDI cases detected by EIA (toxins A + B) with cases detected by PCR (toxin negative, PCR positive) over a 16-month period. Only patients with an initial Clostridium difficile infection episode that fulfilled a standardized definition were included., Results: During the study period, 107 episodes of CDI were detected. Seventy-four patients (69%) had positive glutamate dehydrogenase (GDH) antigen and EIA determinations (EIA positive patients). Thirty-three patients (31%) had GDH positive, negative toxin EIA and positive PCR determination (PCR positive patients). PCR positive patients were younger, 57 (27) years (mean [SD]), than EIA positive patients, 71 (16) years, (p < 0.001). Fewer PCR positive patients were receiving proton pump inhibitors (21 patients, 64%) than EIA positive patients (61 patients, 82%, p = 0.034). The clinical presentation was similar in both groups. In the multivariate analysis, lower age was identified as the only independent variable associated with PCR positive patients., Conclusions: One third of Clostridium difficile infection patients present negative toxin EIA and PCR positive tests. Performing PCR determination after the negative EIA test is more relevant in younger patients.

Published
2016
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93. [Vogt-Koyanagi-Harada disease].

Author

Ortiz Balbuena J, Tutor de Ureta P, Rivera Ruiz E, and Mellor Pita S

Subjects
Adult, Delayed Diagnosis, Female, Glucocorticoids therapeutic use, Headache etiology, Humans, Meningitis, Aseptic etiology, Phenotype, Retinal Detachment etiology, Retrospective Studies, Uveomeningoencephalitic Syndrome blood, Uveomeningoencephalitic Syndrome diagnosis, Uveomeningoencephalitic Syndrome drug therapy, Uveomeningoencephalitic Syndrome epidemiology
Published
2016
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94. [Microbiology of pressure and vascular ulcer infections].

Author

Ortiz Balbuena J, García Madero R, Segovia Gómez T, Cantero Caballero M, Sánchez Romero I, and Ramos Martínez A

Subjects
Adult, Aged, Aged, 80 and over, Cross-Sectional Studies, Female, Humans, Male, Middle Aged, Bacteria isolation & purification, Pressure Ulcer microbiology, Ulcer microbiology, Vascular Diseases microbiology
Abstract

Introduction: Pressure ulcer (PU) infection is a significant clinical problem in many elderly patients., Material and Methods: To determine the microbiology of PU and vascular ulcer (VU) infections by conducting a cross-sectional study of outpatients treated in a chronic wounds unit over an 18 month period., Results: Sixty six patients with PU infection and 159 patients with an infected VU were identified. The PUs were located below the knee in 36 patients (52%). Patients with pressure ulcers had a higher proportion of institutionalization, cognitive impairment, inability to walk, and sphincter incontinence. There was a greater number of infections caused by Enterobacteriaceae (52%, P=.002) and fewer S. aureus infections (24%, P<.001) in patients with a PU compared to those with those with a VU. Forty-one percent of S. aureus strains isolated in all the patients were resistant to methicillin (MRSA). The proportion of Enterobacteriaceae infections was similar in patients with infection of pelvic girdle PU and in those located below the knee., Conclusions: PU patients suffer a higher rate of infection by enterobacteria. The most common pathogen in UV infections is S. aureus. The proportion of MRSA infection in patients with chronic wounds is high. The microbiology of the infection in the pelvic girdle PU is similar to those located below the knee., (Copyright © 2014 SEGG. Published by Elsevier Espana. All rights reserved.)

Published
2015
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95. Risk factors for Clostridium difficile diarrhea in patients with inflammatory bowel disease.

Author

Ramos-Martínez A, Ortiz-Balbuena J, Curto-García I, Asensio-Vegas Á, Martínez-Ruiz R, Múñez-Rubio E, Cantero-Caballero M, Sánchez-Romero I, González-Partida I, and Vera-Mendoza MI

Subjects
Adult, Age Factors, Community-Acquired Infections, Cross Infection, Diarrhea drug therapy, Diarrhea etiology, Enterocolitis, Pseudomembranous complications, Enterocolitis, Pseudomembranous drug therapy, Female, Humans, Inflammatory Bowel Diseases complications, Inflammatory Bowel Diseases drug therapy, Male, Middle Aged, Prospective Studies, Proton Pump Inhibitors therapeutic use, Risk Factors, Clostridioides difficile, Diarrhea microbiology, Enterocolitis, Pseudomembranous microbiology, Inflammatory Bowel Diseases microbiology
Abstract

Background: Despite the growing incidence of Clostridium difficile diarrhea (CCD) in patients with inflammatory bowel disease (IBD), little is known about the associated risk factors., Method: A retrospective study comparing cases of CCD in patients with IBD to IBD carriers who did not develop CCD. A comparison was also made with patients who developed CCD but did not suffer IBD., Results: Three cases (20%) with IBD and CCD had received antibiotics during the previous three months versus none of the controls (IBD without CCD, p = 0.22). Ten cases (67%) received treatment with proton pump inhibitors (PPIs) versus 2 (13%) in the control group (IBD without CCD, p = 0.001). Seven cases underwent colonoscopy and pseudomembranes were seen in one (14%). Fourteen (93%) patients demonstrated a favourable response to metronidazole. Patients with IBD and CCD presented with younger age (36 ± 10 years), a higher degree of community-acquired infection (13 patients, 87%), immunosuppressive treatment (7 patients, 47%) and less patients had received previous antibiotic treatment (3 patients, 20%) than those with CCD without IBD. The proportion of patients who received treatment with PPIs was similar (66% and 80%, respectively p = 0.266)., Conclusions: CCD in IBD carriers affects younger patients, the majority are community acquired (less nosocomial) and it is more related to previous treatment with PPIs than with the antibiotic treatment. Clinical evolution is also favourable.

Published
2015

96. ABCG2 is required to control the sonic hedgehog pathway in side population cells with stem-like properties.

Author

Balbuena J, Pachon G, Lopez-Torrents G, Aran JM, Castresana JS, and Petriz J

Subjects
ATP Binding Cassette Transporter, Subfamily G, Member 2, Benzimidazoles analysis, Blotting, Western, Carbazoles pharmacology, Flow Cytometry, Hedgehog Proteins metabolism, Humans, Hydroxycholesterols pharmacology, Indole Alkaloids pharmacology, KB Cells, Mitoxantrone metabolism, Patched Receptors, Receptors, Cell Surface metabolism, Side-Population Cells drug effects, Signal Transduction, Transfection, ATP-Binding Cassette Transporters metabolism, Hedgehog Proteins antagonists & inhibitors, Neoplasm Proteins metabolism, Side-Population Cells metabolism, Veratrum Alkaloids pharmacology
Abstract

The Sonic Hedgehog (Hh) pathway has been implicated in the maintenance of stem or progenitor cells in many adult tissues. Importantly, abnormal Hh pathway activation is also associated with initiation of neoplasia, but its role in tumor growth is still unclear. Here, we demonstrate that cyclopamine, a plant-derived alkaloid product used to inhibit the Hh signaling pathway, reduces the Side Population (SP) obtained by Hoechst 33342 (Ho342) dye measurements. In addition, cyclopamine is able to modulate, along with oxysterols and other products, the ABCG2 transporter by increasing Ho342 and mitoxantrone uptake. Therefore, if the SP is solely measured as a Ho342 dye extruding fraction, this may be significantly modulated by the inhibition of ABCG2 transport fraction, independently from the action of cyclopamine on the Hh pathway. Our results indicate that ABCG2 may act in the upstream regulation of the Hh signaling pathway to protect the stemness of the SP compartment, giving support to the cancer stem cell hypothesis and suggesting that ABCG2 is not only critical for increased resistance to anticancer agents., (Copyright © 2011 International Society for Advancement of Cytometry.)

Published
2011
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97. Analysis of stemness gene expression and CD133 abnormal methylation in neuroblastoma cell lines.

Author

Schiapparelli P, Enguita-Germán M, Balbuena J, Rey JA, Lázcoz P, and Castresana JS

Subjects
AC133 Antigen, Antigens, CD biosynthesis, Cell Line, Tumor, Epigenomics, Flow Cytometry, Gene Expression Regulation, Neoplastic, Glycoproteins biosynthesis, Humans, Neoplastic Stem Cells metabolism, Neoplastic Stem Cells pathology, Neuroblastoma metabolism, Neuroblastoma pathology, Reverse Transcriptase Polymerase Chain Reaction, Antigens, CD genetics, DNA Methylation, Glycoproteins genetics, Neoplastic Stem Cells physiology, Neuroblastoma genetics, Peptides genetics
Abstract

Neuroblastoma is the most common extracranial solid tumor in children, accounting for up to 10% of all childhood malignancies. Cellular heterogeneity is a hallmark of this embryonal cancer, as distinct neural crest lineages can be found within the same tumor sample. The aim of our study was to investigate the presence of a subpopulation of immature cells with features of cancer-like stem cells in 10 neuroblastoma cell lines. RT-PCR and flow cytometry were performed in order to analyze different kinds of 'stemness genes' such as: NESTIN (NES), CD133, SOX-2, BMI1, c-KIT, MELK1, MUSASHI-1 (MSI1), FAS, CD44 and VIMENTIN (VIM). In addition, glial and neuronal markers such as NCAM1, GFAP and B-TUBULIN III (TUBB3) were analyzed. Epigenetic changes within the CD133 (Prominin-1) gene promoter were also analyzed. Neuroblastoma cell lines showed a particular pattern of expression, suggesting the presence of an immature cancer stem cell-like subpopulation. The CD133 protein, commonly used to enrich putative cancer propagating stem cell-like populations in different kinds of solid tumors, presented a half-methylated DNA state in 7 of the 12 neuroblastoma cell lines analyzed. An increase in RNA and protein levels of CD133 was achieved following demethylation by assays using 5-aza-2'-deoxycytidine (5-Aza-dC). Since cancer stem cells are believed to be responsible for tumor metastasis, escape from anticancer therapies and disease relapse, their therapeutic targeting and analysis is crucial in neuroblastoma. Moreover, the regulation of CD133 by epigenetic changes may provide an innovative mechanism of CD133 expression as its regulation still remains unclear.

Published
2010
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98. Growth and emigration of third-stage larvae of Hysterothylacium aduncum (Nematoda: Anisakidae) in larval herring Clupea harengus.

Author

Balbuena JA, Karlsbakk E, Kvenseth AM, Saksvik M, and Nylund A

Subjects
Animals, Ascaridida Infections parasitology, Ascaridoidea growth & development, Female, Fishes, Larva growth & development, Larva parasitology, Larva physiology, Male, Ascaridida Infections veterinary, Ascaridoidea physiology, Fish Diseases parasitology
Abstract

The growth and emigration of Hystherothylacium aduncum in laboratory-reared herring larvae Clupea harengus was studied. Experimental infections of 36-day-old herring larvae resulted in 126 hosts infected with 306 H. aduncum larvae. Regression analyses showed a significant worm emigration from the rectum to the head of the fish, accompanied by an increase in worm body length. The emigration was independent of worm intensity, which suggests an ontogenetic process. Some worms departed from this pattern by moving posteriorly or by penetrating into the muscle, and in 5 cases, the larvae were observed to leave living fish. This individual variation has not been observed in previous studies and might be explained by host signals related to condition or development stage. Indirect evidence suggested parasite-induced mortality in the tanks due to the emigrations because only 4 of the 126 infected fish survived 8 days postinfection; the emigration of H. aduncum affected vital organs, such as the heart and brain, and the larvae penetrating or leaving the host's tissues can cause extensive damage to the delicate herring larvae.

Published
2000
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99. Anisakid larvae in the musculature of the Argentinean hake, Merluccius hubbsi.

Author

Herreras MV, Aznar FJ, Balbuena JA, and Raga JA

Subjects
Animals, Anisakiasis epidemiology, Anisakiasis parasitology, Anisakis growth & development, Argentina epidemiology, Fish Diseases parasitology, Fishes, Larva, Prevalence, Spain, Anisakiasis veterinary, Anisakis isolation & purification, Fish Diseases epidemiology, Food Microbiology, Muscles parasitology, Seafood parasitology
Abstract

We report the infection levels of third-stage anisakid larva in the muscle of the Argentinean hake, Merluccius hubbsi, in relation to fish size and location in the musculature. The musculature of 42 hake was separated into hypaxial (ventral) and epiaxial (dorsal) parts and surveyed for nematode larvae. Two anisakid species were detected: Anisakis sp. (prevalence, 52.4%; mean +/- SD abundance, 1.2 +/- 1.7) and Pseudoterranova sp. (prevalence, 9.5%; mean +/- SD abundance, 0.2 +/- 0.7). Since the fish were gutted after capture, the occurrence of anisakids in the flesh indicates that the worms had migrated into the muscle before capture. The number of Anisakis sp. in muscle was not correlated with fish length or weight. Therefore, fish size cannot be used as a predictor of parasite loads in the muscle. Only one Anisakis sp. and one Pseudoterranova sp. appeared in the epiaxial musculature. The density of Anisakis sp. in the hypaxial muscles was significantly higher than that in the epiaxial ones. This suggests that removal of the hypaxial musculature can reduce the risk of anisakid-induced allergies and gastrointestinal anisakidoses among consumers.

Published
2000
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100. The impact of parasites on marine mammals: a review.

Author

Raga JA, Balbuena JA, Aznar J, and Fernández M

Subjects
Animals, Host-Parasite Interactions, Parasitic Diseases, Animal mortality, Parasitic Diseases, Animal parasitology, Periodicity, Population Dynamics, Caniformia parasitology, Cetacea parasitology, Marine Biology, Parasitic Diseases, Animal epidemiology
Abstract

The design and implementation of conservation plans for marine mammals is a matter of public concern. However, very little is known about the role of parasites in the dynamics of marine mammal populations. This is probably due to methodological constraints concerning sampling biases, poor knowledge of the biology of the hosts and parasites and difficulty and costy of experimental studies. However, current evidence supports the theory that parasites may regulate marine mammal populations. Crassicauda species in cetaceans and Uncinaria lucasi in pinnipeds seem good candidates as regulating agents. In addition, parasite-induced mass mortalities may be important in marine mammal populations. Well documented cases are the PDV virus which decimated the European common seal (Phoca vitulina) populations in 1988 and the Mediterranean striped dolphin (Stenella coeruleoalba) morbillivirus infection of 1990-1992. Due to the social organisation patterns of marine mammals it is possible that such die-offs occur at very low densities, representing a potential threat to endangered species like the Mediterranean monk seal (Monachus monachus), the Hawaiian monk seal (M. schauinslandi) or the Finish Saimaa seal (Phoca hispida saimensis). It is concluded that parasites can play an important role in marine mammal populations not only at the ecological scale but at the evolutionary one too.

Published
1997

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