PULMONARY SURFACTANT, ALPHA 1 ANTITRYPSIN INHIBITOR DEFICIENCY, AND CYSTIC FIBROSIS DR. NABIL BASHIR BIOCHEMISTRY/RESPIRATORY SYSTEM

Similar documents
Respiratory Pharmacology: Treatment of Cystic Fibrosis

PHOSPHOLIPIDS METABOLISM. BY Dr. Walid Said Zaki Dr. Marwa Ali LECTURER OF BIOCHEMISTRY AND MOLECULAR BIOLOGY

Cystic Fibrosis. Presented by: Chris Belanger & Dylan Medd

Pulmonary Surfactant. Jian kang, M.D. Pediatric PGY-2

Human Genetic Diseases (Ch. 15)

Evaluation of Patients with Diffuse Bronchiectasis

Human Genetic Disorders

Human Genetic Diseases. AP Biology

What is the inheritance pattern (e.g., autosomal, sex-linked, dominant, recessive, etc.)?

Lesson Overview. Human Genetic Disorders. Lesson Overview Human Genetic Disorders

Tay Sachs, Cystic Fibrosis, Sickle Cell Anemia and PKU. Tay Sachs Disease (also called Hexosaminidase deficiency)

UNDERSTANDING CYSTIC FIBROSIS

Human Genetic Diseases. AP Biology

Case Study What is the Relationship Between the Cell Membrane and Cystic Fibrosis?

Diseases of the gastrointestinal system. H Awad Lecture 2: small intestine/ part 2 and appendix

Lesson Overview. Human Genetic Disorders. Lesson Overview Human Genetic Disorders

What is Cystic Fibrosis? CYSTIC FIBROSIS. Genetics of CF

Cystic Fibrosis. Parkland College. Monica Rahman Parkland College. Recommended Citation

A Case of Cystic Fibrosis

Human Genetic Disorders. Lesson Overview. Lesson Overview Human Genetic Disorders

B1 Question 1 Foundation

Alpha-1 Antitrypsin Deficiency AATD

E-BOOK # PANCREATIC ENZYMES FOR CYSTIC FIBROSIS ARCHIVE

What You ll Learn. Genetics Since Mendel. ! Explain how traits are inherited by incomplete dominance

Week 3 The Pancreas: Pancreatic ph buffering:

BIO113 Exam 2 Ch 4, 10, 13

Cystic Fibrosis. Information for Caregivers

Atypical cystic fibrosis: from the genetic causes to current and future treatments

FACTS ABOUT. Cystic Fibrosis. What Is Cystic Fibrosis. What Are the Signs and Symptoms of CF?

Genetic diseases. - chromosomal disorders (aneuploidy) - mitochondrial inherited diseases (female lineage transmission)

Pediatrics Grand Rounds 18 Sept University of Texas Health Science Center. + Disclosure. + Learning Objectives.

CYSTIC FIBROSIS OBJECTIVES NO CONFLICT OF INTEREST TO DISCLOSE

Biochemistry #03 Dr. Nabil Bashir Maryam Alsourti

Each person has a unique set of characteristics, such as eye colour, height and blood group.

PATIENT EDUCATION. Cystic Fibrosis Carrier Testing

Caring for a person with cystic fibrosis

Friday, January 4. Bell Work:

Cystic Fibrosis. Jennifer McDaniel, BS, RRT-NPS

Essential Questions. Basic Patterns of Human Inheritance. Copyright McGraw-Hill Education

Cystic Fibrosis. Na+ 2Cl - K+ Na+ Na+

The Role of Amniotic Fluid Phospholipids in Determining Fetal Lung Maturity

Genetic Diseases. Genetic diseases occur when an individual s DNA has one or more abnormalities.

The Cell Membrane. Page by: OpenStax

THE ROLE OF CFTR MUTATIONS IN CAUSING CYSTIC FIBROSIS (CF)

GENETIC TESTING: IN WHOM AND WHEN

Diseases of exocrine pancreas

Figure 1: Transmission of Wing Shape & Body Color Alleles: F0 Mating. Figure 1.1: Transmission of Wing Shape & Body Color Alleles: Expected F1 Outcome

Cystic Fibrosis Foundation Patient Registry 2013

A review of Cystic Fibrosis

Liver Disease in Cystic Fibrosis

Hths 2231 Laboratory 3 Genetics

Genome - Wide Linkage Mapping

Medical Policy An independent licensee of the Blue Cross Blue Shield Association

NOTES: : HUMAN HEREDITY

Questions Q1. ) in the box next to your answer. (1) A FF B Ff C ff. D ff (ii) Explain why a person with cystic fibrosis (CF) may lose body mass.

Chapters 9 and 10 Lipids and Membranes

Cystic fibrosis: hitting the target

Medical Policy An independent licensee of the Blue Cross Blue Shield Association

Symdeko. Symdeko (tezacaftor and ivacaftor) Description

TEST INFORMATION Test: CarrierMap GEN (Genotyping) Panel: CarrierMap Expanded Diseases Tested: 311 Genes Tested: 299 Mutations Tested: 2647

Recessive Genetic Disorders! A recessive trait is expressed when the individual is homozygous recessive for the trait.

"Management and Treatment of Patients with Cystic fibrosis (CF)

water flows over gills What is meant by the term gas exchange? (1) Suggest three ways in which fish gills are adapted for efficient gas exchange.

Cystic Fibrosis 8/23/2014 GROWTH DEFICIENCY IN CYSTIC FIBROSIS IS

Pulmo-Park Pom-Pom Shooter: Measuring the Effect of Restricted Breathing on Peak Expiratory Flow (PEF) Student Information Page Activity 5D


PomPom SHOOTER. Activity Background: Common Obstructive Lung Disorders:

Cystic Fibrosis Carrier Testing

The Cell Membrane & Movement of Materials In & Out of Cells PACKET #11

Phospholipids Metabolism

The Cystic Fibrosis Gene. about. CF is one of the most common genetic diseases that cause death in both children and

IN SCHOOL ARTICLE Vitamin D3 Blocks NFkB Activation in an In Vitro Model of Cystic Fibrosis

Biochemistry of Lungs. Lecture # 35 Lecturer: Alexander Koval

Pathophysiology. Tutorial 1 Genetic Diseases

CYSTIC FIBROSIS Risk Factors Epidemiology Pathogenesis Defective protein synthesis (10%) Abnormal protein folding, processing & trafficking

Update on ChILD. R. Paul Guillerman, MD Associate Professor Department of Pediatric Radiology

Cell Membrane Study Guide

Transformational Treatments. PRESTON W. CAMPBELL, III, M.D. Executive Vice President for Medical Affairs

Cystic Fibrosis New Patient Binder Cystic Fibrosis Center Pediatric Pulmonary Division

IVACAFTOR THE ISRAELI EXPERIENCE ADI DAGAN MD THE ISRAELI CF CENTER SHEBA MEDICAL CENTER, TEL-HASHOMER

Bronchitis. Anatomy of the Lungs The lungs allow us to fill our blood with oxygen. The oxygen we breathe is absorbed into our blood in the lungs.

The Cell Membrane (Ch. 7)

Two copies of each autosomal gene affect phenotype.

Orkambi. Orkambi (lumacaftor/ivacaftor) Description

Kalydeco. Kalydeco (ivacaftor) Description

Notes to complete gas exchange in mammals

Corporate Medical Policy

Function of the skeleton

Genetic Diseases. SCPA202: Basic Pathology

Lab Activity Report: Mendelian Genetics - Genetic Disorders

End of Course Assessment Review Packet Due: Monday, June 2nd

SCIENCE OLYMPIAD CAPTAINS TRYOUTS DIVISION C ANATOMY & PHYSIOLOGY. Written by Monta Vista Science Olympiad

Classification of Lipids

Chapter 10 Respiration

Monosaccharides: Little amounts Don t need any digestion

Familial Hypercholesterolaemia

Section 37 1 The Circulatory System (pages )

Section 37 1 The Circulatory System (pages )

10.4 Interference with Gas Exchange

Cystic Fibrosis the future

Transcription:

PULMONARY SURFACTANT, ALPHA 1 ANTITRYPSIN INHIBITOR DEFICIENCY, AND CYSTIC FIBROSIS DR. NABIL BASHIR BIOCHEMISTRY/RESPIRATORY SYSTEM

Pulmonary surfactant Pulmonary surfactant is (phospholipoprotein) complex The proteins and lipids that make up the surfactant have both hydrophilic and hydrophobic regions. By adsorbing to the air-water interface of alveoli, with hydrophilic head groups in the water and the hydrophobic tails facing towards the air, the main lipid component of surfactant, dipalmitoylphosphatidylcholine (DPPC), reduces surface tension.

Composition -40% dipalmitoylphosphatidylcholine (DPPC); -40% other phospholipids (PCs); -5% surfactant proteins (SP-A, SP-B, SP-C and SP-D); -Cholesterol (neutral lipids)

09 تشرين الثاني 17 4

09 تشرين الثاني 17 5

09 تشرين الثاني 17 6

09 تشرين الثاني 17 7

Proteins Proteins make up the remaining 10% of the surfactant. Half of this 10% is plasma proteins the rest is formed by the apolipoproteins, surfactant proteins SP-A, SP-B, SP-C, and SP-D.

SP-A and SP-D confer innate immunity SP-A is involved in a negative feedback mechanism to control the production of surfactant. SP-B and SP-C are hydrophobic membrane proteins that increase the rate that surfactant spreads over the surface-- lower surface tension. congenital absence of SP-B ----- respiratory failure congenital absence of SP-C ----- progressive interstitial pneumonitis.

Infant respiratory distress syndrome (IRDS) Infant respiratory distress syndrome (IRDS), also called neonatal respiratory distress syndrome (NRDS), respiratory distress syndrome of newborn. developmental insufficiency of pulmonary surfactant production and structural immaturity in the lungs. It can also be a consequence of neonatal infection. It can also result from a genetic problem with the production of surfactant associated proteins

Surfactant metabolism dysfunction SFTPB mutations.: complete lack of mature SP-B protein. autosomal recessive manner. SFTPC mutations : autosomal dominant pattern, although the onset and severity of lung disease are highly variable, even within the same family.

Lecithins Lecithins are mixtures of glycerophospholipids including: - phosphatidylcholine, - phosphatidylethanolamine, - phosphatidylinositol, - phosphatidic acid.

Biochemical tests to determine lung maturity 1. Lecithin/sphingomyelin (L/S) ratio : A ratio >2 indicates low risk for RDS. 2. Phosphatidylglycerol (PG): Value >0.3 is associated with low risk for RDS. 09 تشرين الثاني 17 13

Alpha-1 Antitrypsin Deficiency Alpha-1 antitrypsin deficiency is an inherited disorder that may cause lung disease and liver disease. Affected individuals often develop emphysema, damage to alveoli. Smoking or exposure to tobacco smoke accelerates the appearance of emphysema symptoms and damage to the lungs.

Genetic changes Mutations in the SERPINA1 gene cause alpha- 1 antitrypsin deficiency. alpha-1 antitrypsin protects the body from a powerful enzyme called neutrophil elastase. Neutrophil elastase is released from white blood cells to fight infection, but it can attack normal tissues (especially the lungs) if not tightly controlled by alpha-1 antitrypsin.

More than 120 mutations in the SERPINA1 gene have been identified. The most common mutation replaces the amino acid glutamic acid - lysine at protein position 342 (written as Glu342Lys or E342K). This mutation results in a version of the SERPINA1 gene called the Z allele that produces very little alpha-1 antitrypsin.

Inheritance patterns This condition is inherited in an autosomal codominant pattern. Codominance means that two different versions of the gene may be active (expressed), and both versions contribute to the genetic trait. The most common version (allele) of the SERPINA1 gene, called M, produces normal levels of alpha-1 antitrypsin. Most people in the general population have two copies of the M allele (MM) in each cell.

M--- normal S --- low levels alpha-1 antitrypsin Z --- very little alpha-1 antitrypsin. ZZ --- have alpha-1 antitrypsin deficiency. SZ --- increased risk of developing lung diseases (such as emphysema), particularly if they smoke.

Cystic Fibrosis Cystic fibrosis : recessive genetic mutations in the Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) gene. Classic cystic fibrosis is characterized by chronic bacterial infection of the airways,fat maldigestion due to pancreatic exocrine insufficiency, infertility in males due to obstructive azoospermia, and elevated concentrations of chloride in sweat.

Molecular Genetics and Gene Function Gene Structure: 250,000 bp long and contains 27 exons. mrna: 6129 bp long. Protein Size: The CFTR protein is 1480 amino acids long and has a molecular weight of 168,173 Da. Protein Function: chloride channel protein found in membranes of cells that line passageways of the lungs, liver, pancreas, intestines, reproductive tract, and skin.

CFTR controls chloride ion movement in and out of the cell. CFTR FUNCTION

CFTR FUNCTION.

Protein Structure and Function CFTR transports chloride ions (Cl-) ions across the membranes of cells in the lungs, liver, pancreas, digestive tract, reproductive tract, and skin. CFTR is made up of five domains: two membrane-spanning domains (MSD1 and MSD2) that form the chloride ion channel two nucleotide-binding domains (NBD1 and NBD2) that bind and hydrolyze ATP (adenosine triphosphate) and a regulatory (R) domain. Delta F508, the most common CF-causing mutation, occurs in the DNA sequence that codes for the first nucleotide-binding domain (NBD1).

delta F508 mutation Incorrect folding- degradation. - never reaches the cell membrane. homozygous for delta F508 mutation -- critical loss of chloride ion transport. This upsets the sodium and chloride ion balance needed to maintain the normal, thin mucus layer that is easily removed by cilia lining the lungs and other organs. The sodium and chloride ion imbalance creates a thick, sticky mucus layer that cannot be removed by cilia and traps bacteria, resulting in chronic infections.

Presentation of Disease

Gene Therapy In the case of CF, gene therapy involves inhaling a spray that delivers normal DNA to the lungs.

2024 © healthdocbox.com Privacy Policy | Terms of Service | Feedback