Verfügbarkeit: Vaccines :: THWS Bibkatalog

Vaccines: [with 20 tables]

Gespeichert in:

Bibliographische Detailangaben
Format:	Buch
Sprache:	English
Veröffentlicht:	Berlin [u.a.] Springer 1999
Schriftenreihe:	Handbook of experimental pharmacology 133
Schlagworte:	Vaccines Pharmacology Infection Vaccins Immune System > physiopathology Vaccines > pharmacology Vaccines > therapeutic use Impfstoff Aufsatzsammlung
Online-Zugang:	Inhaltsverzeichnis
Beschreibung:	XXV, 534 S. Ill., graph. Darst.
ISBN:	3540647406

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MARC


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Datensatz im Suchindex

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adam_text	CONTENTS CHAPTER 1 VACCINES: PAST, PRESENT AND FUTURE G. S CHILD , M. C ORBEL , P. C ORRAN , AND P. M INOR . 1 A. BACTERIAL VACCINES: PAST, PRESENT AND FUTURE . 1 I. PAST . 1 II. PRESENT . 4 1. PURIFIED SUB-UNIT VACCINES . 5 A) POLYSACCHARIDES . 5 B) PROTEIN-POLYSACCHARIDE CONJUGATE VACCINES . 5 2. PURIFIED PROTEIN SUB-UNITS . 6 3. GENETICALLY MODIFIED STRAINS . 7 III. FUTURE . . . . . 7 1. SYNTHETIC PEPTIDES . 7 2. ANTI-IDIOTYPES . 8 3. NUCLEIC ACIDS . 8 4. LIVE RECOMBINANTS . 8 5. MULTIVALENT COMBINATIONS . 9 6. SLOW-RELEASE/SINGLE-DOSE VACCINES . 9 7. ORAL/MUCOSAL DELIVERY SYSTEMS . 9 B. VIRAL VACCINES . 10 I. PAST . 10 II. PRESENT . 11 III. FUTURE . 13 C. PARASITE VACCINES . 14 I. PAST . 14 II. PRESENT . 14 1. KILLED AND ATTENUATED VACCINES . 15 2. PEPTIDE VACCINES . 15 3. VACCINES BASED ON EXPRESSED PARASITE PROTEINS . 15 4. LIVE CARRIERS . 16 5. OTHER APPROACHES . 16 III. FUTURE . 16 1. DNA VACCINES . 17 2. ADJUVANTS . 17 REFERENCES . 17 XII CONTENTS CHAPTER 2 IMMUNOLOGY OF INFECTION S.H.E. K AUFMANN AND J. R EIMANN . WITH 4 FIGURES . 21 A. INTRODUCTION . 21 B. THE ADAPTIVE (ACQUIRED) IMMUNE RESPONSE . 22 C. THE CELLULAR IMMUNE SYSTEM: T CELLS . 23 I. MHC-RESTRICTED PRESENTATION OF EPITOPES TO T CELLS . 23 II. CONVENTIONAL MHC-I OR MHC-II RESTRICTED TCRA/5 T CELLS . 24 III. CONVENTIONAL MHC-IA RESTRICTED CD8 + TCRA/F T CELLS . 27 IV. UNCONVENTIONAL MHC-IB RESTRICTED CD8 + TCRA/3 T CELLS . 28 V. UNCONVENTIONAL DOUBLE-NEGATIVE (DN, CD4 " CD8 ), CDL-RESTRICTED TCRA/3 T CELLS . 28 VI. UNCONVENTIONAL CDL-RESTRICTED CD4 + OR DN NK1 + TCRA/3 T CELLS . 29 VII. TCRYD T CELLS . 29 D. CYTOKINES . 30 E. THE EARLY DECISION ON THE TYPE OF EFFECTOR FUNCTIONS THAT PREVAIL IN AN IMMUNE RESPONSE . 33 F. THE HUMORAL IMMUNE SYSTEM: B CELLS . 34 G. T AND B CELL MEMORY . 35 H. MUCOSAL IMMUNITY . 35 I. UNSUCCESSFUL INDUCTION OF SPECIFIC IMMUNE RESPONSES . 36 J. IMPLICATIONS FOR RATIONAL VACCINE DESIGN . 37 REFERENCES . 39 CHAPTER 3 DNA VACCINES: IMMUNOGENICITY AND PRECLINICAL EFFICACY J.B. U LMER , J.J. D ONNELLY , AND M.A. LIU . 43 A. OVERVIEW . 43 B. BACKGROUND . 43 C. EFFECTIVENESS OF DNA VACCINES IN ANIMAL MODELS . 45 I. MISCELLANEOUS . 45 II. FERRETS . 45 III. NONHUMAN PRIMATES . 46 D. MUCOSAL IMMUNIZATION . 48 E. DELIVERY SYSTEMS AND ADJUVANTS . 50 I. DNA DELIVERY . 50 II. DNA AS ADJUVANT . 50 F. SUMMARY . 52 REFERENCES . 52 CONTENTS - XIII CHAPTER 4 ANTIGEN-PRESENTATION SYSTEMS, IMMUNOMODULATORS, AND IMMUNE RESPONSES TO VACCINES C.-A. S IEGRIST AND P.-H. L AMBERT . 57 A. FROM EMPIRICAL APPROACHES TO RATIONALLY SELECTED ANTIGEN PRESENTATION SYSTEMS AND IMMUNOMODULATORS FOR VACCINE MEDIATED PROTECTION AGAINST INFECTIOUS DISEASES . 57 B. WHAT ARE THE ESSENTIAL PARAMETERS OF VACCINE-INDUCED EFFECTOR MECHANISMS? . 59 I. ANTIBODY-MEDIATED VACCINE RESPONSES . 59 II. VACCINE-SPECIFIC T CELL RESPONSES . 61 1. CD4 T CELL VACCINE RESPONSES . 61 2. CHARACTERISTICS OF VACCINE-SPECIFIC CD8 CYTOTOXIC RESPONSES . 61 C. WHAT FUNDAMENTAL IMMUNOLOGICAL MECHANISMS CAN BE MODULATED BY ANTIGEN-DELIVERY SYSTEMS AND IMMUNOMODULATORS? . 62 I. MODULATION OF ANTIGEN PRESENTATION TO T/B CELLS . 62 1. ANTIGEN CONFORMATION . 62 2. ANTIGEN PERSISTENCE . 63 3. TARGETING OF PROFESSIONAL ANTIGEN-PRESENTING CELLS . 64 II. MODULATION OF CD4 T CELL RESPONSES . 64 III. INDUCTION OF CD8 T CELL RESPONSES . 65 D. WHAT IS THE EFFECT OF SPECIFIC DELIVERY SYSTEMS AND IMMUNOMODULATORS ON RESPONSES TO VACCINE ANTIGENS? . 65 I. EFFECT OF ANTIGEN-DELIVERY SYSTEMS . 65 1. LIVE BACTERIAL AND VIRAL VECTORS . 65 A) BACTERIAL VECTORS . 65 B) VIRAL VECTORS . 66 2. DNA VACCINES . 67 II. EFFECT OF PARTICULATE SUBSTANCES ON VACCINE RESPONSES . 68 1. ALUMINUM AND CALCIUM SALTS . 68 2. WATER AND OIL EMULSIONS . 69 3. LIPOSOMES AND VIROSOMES . 69 4. PROTEOSOMES . 70 5. MICRO AND NANOSPHERES OF BIODEGRADABLE POLYMERS . 70 III. EFFECT OF IMMUNOMODULATORS THAT CAN BE INCORPORATED INTO ANTIGEN-PRESENTATION SYSTEMS . 71 1. LIPID A AND DERIVATIVES . 72 2. SAPONINS (QUIL A, QS21) . 72 3. NONIONIC BLOCK COPOLYMERS . 72 4. MDP AND DERIVATIVES . 73 5. CYTOKINES AND INTERFERONS . 73 XIV CONTENTS IV. EFFECT OF VACCINE FORMULATIONS THAT COMBINE ANTIGEN-DELIVERY SYSTEMS AND IMMUNOMODULATORY SUBSTANCES . 74 1. IMMUNE-STIMULATING COMPLEXES . 74 2. W/O EMULSIONS WITH BUILT-IN IMMUNOMODULATORS . 75 3. O/W EMULSIONS WITH BUILT-IN IMMUNOMODULATORS . 76 4. FORMULATIONS BASED ON LIPOSOMES WITH BUILT-IN IMMUNOMODULATORS . 77 E. HOW CAN VACCINES BE DESIGNED FOR SELECTED TARGET POPULATIONS WITH VARIABLE LEVELS OF IMMUNOCOMPETENCE? . 77 I. INDUCING EFFICIENT VACCINE RESPONSES IN EARLY LIFE . 77 1. CHARACTERISTICS OF IMMUNE RESPONSES IN EARLY LIFE . 77 2. SELECTING ANTIGEN-PRESENTATION SYSTEMS/ IMMUNOMODULATORS FOR USE IN EARLY LIFE . 78 A) INDUCING PROTECTIVE ANTIBODY RESPONSES IN INFANTS AND NEONATES . 79 B) INDUCING STRONG TH1 AND CTL RESPONSES IN INFANTS AND NEONATES . 79 C) INDUCING VACCINE RESPONSES IN PRESENCE OF MATERNAL ANTIBODIES . 80 II. INDUCING EFFICIENT VACCINE RESPONSES IN THE ELDERLY . 81 III. INDUCING EFFICIENT VACCINE RESPONSES IN IMMUNODEFICIENT PATIENTS . 82 1. ENHANCING VACCINE RESPONSES IN IMMUNOSUPPRESSED PATIENTS . 82 2. ENHANCING VACCINE RESPONSES IN HIV-1 INFECTED PATIENTS . 82 F. CONCLUSIONS . 83 REFERENCES . 84 CHAPTER 5 VACCINES AGAINST MEASLES, MUMPS, RUBELLA, AND VARICELLA E. N ORRBY . 93 A. INTRODUCTION . 93 B. MEASLES VACCINE . 94 I. SAFETY AND EFFICACY OF LIVE MEASLES VACCINE . 95 II. EPIDEMIOLOGICAL CONSEQUENCES OF USING LIVE MEASLES VACCINE . 97 III. NEW KINDS OF MEASLES VACCINES . 99 IV. REMAINING PROBLEMS IN USING MEASLES VACCINE AND PROJECTED FUTURE DEVELOPMENTS . 99 C. MUMPS VACCINE . 100 I. SAFETY AND EFFICACY OF LIVE MUMPS VACCINE . 101 CONTENTS XV II. EPIDEMIOLOGICAL CONSEQUENCES OF USING LIVE MUMPS VACCINE USE . 102 III. NEW KINDS OF MUMPS VACCINES . 103 IV. REMAINING PROBLEMS IN USING MUMPS VACCINE AND PROJECTED FUTURE DEVELOPMENTS . 103 D. RUBELLA VACCINE . 103 I. SAFETY AND EFFICACY OF LIVE RUBELLA VACCINE . 104 II. EPIDEMIOLOGICAL CONSEQUENCES OF USING LIVE RUBELLA VACCINE . 106 III. NEW KINDS OF RUBELLA VACCINES . 106 IV. REMAINING PROBLEMS IN USING RUBELLA VACCINE AND PROJECTED FUTURE DEVELOPMENTS . 107 E. VARICELLA VACCINE . 108 I. SAFETY AND EFFICACY OF LIVE VARICELLA VACCINE . 109 II. EPIDEMIOLOGICAL CONSEQUENCES OF USING LIVE VARICELLA VACCINE . 110 III. NEW KINDS OF VARICELLA VACCINES . ILL IV. REMAINING PROBLEMS IN USING VARICELLA VACCINE AND PRIORITIES FOR THE FUTURE . 112 F. EPILOGUE . 112 REFERENCES . 113 CHAPTER 6 HEPATITIS AND POLIO VACCINES F. S CHODEL AND P. M INOR . WITH 3 FIGURES . 121 A. INTRODUCTION . 121 B. HEPATITIS A VIRUS . 122 I. THE VIRUS . 122 II. THE ANTIGENS . 122 III. THE DISEASE . 123 IV. IMMUNITY AND VACCINES . 124 1. PASSIVE IMMUNIZATION . 124 2. INACTIVATED WHOLE VIRUS VACCINES . 124 3. LIVE ATTENUATED VACCINES . 126 C. HEPATITIS B VIRUS . 126 I. THE VIRUS . 126 II. THE ANTIGENS . 127 1. ENVELOPE PROTEINS . 127 2. NUCLEOCAPSID ANTIGEN . 128 III. THE DISEASE . 129 IV. IMMUNITY AND VACCINES . 131 1. PROTECTIVE IMMUNITY . 131 2. PASSIVE IMMUNIZATION . 131 3. ACTIVE IMMUNIZATION . 131 XVI CONTENTS A) TARGETS . 131 B) CURRENT VACCINES: PLASMA-DERIVED VACCINES . 131 C) RECOMBINANT VACCINES . 133 A) HBSAG-BASED . 133 \|3) PRE-S CONTAINING VACCINES . 135 Y) ALTERNATIVE VACCINATION APPROACHES . 138 B) THERAPEUTIC VACCINATION? . 143 E) ERADICATION OF HEPATITIS B? . 145 D. HEPATITIS C VIRUS . 145 I. THE VIRUS . 145 II. THE ANTIGENS . 146 III. THE DISEASE . 146 IV. VACCINE DEVELOPMENT . 147 E. HEPATITIS E VIRUS . 147 I. THE VIRUS . 147 II. THE ANTIGENS . 148 III. THE DISEASE . 148 IV. CANDIDATE VACCINES . 148 F. POLIOVIRUS . 148 I. THE VIRUS . 148 II. THE ANTIGENS . 149 III. THE DISEASE . 150 IV. INACTIVATED POLIOVACCINES . 151 V. ORAL POLIOVACCINES . 152 VI. ERADICATION OF POLIOMYELITIS . 154 REFERENCES . 157 CHAPTER 7 HERPES A. V AHLNE , T. B ERGSTROM , AND B. S VENNERHOLM . 171 A. HERPESVIRIDAE . 171 B. HISTORICAL BACKGROUND . 172 I. HSV . 172 II. CMV . 173 III. EBV . 173 C. THE GLYCOPROTEINS . 173 D. EARLY EVENTS OF HUMAN HERPES VIRUS REPLICATION . 175 E. LATENCY . 176 F. REACTIVATION . 177 G. CLINICAL INFECTIONS . 179 I. HSV . 179 II. CMV . 180 III. EBV . 181 CONTENTS XVII H. IMMUNOLOGY . 181 I. THERAPEUTIC VACCINES . 183 I. KILLED VACCINES . 183 II. SUBUNIT VACCINES . 184 J. PROPHYLACTIC VACCINES . 185 I. HSV . 185 II. CMV . 186 1. LIVE VACCINE . 187 2. SUBUNIT VACCINE . 187 III. EBV . 188 1. SUBUNIT VACCINES . 188 2. LIVE VACCINES . 188 K. CONCLUSIONS . 189 REFERENCES . 189 CHAPTER 8 TOXIN-BASED VACCINES (DIPHTHERIA, TETANUS, PERTUSSIS) R. R APPUOLI AND M. P IZZA . 201 A. INTRODUCTION . 201 B. DIPHTHERIA TOXIN . 202 C. TETANUS TOXIN . 203 D. PRODUCTION, EFFECTIVENESS, AND PROBLEMS OF CONVENTIONAL DIPHTHERIA AND TETANUS VACCINES . 204 I. PRODUCTION AND DETOXIFICATION OF DIPHTHERIA AND TETANUS TOXOIDS . 204 II. PRODUCTION AND DETOXIFICATION OF PURIFIED DIPHTHERIA AND TETANUS TOXOIDS . 205 E. FUTURE PROSPECTS . 206 I. ENGINEERED LIVE-ATTENUATED STRAINS . 206 II. RECOMBINANT MOLECULES . 207 III. MUCOSAL VACCINATION . 207 IV. CRM 197 . 208 F. DIPHTHERIA AND TETANUS TOXOIDS AS CARRIERS FOR POLYSACCHARIDE VACCINES . 209 G. PERTUSSIS . 209 I. THE DISEASE . 209 II. HISTORY OF ACELLULAR VACCINES . 210 III. PERTUSSIS TOXIN . 211 IV. GENETIC DETOXIFICATION . 211 V. ACELLULAR VACCINES PROPOSED . 212 VI. CLINICAL TRIALS . 212 VIL OTHER CLINICAL STUDIES . 217 REFERENCES . 218 XVIII CONTENTS CHATER 9 OUTER MEMBRANE PROTEIN VACCINES J. P OOLMAN . 225 A. INTRODUCTION . 225 B. NEISSERIA GONORRHOEAE . 225 I. PILI . 225 II. OUTER MEMBRANE PROTEIN PI OR POR . 226 III. PII OR OPACITY-ASSOCIATED PROTEINS . 227 IV. LIPOPOLYSACCHARIDES . 227 V. FE LIMITATION INDUCIBLE OMPS . 228 VI. MISCELLANEOUS . 228 C. NEISSERIA MENINGITIDIS . 229 I. THE SEROGROUP B CAPSULAR POLYSACCHARIDE . 229 II. OMP VACCINES . 230 III. OPA AND OPC . 233 IV. PILI . 233 V. LIPOPOLYSACCHARIDES . 233 VI. FE LIMITATION INDUCIBLE OMPS . 234 VIL MISCELLANEOUS . 234 D. NONTYPABLE HAEMOPHILUS INFLUENZAE . 234 I. PL, P2, P4 . 235 II. P6 AND PCP . 235 III. PILI, FIMBRIAE, P5 . 235 IV. HIGH MOLECULAR WEIGHT ADHESINS . 235 V. LIPOPOLYSACCHARIDE OR LIPO-OLIGOSACCHARIDE . 236 VI. FE LIMITATION INDUCIBLE OMPS . 236 VIL MISCELLANEOUS . 236 E. MORAXELLA CATARRHALIS . 236 I. OMP CD, OMP E . 237 II. PILI/FIMBRIAE/HIGH MOLECULAR WEIGHT OMPS . 237 III. LIPOPOLYSACCHARIDE OR LIPO-OLIGOSACCHARIDE . 237 IV. FE LIMITATION INDUCIBLE OMPS . 237 F. ANIMAL MODELS . 237 REFERENCES . 238 CHAPTER 10 CARBOHYDRATE-BASED BACTERIAL VACCINES J.T. P OOLMAN , C. L AFERRIERE , AND S.B. S VENSON . 249 A. INTRODUCTION . 249 B. THE HIB EXPERIENCE . 250 C. MENINGOCOCCAL POLYSACCHARIDE AND CONJUGATE VACCINES . 252 D. PNEUMOCOCCAL POLYSACCHARIDE AND CONJUGATE VACCINES . 253 I. PROTEIN CARRIER . 254 CONTENTS XIX II. POLYSACCHARIDE SIZE . 255 III. COUPLING CHEMISTRY . 255 IV. POLYSACCHARIDE-PROTEIN RATIO . 255 V. ADJUVANT . 256 VI. ANIMAL MODELS AND CORRELATES OF PROTECTION . 256 VII. CLINICAL TRIALS OF PNEUMOCOCCAL POLYSACCHARIDE-PROTEIN CONJUGATE VACCINES . 257 VIII. THE FUTURE OF PNEUMOCOCCAL VACCINES . 259 E. SALMONELLA, SHIGELLA, AND E. COLL . 259 I. SALMONELLA: O-ANTIGEN SPECIFIC CONJUGATES . 259 II. S. TYPHI: VI-ANTIGEN SPECIFIC CONJUGATES . 261 III. SHIGELLA: O-ANTIGEN SPECIFIC CONJUGATES . 261 IV. E. COLI: O-ANTIGEN SPECIFIC CONJUGATES . 262 REFERENCES . 262 CHAPTER 11 MYCOBACTERIA R. J ANSSEN , D. Y OUNG , AND J. T HOLE . 273 A. INTRODUCTION . 273 B. THE CELLULAR RESPONSE TO MYCOBACTERIA . 273 I. MACROPHAGE INTERACTIONS . 273 II. RECOGNITION BY CD4 T CELLS . 275 III. THE CD8 RESPONSE . 276 IV. OTHER SUBSETS . 277 C. MYCOBACTERIAL ANTIGENS . 278 D. PROTECTION VERSUS DISEASE . 279 E. MYCOBACTERIAL VACCINES . 280 I. LIVE VACCINES . 280 II. SUBUNIT VACCINES . 282 III. DNA VACCINES . 283 F. FUTURE PROSPECTS . 284 REFERENCES . 284 CHAPTER 12 VACCINES AGAINST DIARRHEAL DISEASES J. H OLMGREN AND A.-M. S VENNERHOLM . 291 A. INTRODUCTION . 291 B. OVERVIEW OF THE MAIN DIARRRHEAL PATHOGENS . 293 I. VIBRIO CHOLERAE . 293 II. ENTEROTOXIGENIC ESCHERICHIA COLI . 294 III. SHIGELLA SPP . 294 IV. CAMPYLOBACTER JEJUNI . 295 V. ROTAVIRUS . 295 XX CONTENTS C. MECHANISMS OF DISEASE AND IMMUNITY IN DIARRHEAL DISEASES . 295 I. ENTEROTOXINS AND ANTITOXIC IMMUNITY . 296 II. COLONIZATION AND ANTIBACTERIAL IMMUNITY IN CHOLERA AND ETEC INFECTIONS . 297 III. PATHOGENIC AND IMMUNE MECHANISMS IN SHIGELLA INFECTIONS . 299 IV. PROTECTIVE IMMUNITY IN ROTAVIRUS INFECTIONS . 301 D. CHOLERA VACCINES . 302 I. ORAL INACTIVATED VACCINES . 302 II. ORAL LIVE VACCINES . 305 III. COMBINED VACCINES AGAINST O1 AND 0139 CHOLERA . 307 E. ETEC VACCINES . 308 I. ORAL INACTIVATED VACCINES . 309 II. ORAL LIVE VACCINES . 313 F. SHIGELLA VACCINES . 314 I. PARENTERAL VACCINES . 315 II. ORAL LIVE VACCINES . 315 G. CAMPYLOBACTER JEJUNI VACCINES . 317 H. ROTAVIRUS VACCINES . 318 REFERENCES . 321 CHAPTER 13 SEXUALLY TRANSMITTED DISEASES E.G. S ANDSTROM . 329 A. INTRODUCTION . 329 B. SPECIAL CHALLENGES . 330 C. GONORRHEA . 331 I. EPIDEMIOLOGY . 331 II. NATURAL INFECTION . 331 III. ANTIGENIC VARIATION . 332 IV. WHOLE-CELL VACCINES . 332 V. SUBCOMPONENT VACCINES . 332 1. PORIN . 332 2. LIPO-OLIGOSACCHARIDES . 333 3. PILI . 333 4. OPACITY PROTEINS . 334 5. TRANSFERRIN BINDING PROTEINS . 334 6. IGA PROTEASE . 334 VI. PROSPECTS . 334 D. CHLAMYDIA INFECTION . 335 I. EPIDEMIOLOGY . 335 II. NATURAL INFECTION . 335 III. PATHOGENESIS . 336 CONTENTS XXI IV. WHOLE-CELL VACCINES . 336 V. SUBCOMPONENT VACCINES . 337 1. MAJOR OUTER MEMBRANE PROTEIN . 337 2. HEAT SHOCK PROTEIN 75 KDA . 338 VI. PROSPECTS . 338 E. GENITAL ULCERS CAUSED BY HAEMOPHILUS DUCREYI . 339 I. EPIDEMIOLOGY . 339 II. NATURAL INFECTION . 339 III. SUBCOMPONENT VACCINES . 339 IV. PROSPECTS . 340 F. SYPHILIS . 340 I. EPIDEMIOLOGY . 340 II. NATURAL INFECTION . 340 III. ANTIGENIC VARIATION . 341 IV. WHOLE-CELL VACCINES . 341 V. SUBCOMPONENT VACCINES . 341 1. CARDIOLIPIN . 341 2. TREPONEMAL PROTEINS . 341 VI. PROSPECTS . 342 G. HUMAN GENITAL PAPILLOMA VIRUS INFECTION . 342 I. EPIDEMIOLOGY . 342 II. NATURAL INFECTION . 342 III. WHOLE-VIRAL VACCINES . 343 IV. SUBCOMPONENT VACCINES . 343 V. PROSPECTS . 344 H. HERPES SIMPLEX INFECTION . 344 I. EPIDEMIOLOGY . 344 II. NATURAL INFECTION . 345 III. WHOLE-VIRAL VACCINES . 345 IV. SUBCOMPONENT VACCINES . 345 V. PROSPECTS . 347 I. CONCLUSION . 347 REFERENCES . 348 CHAPTER 14 DESIGNING A VACCINE AGAINST HIV A.M. S CHULTZ . 357 A. PERSPECTIVE . 357 I. THE NEED FOR A VACCINE . 357 II. THE FIRST DECADE: 1985-1995 . 357 III. NEW PARADIGMS . 359 IV. WHAT SHOULD THE VACCINE DO? . 360 V. DESIGN CONSIDERATIONS . 361 XXII CONTENTS B. THE ROLE OF ANTIBODY . 362 I. PASSIVE TRANSFER . 362 II. DOES HIV HAVE SEROTYPES? . 363 III. DO CORECEPTOR FAMILIES OF HIV REPRESENT SEROTYPES? . . . 364 IV. DESIGN CONSIDERATIONS . 365 1. THE IDEAL IMMUNOGEN . 365 2. OBSTACLES TO INDUCING A BROAD RESPONSE . 366 3. HUMAN MONOCLONAL ANTIBODIES AS CLUES . 368 4. IS NEUTRALIZATION REQUIRED FOR PROTECTION? . 368 C. THE ROLE OF CYTOTOXIC T-CELLS . 369 I. EVIDENCE FROM VACCINATION AND CHALLENGE . 369 II. EVIDENCE FROM INFECTION . 370 III. ADDRESSING THE HETEROGENEITY OF HIV . 371 IV. DESIGN CONSIDERATIONS . 372 D. OTHER T-CELL ACTIVITIES . 372 E. MUCOSAL IMMUNITY . 373 F. VACCINE APPROACHES . 375 I. LIVE-ATTENUATED VACCINE . 375 II. WHOLE, INACTIVATED VIRUS . 376 III. RECOMBINANT VECTORS . 377 IV. PLASMID IMMUNIZATION . 378 V. SUBUNIT PROTEINS AND PEPTIDES . 379 VI. COMBINATIONS . 379 G. PROSPECTUS . 380 I. DESIGN CONSIDERATIONS . 380 II. EVALUATION CONSIDERATIONS . 382 REFERENCES . 382 CHAPTER 15 AN OVERVIEW OF MALARIA VACCINE DEVELOPMENT EFFORTS S. K UMAR , D.C. K ASLOW , AND S.L. H OFFMAN . WITH 1 FIGURE . 397 A. EPIDEMIOLOGY . 397 B. THE PARASITE . 397 C. APPROACHES TO MALARIA VACCINE DEVELOPMENT: PREVENTING ERYTHROCYTIC STAGE INFECTION OR REDUCING MORBIDITY AND MORTALITY WITHOUT PREVENTING INFECTION . 398 D. PREERYTHROCYTIC STAGE VACCINES . 399 I. PREVENTING SPOROZOITE INVASION OF HEPATOCYTES . 399 II. ATTACKING INFECTED HEPATOCYTES . 402 E. ERYTHROCYTIC STAGE VACCINES: REDUCING PARASITE BURDEN AND BLOCKING PATHOGENESIS . 405 I. APPROACHES TO REDUCING PARASITE BURDEN . 406 1. PREVENTING MEROZOITE INVASION OF ERYTHROCYTES . 406 CONTENTS XXIII 2. ATTACKING INFECTED ERYTHROCYTES . 406 II. ANTIPARASITE IMMUNE MECHANISMS THAT CONTRIBUTE TO PARASITE REDUCTION . 407 1. REDUCTION IN PARASITE BURDEN: THE DIRECT EFFECTS OF ANTIBODIES . 407 2. REDUCTION IN PARASITE BURDEN: THE ROLE OF CELLULAR MECHANISMS THROUGH DIRECT EFFECTS OF CYTOKINES AND OTHER BIOACTIVE MOLECULES . 407 A) THE ROLE OF CD4 + T CELLS . 407 B) THE ROLE OF Y/D T CELLS . 409 C) THE ROLE OF CYTOKINES . 410 III. DATA SUPPORTING REDUCTION IN PARASITE BURDEN AND THE STATUS OF EXPERIMENTAL ERYTHROCYTIC STAGE VACCINES DESIGNED TO REDUCE PARASITE BURDEN . 411 1. MSP1 . 412 2. MSP2 . 414 3. AMA1 . 414 4. EBA-175 . 415 5. SERA . 416 6. RESA . 416 7. SYNTHETIC SPF66 VACCINE . 417 IV. BLOCKING PATHOGENESIS . _ . 417 1. INHIBITING ADHERENCE OF INFECTED ERYTHROCYTES TO ENDOTHELIAL CELLS . 418 2. INHIBITING ADHERENCE OF INFECTED ERYTHROCYTES TO OTHER ERYTHROCYTES (RESETTING) . 419 3. INHIBITING MALARIA TOXINS . 420 F. TRANSMISSION BLOCKING VACCINES . 420 I. GAMETE AND EARLY ZYGOTE SURFACE TARGET ANTIGENS . 422 II. LATE ZYGOTE OOKINETE SURFACE TARGET ANTIGENS . 422 III. OOKINETE SECRETED AND MOSQUITO DERIVED TARGET ANTIGENS . 424 IV. PROGRESS TOWARDS A TRANSMISSION BLOCKING VACCINE . 425 G. CONCLUSIONS . 426 REFERENCES . 426 CHAPTER 16 ANTIFERTILITY VACCINES V.C. S TEVENS . WITH 4 FIGURES . 443 A. INTRODUCTION . 443 B. CURRENT STATUS OF VACCINE DEVELOPMENT . 445 I. ANTISPERM VACCINES . 445 II. OVUM ANTIGENS . 446 III. ANTIHORMONE VACCINES . 449 XXIV CONTENTS 1. GONADOTROPIN-RELEASING HORMONE . 449 2. FOLLICLE-STIMULATING HORMONE . 450 3. HUMAN CHORIONIC GONADOTROPIN . 452 C. PROBLEMS AND PROSPECTS . 456 REFERENCES . 457 CHAPTER 17 CANCER VACCINES K.E. H ELLSTROM AND I. H ELLSTROM . 463 A. INTRODUCTION . 463 B. TUMOR ANTIGENS . 463 I. RECOGNITION BY ANTIBODIES . 464 II. RECOGNITION BY T LYMPHOCYTES . 464 III. TUMOR PEPTIDES AS T CELL TARGETS . 465 IV. ANTIGEN PRESENTATION . 466 C. TYPES OF TUMOR VACCINES . 468 D. DOWNREGULATORY MECHANISMS . 471 E. CONCLUSIONS AND OUTLOOK . 472 REFERENCES . 473 CHAPTER 18 PREVENTION OF AUTOIMMUNITY A.J. S LAVIN AND H.L. W EINER . WITH 2 FIGURES . 479 A. OVERVIEW OF AUTOIMMUNE DISEASES . 479 B. AUTOREACTIVE T CELLS . 479 C. ANTIGEN-SPECIFIC THERAPY . 480 I. ALTERED PEPTIDE LIGANDS . 480 II. ORAL TOLERANCE . 480 1. MECHANISMS OF ORAL TOLERANCE . 481 2. BYSTANDER SUPPRESSION . 484 3. MODULATION OF ORAL TOLERANCE . 485 III. NASAL AND AEROSOL MUCOSAL TOLERANCE . 487 IV. TREATMENT OF AUTOIMMUNE DISEASES IN ANIMALS . 488 1. EXPERIMENTAL AUTOIMMUNE ENCEPHALOMYELITIS . 488 2. ARTHRITIS . 488 3. UVEITIS . 488 4. MYASTHENIA GRAVIS . 489 5. DIABETES . 489 6. TRANSPLANTATION AND OTHER MODELS . 489 V. TREATMENT OF AUTOIMMUNE DISEASES IN HUMANS . 490 D. FUTURE DIRECTIONS . 491 REFERENCES . 492 CONTENTS XXV CHAPTER 19 VACCINES AGAINST ALLERGIES L. H ELLMAN . WITH 2 FIGURES . 499 A. INTRODUCTION . 499 B. THE ALLERGIC IMMUNE RESPONSE . 499 C. TRADITIONAL IMMUNOTHERAPY . 506 I. MODIFIED ALLERGENS OR ALLERGEN EXTRACTS . 507 II. ORAL ADMINISTRATION OF RECOMBINANT ALLERGENS OR ALLERGEN EXTRACTS . 509 III. PEPTIDE VACCINES . 510 IV. CYTOKINE AGONISTS AND ANTAGONISTS . 512 V. LOW MOLECULAR WEIGHT COMPOUNDS INTERFERING WITH THE INTERACTION BETWEEN IGE AND ITS HIGH-AFFINITY RECEPTOR . . 513 VI. DEPLETION OF PLASMA AND MAST CELL BOUND IGE BY TREATMENT WITH MONOCLONAL ANTI-IGE ANTIBODIES . 514 VII. INDUCTION OF A STRONG ANTI-IGE RESPONSE BY VACCINATION . . 516 D. CONCLUSIONS . 519 REFERENCES . 519 SUBJECT INDEX . 527
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spelling	Vaccines [with 20 tables] contributors T. Bergström ... Ed. P. Perlmann and H. Wigzell Berlin [u.a.] Springer 1999 XXV, 534 S. Ill., graph. Darst. txt rdacontent n rdamedia nc rdacarrier Handbook of experimental pharmacology 133 Vaccines cabt Pharmacology cabt Infection cabt Vaccins gtt Immune System physiopathology Vaccines Vaccines pharmacology Vaccines therapeutic use Impfstoff (DE-588)4026655-2 gnd rswk-swf (DE-588)4143413-4 Aufsatzsammlung gnd-content Impfstoff (DE-588)4026655-2 s DE-604 Perlmann, Peter Sonstige oth Bergström, Tomas Sonstige oth Handbook of experimental pharmacology 133 (DE-604)BV002390716 133 DNB Datenaustausch application/pdf http://bvbr.bib-bvb.de:8991/F?func=service&doc_library=BVB01&local_base=BVB01&doc_number=008261306&sequence=000001&line_number=0001&func_code=DB_RECORDS&service_type=MEDIA Inhaltsverzeichnis
spellingShingle	Vaccines [with 20 tables] Handbook of experimental pharmacology Vaccines cabt Pharmacology cabt Infection cabt Vaccins gtt Immune System physiopathology Vaccines Vaccines pharmacology Vaccines therapeutic use Impfstoff (DE-588)4026655-2 gnd
subject_GND	(DE-588)4026655-2 (DE-588)4143413-4
title	Vaccines [with 20 tables]
title_auth	Vaccines [with 20 tables]
title_exact_search	Vaccines [with 20 tables]
title_full	Vaccines [with 20 tables] contributors T. Bergström ... Ed. P. Perlmann and H. Wigzell
title_fullStr	Vaccines [with 20 tables] contributors T. Bergström ... Ed. P. Perlmann and H. Wigzell
title_full_unstemmed	Vaccines [with 20 tables] contributors T. Bergström ... Ed. P. Perlmann and H. Wigzell
title_short	Vaccines
title_sort	vaccines with 20 tables
title_sub	[with 20 tables]
topic	Vaccines cabt Pharmacology cabt Infection cabt Vaccins gtt Immune System physiopathology Vaccines Vaccines pharmacology Vaccines therapeutic use Impfstoff (DE-588)4026655-2 gnd
topic_facet	Vaccines Pharmacology Infection Vaccins Immune System physiopathology Vaccines pharmacology Vaccines therapeutic use Impfstoff Aufsatzsammlung
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work_keys_str_mv	AT perlmannpeter vaccineswith20tables AT bergstromtomas vaccineswith20tables

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