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Bleeding disorder &
Periodontitis
Department Of Periodontics
Dr Sachin RathodDr Sachin Rathod
Email:- drsachin.rathod@yahoo.comEmail:- drsachin.rathod@yahoo.com
Content
• Definition
• Etiology
• Evaluation
• Dental management
• Summary
Definition
• Periodontitis
Periodontitis is a set of inflammatory diseases affecting the
periodontium, i.e., the tissues that surround and support
the teeth.
• Bleeding disorders
Bleeding disorders are a group of conditions in which there is a
problem with the body's blood clotting process. These disorders
can lead to heavy and prolonged bleeding after an injury.
Etiology of bleeding disorder
 1. Thrombocytopenia purpuras
 2. Disorders of coagulation
Etiology Of Periodontitis
• Periodontitis is caused by microorganisms that adhere to
and grow on the tooth's surfaces, along with an overly
aggressive immune response against these
microorganisms.
• Periodontitis is an inflammation of
the periodontium, i.e., the tissues that
support the teeth. The periodontium consists
of four tissues:
• gingiva, or gum tissue,
• cementum, or outer layer of the roots of
teeth,
• alveolar bone, or the bony sockets into
which the teeth are anchored, and
• periodontal ligaments (PDLs), which are
the connective tissue fibers that run
between the cementum and the alveolar
bone.
Signs and symptoms
• Redness or bleeding of gums while brushing teeth
• Gum swelling that recurs
• Spitting out blood after brushing teeth
• Halitosis, or bad breath, and a persistent metallic
taste in the mouth
• Gingival recession, resulting in apparent
lengthening of teeth.
• Deep pockets between the teeth and the gums
• Loose teeth, in the later stage
Treatment
• Excellent Oral Hygiene : This includes
twice-daily brushing with daily flossing.
• use of an interdental brush is helpful if
space between the teeth allows.
• Removal of microbial plaque and calculus
is necessary to establish periodontal health
• periodontal surgery may be needed to stop
progressive bone loss and regenerate lost
bone where possible.
Etiology of bleeding disorders
 Thrombotic Thrombocytopenia purpuras (TTP) :
1. primary
2. secondary : Chemicals, ex: mitomycin C
Physical agent (radiation)
Systemic disease (leukemia)
Character:
1. 1.Thrombocytpenia 2. Micro-angiopathic hemolytic
anemia(MAHA) 3. Fever 4. Hyporenal function 5. Neural systemic
disturbance due to ischemic
2. Considered to be an emergency
3. Tx: plasma exchange and glucocortisone application
Etiology of bleeding disorders
 Disorders of coagulation
1. Inherited : Hemophilia A
Christmas disease
von Willebrandis Disease
2. Acquired : Liver disease
Vitamin K deficiency
Anticoagulation drugs (heparin, coumarin)
Anemia
Evaluation of bleeding disorders
 1. Take history
 2. Physical examination
 3. Screening clinical laboratory tests
 4. Observation of excessive bleeding following a surgical
procedure
History
 Bleeding problems in relatives
 Bleeding problems following operations and tooth
extractions, trauma
 Use of drugs for prevention of coagulation or pain
 Spontaneous bleeding from nose mouth etc..
Physical examination
 Jaundice
 Petechiae : < 0.2 cm
 Purpura : 0.2 cm-1 cm
 Eccymoses : > 1 cm
 Spider angioma
 Oral ulcer
 Hyperplasia of gingiva
 Hemarthrosis
Screening laboratory tests
 1. Platelet count
 2. BT (Bleeding Time)
 3. PT (Prothrombin Time)
 4. aPTT (active Partial Thrombopastin Time)
 5. TT (Thrombin Time)
primary
secondary
Platelet count
 Test platelet phase: evaluation of platelet function
 Normal (140,000 to 400,000/mm3)
 Thrombocytopenia : < 140,000/mm3
 Clinical bleeding problem : <50,000/mm3
 Spontaneous bleeding with life theartening : <20,000/mm3
BT (Ivy method)
 Test platelet & vascular phase
 Normal if adequate number of platelets of good quality
present intact vascular walls
 Normal ( 1 to 6 minutes )
PT (Prothrombin Time)
 Activated by tissue thromboplastin
 Tests extrinsic ( factor VII ) and common ( I,II,V,X )
pathways
 Normal ( 11-15sec )
 Coumarin therapy- PT at 1.5 to 2.5 time
 International normalized ratio= INR, (1) surgery can be
done under INR< 3.0 (2) when INR=3.0-3.5, consultation
is needed (3) delay surgery when INR>3.5
Activated PTT (aPTT)
 Activated by contact activator (kaolin)
 Tests intrinsic and common pathway
 Normal ( 25-35 sec )
 Heparin therapy- PTT in 50-65 sec range by promote AT
III
TT (Thrombin Time)
 Activated by thrombin
 Tests ability to form initial clot from fibrinogen
 Normal ( 9 to 13 seconds )
Patient at low risk
 1. patient with no history of bleeding disorders,
normal
examinations, no medications associated with
bleeding
disorders and normal bleeding parameters
 2. patients with nonspecific history of excessive
bleeding
with normal bleeding parameters (PT, PTT, BT,
platelet count, are within normal time)
Patient at moderate risk
 1. patients in chronic oral anticoagulant therapy
(coumadin)
 2. patients on chronic aspirin therapy
Patient at high risk
 1. patients with known bleeding disorders
Thrombocytopenia
Thrombocytopathy
Clotting factor defects
 2. Patient without known bleeding disorders found to
have abnormal , platelet count, BT, PT, PTT
Dental management of bleeding disorders
 Replacement therapy :
1. platelet concentrate : thrombocytopenia ( 1 unit= 30,000/
uL enough for 1 day )
2. Fresh frozen plasma : liver disease, Hemophilia B, vWD
type III
3. Factor VIII,IX concentrate : Hemophilia A ( 1 unit /kg can
add 2%, so 50 unit /kg add 100% )
4. Factor IX concentrate : Hemophilia B
5. 1-desamino-8-darginine vesopressin (DDAVP) :
Hemophilia A, vWD type I, II
 Antifibrinolytic therapy:
1. E-aminocaproic acid (EACA, Plaslloid)
2. Tranexamic acid (AMCA, Transamin)
Local hemostatic methods
 splints, pressure packs, sutures; gelfoam with thrombin,
surgicel, oxycel, microfibrillar collagen(avitene), topical
AHF
Heparin (anticoagulant)
 Complex inhibited ( IXa, Xa, XIa, XIIa )
 Used in deep vein thrombosis , renal dialysis
 Rapid onset, Duration 4-6hrs ( given IV )
 Monitoring by aPTT: 50-65 sec
 Discontinue 6 hrs before surgery then reinstituting therapy
6-12hrs post –op
 Protamine sulfate can reverse the effect
Coumarin (Vit k anatagonist)
 Inhibit Vit K action (Factor II,VII,IX,X)
 Used venous thrombosis, cerebrovascular disease
 Duration haft-life 40hrs
 Monitored by PT : INR 1.5-2.5
 PT>2.5, reduction coumarin dosage ( 2-3 days )
 Vit. K can reverse the effect
Aspirin (antiplatelet)
 Inhibit cycloxygenase, TxA2 formation
 Analgesic drug impairs platelet function
 Aterial thrombosis, MI
 Tests-BT, aPTT
 If tests are abnormal , MD should be consulted before
dental surgery is done
 Stop aspirin for 5 days, substitute alternative drug in
consultation with MD
Thrombocytopenia
 Disease in number of circulation platelets
 Idiopathic thrombocytopenia, secondary thrombocytopenia
 TX : is none indicated unless
platelets<20000/mm3, or excessive bleeding
 TX : Steroid, platelet transfusion
Von Willebrandis Disease
Gene mutation on Von Willebrandis factor; most common
Inherited disease in America ( 1% )
• Type I : 70%-80%, partial loss on quantity
• Type II : poor on quality
• Type III : severe loss on quantity, inactive to DDAVP
Hemophilia
 Sex-linked recessive trait, X chromosome, male > female
 Prolong aPTT, normal BT,PT
 Hemophilia A (factor VIII deficiency)
 Hemophilia B or Christmas disease (factor IX deficiency)
 Severity of disorder : severe<1%, moderate 1-5%,
mild 6-30%
 TX : Replacement factors, antifibrinilytic agents, steroids
Hemophilia-dental management
 Preventive dentistry
1. tooth brushing, flossing, rubber cup prophylaxis &
topical fluoride, supragingival scaling
2. without prior replacement therapy
 Pain control
1. block anesthesia: factor level>50%
2. Avoid aspirin, NSAIDs
Hemophilia-dental management
 Orthodontic treatment :
1. no contraindication in well-motivated patients
2. care with placement of bands and wires
 Operative dentistry
1. rubber dam to protect tissue against accidental
laceration
2. wedges should be place to protect and retract
papilla
Hemophilia-dental management
 Pulp therapy
1. Preferable to extraction
2. Avoid overinstrumentation and overfilling
 Periodontal therapy
1. no contraindication of probing and supragingival
scaling
2. deep scaling, curettage, surgery need replacement
therapy
Hemophilia-dental management
 Oral surgery :
1. Dental extraction: 40%-50% level
2. Maxillofacial surgery (including surgery
extraction of impaction teeth): 80-100%
3. Antifribrinilytic therapy & local hemastatic
measure
4. do not open lingual tissue in lower molar regions to
avoid hemorrhage track down a endanger airway
Summary
 History, PE, Lab data
 Consultation with physician
 Antibiotics to prevent post-op infection
 Avoid aspirin and NSAIDs
 Local hemostatic measure is very important
The End
• Thank you!
Dr Sachin RathodDr Sachin Rathod
Email:- drsachin.rathod@yahoo.comEmail:- drsachin.rathod@yahoo.com

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Bleeding disorder & periodontitis By Dr sachin Rathod

  • 1. Bleeding disorder & Periodontitis Department Of Periodontics Dr Sachin RathodDr Sachin Rathod Email:- drsachin.rathod@yahoo.comEmail:- drsachin.rathod@yahoo.com
  • 2. Content • Definition • Etiology • Evaluation • Dental management • Summary
  • 3. Definition • Periodontitis Periodontitis is a set of inflammatory diseases affecting the periodontium, i.e., the tissues that surround and support the teeth. • Bleeding disorders Bleeding disorders are a group of conditions in which there is a problem with the body's blood clotting process. These disorders can lead to heavy and prolonged bleeding after an injury.
  • 4. Etiology of bleeding disorder  1. Thrombocytopenia purpuras  2. Disorders of coagulation Etiology Of Periodontitis • Periodontitis is caused by microorganisms that adhere to and grow on the tooth's surfaces, along with an overly aggressive immune response against these microorganisms.
  • 5. • Periodontitis is an inflammation of the periodontium, i.e., the tissues that support the teeth. The periodontium consists of four tissues: • gingiva, or gum tissue, • cementum, or outer layer of the roots of teeth, • alveolar bone, or the bony sockets into which the teeth are anchored, and • periodontal ligaments (PDLs), which are the connective tissue fibers that run between the cementum and the alveolar bone.
  • 6. Signs and symptoms • Redness or bleeding of gums while brushing teeth • Gum swelling that recurs • Spitting out blood after brushing teeth • Halitosis, or bad breath, and a persistent metallic taste in the mouth • Gingival recession, resulting in apparent lengthening of teeth. • Deep pockets between the teeth and the gums • Loose teeth, in the later stage
  • 7. Treatment • Excellent Oral Hygiene : This includes twice-daily brushing with daily flossing. • use of an interdental brush is helpful if space between the teeth allows. • Removal of microbial plaque and calculus is necessary to establish periodontal health • periodontal surgery may be needed to stop progressive bone loss and regenerate lost bone where possible.
  • 8. Etiology of bleeding disorders  Thrombotic Thrombocytopenia purpuras (TTP) : 1. primary 2. secondary : Chemicals, ex: mitomycin C Physical agent (radiation) Systemic disease (leukemia) Character: 1. 1.Thrombocytpenia 2. Micro-angiopathic hemolytic anemia(MAHA) 3. Fever 4. Hyporenal function 5. Neural systemic disturbance due to ischemic 2. Considered to be an emergency 3. Tx: plasma exchange and glucocortisone application
  • 9. Etiology of bleeding disorders  Disorders of coagulation 1. Inherited : Hemophilia A Christmas disease von Willebrandis Disease 2. Acquired : Liver disease Vitamin K deficiency Anticoagulation drugs (heparin, coumarin) Anemia
  • 10. Evaluation of bleeding disorders  1. Take history  2. Physical examination  3. Screening clinical laboratory tests  4. Observation of excessive bleeding following a surgical procedure
  • 11. History  Bleeding problems in relatives  Bleeding problems following operations and tooth extractions, trauma  Use of drugs for prevention of coagulation or pain  Spontaneous bleeding from nose mouth etc..
  • 12. Physical examination  Jaundice  Petechiae : < 0.2 cm  Purpura : 0.2 cm-1 cm  Eccymoses : > 1 cm  Spider angioma  Oral ulcer  Hyperplasia of gingiva  Hemarthrosis
  • 13. Screening laboratory tests  1. Platelet count  2. BT (Bleeding Time)  3. PT (Prothrombin Time)  4. aPTT (active Partial Thrombopastin Time)  5. TT (Thrombin Time) primary secondary
  • 14. Platelet count  Test platelet phase: evaluation of platelet function  Normal (140,000 to 400,000/mm3)  Thrombocytopenia : < 140,000/mm3  Clinical bleeding problem : <50,000/mm3  Spontaneous bleeding with life theartening : <20,000/mm3
  • 15. BT (Ivy method)  Test platelet & vascular phase  Normal if adequate number of platelets of good quality present intact vascular walls  Normal ( 1 to 6 minutes )
  • 16. PT (Prothrombin Time)  Activated by tissue thromboplastin  Tests extrinsic ( factor VII ) and common ( I,II,V,X ) pathways  Normal ( 11-15sec )  Coumarin therapy- PT at 1.5 to 2.5 time  International normalized ratio= INR, (1) surgery can be done under INR< 3.0 (2) when INR=3.0-3.5, consultation is needed (3) delay surgery when INR>3.5
  • 17. Activated PTT (aPTT)  Activated by contact activator (kaolin)  Tests intrinsic and common pathway  Normal ( 25-35 sec )  Heparin therapy- PTT in 50-65 sec range by promote AT III
  • 18. TT (Thrombin Time)  Activated by thrombin  Tests ability to form initial clot from fibrinogen  Normal ( 9 to 13 seconds )
  • 19. Patient at low risk  1. patient with no history of bleeding disorders, normal examinations, no medications associated with bleeding disorders and normal bleeding parameters  2. patients with nonspecific history of excessive bleeding with normal bleeding parameters (PT, PTT, BT, platelet count, are within normal time)
  • 20. Patient at moderate risk  1. patients in chronic oral anticoagulant therapy (coumadin)  2. patients on chronic aspirin therapy
  • 21. Patient at high risk  1. patients with known bleeding disorders Thrombocytopenia Thrombocytopathy Clotting factor defects  2. Patient without known bleeding disorders found to have abnormal , platelet count, BT, PT, PTT
  • 22. Dental management of bleeding disorders  Replacement therapy : 1. platelet concentrate : thrombocytopenia ( 1 unit= 30,000/ uL enough for 1 day ) 2. Fresh frozen plasma : liver disease, Hemophilia B, vWD type III 3. Factor VIII,IX concentrate : Hemophilia A ( 1 unit /kg can add 2%, so 50 unit /kg add 100% ) 4. Factor IX concentrate : Hemophilia B 5. 1-desamino-8-darginine vesopressin (DDAVP) : Hemophilia A, vWD type I, II  Antifibrinolytic therapy: 1. E-aminocaproic acid (EACA, Plaslloid) 2. Tranexamic acid (AMCA, Transamin)
  • 23. Local hemostatic methods  splints, pressure packs, sutures; gelfoam with thrombin, surgicel, oxycel, microfibrillar collagen(avitene), topical AHF
  • 24. Heparin (anticoagulant)  Complex inhibited ( IXa, Xa, XIa, XIIa )  Used in deep vein thrombosis , renal dialysis  Rapid onset, Duration 4-6hrs ( given IV )  Monitoring by aPTT: 50-65 sec  Discontinue 6 hrs before surgery then reinstituting therapy 6-12hrs post –op  Protamine sulfate can reverse the effect
  • 25. Coumarin (Vit k anatagonist)  Inhibit Vit K action (Factor II,VII,IX,X)  Used venous thrombosis, cerebrovascular disease  Duration haft-life 40hrs  Monitored by PT : INR 1.5-2.5  PT>2.5, reduction coumarin dosage ( 2-3 days )  Vit. K can reverse the effect
  • 26. Aspirin (antiplatelet)  Inhibit cycloxygenase, TxA2 formation  Analgesic drug impairs platelet function  Aterial thrombosis, MI  Tests-BT, aPTT  If tests are abnormal , MD should be consulted before dental surgery is done  Stop aspirin for 5 days, substitute alternative drug in consultation with MD
  • 27. Thrombocytopenia  Disease in number of circulation platelets  Idiopathic thrombocytopenia, secondary thrombocytopenia  TX : is none indicated unless platelets<20000/mm3, or excessive bleeding  TX : Steroid, platelet transfusion
  • 28. Von Willebrandis Disease Gene mutation on Von Willebrandis factor; most common Inherited disease in America ( 1% ) • Type I : 70%-80%, partial loss on quantity • Type II : poor on quality • Type III : severe loss on quantity, inactive to DDAVP
  • 29. Hemophilia  Sex-linked recessive trait, X chromosome, male > female  Prolong aPTT, normal BT,PT  Hemophilia A (factor VIII deficiency)  Hemophilia B or Christmas disease (factor IX deficiency)  Severity of disorder : severe<1%, moderate 1-5%, mild 6-30%  TX : Replacement factors, antifibrinilytic agents, steroids
  • 30. Hemophilia-dental management  Preventive dentistry 1. tooth brushing, flossing, rubber cup prophylaxis & topical fluoride, supragingival scaling 2. without prior replacement therapy  Pain control 1. block anesthesia: factor level>50% 2. Avoid aspirin, NSAIDs
  • 31. Hemophilia-dental management  Orthodontic treatment : 1. no contraindication in well-motivated patients 2. care with placement of bands and wires  Operative dentistry 1. rubber dam to protect tissue against accidental laceration 2. wedges should be place to protect and retract papilla
  • 32. Hemophilia-dental management  Pulp therapy 1. Preferable to extraction 2. Avoid overinstrumentation and overfilling  Periodontal therapy 1. no contraindication of probing and supragingival scaling 2. deep scaling, curettage, surgery need replacement therapy
  • 33. Hemophilia-dental management  Oral surgery : 1. Dental extraction: 40%-50% level 2. Maxillofacial surgery (including surgery extraction of impaction teeth): 80-100% 3. Antifribrinilytic therapy & local hemastatic measure 4. do not open lingual tissue in lower molar regions to avoid hemorrhage track down a endanger airway
  • 34. Summary  History, PE, Lab data  Consultation with physician  Antibiotics to prevent post-op infection  Avoid aspirin and NSAIDs  Local hemostatic measure is very important
  • 35. The End • Thank you! Dr Sachin RathodDr Sachin Rathod Email:- drsachin.rathod@yahoo.comEmail:- drsachin.rathod@yahoo.com