Description

Thanks to this 100% online program, you will acquire a deep understanding of Multidrug-Resistant Bacteria, from their epidemiology to their resistance mechanisms and the best practices for their clinical management"

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Currently, Multidrug-Resistant Bacteria pose a significant challenge to Nursing, due to their ability to resist multiple antibiotics, which complicates treatments and increases mortality and morbidity in hospitalized patients. Therefore, the implementation of strict infection control measures, including hand washing, proper use of personal protective equipment and surface disinfection, is crucial for prevention.

In this scenario, TECH presents this program, which will examine Multidrug-Resistant Bacteria in human pathology, providing a solid foundation on the biology and epidemiology of these infections. It will also delve into the management of patients with BMR infections in Intensive Care Units (ICU), where nurses will utilize advanced clinical management techniques and infection control measures crucial to these critical settings.

In addition, the study plan will focus on Multidrug-Resistant Gram Negative Bacteria, addressing the specific challenges they present, and analyzing antibiotic resistance in Streptococcus, Enterococcus and Staphylococcus, providing a detailed understanding of these common and dangerous pathogens. Without overlooking Proteomics in Clinical Microbiology, which will offer an advanced perspective on protein analysis in the study of Multidrug-Resistant Bacteria.

Finally, the presence and management of Multidrug-Resistant Bacteria in the food chain and animal health, respectively, highlighting the importance of an integrated approach to control antimicrobial resistance in different sectors. In addition, emerging strategies and new antimicrobial molecules will be explored and the use of Artificial Intelligence in Clinical Microbiology and infectious diseases will be introduced.

In this way, TECH has designed a comprehensive, fully online program, which will allow graduates to avoid worries, such as traveling to a fixed center or adjusting to a pre-established schedule. Additionally, it is based on the innovative Relearning methodology, consisting of the repetition of key concepts for an optimal and organic assimilation of the contents.

This program will equip you with the knowledge and skills necessary to face one of the most pressing challenges in contemporary medicine: Multidrug-Resistant Bacteria"

This Professional master’s degree in Multidrug-Resistant Bacteria for Nursing contains the most complete and up-to-date scientific program on the market. The most important features include:

  • The development of practical cases presented by experts in Microbiology, Medicine and Parasitology
  • The graphic, schematic and eminently practical contents with which it is conceived gather scientific and practical information on those disciplines that are indispensable for professional practice
  • Practical exercises where the self-assessment process can be carried out to improve learning
  • Its special emphasis on innovative methodologies
  • Theoretical lessons, questions to the expert, debate forums on controversial topics, and individual reflection assignments
  • Content that is accessible from any fixed or portable device with an Internet connection

You will delve into advanced topics such as Proteomics in Clinical Microbiology, emerging strategies against Multidrug-Resistant Bacteria and the development of new antimicrobial molecules. What are you waiting to enroll?"

The program’s teaching staff includes professionals from the sector who contribute their work experience to this specializing program, as well as renowned specialists from leading societies and prestigious universities.

The multimedia content, developed with the latest educational technology, will provide the professional with situated and contextual learning, i.e., a simulated environment that will provide immersive education programmed to learn in real situations.

This program is designed around Problem-Based Learning, whereby the professional must try to solve the different professional practice situations that arise during the course. For this purpose, students will be assisted by an innovative interactive video system created by renowned and experienced experts.

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You will delve into Multidrug-Resistant Gram Negative Bacteria, with a specific focus on organisms such as Klebsiella pneumoniae and Pseudomonas aeruginosa. With all TECH's quality guarantees!"

Syllabus

The contents of the program will include the detailed study of the epidemiology and pathogenesis of Multidrug-Resistant Bacteria for Nursing, as well as the molecular mechanisms of resistance. In addition, nurses will analyze advanced microbiological diagnostic strategies and methods of hospital infection control. The clinical management of patients with these infections in different care settings, from Intensive Care Units to Primary Care, will also be discussed. Topics such as Proteomics in Clinical Microbiology, the development of new antimicrobial therapies and the role of Artificial Intelligence in the management of infectious diseases will complement the program.

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You will address the advanced management of infected patients in critical settings, such as Intensive Care Units (ICU), as well as infection control strategies to prevent nosocomial spread"

Module 1. Multidrug-Resistant Bacteria in Human Pathology

1.1. Mechanisms of Acquired Resistance to Antibiotics

1.1.1. Acquisition of Resistance Genes
1.1.2. Mutations
1.1.3. Acquisition of Plasmids

1.2. Mechanisms of Intrinsic Resistance to Antibiotics

1.2.1. Blockage of Antibiotic Entry
1.2.2. Modification of the Antibiotic Target
1.2.3. Inactivation of the Antibiotic
1.2.4. Antibiotic Expulsion

1.3. Chronology and Evolution of Antibiotic Resistance

1.3.1. Discovery of Antibiotic Resistance
1.3.2. Plasmids
1.3.3. Evolution of Resistance
1.3.4. Current Trends in the Evolution of Antibiotic Resistance

1.4. Antibiotic Resistance in Human Pathology

1.4.1. Increased Mortality and Morbidity
1.4.2. Impact of Resistance on Public Health
1.4.3. Economic Cost Associated with Antibiotic Resistance

1.5. Multidrug-Resistant Human Pathogens

1.5.1. Acinetobacter Baumannii
1.5.2. Pseudomonas Aeruginosa
1.5.3. Enterobacteriaceae
1.5.4. Enterococcus Faecium
1.5.5. Staphylococcus Aureus
1.5.6. Helicobacter Pylori
1.5.7. Campylobacter Spp
1.5.8. Salmonellae
1.5.9. Neisseria Gonorrhoeae
1.5.10 Streptococcus Pneumoniae
1.5.11 Hemophilus Influenzae
1.5.12 Shigella Spp

1.6. Bacteria Highly Dangerous to Human Health: Update of the WHO List

1.6.1. Critical Priority Pathogens
1.6.2. High Priority Pathogens
1.6.3. Pathogens with Medium Priority

1.7. Analysis of the Causes of Antibiotic Resistance

1.7.1. Lack of New Antibiotics
1.7.2. Socioeconomic Factors and Health Policies
1.7.3. Poor Hygiene and Sanitation
1.7.4. Health Policies and Antibiotic Resistance
1.7.5. International Travel and Global Trade
1.7.6. Dispersal of High-Risk Clones
1.7.7. Emerging Pathogens with Resistance to Multiple Antibiotics

1.8. Antibiotic Use and Abuse in the Community

1.8.1. Prescription
1.8.2. Acquisition
1.8.3. Misuse of Antibiotics

1.9. Current Status of Antibiotic Resistance in the World

1.9.1. Global Statistics
1.9.2. Central and South America
1.9.3. Africa
1.9.4. North America
1.9.5. Asia and Oceania

1.10. Perspectives on Antibiotic Resistance

1.10.1. Strategies to Mitigate the Problem of Multidrug-Resistance
1.10.2. International Actions
1.10.3. Actions at the Global Level

Module 2. Management of Patients with Multidrug-Resistant Bacterial Infections in Intensive Care Units (ICU)

2.1. Colonization and Infection of Patients in ICUs

2.1.1. Types of ICUs
2.1.2. Epidemiology
2.1.3. Risk Factors Associated with Infection in ICUs

2.2. Impact of Nosocomial Infections in the Critically Ill Patient

2.2.1. Importance of Nosocomial Infections in ICUs
2.2.2. Risk Factors for Nosocomial Infections

2.2.2.1. Patient Factors
2.2.2.2. Factors of the ICU Environment
2.2.2.3. Factors Related to the Healthcare Personnel

2.2.3. Impact of Nosocomial Infections in Immunocompromised Patients
2.2.4. Impact on Length of Stay in the ICU

2.3. Pneumonia Associated with Mechanical Ventilation

2.3.1. Etiology
2.3.2. Diagnosis
2.3.3. Treatment

2.4. Urinary Tract Infections Associated with Catheters

2.4.1. Etiology
2.4.2. Diagnosis
2.4.3. Treatment

2.5. Primary Bacteremias and Catheter-Related Bacteremias

2.5.1. Etiology
2.5.2. Diagnosis
2.5.3. Treatment

2.6. Pseudomembranous Colitis

2.6.1. Etiology
2.6.2. Diagnosis
2.6.3. Treatment

2.7. Infections by Opportunistic Pathogens

2.7.1. Etiology
2.7.2. Diagnosis
2.7.3. Treatment

2.8. Appropriate Use of Antibiotics

2.8.1. Programs for the Optimization of Antibiotic use (PROA) in the ICU
2.8.2. Antibiotic Therapy Strategies for the Treatment of Gram-Negative Patients
2.8.3. Antibiotic Therapy Strategies for the Treatment of Gram-Positive Patients
2.8.4. Antibiotic Therapy Strategies for the Treatment of Co-Infections

2.9. Strategies for the Prevention of BMR Infections in the ICU

2.9.1. Hygiene Measures
2.9.2. Infection Control Measures
2.9.3. Protocols and Clinical Practice Guidelines
2.9.4. Education and Training of ICU Personnel
2.9.5. Participation of Patients and their Families

2.10. Infection Prevention Strategies in the ICU

2.10.1. Infection Prevention Strategies in the ICU According to the Focus

2.10.1.1. Pneumonia
2.10.1.2. Bacteremia
2.10.1.3. Urinary Infection

2.10.2. Evaluation and Quality Indicators in the Prevention of Infections
2.10.3. Evaluation and Continuous Improvement Tools
2.10.4. Successful Examples of Infection Prevention in ICUs

Module 3. Multidrug-Resistant Gram Negative Bacteria

3.1. Infections Due to Gram-Negative Microorganisms

3.1.1. Epidemiology of Gram-Negative Microorganisms
3.1.2. Community and Nosocomial Infections by Gram-Negative Microorganisms
3.1.3. Relevance of Infections by Multidrug-Resistant Gram-Negative Microorganisms

3.2. Pathogenesis of Infections by Gram-Negative Microorganisms

3.2.1. Factors Related to Gram-Negative Microorganisms
3.2.2. Patient Factors in Gram-Negative Infections
3.2.3. Other Factors in Gram-Negative Infections

3.3. Clinical Evaluation of Patients with Multidrug-Resistant Gram-Negative Infections

3.3.1. Medical History
3.3.2. Clinical Evaluation of Patients
3.3.3. Other Data of Interest

3.4. Complementary Tests in Infections by Multidrug-Resistant Gram-Negative Microorganisms

3.4.1. Blood Tests
3.4.2. Imaging Tests
3.4.3. Microbiological Techniques

3.5. Estimation of Severity in Patients with Infections by Multidrug-Resistant Gram-Negative Microorganisms

3.5.1. Gram-Negative Multidrug-Resistant Microorganisms
3.5.2. Traditional Approach to Severity Estimation
3.5.3. Practical Conclusions

3.6. Risk of Acquiring Infections by Multidrug-Resistant Gram-Negative Microorganisms

3.6.1. Clinical Factors in the Acquisition of Infections by Multidrug-Resistant Gram-Negative Microorganisms
3.6.2. Other Factors in the Acquisition of Infections by Multidrug-Resistant Gram-Negative Microorganisms
3.6.3. Tools to Calculate the Risk of Presence of Multidrug-Resistant Gram-Negative Microorganisms

3.7. Empirical Treatment in the Suspicion of Infections by Multidrug-Resistant Gram-Negative Microorganisms

3.7.1. Microorganisms Involved According to Localization
3.7.2. Comprehensive Assessment of Patients with Suspected Infections by Multidrug-Resistant Gram-Negative Microorganisms
3.7.3. Selection of Empirical Antibiotic Treatment

3.8. Targeted Therapy in Infections by Multidrug-Resistant Gram-Negative Microorganisms

3.8.1. Adjustment of Antibiotic Therapy According to Microbiological Results
3.8.2. Follow-up of Multidrug-Resistant Gram-Negative Microorganism Infection
3.8.3. Most Relevant Side Effects of Antibiotherapy

3.9. Duration of Antibiotherapy in Infections by Multidrug-Resistant Gram-Negative Microorganisms

3.9.1. Estimation of the Duration of Antibiotic Treatment in Infections by Multidrug-Resistant Gram-Negative Microorganisms
3.9.2. Relevance of Focus Control in Infections by Multidrug-Resistant Gram-Negative Microorganisms
3.9.3. Special Considerations Related to Antibiotic Therapy in These Infections

3.10. PROA Teams in Infections Caused by Multidrug-Resistant Gram-Negative Microorganisms

3.10.1. PROA Teams: History
3.10.2. Impact of PROA Teams on the Correct Use of Antibiotic Treatments
3.10.3. Challenge of PROA Teams in the Treatment of Infections Caused by Multiresistant Gram-Negative Microorganisms

Module 4. Antibiotic Resistance in Streptococcus, Enterococcus and Staphylococcus

4.1. Infections Due to Gram-Positive Bacteria

4.1.1. Natural Habitat of Gram-Positive Pathogens
4.1.2. Nosocomial Infections due to Gram-Positive Bacteria
4.1.3. Community-Acquired Infections by Gram-Positive Bacteria

4.2. In Vitro and in Vivo Systems for the Study of Resistance in Gram-Positive Bacteria

4.2.1. Biofilms
4.2.2. Cellular Models
4.2.3. Animal Models

4.3. Streptococcus Pneumoniae

4.3.1. Clinical Significance
4.3.2. Resistance Mechanisms
4.3.3. Biofilms
4.3.4. Treatment Options

4.4. Streptococcus Pyogenes

4.4.1. Clinical Significance
4.4.2. Resistance Mechanisms
4.4.3. Biofilms
4.4.4. Treatment Options

4.5. Streptococcus Agalactiae

4.5.1. Clinical Significance
4.5.2. Resistance Mechanisms
4.5.3. Biofilms
4.5.4. Treatment Options

4.6. Enterococcus Faecalis

4.6.1. Clinical Significance
4.6.2. Resistance Mechanisms
4.6.3. Biofilms
4.6.4. Treatment Options

4.7. Enterococcus Faecium

4.7.1. Clinical Significance
4.7.2. Resistance Mechanisms
4.7.3. Biofilms
4.7.4. Treatment Options

4.8. Staphylococcus Aureus

4.8.1. Clinical Significance
4.8.2. Resistance Mechanisms
4.8.3. Biofilms
4.8.4. Treatment Options

4.9. Mycobacterium Tuberculosis

4.9.1. Clinical Significance
4.9.2. Resistance Mechanisms
4.9.3. Treatment Options

4.10. Resistance in Other Gram-Positive Bacteria

4.10.1. Coagulase-Negative Staphylococcus
4.10.2. Clostridioides Difficile
4.10.3. Emerging Gram Positive Pathogens

Module 5.  Proteomics in Clinical Microbiology

5.1. Proteomics in the Microbiology Laboratory

5.1.1. Evolution and Development of Proteomics
5.1.2. Importance in Microbiological Diagnosis
5.1.3. Proteomics of Multi-Resistant Bacteria

5.2. Qualitative Protein Separation Techniques

5.2.1. Two-Dimensional Electrophoresis (2DE)
5.2.2. DIGE Technology
5.2.3. Applications in Microbiology

5.3. Quantitative Protein Separation Techniques

5.3.1. Isotopic Labelling
5.3.2. High Performance Liquid Chromatography (HPLC)
5.3.3. Mass Spectrometry (MS)

5.3.3.1. MALDI-TOF Technologies in the Clinical Microbiology Laboratory

5.3.3.1.1. VITEK®MS System
5.3.3.1.2. MALDI Biotyper® System

5.4. MALDI-TOF Applications in Clinical Microbiology

5.4.1. Identification of Microorganisms
5.4.2. Characterization of Antibiotic Resistance
5.4.3. Bacterial Typing

5.5. Bioinformatics Tools for Proteomics

5.5.1. Proteomic Databases
5.5.2. Protein Sequence Analysis Tools
5.5.3. Visualization of Proteomic Data

5.6. Genomics in the Microbiology Laboratory

5.6.1. Evolution and Development of Genomics
5.6.2. Importance in Microbiological Diagnosis
5.6.3. Genomics of Multi-Resistant Bacteria

5.7. Types of Sequencing

5.7.1. Sequencing of Genes with Taxonomic Value
5.7.2. Sequencing of Genes of Taxonomic Value
5.7.3. Bulk Sequencing

5.8. Applications of Massive Sequencing in Clinical Microbiology

5.8.1. Whole Bacterial Genome Sequencing
5.8.2. Comparative Genomics
5.8.3. Epidemiological Surveillance
5.8.4. Microbial Diversity and Evolution Studies

5.9. Bioinformatics Tools for Genomics

5.9.1. Genomic Databases
5.9.2. Sequence Analysis Tools
5.9.3. Visualization of Genomic Data

5.10. Future of Genomics and Proteomics in the Clinical Laboratory

5.10.1. Recent and Future Developments in Genomics and Proteomics
5.10.2. Development of New Therapeutic Strategies
5.10.3. Technical and Bioinformatics Challenges
5.10.4. Ethical and Regulatory Implications

Module 6. Multidrug-Resistant Bacteria in the Food Chain

6.1. Multidrug-Resistant Bacteria in the Food Chain

6.1.1. The Role of the Food Chain in the Spread of Antimicrobial Resistance
6.1.2. Antimicrobial Resistances in Food (ESBL, MRSA, and Colistin)
6.1.3. The Food Chain within the One Health Approach

6.2. Dissemination of Antimicrobial Resistance through Food

6.2.1. Food of Animal Origin
6.2.2. Food of Plant Origin
6.2.3. Dissemination of Resistant Bacteria through Water

6.3. Spread of Resistant Bacteria in Food Production

6.3.1. Spread of Resistant Bacteria in Food Production Environments
6.3.2. Spread of Resistant Bacteria through Food Handlers
6.3.3. Cross-Resistance between Biocides and Antibiotics

6.4. Antimicrobial Resistance in Salmonella Spp

6.4.1. AmpC-, ESBL- and Carbapenemase-Producing Salmonella Spp
6.4.2. Resistant Salmonella Spp in Humans
6.4.3. Antibiotic Resistant Salmonella Spp in Farm and Meat Animals
6.4.4. Multidrug-Resistant Salmonella Spp

6.5. Antimicrobial Resistance in Campylobacter Spp

6.5.1. Antimicrobial Resistance in Campylobacter Spp
6.5.2. Antimicrobial Resistant Campylobacter Spp in Foods
6.5.3. Multidrug-Resistant Campylobacter Spp

6.6. Antimicrobial Resistances in Escherichia Coli

6.6.1. AmpC, ESBL and Carbapenemase Producing E. Coli
6.6.2. Antimicrobial Resistant E. Coli in Farm Animals
6.6.3. Antimicrobial Resistant E. Coli in Foodstuffs
6.6.4. Multidrug-Resistant E. Coli

6.7. Antimicrobial Resistance in Staphylococci

6.7.1. Methicillin-Resistant S. Aureus (MRSA)
6.7.2. MRSA in Food and Farm Animals
6.7.3. Methicillin-Resistant Staphylococcuys Epidermidis (MRSE)
6.7.4. Multidrug-Resistant Staphylococcus Spp

6.8. Antimicrobial Resistance in Enterobacteria

6.8.1. Shigella Spp
6.8.2. Enterobacter Spp
6.8.3. Other Environmental Enterobacteriaceae

6.9. Antimicrobial Resistance in Other Food-Borne Pathogens

6.9.1. Listeria Monocytogenes
6.9.2. Enterococcus Spp
6.9.3. Pseudomonas Spp
6.9.4. Aeromonas Spp and Plesiomonas Spp

6.10. Strategies to Prevent and Control the Spread of Microbial Resistance in the Food Chain

6.10.1. Preventive and Control Measures in Primary Production
6.10.2. Preventive and Control Measures in Slaughterhouses
6.10.3. Preventive and Control Measures in Food Industries

Module 7. Antimicrobial Resistance in Animal Health

7.1. Antibiotics in the Veterinary Field

7.1.1. Prescription
7.1.2. Acquisition
7.1.3. Misuse of Antibiotics

7.2. Multidrug-Resistant Bacteria in the Veterinary Field

7.2.1. Causes of Bacterial Resistance in the Veterinary Field
7.2.2. Dissemination of Antibiotic Resistance Genes (ARGs), Especially through Horizontal Transmission Mediated by Plasmids
7.2.3. Mobile Colistin Resistance Gene (mcr)

7.3. Multidrug-Resistant Bacterial Species of Veterinary Importance

7.3.1. Pet Pathogens
7.3.2. Cattle Pathogens
7.3.3. Pig Pathogens
7.3.4. Poultry Pathogens
7.3.5. Goat and Sheep Pathogens
7.3.6. Fish and Aquatic Animal Pathogens

7.4. Impact of Multi-Resistant Bacteria in Animal Health

7.4.1. Animal Suffering and Losses
7.4.2. Impact on Household Livelihoods
7.4.3. Generation of "Superbugs”

7.5. Multidrug-Resistant Bacteria in the Environment and Wildlife

7.5.1. Antibiotic Resistant Bacteria in the Environment
7.5.2. Antibiotic Resistant Bacteria in Wildlife
7.5.3. Antimicrobial Resistant Bacteria in Marine and Inland Waters

7.6. Impact of Resistances Detected in Animals and in the Environment on Public Health

7.6.1. Shared Antibiotics in Veterinary Medicine and Human Medicine
7.6.2. Transmission of Resistance from Animals to Humans
7.6.3. Transmission of Resistance from the Environment to Humans

7.7. Prevention and Control

7.7.1. Preventive Measures Against Bacterial Resistance in Animals
7.7.2. Systems and Processes for the Effective Use of Antibiotics
7.7.3. Role of Veterinarians and Pet Owners in the Prevention of Bacterial Resistance
7.7.4. Treatments and Alternatives to Antibiotics in Animals
7.7.5. Tools for Limiting the Emergence of Antimicrobial Resistance and its and Spread in the Environment

7.8. Strategic Plans to Reduce the Risk of Selection and Spread of Antimicrobial Resistance

7.8.1. Monitoring and Surveillance of the Use of Critical Antibiotics
7.8.2. Training and Research
7.8.3. Communication and Prevention

7.9. One Health Strategy

7.9.1. Definition and Objectives of the One Health Strategy
7.9.2. Application of the One Health Strategy in the Control of Multidrug-Resistant Bacteria
7.9.3. Success Stories Using the One Health Strategy

7.10. Climate Change and Antibiotic Resistance

7.10.1. Increase in Infectious Diseases
7.10.2. Extreme Climatic Conditions
7.10.3. Displacement of Populations

Module 8. Emerging Strategies for Multidrug-Resistant Bacteria

8.1. CRISPR-Cas9 Gene Editing

8.1.1. Molecular Mechanism of Action
8.1.2. Applications

8.1.2.1. CRISPR-Cas9 as a Therapeutic Tool
8.1.2.2. Engineering of Probiotic Bacteria
8.1.2.3. Rapid Detection of Resistance
8.1.2.4. Elimination of Resistance Plasmids
8.1.2.5. Development of New Antibiotics
8.1.2.6. Safety and Stability

8.1.3. Limitations and Challenges

8.2. Temporary Collateral Sensitization (SCT)

8.2.1. Molecular Mechanism
8.2.2. Advantages and Applications of SCT
8.2.3. Limitations and Challenges

8.3. Gene Silencing

8.3.1. Molecular Mechanism
8.3.2. RNA Interference
8.3.3. Antisense Oligonucleotides
8.3.4. Benefits and Applications of Gene Silencing
8.3.5. Limitations

8.4. High-Throughput Sequencing

8.4.1. Stages of High-Throughput Sequencing
8.4.2. Bioinformatics Tools for Combating Multidrug-Resistant Bacteria
8.4.3. Challenges

8.5. Nanoparticles

8.5.1. Mechanisms of Action against Bacteria
8.5.2. Clinical Applications
8.5.3. Limitations and Challenges

8.6. Engineering of Probiotic Bacteria

8.6.1. Production of Antimicrobial Molecules
8.6.2. Bacterial Antagonism
8.6.3. Modulation of the Immune System
8.6.4. Clinical Applications

8.6.4.1. Prevention of Nosocomial Infections
8.6.4.2. Reducing the Incidence of Respiratory Infections
8.6.4.3. Adjunctive Therapy in the Treatment of Urinary Tract Infections
8.6.4.4. Prevention of Resistant Skin Infections

8.6.5. Limitations and Challenges

8.7. Antibacterial Vaccines

8.7.1. Types of Vaccines against Diseases Caused by Bacteria
8.7.2. Vaccines in Development against Major Multidrug-Resistant Bacteria
8.7.3. Challenges and Considerations

8.8. Bacteriophages

8.8.1. Mechanism of Action
8.8.2. Lytic Cycle of Bacteriophages
8.8.3. Lysogenic Cycle of Bacteriophages

8.9. Phage Therapy

8.9.1. Isolation and Transport of Bacteriophages
8.9.2. Purification and Handling of Bacteriophages in the Laboratory
8.9.3. Phenotypic and Genetic Characterisation of Bacteriophages
8.9.4. Preclinical and Clinical Trials
8.9.5. Compassionate Use of Phages and Success Stories

8.10. Antibiotic Combination Therapy

8.10.1. Mechanisms of Action
8.10.2. Efficacy and Risks
8.10.3. Challenges and Constraints
8.10.4. Combined Antibiotic and Phage Therapy

Module 9. New Antimicrobial Molecules

9.1. New Antimicrobial Molecules

9.1.1. The Need for New Antimicrobial Molecules
9.1.2. Impact of New Molecules on Antimicrobial Resistance
9.1.3. Challenges and Opportunities in the Development of New Antimicrobial Molecules

9.2. Methods of Discovery of New Antimicrobial Molecules

9.2.1. Traditional Discovery Approaches
9.2.2. Advances in Screening Technology
9.2.3. Rational Drug Design Strategies
9.2.4. Biotechnology and Functional Genomics
9.2.5. Other Innovative Approaches

9.3. New Penicillins: New Drugs, their Future Role in Anti-Infective Therapeutics

9.3.1. Classification
9.3.2. Mechanism of Action
9.3.3. Antimicrobial Spectrum
9.3.4. Therapeutic Uses
9.3.5. Adverse Effects
9.3.6. Presentation and Dosage

9.4. Cephalosporins

9.4.1. Classification
9.4.2. Mechanism of Action
9.4.3. Antimicrobial Spectrum
9.4.4. Therapeutic Uses
9.4.5. Adverse Effects
9.4.6. Presentation and Dosage

9.5. Carbapenemics and Monobactams

9.5.1. Classification
9.5.2. Mechanism of Action
9.5.3. Antimicrobial Spectrum
9.5.4. Therapeutic Uses
9.5.5. Adverse Effects
9.5.6. Presentation and Dosage

9.6. Cyclic Glycopeptides and Lipopeptides

9.6.1. Classification
9.6.2. Mechanism of Action
9.6.3. Antimicrobial Spectrum
9.6.4. Therapeutic Uses
9.6.5. Adverse Effects
9.6.6. Presentation and Dosage

9.7. Macrolides, Ketolides and Tetracyclines

9.7.1. Classification
9.7.2. Mechanism of Action
9.7.3. Antimicrobial Spectrum
9.7.4. Therapeutic Uses
9.7.5. Adverse Effects
9.7.6. Presentation and Dosage

9.8. Aminoglycosides and Quinolones

9.8.1. Classification
9.8.2. Mechanism of Action
9.8.3. Antimicrobial Spectrum
9.8.4. Therapeutic Uses
9.8.5. Adverse Effects
9.8.6. Presentation and Dosage

9.9. Lincosamides, Streptogramins and Oxazolidinones

9.9.1. Classification
9.9.2. Mechanism of Action
9.9.3. Antimicrobial Spectrum
9.9.4. Therapeutic Uses
9.9.5. Adverse Effects
9.9.6. Presentation and Dosage

9.10. Rifamycins and other Developmental Antimicrobial Molecules

9.10.1. Rifamycins: Classification

9.10.1.1. Mechanism of Action
9.10.1.2. Antimicrobial Spectrum
9.10.1.3. Therapeutic Uses
9.10.1.4. Adverse Effects
9.10.1.5. Presentation and Dosage

9.10.2. Antibiotics of Natural Origin
9.10.3. Synthetic Antimicrobial Agents
9.10.4. Antimicrobial Peptides
9.10.5. Antimicrobial Nanoparticles

Module 10. Artificial Intelligence in Clinical Microbiology and Infectious Diseases

10.1. Artificial Intelligence (AI) in Clinical Microbiology and Infectious Diseases

10.1.1. Current Expectation of AI in Clinical Microbiology
10.1.2. Emerging Areas Interrelated to AI
10.1.3. Transversality of AI

10.2. Artificial Intelligence (AI) Techniques and other Complementary Technologies applied to Clinical Microbiology and Infectious Diseases

10.2.1. AI Logic and Models
10.2.2. Technologies for AI

10.2.2.1. Machine Learning
10.2.2.2. Deep Learning
10.2.2.3. Data Science and Big Data

10.3. Artificial Intelligence (AI) in Microbiology

10.3.1. AI in Microbiology: History and Evolution
10.3.2. AI Technologies that can be Used in Microbiology
10.3.3. Research Objectives of AI in Microbiology

10.3.3.1. Understanding Bacterial Diversity
10.3.3.2. Exploring Bacterial Physiology
10.3.3.3. Investigation of Bacterial Pathogenicity
10.3.3.4. Epidemiological Surveillance
10.3.3.5. Development of Antimicrobial Therapies
10.3.3.6. Microbiology in Industry and Biotechnology

10.4. Classification and Identification of Bacteria using Artificial Intelligence (AI)

10.4.1. Machine Learning Techniques for Bacterial Identification
10.4.2. Taxonomy of Multi-Resistant Bacteria using AI
10.4.3. Practical Implementation of AI in Clinical and Research Laboratories in Microbiology

10.5. Bacterial Protein Decoding

10.5.1. AI Algorithms and Models for Protein Structure Prediction
10.5.2. Applications in the Identification and Understanding of Resistance Mechanisms
10.5.3. Practical Application AlphaFold and Rosetta

10.6. Decoding the Genome of Multi-Resistant Bacteria

10.6.1. Identification of Resistance Genes
10.6.2. Genomic Big Data Analysis: AI-Assisted Sequencing of Bacterial Genomes
10.6.3. Practical Application Identification of Resistance Genes

10.7. Artificial Intelligence (AI) Strategies in Microbiology and Public Health

10.7.1. Infectious Outbreak Management
10.7.2. Epidemiological Surveillance
10.7.3. AI for Personalized Treatments

10.8. Artificial Intelligence (AI) to Combat Antibiotic Resistance in Bacteria

10.8.1. Optimizing Antibiotic Use
10.8.2. Predictive Models for the Evolution of Antimicrobial Resistance
10.8.3. Targeted Therapy Based on Development of New Antibiotics by IA

10.9. Future of Artificial Intelligence in Microbiology

10.9.1. Synergies between Microbiology and IA
10.9.2. Lines of AI Implementation in Microbiology
10.9.3. Long-Term Vision of the Impact of AI in the Fight against Multi-Drug Resistant Bacteria

10.10. Technical and Ethical Challenges in the Implementation of Artificial Intelligence (AI) in Microbiology

10.10.1. Legal Considerations
10.10.2. Ethical and Liability Considerations
10.10.3. Barriers to AI Implementation

10.10.3.1. Technical Barriers
10.10.3.2. Social Barriers
10.10.3.3. Economic Barriers
10.10.3.4. Cybersecurity 

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