Bloodkb 160720181259
Bloodkb 160720181259
Bloodkb 160720181259
disorders
Presented by:
Dr. Jeena Raj
CONTENTS
• Introduction
• Red blood cell and its disorders
• White blood cell and its disorders
• Platelet and its disorders
• Coagulation disorders
• Anticoagulant-Related Coagulopathies
• Disease-Related Coagulopathies
• Conclusion
RED BLOOD CELL AND ITS DISORDERS
Physiological variations
A. Increase in RBC:
1. Age
2. Sex
3. High altitude
4. Muscular exercise
5. Emotional conditions
6. Increase environmental temperature
7. After meals
B. Decrease in RBC:
1. High barometric pressures
2. After sleep
3. Pregnancy
Pathological variation:
1. Polycythemia
2. Anemia
RED BLOOD CELL DISORDERS
• Erythrocytoses
• Polycythemia vera
• Anemia
Iron deficiency anemia
Anemia owing to hemolysis
Sickle cell anemia
Erythroblastosis fetalis
Thalassemia
Pernicious anemia
Aplastic anemia
Erythrocytoses
• Asymptomatic
• Pruritis
• Vertigo
• Gastrointestinal pain
• Headache
• Paresthesias, fatigue, weakness,
• visual disturbances, tinnitus,
Oral Manifestations
• Erythema (red-purple color) of mucosa,
• Glossitis,
• Erythematous & edematous gingiva
• Spontaneous gingival bleeding
Laboratory findings
• RBC- normochromic normocytic- >10,000.000/cubic mm
• HEMOGLOBIN: >20gm/dl
• PLATELETS- 400,000-800,000/dl
• BONE MARROW- hypercellular, megakaryocytes are increased
TREATMENT
• Phlebotomy
• Chemotherapy
• Radioactive phosphorus
ANEMIA
• Anemia refers to reduction in
1. Red blood cell count
2. Hemoglobin content
3. Packed cell volume
Etiology
• Chronic blood loss
• Inadequate dietary intake
• Faulty iron absorption
• Increased for iron- infancy, childhood,
requirements
pregnancy.
Clinical Manifestations
• Chronic fatigue
• Pallor of the conjunctiva, lips, and
oral
mucosa;
• Brittle nails with spooning, cracking,
• Splitting of nail beds, koilonychia
• Palmar creases
• Palpitations
• Shortness of breath, numbness
• Bone pain
Oral Manifestations
• Angular cheilitis,
• Glossitis with different degrees of atrophy
of fungiform and filliform papillae
• Pale oral mucosa
• Oral candidiasis
• Recurrent aphthous stomatitis
• Erythematous mucositis
• Burning mouth
Laboratory findings
Etiopathogenesis :
• Unknown - iron deficiency.
• Malnutrition,
• Genetic predisposition and Autoimmune processes.
Laboratory findings:
• An elevated reticulocyte count is the most useful
indicator of hemolysis, reflecting erythroid hyperplasia
of the bone marrow.
Sickle Cell Disease/Sickle Cell Anemia
• Hereditary type of chronic hemolytic anemia transmitted as
a mendalian dominant, nongender linked characteristic.
• Exclusively in blacks and in whites of Mediterranean origin.
• A concordance exists between the prevalence of malaria and
HbS
Obstructs microcirculation
Hypoxia → promotes
sickling
Clinical Manifestations
Blood smear:
• Typical sickle- shaped RBCs seen
Treatment :
• Management of vaso-occlusive crisis
• Management of chronic pain syndrome
• Management of chronic hemolytic anemia
• Prevention and treatment of infections
• Management of the complications.
Erythroblastosis fetalis
Oral manifestation
• Deposition of blood pigments in the enamel and dentin
• Ground sections- positive test for bilirubin
• Intrinsic stains
• Enamel hypoplasia
• Rh hump
Laboratory findings
• RBC count decreased, large number of normoblasts or
nucleated red cells
• Icterus index high
• Positive direct coombs test on cord blood
Treatment
• At present, Rh-negative mothers are being given anti-
D
gamma globulin to prevent immunization
Thalassemias
• Thalassemia is a group of genetic disorders of
hemoglobin synthesis characterized by a disturbance of
either alpha (α) or beta (β) hemoglobin chain production.
• An estimated 900,000 births are expected to occur in the
next 20 years with clinically significant thalassemia
disorders
• First described by Thomas B Cooley in 1925.
• Thalassa means ‘sea’in Greek.
Pathogenesis:
• Normal adult hemoglobin (HbA)- heme is conjugated to globin.
• Globin- 2 pairs of α chain and β chain.
Laboratory findings
• Hypochromic microcytic
• RBC- exhibiting Poikilocytosis and Anisocytosis.
• Safety pin cells and nucleated RBCs in the circulating RBC
is also a characteristic feature.
• WBC- frequently elevated.
• Bone marrow- cellular hyperplasia with large number
of
immature, primitive and stem form of RBCs.
• Supravital staining- Methyl blue demonstrate
inclusion bodies.
Radiographic findings
• RIB- WITHIN- A- RIB: noted in middle and anterior
portion of the ribs. Long linear density within or
overlapping the medullary space of the rib and running
parallel to its long axis.
• HAIR- ON- END appearance.
• SALT AND PEPPER EFFECT: peculiar trabeculae pattern
of maxilla and mandible, apparent coarsening of some
trabeculae and the blurring and disappearance of others.
Treatment
TREATMENT:
• Weekly intramuscular injections of 1,000 μg of vitamin
B12 for the initial 4 to 6 weeks, followed by 1,000 μg per
week indefinitely.
• Delayed treatment permits progression of the anemia
and neurological complication
Aplastic Anemia
• Aplastic anemia (AA) is a rare blood dyscrasia in which
peripheral blood pancytopenia results from reduced or
absent blood cell production in the bone marrow and
normal hematopoietic tissue in the bone marrow has been
replaced by fatty marrow.
• Environmental exposures, such as to drugs, viruses, and
toxins, are thought to trigger the aberrant immune
response in some patients, but most cases are classified as
idiopathic
2 chief forms:
• Primary aplastic anemia: unknown etiology.
young adults, develops rapidly and terminates fatally.
FANCONI’S SYNDROME: congenital, sometimes familial,
aplastic anemia is associated with other congenital defects
including bone abnormalities, microcephaly, hypogenitalism
and generalized olive brown pigmentation of the skin.
Laboratory findings
• RBC- diminished as low as 1,000,000 cells per cubic mm
• ↓ in hemoglobin level.
• A paucity of granulocytes, monocytes and reticulocytes is
found.
• Prolonged bleeding time
• Tourniquet test is positive.
BONE MARROW SMEAR:
• Anemia: erythropoietic depression, appears
marrow normal or even hyperplastic.
• Pancytopenia- hypoplasia of all marrow
• element
Severe cases- hypocellular bone marrow with fatty
replacement and relatively increased nonhematopoietic
element such as plasma cell and mast cell.
Treatment
• Blood transfusions to correct anemia and thrombocytopenia
• Immunosuppression with antithymocyte globulins
and
cyclosporine is effective at restoring blood cell production
Oral Health Considerations
• Neutropenia leads to an increased susceptibility to infection,
• Thrombocytopenia leads to bruising and mucosal bleeding.
• Neutropenic fevers must be treated aggressively with
parenteral, broad-spectrum antibiotics.
• Antifungal therapy should be added
• Attention to details of oral hygiene and hand washing and
avoidance of minor injuries or casual exposure to infectious
agents can reduce the risk of serious complications.
WHITE BLOOD CELLS AND ITS DISORDERS
• White blood cells (WBCs),
also called leukocytes or leucocytes, are the cells
of the immune system that are involved in protecting the
body against both infectious disease and foreign invaders.
• All white blood cells are produced and derived from
multipotent cells in the bone marrow known
as hematopoietic stem cells.
• Leukocytes are found throughout the body, including
the blood and lymphatic system
• 2 types: granulocytes and agranulocytes
Variations in the number of white blood cells
PHYSIOLOGICAL
VARIATIONS:
• Age
• Sex
• Diurnal variations
• Exercise
• Emotional condition
• Pregnancy
• Sleep
PATHOLOGICAL
VARIATIONS
• Leukopania
• Leukocytosis
• Neutrophilia
• Eosinophilia
• Basophilia
• Monocytosis
• Lymphocytosis
• Leukemia
Disorders
• Leukocytosis
• Leukopenia
• Agranulocytosis
• Neutropenia
• Chediak – Higashi Syndrome
• Acute Leukemia
• Chronic leukemia
LEUKOCYTOSIS
• Defined as abnormal increase in the number of circulating
WBCs.
• Considered to be a manifestation of the reaction of the body
to a pathologic situation.
• It may also occur after exercise, convulsions such as
epilepsy, emotional stress, pregnancy, anesthesia, and
epinephrine administration.
• There are five principal types of leukocytosis:
1. Neutrophilia (the most common form)
2. Lymphocytosis
3. Monocytosis
4. Eosinophilia
5. Basophilia
Neutrophilia
• Physiologic- in new born, during labor, after exercise,
convulsions
• Acute infections- certain bacilli, fungi, viruses, parasites.
• Inflammatory conditions- Gout, Burns, Vascular
disease, Hypersensitivity reactions
• Intoxications- Uremia, Poisoning by chemicals and drugs- lead,
mercury.
• Acute hemorrhage
• Acute hemolysis
• Polycythemia, myelotic leukemia.
Eosinophilia
• Allergic disorders- bronchial asthma, hay fever
• Skin disease- phemphigus, erythema multiforme
• Scarlet fever,
• Parasitic infection- malaria.
• Diseases of the hemopoietic system- chronic myeloid
leukemia, polycythema vera, hodgkins disease, pernicious
anemia
• Following irradiation
• Sarcoidosis, rheumatoid arthritis.
Basophilia
• Splenectomy
• Blood disease- CML, polycythemia vera, hodgkin’s
anemia
• Infection- smallpox, chickenpox
• After injection of foreign proteins
Lymphocytosis
• Acute Infections- infectious mononucleosis,
• Chronic Infections- tuberculosis, syphilis,
• Lymphocytic leukemia, lymphosarcoma
• Hemopoietic disorders- lymphocytosis,
• Mumps, german measles, thyrotoxicosis.
Monocytosis
• Bacterial infections- tuberculosis, SABE, syphilis,
• Protozoal and Rickettsial- malaria, typhus, kala-azar
• CML, hodgkin’s disease, multiple myeloma
• Lipid storage disease- Gaucher’s disease
• Granulomatous disease- sarcoidosis, ulcerative colitis
• Collagen vascular disease- lupus
erythematosus,
rheumatoid arthritis.
LEUKOPENIA
• Leukopenia is a decrease in the number of white blood
cells (leukocytes) found in the blood, which places individuals
at increased risk of infection.
CAUSES:
1) Infections:
• A) Bacterial – typhoid fever, Paratyphoid fever, Brucellosis
• B) Viral and Rickettsial- Influenza, Measles,
Chickenpox, Dengue, Infectious Hepatitis
• C) Protozoal- Malaria, Kala-azar
2) Hemopoietic disorders:
• Gaucher’s disease, Pernicious anemia, Aplastic
anemia, Chronic hypochromic anemia,
Agranuocytosis
3) Chemical agents:
• Mustards, Benzene, Urethane.
• Analgesics, Anticonvulsants, Sulfonamides,
Antihistamines, Antithyroid drugs.
4) X-ray radiations
5) Anaphylactid shock
6) Liver cirrhosis, DLE
Agranulocytosis
(Neutropenia/Granulocytopenia)
Types:
• Primary Agranulocytosis- unknown etiology
• Secondary Agranulocytosis- known etiology.
ETIOLOGY
• Antineoplastics, Drugs → hapten
• Antibiotics,
• Anticonvulsants, Induce Antibody formation
Laboratory findings
• WBC are often below 2000 cells per cubic mm
• Almost complete absence of granulocytes or
PMNs.
• RBC and platelet counts are normal
Treatment
Laboratory findings:
• Patient exhibit a normal blood count which, over a period
of 4-5 days, begins to show a precipitous decline in
neutrophil count compensated by an increase in
monocytes and lymphocytes.
• Neutrophil count completely disappear for 1-2 days,
however cells begins to reappear within 4-5 days.
Treatment
• No specific treatment
• Splenectomy may be beneficial.
Chédiak-Higashi Syndrome
Laboratory findings
• Exhibit giant abnormal granules in the peripheral
circulating leukocytes and in the marrow precursors.
• Granules represent abnormal lysosomes bear resemblanc to toxic
granulations and Dohle bodies.
• Pancytopenia may be present.
Treatment
• No specific treatment
• Most of the therapy available in CHS is symptomatic, such
as childhood immunizations and antibiotics for infections.
Oral Health Considerations
• When oral surgical procedures are planned, excessive
operative blood loss should be anticipated secondary to
qualitive defects in platelet function.
• Intramuscular injections should be avoided.
• Patients often have photophobia and may be sensitive to the
bright operatory lights.
• Patients can be encouraged to bring sunglasses to dental
appointments.
Leukemia
• Leukemia is a disease characterized by the progressive
overproduction of WBCs which usually appear in the
circulating blood in an immature form.
• True malignant neoplasm- proliferation of WBC or
their precursors occurs in such as uncoordinated and
independent fashion.
• Leukemic cells multiply at the expense of normal
hematopoietic cell lines, resulting in marrow failure,
altered blood cell counts, and, when untreated, death from
infection, bleeding, or both.
Leukemia is classified into:
• Lymphoid (lymphoblastic, lymphocytic) leukemia- involving
the lymphocytic series.
• Myeloid (myelogenous) leukemia- involving progenitor cells
that gives rise to terminally differentiated cells of the myeloid
series (erythrocytes, granulocytes, monocytes, platelets).
• Weakness,
• Fever, headache
• Generalized swelling of lymph node
• Petechial or ecchymotic hemorrhages in the skin
and mucous membrane
• Anemia
• Spleen, liver and kidney become enlarged owing
to leukemic infiltration.
• Hemorrhage
CHRONIC LEUKEMIA
Laboratory findings
• Platelet count is usually below 60,000 platelets/cubic mm
• Bleeding time is prolonged
• Coagulation time- normal
Treatment
• No specific treatment
• Splenomegaly
• Corticosteroids
Laboratory findings
• Fragmented RBCs consistent with hemolysis are noted in
the peripheral smear.
• Reticulocyte count is also elevated
• PT and PTT are within normal limits
• LDH levels are increased
• Urinalysis- proteinuria and hematuria
Histologic features
• Widespread microthrombi in the arterioles, venules and
capillaries.
• Intravascular thrombi are composed of loose aggregates
of platelets that become organized into amorphous plugs
which are than replaced by fibrins.
Treatment
• Corticosteroids
• Platelet aggregation inhibitors
• Splenectomy
• Exchange transfusion
Thrombocytasthenia
Oral manifestation
• Spontaneous gingival bleeding
• Mucosal ecchymosis
• Excessive and prolonged bleeding from extraction socket
Laboratory findings
• Platelet count- nearly normal
• Bleeding time- is either normal or prolonged
• Normal capillary plugging is impaired
Treatment
• Conventional hemostatic agents
• Blood transfusion
Thrombocythemia/ Thrombocytosis
Oral manifestations
• Spontaneous gingival bleeding
• Excessive and prolonged bleeding
Laboratory findings
• Platelet count is increased
• Clotting time, PT, clot retraction and tourniquet test- all
are normal
Treatment
• Radioactive phosphorus
• Blood transfusion
• Corticosteroids
• Aspirin, heparin
Congenital coagulopathies
Hemophilia
• Blood disease characterized by prolonged coagulation time
and
hemorrhagic tendencies.
• Hereditary disease, defect being carried by x-chromosome,
• Transmitted as a gender-linked Mendelian recessive trait.
• Occurs only in males, transmitted through an unaffected daughter to
a grandson.
Etiology
• Hemophilia A- Plasma Thromboplastinogen (AHG factor VIII)
• Hemophilia B- Plasma Thromboplastin component (PTC factor IX)
• Hemophilia C- Plasma Thromboplastin antecedent (PTA factor XI)
Hemophilia A
• A deficiency of F VIII, the antihemophilic factor, is
inherited as an X-linked recessive trait that affects males.
The trait is carried in the female without clinical evidence
of the disease.
Clinical signs:
• hematomas, hemarthroses, hematuria,
• gastrointestinal bleeding, and
• bleeding from lacerations
• head trauma or spontaneous intracranial bleeding
• Joint synovitis, hemophilic arthropathies
• Intramuscular bleed and pseudotumors
Hemophilia B
• Due to PTC deficiency also known as Christmas disease.
• 2 forms- apparently normal levels of the inactive protein
and another in which there is deficient level of the
coagulant factor.
Hemophilia C
• Mild disorder seen in pedigrees of Jewish descent; it is
transmitted as an autosomal dominant trait.
• Bleeding symptoms do occur but are usually mild.
Oral manifeststions
• Gingival Hemorrhage- massive and prolonged
• Pseudotumor
Laboratory findings
• Prolonged coagulation time
• Bleeding time- normal
• PTT is prolonged
Treatment
• Preoperative transfusion of whole blood
• Administration of antihemophilic factor
• Protected from traumatic injuries