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1. Adipose tissue in evolution

Author

Fantuzzi, G, Braunschweig, C, Fantuzzi, G ( G ), Braunschweig, C ( C ), Isler, Karin, Fantuzzi, G, Braunschweig, C, Fantuzzi, G ( G ), Braunschweig, C ( C ), and Isler, Karin

Published
2014

2. Differential susceptibility to lethal endotoxaemia in mice deficient in IL-1alpha, IL-1beta or IL-1 receptor type I.

Author

Joosten, L.A.B., Veerdonk, F.L. van de, Vonk, A.G., Boerman, O.C., Keuter, M., Fantuzzi, G., Verschueren, I., Poll, T. van der, Dinarello, C.A., Kullberg, B.J., Meer, J.W.M. van der, Netea, M.G., Joosten, L.A.B., Veerdonk, F.L. van de, Vonk, A.G., Boerman, O.C., Keuter, M., Fantuzzi, G., Verschueren, I., Poll, T. van der, Dinarello, C.A., Kullberg, B.J., Meer, J.W.M. van der, and Netea, M.G.

Abstract

01 december 2010, Contains fulltext : 88883.pdf (publisher's version ) (Closed access), The role of intereukin-1 (IL-1) in mortality caused by endotoxaemia remains controversial. While IL-1 receptor antagonist (IL-1Ra) protects mice from lethal endotoxaemia, mice deficient in IL-1beta (IL-1beta( /)) display normal susceptibility to lipopolysaccharide (LPS). The aim of this study was to identify the source of these discrepancies. Mice deficient in IL-1alpha, IL-1beta or IL-1R type I were injected intraperitoneally with Escherichia coli or Salmonella typhimurium LPS. Survival of the mice was examined and compared with C57/Bl6 wild-type mice. In addition, serum cytokine concentrations were determined after LPS challenge and in vitro cytokine production by peritoneal macrophages was analysed. Clearance of radioactive IL-1alpha was examined in IL-1alpha(/) and wild-type mice. IL-1beta(/) mice were normally susceptible to endotoxaemia and cytokine production did not differ from that in control mice. Surprisingly, LPS mortality in IL-1alpha(/) mice was significantly greater than that in control mice, accompanied by higher interferon-gamma release. These effects were mediated by a distorted homeostasis of IL-1RI receptors, as shown by a strongly delayed clearance of IL-1alpha. In contrast to the IL-1alpha(/) and IL-1beta(/) mice, IL-1RI(/) mice were completely resistant to high doses of LPS. In conclusion, IL-1RI-mediated signals are crucial in mediating mortality occurring as a result of lethal endotoxaemia. Investigation of IL-1-mediated pathways in IL-1 knock-out mice is complicated by a distorted homeostasis of IL-1Rs.

Published
2010

3. The inflammasome-mediated caspase-1 activation controls adipocyte differentiation and insulin sensitivity.

Author

Stienstra, R., Joosten, L.A.B., Koenen, T.B., Tits, B. van, Diepen, J.A. van, Berg, S.W. van den, Rensen, P.C., Voshol, P.J., Fantuzzi, G., Hijmans, A.G.M., Kersten, S., Muller, M., Berg, W.B. van den, Rooijen, N. van, Wabitsch, M., Kullberg, B.J., Meer, J.W.M. van der, Kanneganti, T., Tack, C.J.J., Netea, M.G., Stienstra, R., Joosten, L.A.B., Koenen, T.B., Tits, B. van, Diepen, J.A. van, Berg, S.W. van den, Rensen, P.C., Voshol, P.J., Fantuzzi, G., Hijmans, A.G.M., Kersten, S., Muller, M., Berg, W.B. van den, Rooijen, N. van, Wabitsch, M., Kullberg, B.J., Meer, J.W.M. van der, Kanneganti, T., Tack, C.J.J., and Netea, M.G.

Abstract

Contains fulltext : 87798.pdf (publisher's version ) (Closed access), Obesity-induced inflammation originating from expanding adipose tissue interferes with insulin sensitivity. Important metabolic effects have been recently attributed to IL-1beta and IL-18, two members of the IL-1 family of cytokines. Processing of IL-1beta and IL-18 requires cleavage by caspase-1, a cysteine protease regulated by a protein complex called the inflammasome. We demonstrate that the inflammasome/caspase-1 governs adipocyte differentiation and insulin sensitivity. Caspase-1 is upregulated during adipocyte differentiation and directs adipocytes toward a more insulin-resistant phenotype. Treatment of differentiating adipocytes with recombinant IL-1beta and IL-18, or blocking their effects by inhibitors, reveals that the effects of caspase-1 on adipocyte differentiation are largely conveyed by IL-1beta. Caspase-1 and IL-1beta activity in adipose tissue is increased both in diet-induced and genetically induced obese animal models. Conversely, mice deficient in caspase-1 are more insulin sensitive as compared to wild-type animals. In addition, differentiation of preadipocytes isolated from caspase-1(-/-) or NLRP3(-/-) mice resulted in more metabolically active fat cells. In vivo, treatment of obese mice with a caspase-1 inhibitor significantly increases their insulin sensitivity. Indirect calorimetry analysis revealed higher fat oxidation rates in caspase-1(-/-) animals. In conclusion, the inflammasome is an important regulator of adipocyte function and insulin sensitivity, and caspase-1 inhibition may represent a novel therapeutic target in clinical conditions associated with obesity and insulin resistance.

Published
2010

4. Differential susceptibility to lethal endotoxaemia in mice deficient in IL-1alpha, IL-1beta or IL-1 receptor type I.

Author

Joosten, L.A.B., Veerdonk, F.L. van de, Vonk, A.G., Boerman, O.C., Keuter, M., Fantuzzi, G., Verschueren, I., Poll, T. van der, Dinarello, C.A., Kullberg, B.J., Meer, J.W.M. van der, Netea, M.G., Joosten, L.A.B., Veerdonk, F.L. van de, Vonk, A.G., Boerman, O.C., Keuter, M., Fantuzzi, G., Verschueren, I., Poll, T. van der, Dinarello, C.A., Kullberg, B.J., Meer, J.W.M. van der, and Netea, M.G.

Abstract

01 december 2010, Contains fulltext : 88883.pdf (publisher's version ) (Closed access), The role of intereukin-1 (IL-1) in mortality caused by endotoxaemia remains controversial. While IL-1 receptor antagonist (IL-1Ra) protects mice from lethal endotoxaemia, mice deficient in IL-1beta (IL-1beta( /)) display normal susceptibility to lipopolysaccharide (LPS). The aim of this study was to identify the source of these discrepancies. Mice deficient in IL-1alpha, IL-1beta or IL-1R type I were injected intraperitoneally with Escherichia coli or Salmonella typhimurium LPS. Survival of the mice was examined and compared with C57/Bl6 wild-type mice. In addition, serum cytokine concentrations were determined after LPS challenge and in vitro cytokine production by peritoneal macrophages was analysed. Clearance of radioactive IL-1alpha was examined in IL-1alpha(/) and wild-type mice. IL-1beta(/) mice were normally susceptible to endotoxaemia and cytokine production did not differ from that in control mice. Surprisingly, LPS mortality in IL-1alpha(/) mice was significantly greater than that in control mice, accompanied by higher interferon-gamma release. These effects were mediated by a distorted homeostasis of IL-1RI receptors, as shown by a strongly delayed clearance of IL-1alpha. In contrast to the IL-1alpha(/) and IL-1beta(/) mice, IL-1RI(/) mice were completely resistant to high doses of LPS. In conclusion, IL-1RI-mediated signals are crucial in mediating mortality occurring as a result of lethal endotoxaemia. Investigation of IL-1-mediated pathways in IL-1 knock-out mice is complicated by a distorted homeostasis of IL-1Rs.

Published
2010

5. The inflammasome-mediated caspase-1 activation controls adipocyte differentiation and insulin sensitivity.

Author

Stienstra, R., Joosten, L.A.B., Koenen, T.B., Tits, B. van, Diepen, J.A. van, Berg, S.W. van den, Rensen, P.C., Voshol, P.J., Fantuzzi, G., Hijmans, A.G.M., Kersten, S., Muller, M., Berg, W.B. van den, Rooijen, N. van, Wabitsch, M., Kullberg, B.J., Meer, J.W.M. van der, Kanneganti, T., Tack, C.J.J., Netea, M.G., Stienstra, R., Joosten, L.A.B., Koenen, T.B., Tits, B. van, Diepen, J.A. van, Berg, S.W. van den, Rensen, P.C., Voshol, P.J., Fantuzzi, G., Hijmans, A.G.M., Kersten, S., Muller, M., Berg, W.B. van den, Rooijen, N. van, Wabitsch, M., Kullberg, B.J., Meer, J.W.M. van der, Kanneganti, T., Tack, C.J.J., and Netea, M.G.

Abstract

Contains fulltext : 87798.pdf (publisher's version ) (Closed access), Obesity-induced inflammation originating from expanding adipose tissue interferes with insulin sensitivity. Important metabolic effects have been recently attributed to IL-1beta and IL-18, two members of the IL-1 family of cytokines. Processing of IL-1beta and IL-18 requires cleavage by caspase-1, a cysteine protease regulated by a protein complex called the inflammasome. We demonstrate that the inflammasome/caspase-1 governs adipocyte differentiation and insulin sensitivity. Caspase-1 is upregulated during adipocyte differentiation and directs adipocytes toward a more insulin-resistant phenotype. Treatment of differentiating adipocytes with recombinant IL-1beta and IL-18, or blocking their effects by inhibitors, reveals that the effects of caspase-1 on adipocyte differentiation are largely conveyed by IL-1beta. Caspase-1 and IL-1beta activity in adipose tissue is increased both in diet-induced and genetically induced obese animal models. Conversely, mice deficient in caspase-1 are more insulin sensitive as compared to wild-type animals. In addition, differentiation of preadipocytes isolated from caspase-1(-/-) or NLRP3(-/-) mice resulted in more metabolically active fat cells. In vivo, treatment of obese mice with a caspase-1 inhibitor significantly increases their insulin sensitivity. Indirect calorimetry analysis revealed higher fat oxidation rates in caspase-1(-/-) animals. In conclusion, the inflammasome is an important regulator of adipocyte function and insulin sensitivity, and caspase-1 inhibition may represent a novel therapeutic target in clinical conditions associated with obesity and insulin resistance.

Published
2010

6. Differential susceptibility to lethal endotoxaemia in mice deficient in IL-1alpha, IL-1beta or IL-1 receptor type I.

Author

Joosten, L.A.B., Veerdonk, F.L. van de, Vonk, A.G., Boerman, O.C., Keuter, M., Fantuzzi, G., Verschueren, I., Poll, T. van der, Dinarello, C.A., Kullberg, B.J., Meer, J.W.M. van der, Netea, M.G., Joosten, L.A.B., Veerdonk, F.L. van de, Vonk, A.G., Boerman, O.C., Keuter, M., Fantuzzi, G., Verschueren, I., Poll, T. van der, Dinarello, C.A., Kullberg, B.J., Meer, J.W.M. van der, and Netea, M.G.

Abstract

01 december 2010, Contains fulltext : 88883.pdf (publisher's version ) (Closed access), The role of intereukin-1 (IL-1) in mortality caused by endotoxaemia remains controversial. While IL-1 receptor antagonist (IL-1Ra) protects mice from lethal endotoxaemia, mice deficient in IL-1beta (IL-1beta( /)) display normal susceptibility to lipopolysaccharide (LPS). The aim of this study was to identify the source of these discrepancies. Mice deficient in IL-1alpha, IL-1beta or IL-1R type I were injected intraperitoneally with Escherichia coli or Salmonella typhimurium LPS. Survival of the mice was examined and compared with C57/Bl6 wild-type mice. In addition, serum cytokine concentrations were determined after LPS challenge and in vitro cytokine production by peritoneal macrophages was analysed. Clearance of radioactive IL-1alpha was examined in IL-1alpha(/) and wild-type mice. IL-1beta(/) mice were normally susceptible to endotoxaemia and cytokine production did not differ from that in control mice. Surprisingly, LPS mortality in IL-1alpha(/) mice was significantly greater than that in control mice, accompanied by higher interferon-gamma release. These effects were mediated by a distorted homeostasis of IL-1RI receptors, as shown by a strongly delayed clearance of IL-1alpha. In contrast to the IL-1alpha(/) and IL-1beta(/) mice, IL-1RI(/) mice were completely resistant to high doses of LPS. In conclusion, IL-1RI-mediated signals are crucial in mediating mortality occurring as a result of lethal endotoxaemia. Investigation of IL-1-mediated pathways in IL-1 knock-out mice is complicated by a distorted homeostasis of IL-1Rs.

Published
2010

7. The inflammasome-mediated caspase-1 activation controls adipocyte differentiation and insulin sensitivity

Author

Stienstra, R., Joosten, L.A., Koenen, T., van Tits, B., van Diepen, J.A., van den Berg, S.A.A., Rensen, P.C., Voshol, P.J., Fantuzzi, G., Hijmans, A., Kersten, A.H., Müller, M.R., van den Berg, W.B., van Rooijen, N., Wabitsch, M., Kullberg, B.J., van der Meer, J.W., Kanneganti, T., Tack, C.J., Netea, M.G., Stienstra, R., Joosten, L.A., Koenen, T., van Tits, B., van Diepen, J.A., van den Berg, S.A.A., Rensen, P.C., Voshol, P.J., Fantuzzi, G., Hijmans, A., Kersten, A.H., Müller, M.R., van den Berg, W.B., van Rooijen, N., Wabitsch, M., Kullberg, B.J., van der Meer, J.W., Kanneganti, T., Tack, C.J., and Netea, M.G.

Abstract

Obesity-induced inflammation originating from expanding adipose tissue interferes with insulin sensitivity. Important metabolic effects have been recently attributed to IL-1ß and IL-18, two members of the IL-1 family of cytokines. Processing of IL-1ß and IL-18 requires cleavage by caspase-1, a cysteine protease regulated by a protein complex called the inflammasome. We demonstrate that the inflammasome/caspase-1 governs adipocyte differentiation and insulin sensitivity. Caspase-1 is upregulated during adipocyte differentiation and directs adipocytes toward a more insulin-resistant phenotype. Treatment of differentiating adipocytes with recombinant IL-1ß and IL-18, or blocking their effects by inhibitors, reveals that the effects of caspase-1 on adipocyte differentiation are largely conveyed by IL-1ß. Caspase-1 and IL-1ß activity in adipose tissue is increased both in diet-induced and genetically induced obese animal models. Conversely, mice deficient in caspase-1 are more insulin sensitive as compared to wild-type animals. In addition, differentiation of preadipocytes isolated from caspase-1(-/-) or NLRP3(-/-) mice resulted in more metabolically active fat cells. In vivo, treatment of obese mice with a caspase-1 inhibitor significantly increases their insulin sensitivity. Indirect calorimetry analysis revealed higher fat oxidation rates in caspase-1(-/-) animals. In conclusion, the inflammasome is an important regulator of adipocyte function and insulin sensitivity, and caspase-1 inhibition may represent a novel therapeutic target in clinical conditions associated with obesity and insulin resistance

Published
2010

8. Inflammatory arthritis in caspase 1 gene-deficient mice: contribution of proteinase 3 to caspase 1-independent production of bioactive interleukin-1beta.

Author

Joosten, L.A.B., Netea, M.G., Fantuzzi, G., Koenders, M.I., Helsen, M.M.A., Sparrer, H., Pham, C.T., Meer, J.W.M. van der, Dinarello, C.A., Berg, W.B. van den, Joosten, L.A.B., Netea, M.G., Fantuzzi, G., Koenders, M.I., Helsen, M.M.A., Sparrer, H., Pham, C.T., Meer, J.W.M. van der, Dinarello, C.A., and Berg, W.B. van den

Abstract

Contains fulltext : 80189.pdf (publisher's version ) (Closed access), OBJECTIVE: Caspase 1, a known cysteine protease, is a critical component of the inflammasome. Both caspase 1 and neutrophil serine proteases such as proteinase 3 (PR3) can process pro-interleukin-1beta (proIL-1beta), a crucial cytokine linked to the pathogenesis of rheumatoid arthritis. This study was undertaken to establish the relative importance of caspase 1 and serine proteases in mouse models of acute and chronic inflammatory arthritis. METHODS: Acute and chronic arthritis were induced in caspase 1-/- mice, and the lack of caspase 1 was investigated for its effects on joint swelling, cartilage metabolism, and histopathologic features. In addition, caspase 1 activity was inhibited in mice lacking active cysteine proteases, and the effects of dual blockade of caspase 1 and serine proteases on arthritis severity and histopathologic features were evaluated. RESULTS: Surprisingly, caspase 1-/- mice, in a model of acute (neutrophil-dominated) arthritis, developed joint swelling to an extent similar to that in wild-type control mice. Joint fluid concentrations of bioactive IL-1beta were comparable in caspase 1-/- mice and controls. In contrast, induction of chronic arthritis (characterized by minimal numbers of neutrophils) in caspase 1-/- mice led to reduced joint inflammation and less cartilage damage, implying a caspase 1-dependent role in this process. In mice lacking neutrophil serine PR3, inhibition of caspase 1 activity resulted in decreased bioactive IL-1beta concentrations in the synovial tissue and less suppression of chondrocyte anabolic function. In addition, dual blockade of both PR3 and caspase 1 led to protection against cartilage and bone destruction. CONCLUSION: Caspase 1 deficiency does not affect neutrophil-dominated joint inflammation, whereas in chronic arthritis, the lack of caspase 1 results in reduced joint inflammation and cartilage destruction. These findings suggest that inhibitors of caspase 1 are not able to interfere with the whole spectr

Published
2009

9. Inflammatory arthritis in caspase 1 gene-deficient mice: contribution of proteinase 3 to caspase 1-independent production of bioactive interleukin-1beta.

Author

Joosten, L.A.B., Netea, M.G., Fantuzzi, G., Koenders, M.I., Helsen, M.M.A., Sparrer, H., Pham, C.T., Meer, J.W.M. van der, Dinarello, C.A., Berg, W.B. van den, Joosten, L.A.B., Netea, M.G., Fantuzzi, G., Koenders, M.I., Helsen, M.M.A., Sparrer, H., Pham, C.T., Meer, J.W.M. van der, Dinarello, C.A., and Berg, W.B. van den

Abstract

Contains fulltext : 80189.pdf (publisher's version ) (Closed access), OBJECTIVE: Caspase 1, a known cysteine protease, is a critical component of the inflammasome. Both caspase 1 and neutrophil serine proteases such as proteinase 3 (PR3) can process pro-interleukin-1beta (proIL-1beta), a crucial cytokine linked to the pathogenesis of rheumatoid arthritis. This study was undertaken to establish the relative importance of caspase 1 and serine proteases in mouse models of acute and chronic inflammatory arthritis. METHODS: Acute and chronic arthritis were induced in caspase 1-/- mice, and the lack of caspase 1 was investigated for its effects on joint swelling, cartilage metabolism, and histopathologic features. In addition, caspase 1 activity was inhibited in mice lacking active cysteine proteases, and the effects of dual blockade of caspase 1 and serine proteases on arthritis severity and histopathologic features were evaluated. RESULTS: Surprisingly, caspase 1-/- mice, in a model of acute (neutrophil-dominated) arthritis, developed joint swelling to an extent similar to that in wild-type control mice. Joint fluid concentrations of bioactive IL-1beta were comparable in caspase 1-/- mice and controls. In contrast, induction of chronic arthritis (characterized by minimal numbers of neutrophils) in caspase 1-/- mice led to reduced joint inflammation and less cartilage damage, implying a caspase 1-dependent role in this process. In mice lacking neutrophil serine PR3, inhibition of caspase 1 activity resulted in decreased bioactive IL-1beta concentrations in the synovial tissue and less suppression of chondrocyte anabolic function. In addition, dual blockade of both PR3 and caspase 1 led to protection against cartilage and bone destruction. CONCLUSION: Caspase 1 deficiency does not affect neutrophil-dominated joint inflammation, whereas in chronic arthritis, the lack of caspase 1 results in reduced joint inflammation and cartilage destruction. These findings suggest that inhibitors of caspase 1 are not able to interfere with the whole spectr

Published
2009

10. Inflammatory arthritis in caspase 1 gene-deficient mice: contribution of proteinase 3 to caspase 1-independent production of bioactive interleukin-1beta.

Author

Joosten, L.A.B., Netea, M.G., Fantuzzi, G., Koenders, M.I., Helsen, M.M.A., Sparrer, H., Pham, C.T., Meer, J.W.M. van der, Dinarello, C.A., Berg, W.B. van den, Joosten, L.A.B., Netea, M.G., Fantuzzi, G., Koenders, M.I., Helsen, M.M.A., Sparrer, H., Pham, C.T., Meer, J.W.M. van der, Dinarello, C.A., and Berg, W.B. van den

Abstract

Contains fulltext : 80189.pdf (publisher's version ) (Closed access), OBJECTIVE: Caspase 1, a known cysteine protease, is a critical component of the inflammasome. Both caspase 1 and neutrophil serine proteases such as proteinase 3 (PR3) can process pro-interleukin-1beta (proIL-1beta), a crucial cytokine linked to the pathogenesis of rheumatoid arthritis. This study was undertaken to establish the relative importance of caspase 1 and serine proteases in mouse models of acute and chronic inflammatory arthritis. METHODS: Acute and chronic arthritis were induced in caspase 1-/- mice, and the lack of caspase 1 was investigated for its effects on joint swelling, cartilage metabolism, and histopathologic features. In addition, caspase 1 activity was inhibited in mice lacking active cysteine proteases, and the effects of dual blockade of caspase 1 and serine proteases on arthritis severity and histopathologic features were evaluated. RESULTS: Surprisingly, caspase 1-/- mice, in a model of acute (neutrophil-dominated) arthritis, developed joint swelling to an extent similar to that in wild-type control mice. Joint fluid concentrations of bioactive IL-1beta were comparable in caspase 1-/- mice and controls. In contrast, induction of chronic arthritis (characterized by minimal numbers of neutrophils) in caspase 1-/- mice led to reduced joint inflammation and less cartilage damage, implying a caspase 1-dependent role in this process. In mice lacking neutrophil serine PR3, inhibition of caspase 1 activity resulted in decreased bioactive IL-1beta concentrations in the synovial tissue and less suppression of chondrocyte anabolic function. In addition, dual blockade of both PR3 and caspase 1 led to protection against cartilage and bone destruction. CONCLUSION: Caspase 1 deficiency does not affect neutrophil-dominated joint inflammation, whereas in chronic arthritis, the lack of caspase 1 results in reduced joint inflammation and cartilage destruction. These findings suggest that inhibitors of caspase 1 are not able to interfere with the whole spectr

Published
2009

11. Work-related injuries in young workers: An Italian multicentric epidemiological survey

Author

Aggazzotti, G, Righi, E, Patorno, E, Fantuzzi, G, Fabiani, L, Giuliani, A, Grappasonni, I, Petrelli, F, Ricciardi, W, La Torre, G, Sciacca, S, Angelillo, I, Bianco, A, Nobile, C, Gregorio, P, Lupi, S, Perlangeli, V, Bonazzi, M, Laviola, F, Triassi, M, Iorfida, E, Montegrosso, S, Rivosecchi, P, Serra, M, Adorisio, E, Gramiccia, A, Mura, I, Castiglia, P, Romano, G, Poli, A, Tardivo, S, Giuliani, AR, Serra, MC, Tardivo, S., BONAZZI, MARIA CHIARA, Aggazzotti, G, Righi, E, Patorno, E, Fantuzzi, G, Fabiani, L, Giuliani, A, Grappasonni, I, Petrelli, F, Ricciardi, W, La Torre, G, Sciacca, S, Angelillo, I, Bianco, A, Nobile, C, Gregorio, P, Lupi, S, Perlangeli, V, Bonazzi, M, Laviola, F, Triassi, M, Iorfida, E, Montegrosso, S, Rivosecchi, P, Serra, M, Adorisio, E, Gramiccia, A, Mura, I, Castiglia, P, Romano, G, Poli, A, Tardivo, S, Giuliani, AR, Serra, MC, Tardivo, S., and BONAZZI, MARIA CHIARA

Abstract

Emergency departments records from 33 hospitals were reviewed to disclose work-related injuries occurred in teen-subjects living in 14 Italian cities. During January-June 2000, 317 work-related injuries were reported. Male subjects, 17 year old, working in the industrial field, resulted the most affected, probably due to the fact that among young workers this sex and age class is the most represented one. Cluster analysis identified two groups of work-related injuries: one includes mainly transportation injuries causing lower extremities or multiple body sites traumas. The other is more strictly related to specific working tasks and includes mostly traumas and cut wounds in hand/wrist and head, together with eye lesions. A more intensive supervision on the use of protective equipment, a more appropriate training in hazard recognition and safe work practices, including operation of vehicles in the work site, must be implemented to reduce work-related injuries.

Published
2006

12. Regulation of Staphylococcus epidermidis-induced IFN-7 in whole human blood: the role of endogenous IL-18, IL-12, IL-1, and TNF

Author

Stuyt, R.J.L., Kim, S.H., Reznikov, L.L., Fantuzzi, G., Novick, D., Rubinstein, M., Kullberg, B.J., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Stuyt, R.J.L., Kim, S.H., Reznikov, L.L., Fantuzzi, G., Novick, D., Rubinstein, M., Kullberg, B.J., Meer, J.W.M. van der, Dinarello, C.A., and Netea, M.G.

Abstract

Item does not contain fulltext

Published
2003

13. Regulation of Staphylococcus epidermidis-induced IFN-gamma in whole human blood: the role of endogenous IL-18, IL-12, IL-1, and TNF.

Author

Stuyt, R.J.L., Kim, S., Reznikov, L.L., Fantuzzi, G., Novick, D., Rubinstein, M., Kullberg, B.J., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Stuyt, R.J.L., Kim, S., Reznikov, L.L., Fantuzzi, G., Novick, D., Rubinstein, M., Kullberg, B.J., Meer, J.W.M. van der, Dinarello, C.A., and Netea, M.G.

Abstract

Item does not contain fulltext, Interleukin 12 (IL-12) and IL-18 act synergistically to stimulate interferon gamma (IFN-gamma) production; moreover, IL-1 and tumor necrosis factor (TNF) may also augment IFN-gamma synthesis. We have investigated the relative contributions of these cytokines in the production of IFN-gamma and TNF by the Gram-positive bacterium Staphylococcus epidermidis, using the specific cytokine inhibitors IL-18 binding protein (IL-18BP), IL-1 receptor antagonist (IL-1Ra), anti-IL-12 antibodies (anti-IL-12 Ab), and TNF binding protein. Inhibition of caspase-1 reduced IFN-gamma and IL-1beta levels (by 80 and 67%, respectively) when heat-killed S. epidermidis was added to whole human blood cultures. IL-18BP reduced S. epidermidis-induced IFN-gamma (77% maximal suppression). In contrast, blocking IL-1 receptors by IL-1Ra had no effect on IFN-gamma production. Blocking endogenous IL-12 and TNF reduced IFN-gamma production by 69 and 36%. S. epidermidis-induced TNF-alpha was inhibited by IL-18BP and IL-1Ra, but not anti-IL-12 Ab, whereas IL-8 production was unaffected by any of the specific cytokine blocking agents. In conclusion, S. epidermidis stimulates IFN-gamma which is IL-18, IL-12 and TNF-dependent, but IL-1 independent.

Published
2003

14. Regulation of Staphylococcus epidermidis-induced IFN-7 in whole human blood: the role of endogenous IL-18, IL-12, IL-1, and TNF

Author

Stuyt, R.J.L., Kim, S.H., Reznikov, L.L., Fantuzzi, G., Novick, D., Rubinstein, M., Kullberg, B.J., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Stuyt, R.J.L., Kim, S.H., Reznikov, L.L., Fantuzzi, G., Novick, D., Rubinstein, M., Kullberg, B.J., Meer, J.W.M. van der, Dinarello, C.A., and Netea, M.G.

Abstract

Item does not contain fulltext

Published
2003

15. Regulation of Staphylococcus epidermidis-induced IFN-gamma in whole human blood: the role of endogenous IL-18, IL-12, IL-1, and TNF.

Author

Stuyt, R.J.L., Kim, S., Reznikov, L.L., Fantuzzi, G., Novick, D., Rubinstein, M., Kullberg, B.J., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Stuyt, R.J.L., Kim, S., Reznikov, L.L., Fantuzzi, G., Novick, D., Rubinstein, M., Kullberg, B.J., Meer, J.W.M. van der, Dinarello, C.A., and Netea, M.G.

Abstract

Item does not contain fulltext, Interleukin 12 (IL-12) and IL-18 act synergistically to stimulate interferon gamma (IFN-gamma) production; moreover, IL-1 and tumor necrosis factor (TNF) may also augment IFN-gamma synthesis. We have investigated the relative contributions of these cytokines in the production of IFN-gamma and TNF by the Gram-positive bacterium Staphylococcus epidermidis, using the specific cytokine inhibitors IL-18 binding protein (IL-18BP), IL-1 receptor antagonist (IL-1Ra), anti-IL-12 antibodies (anti-IL-12 Ab), and TNF binding protein. Inhibition of caspase-1 reduced IFN-gamma and IL-1beta levels (by 80 and 67%, respectively) when heat-killed S. epidermidis was added to whole human blood cultures. IL-18BP reduced S. epidermidis-induced IFN-gamma (77% maximal suppression). In contrast, blocking IL-1 receptors by IL-1Ra had no effect on IFN-gamma production. Blocking endogenous IL-12 and TNF reduced IFN-gamma production by 69 and 36%. S. epidermidis-induced TNF-alpha was inhibited by IL-18BP and IL-1Ra, but not anti-IL-12 Ab, whereas IL-8 production was unaffected by any of the specific cytokine blocking agents. In conclusion, S. epidermidis stimulates IFN-gamma which is IL-18, IL-12 and TNF-dependent, but IL-1 independent.

Published
2003

17. Role of interleukin-18 in host defense against disseminated Candida albicans infection.

Author

Stuyt, R.J.L., Netea, M.G., Verschueren, C.M.M., Fantuzzi, G., Dinarello, C.A., Meer, J.W.M. van der, Kullberg, B.J., Stuyt, R.J.L., Netea, M.G., Verschueren, C.M.M., Fantuzzi, G., Dinarello, C.A., Meer, J.W.M. van der, and Kullberg, B.J.

Abstract

Item does not contain fulltext, In mice injected intravenously with Candida albicans, administration of anti-interleukin-18 (IL-18) antibodies increased the yeast load in the kidneys. There was no effect on the organ load with Candida when gamma interferon (IFN-gamma)-deficient mice were treated with anti-IL-18 antibodies, suggesting that the protective effect of IL-18 is mediated through endogenous IFN-gamma.

Published
2002

19. Role of interleukin-18 in host defense against disseminated Candida albicans infection.

Author

Stuyt, R.J.L., Netea, M.G., Verschueren, C.M.M., Fantuzzi, G., Dinarello, C.A., Meer, J.W.M. van der, Kullberg, B.J., Stuyt, R.J.L., Netea, M.G., Verschueren, C.M.M., Fantuzzi, G., Dinarello, C.A., Meer, J.W.M. van der, and Kullberg, B.J.

Abstract

Item does not contain fulltext, In mice injected intravenously with Candida albicans, administration of anti-interleukin-18 (IL-18) antibodies increased the yeast load in the kidneys. There was no effect on the organ load with Candida when gamma interferon (IFN-gamma)-deficient mice were treated with anti-IL-18 antibodies, suggesting that the protective effect of IL-18 is mediated through endogenous IFN-gamma.

Published
2002

20. Role of interleukin-18 in host defense against disseminated Candida albicans infection.

Author

Stuyt, R.J.L., Netea, M.G., Verschueren, C.M.M., Fantuzzi, G., Dinarello, C.A., Meer, J.W.M. van der, Kullberg, B.J., Stuyt, R.J.L., Netea, M.G., Verschueren, C.M.M., Fantuzzi, G., Dinarello, C.A., Meer, J.W.M. van der, and Kullberg, B.J.

Abstract

Item does not contain fulltext, In mice injected intravenously with Candida albicans, administration of anti-interleukin-18 (IL-18) antibodies increased the yeast load in the kidneys. There was no effect on the organ load with Candida when gamma interferon (IFN-gamma)-deficient mice were treated with anti-IL-18 antibodies, suggesting that the protective effect of IL-18 is mediated through endogenous IFN-gamma.

Published
2002

22. Neutralization of IL-18 reduces neutrophil tissue accumulation and protects mice against lethal Escherichia coli and Salmonella typhimurium endotoxemia

Author

Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, and Dinarello, C.A.

Abstract

Contains fulltext : 19643.pdf (publisher's version ) (Closed access)

Published
2000

23. Neutralization of IL-18 reduces neutrophil tissue accumulation and protects mice against lethal Escherichia Coli and Salmonella typhimurium endotoxemia

Author

Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, and Dinarello, C.A.

Abstract

Item does not contain fulltext

Published
2000

24. Interleukin-18 mRNA, but not interleukin-18 receptor mRNA, is constitutively expressed in islet beta-cells and up-regulated by interferon-gamma.

Author

Hong, T P, Andersen, N A, Nielsen, K, Karlsen, A E, Puren, AJ, Fantuzzi, G, Eizirik, Decio L., Dinarello, C A, Mandrup-Poulsen, T., Hong, T P, Andersen, N A, Nielsen, K, Karlsen, A E, Puren, AJ, Fantuzzi, G, Eizirik, Decio L., Dinarello, C A, and Mandrup-Poulsen, T.

Abstract

Interleukin-18 (IL-18) mRNA is expressed in islets of NOD mice during the early stages of insulitis and IL-18 has therefore been implicated as a contributing factor in immune-mediated beta-cell destruction. However, a recent study failed to show any effect of human IL-18 on the function of isolated rat islets. Since species differences have been shown between human and murine IL-18, the aims of this study were to investigate 1) if species homologous IL-18 alone or following IL-12 pre-exposure affected rat islet function, 2) if IL-18 dose-dependently modulated IL-1 beta or interferon-gamma (IFN-gamma) + tumor necrosis factor-alpha (TNF-alpha) actions on islet function, and 3) if IL-18 and IL-18 receptor (IL-18R) were expressed in rat islet beta-cells. Insulin release and nitric oxide (NO) production from isolated rat islets were measured after incubation with or without cytokines. RT-PCR was used to quantitate mRNA expression of IL-18 and the IL-18R signaling chain (IL-18R beta). There were no significant effects of 0.625-10 nM recombinant murine (rm) IL-18 alone on accumulated or glucose-challenged insulin release or NO production after 24 hours. Fifteen pg/ml of recombinant human (rh) IL-1 beta as well as 200 U/ml recombinant rat (rr) IFN-gamma + 250 U/ml rhTNF-alpha significantly increased islet NO production and inhibited both accumulated and glucose-challenged islet insulin release. However, rmIL-18 failed to modulate these effects of IL-1 beta or IFN-gamma + TNF-alpha. Although IL-12 induces IL-18R expression in Th1 and B lymphocytes, 24-hours rmIL-12 preincubation neither sensitized islets to effects of 10 nM of rm or rrIL-18 alone nor primed the islets to IL-1 beta actions on insulin release and NO production. IL-18R beta mRNA, which was expressed in human peripheral blood mononuclear cells (PBMC), was not expressed in rat insulinoma (RIN) cells or in isolated rat islets, even after exposure to IL-1 beta and/or IFN-gamma + TNF-alpha or IL-12. IL-18 mRNA was c, In Vitro, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published
2000

25. Neutralization of IL-18 reduces neutrophil tissue accumulation and protects mice against lethal Escherichia coli and Salmonella typhimurium endotoxemia

Author

Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, and Dinarello, C.A.

Abstract

Contains fulltext : 19643.pdf (publisher's version ) (Closed access)

Published
2000

26. Neutralization of IL-18 reduces neutrophil tissue accumulation and protects mice against lethal Escherichia Coli and Salmonella typhimurium endotoxemia

Author

Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, and Dinarello, C.A.

Abstract

Item does not contain fulltext

Published
2000

27. Neutralization of IL-18 reduces neutrophil tissue accumulation and protects mice against lethal Escherichia coli and Salmonella typhimurium endotoxemia

Author

Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, Dinarello, C.A., Netea, M.G., Fantuzzi, G., Kullberg, B.J., Stuyt, R.J.L., Pulido, E.J., McIntyre, R.C., Joosten, L.A.B., Meer, J.W.M. van der, and Dinarello, C.A.

Abstract

Contains fulltext : 19643.pdf (publisher's version ) (Closed access)

Published
2000

28. Interleukin-18 mRNA, but not interleukin-18 receptor mRNA, is constitutively expressed in islet beta-cells and up-regulated by interferon-gamma.

Author

Hong, T P, Andersen, N A, Nielsen, K, Karlsen, A E, Puren, AJ, Fantuzzi, G, Eizirik, Decio L., Dinarello, C A, Mandrup-Poulsen, T., Hong, T P, Andersen, N A, Nielsen, K, Karlsen, A E, Puren, AJ, Fantuzzi, G, Eizirik, Decio L., Dinarello, C A, and Mandrup-Poulsen, T.

Abstract

Interleukin-18 (IL-18) mRNA is expressed in islets of NOD mice during the early stages of insulitis and IL-18 has therefore been implicated as a contributing factor in immune-mediated beta-cell destruction. However, a recent study failed to show any effect of human IL-18 on the function of isolated rat islets. Since species differences have been shown between human and murine IL-18, the aims of this study were to investigate 1) if species homologous IL-18 alone or following IL-12 pre-exposure affected rat islet function, 2) if IL-18 dose-dependently modulated IL-1 beta or interferon-gamma (IFN-gamma) + tumor necrosis factor-alpha (TNF-alpha) actions on islet function, and 3) if IL-18 and IL-18 receptor (IL-18R) were expressed in rat islet beta-cells. Insulin release and nitric oxide (NO) production from isolated rat islets were measured after incubation with or without cytokines. RT-PCR was used to quantitate mRNA expression of IL-18 and the IL-18R signaling chain (IL-18R beta). There were no significant effects of 0.625-10 nM recombinant murine (rm) IL-18 alone on accumulated or glucose-challenged insulin release or NO production after 24 hours. Fifteen pg/ml of recombinant human (rh) IL-1 beta as well as 200 U/ml recombinant rat (rr) IFN-gamma + 250 U/ml rhTNF-alpha significantly increased islet NO production and inhibited both accumulated and glucose-challenged islet insulin release. However, rmIL-18 failed to modulate these effects of IL-1 beta or IFN-gamma + TNF-alpha. Although IL-12 induces IL-18R expression in Th1 and B lymphocytes, 24-hours rmIL-12 preincubation neither sensitized islets to effects of 10 nM of rm or rrIL-18 alone nor primed the islets to IL-1 beta actions on insulin release and NO production. IL-18R beta mRNA, which was expressed in human peripheral blood mononuclear cells (PBMC), was not expressed in rat insulinoma (RIN) cells or in isolated rat islets, even after exposure to IL-1 beta and/or IFN-gamma + TNF-alpha or IL-12. IL-18 mRNA was c, In Vitro, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published
2000

29. Chlorpromazine specifically inhibits peripheral and brain TNF production, and up-regulates IL-10 production, in mice

Author

Mengozzi, M., Fantuzzi, G, Marchant, Arnaud, Goldman, Michel, Orencole, S., Clark, B.D., Sironi, Marina, Benigni, F., Ghezzi, P., Mengozzi, M., Fantuzzi, G, Marchant, Arnaud, Goldman, Michel, Orencole, S., Clark, B.D., Sironi, Marina, Benigni, F., and Ghezzi, P.

Abstract

We have previously shown that chlorpromazine (CPZ) inhibits tumour necrosis factor (TNF) production and protects against endotoxic shock in mice. In this paper we investigated the effect of pretreatment with CPZ, 4 mg/kg i.p. 30 min before, compared with dexamethasone (DEX; 3 mg/kg) on the induction of other endotoxin (lipopolysaccharide; LPS)-induced cytokines in the serum of mice, i.e. interleukin-1 alpha (IL-1 alpha), IL-6 and IL-10, and TNF. We also studied the effect of CPZ on serum and spleen-associated TNF. Both DEX and CPZ inhibited TNF production, whereas induction of IL-1 and IL-6 was inhibited by DEX but not by CPZ. DEX did not affect IL-10, while CPZ potentiated its induction. CPZ also inhibited spleen-associated TNF induction in LPS-treated mice, suggesting an effect on the synthesis of TNF. CPZ inhibited TNF induction by Gram-positive bacteria (heat-killed Staphylococcus epidermidis) and by anti-CD3 monoclonal antibodies. Intraperitoneal administration of CPZ also inhibited the induction of brain-associated TNF induced by intra-cerebroventricular injection of LPS. Therefore, CPZ is a more specific inhibitor of TNF production than DEX; in particular, CPZ increased the induction of IL-10, which is a 'protective' cytokine known to inhibit LPS toxicity and TNF production. CPZ inhibited TNF production in vivo, irrespective of the TNF stimulus used to induce TNF. Finally, CPZ did not induce the 'rebound' effect of DEX that, when given 24 hr before LPS, potentiates TNF production, but it did inhibit TNF production after 24 hr., Journal Article, Research Support, Non-U.S. Gov't, FLWNO, info:eu-repo/semantics/published

Published
1994

30. Chlorpromazine specifically inhibits peripheral and brain TNF production, and up-regulates IL-10 production, in mice

Author

Mengozzi, M., Fantuzzi, G, Marchant, Arnaud, Goldman, Michel, Orencole, S., Clark, B.D., Sironi, Marina, Benigni, F., Ghezzi, P., Mengozzi, M., Fantuzzi, G, Marchant, Arnaud, Goldman, Michel, Orencole, S., Clark, B.D., Sironi, Marina, Benigni, F., and Ghezzi, P.

Abstract

We have previously shown that chlorpromazine (CPZ) inhibits tumour necrosis factor (TNF) production and protects against endotoxic shock in mice. In this paper we investigated the effect of pretreatment with CPZ, 4 mg/kg i.p. 30 min before, compared with dexamethasone (DEX; 3 mg/kg) on the induction of other endotoxin (lipopolysaccharide; LPS)-induced cytokines in the serum of mice, i.e. interleukin-1 alpha (IL-1 alpha), IL-6 and IL-10, and TNF. We also studied the effect of CPZ on serum and spleen-associated TNF. Both DEX and CPZ inhibited TNF production, whereas induction of IL-1 and IL-6 was inhibited by DEX but not by CPZ. DEX did not affect IL-10, while CPZ potentiated its induction. CPZ also inhibited spleen-associated TNF induction in LPS-treated mice, suggesting an effect on the synthesis of TNF. CPZ inhibited TNF induction by Gram-positive bacteria (heat-killed Staphylococcus epidermidis) and by anti-CD3 monoclonal antibodies. Intraperitoneal administration of CPZ also inhibited the induction of brain-associated TNF induced by intra-cerebroventricular injection of LPS. Therefore, CPZ is a more specific inhibitor of TNF production than DEX; in particular, CPZ increased the induction of IL-10, which is a 'protective' cytokine known to inhibit LPS toxicity and TNF production. CPZ inhibited TNF production in vivo, irrespective of the TNF stimulus used to induce TNF. Finally, CPZ did not induce the 'rebound' effect of DEX that, when given 24 hr before LPS, potentiates TNF production, but it did inhibit TNF production after 24 hr., Journal Article, Research Support, Non-U.S. Gov't, FLWNO, info:eu-repo/semantics/published

Published
1994

31. Lead Exposure and Child Development: An International Assessment

Author

Ahmedi, G., Ashby, Paul David, Baghurst, P.A., Beese, I, BELL, A, Bellinger, D.C, Belmont, L, Berger, O, Bergoni, M, Bier, M, Borella, P, BORNSCHEIN, Robert L, Bozovic, R, Bratel, J, Brittenham, G, Brockhaus, A, Bushnell, L, Campagna, R, CARTER, C, Catelli, D, Cavazutti, G B, Cluydts, Raymond, Colakovic, B, Collet, W, Cookman, G, Cooney, G, Cory-Slechta, D C, Davis, J M, Delves, T, Dietrich, K N, Emmern, S, Ernhart, C B, Ewert, T, Fantuzzi, G, Fulton, M, Gashi, E, Goldberg, A, Grandjean, Philippe, Grant, Lester D, Graziano, J, Greenland, R, Grote, J, Hamlin, M, Hammond, Paul B, Hansen, O N, Hargreaves, E, Harvey, P, Hatzakis, A, Haxhiu, R, Hennekes, R, Hepburn, W, Hidalgo, H, Hunter, J, Hunter, R, Kalandidi, A, Katsouyanni, K, Kazantzis, G, Keane, G, King, W, Kline, J, Kokkevi, A, Koutselinis, A, Krafft, K, Krämer, U, Krause, C, Kumar, R, Lansdown, R, Laxen, D P, Lenaerts, C, Leviton, A, Lilienthal, H, Loiacono, N, Lyngbye, T, Maravelias, C, Marler, M, McBride, W, J McMichael, A, Mehmetti, A, Mendes, C, Mitchell, T, Montorsi, R, Moore, Michael.M, Morgan, J, Morrow-Tlulak, M, Muddiman, D, Munoz, C, Mushak, Paul, Murphy, M, Needleman, Herbert L, Nenezic, D, Steenhout, Anne, Otto, D, Pelling, D, Pocock, S J, Popovac, D, Raab, G M, Rabinowitz, Michael, Radovic, L, Rajovic, B, Regan, C, Rice, Deborah C, Roberts, R, Ahmedi, G., Ashby, Paul David, Baghurst, P.A., Beese, I, BELL, A, Bellinger, D.C, Belmont, L, Berger, O, Bergoni, M, Bier, M, Borella, P, BORNSCHEIN, Robert L, Bozovic, R, Bratel, J, Brittenham, G, Brockhaus, A, Bushnell, L, Campagna, R, CARTER, C, Catelli, D, Cavazutti, G B, Cluydts, Raymond, Colakovic, B, Collet, W, Cookman, G, Cooney, G, Cory-Slechta, D C, Davis, J M, Delves, T, Dietrich, K N, Emmern, S, Ernhart, C B, Ewert, T, Fantuzzi, G, Fulton, M, Gashi, E, Goldberg, A, Grandjean, Philippe, Grant, Lester D, Graziano, J, Greenland, R, Grote, J, Hamlin, M, Hammond, Paul B, Hansen, O N, Hargreaves, E, Harvey, P, Hatzakis, A, Haxhiu, R, Hennekes, R, Hepburn, W, Hidalgo, H, Hunter, J, Hunter, R, Kalandidi, A, Katsouyanni, K, Kazantzis, G, Keane, G, King, W, Kline, J, Kokkevi, A, Koutselinis, A, Krafft, K, Krämer, U, Krause, C, Kumar, R, Lansdown, R, Laxen, D P, Lenaerts, C, Leviton, A, Lilienthal, H, Loiacono, N, Lyngbye, T, Maravelias, C, Marler, M, McBride, W, J McMichael, A, Mehmetti, A, Mendes, C, Mitchell, T, Montorsi, R, Moore, Michael.M, Morgan, J, Morrow-Tlulak, M, Muddiman, D, Munoz, C, Mushak, Paul, Murphy, M, Needleman, Herbert L, Nenezic, D, Steenhout, Anne, Otto, D, Pelling, D, Pocock, S J, Popovac, D, Raab, G M, Rabinowitz, Michael, Radovic, L, Rajovic, B, Regan, C, Rice, Deborah C, and Roberts, R

Abstract

0, European Commission and US.Environmental Protection Agency ;Published for the Commission of the European Communities and the U.S. Environmental Protection Agency (M. Smith, L. Grant ,A. Sors, Editors), info:eu-repo/semantics/published

Published
1989

32. Lead Exposure and Child Development: An International Assessment

Author

Ahmedi, G., Ashby, Paul David, Baghurst, P.A., Beese, I, BELL, A, Bellinger, D.C, Belmont, L, Berger, O, Bergoni, M, Bier, M, Borella, P, BORNSCHEIN, Robert L, Bozovic, R, Bratel, J, Brittenham, G, Brockhaus, A, Bushnell, L, Campagna, R, CARTER, C, Catelli, D, Cavazutti, G B, Cluydts, Raymond, Colakovic, B, Collet, W, Cookman, G, Cooney, G, Cory-Slechta, D C, Davis, J M, Delves, T, Dietrich, K N, Emmern, S, Ernhart, C B, Ewert, T, Fantuzzi, G, Fulton, M, Gashi, E, Goldberg, A, Grandjean, Philippe, Grant, Lester D, Graziano, J, Greenland, R, Grote, J, Hamlin, M, Hammond, Paul B, Hansen, O N, Hargreaves, E, Harvey, P, Hatzakis, A, Haxhiu, R, Hennekes, R, Hepburn, W, Hidalgo, H, Hunter, J, Hunter, R, Kalandidi, A, Katsouyanni, K, Kazantzis, G, Keane, G, King, W, Kline, J, Kokkevi, A, Koutselinis, A, Krafft, K, Krämer, U, Krause, C, Kumar, R, Lansdown, R, Laxen, D P, Lenaerts, C, Leviton, A, Lilienthal, H, Loiacono, N, Lyngbye, T, Maravelias, C, Marler, M, McBride, W, J McMichael, A, Mehmetti, A, Mendes, C, Mitchell, T, Montorsi, R, Moore, Michael.M, Morgan, J, Morrow-Tlulak, M, Muddiman, D, Munoz, C, Mushak, Paul, Murphy, M, Needleman, Herbert L, Nenezic, D, Steenhout, Anne, Otto, D, Pelling, D, Pocock, S J, Popovac, D, Raab, G M, Rabinowitz, Michael, Radovic, L, Rajovic, B, Regan, C, Rice, Deborah C, Roberts, R, Ahmedi, G., Ashby, Paul David, Baghurst, P.A., Beese, I, BELL, A, Bellinger, D.C, Belmont, L, Berger, O, Bergoni, M, Bier, M, Borella, P, BORNSCHEIN, Robert L, Bozovic, R, Bratel, J, Brittenham, G, Brockhaus, A, Bushnell, L, Campagna, R, CARTER, C, Catelli, D, Cavazutti, G B, Cluydts, Raymond, Colakovic, B, Collet, W, Cookman, G, Cooney, G, Cory-Slechta, D C, Davis, J M, Delves, T, Dietrich, K N, Emmern, S, Ernhart, C B, Ewert, T, Fantuzzi, G, Fulton, M, Gashi, E, Goldberg, A, Grandjean, Philippe, Grant, Lester D, Graziano, J, Greenland, R, Grote, J, Hamlin, M, Hammond, Paul B, Hansen, O N, Hargreaves, E, Harvey, P, Hatzakis, A, Haxhiu, R, Hennekes, R, Hepburn, W, Hidalgo, H, Hunter, J, Hunter, R, Kalandidi, A, Katsouyanni, K, Kazantzis, G, Keane, G, King, W, Kline, J, Kokkevi, A, Koutselinis, A, Krafft, K, Krämer, U, Krause, C, Kumar, R, Lansdown, R, Laxen, D P, Lenaerts, C, Leviton, A, Lilienthal, H, Loiacono, N, Lyngbye, T, Maravelias, C, Marler, M, McBride, W, J McMichael, A, Mehmetti, A, Mendes, C, Mitchell, T, Montorsi, R, Moore, Michael.M, Morgan, J, Morrow-Tlulak, M, Muddiman, D, Munoz, C, Mushak, Paul, Murphy, M, Needleman, Herbert L, Nenezic, D, Steenhout, Anne, Otto, D, Pelling, D, Pocock, S J, Popovac, D, Raab, G M, Rabinowitz, Michael, Radovic, L, Rajovic, B, Regan, C, Rice, Deborah C, and Roberts, R

Abstract

0, European Commission and US.Environmental Protection Agency ;Published for the Commission of the European Communities and the U.S. Environmental Protection Agency (M. Smith, L. Grant ,A. Sors, Editors), info:eu-repo/semantics/published

Published
1989

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