Infections after hematopoietic stem cell transplantation: Difference between revisions

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==Prevention==
==Prevention==

=== Pre-Transplant Screening ===

* For autoHSCT: HBV, HCV, HEV, and HIV screening

=== By Infection ===
{| class="wikitable"
{| class="wikitable"
!Infection
!Infection
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|Immunization of all HCT recipients. Post-exposure prophylaxis if exposed.
|Immunization of all HCT recipients. Post-exposure prophylaxis if exposed.
|-
|-
|''[[Bordatella pertussis]]''
|''[[Bordetella pertussis]]''
|Ensuring up-to-date immunizations of close contacts.
|Ensuring up-to-date immunizations of close contacts.
|Immunization of all HCT recipients. Post-exposure prophylaxis if exposed.
|Immunization of all HCT recipients. Post-exposure prophylaxis if exposed.
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|[[Toxoplasma gondii]]
|[[Toxoplasma gondii]]
|Provide education about decreasing risk.
|Provide education about decreasing risk.
|Pretransplant screening of IgG antibody (reactivation in 2 to 6% of those who are positive). Consider preemptive therapy or prophylaxis for high-risk (e.g. allogeneic HSCT) recipients. Not needed for autologous transplants.
|Pretransplant screening of IgG antibody (reactivation in 2 to 6% of those who are positive). Consider preemptive therapy or prophylaxis for high-risk (e.g. allogeneic HSCT) recipients; note that prophylaxis with [[TMP-SMX]] may already be indicated for [[Pneumocystis]], above. Not needed for autologous transplants.
|-
|-
|[[Strongyloides stercoralis]]
|[[Strongyloides stercoralis]]
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|Seropositivity is not a contraindication to receiving transplant.
|Seropositivity is not a contraindication to receiving transplant.
|-
|-
|[[Plasmodium species]]
|[[Plasmodium]]
|Exclusion of donors who have traveled to malaria-endemic area in past 1 year, or who have lived in an endemic area in past 3 years. If not feasible to wait, consider treating donor empirically before donation.
|Exclusion of donors who have traveled to malaria-endemic area in past 1 year, or who have lived in an endemic area in past 3 years. If not feasible to wait, consider treating donor empirically before donation.
|Pre-transplant screening of recipients by blood smear, rapid test, or PCR.
|Pre-transplant screening of recipients by blood smear, rapid test, or PCR.
|}
|}


===Antimicrobial Prophylaxis===
===Antimicrobial Prophylaxis in AlloHSCT===
{| class="wikitable"
{| class="wikitable"
! rowspan="2" |Time
! rowspan="2" |Time
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|-
|-
|'''Pre-engraftment'''<br />day 0 to 30
|'''Pre-engraftment'''<br />day 0 to 30
|[[levofloxacin]] or other [[fluoroquinolone]]
|[[levofloxacin]] or other [[fluoroquinolone]] starting D+1 until engraftment (ANC>1 x3d)
|[[HSV]]-positive: ([[valacyclovir|val]])[[acyclovir]]
|[[HSV]]-positive: ([[valacyclovir|val]])[[acyclovir]]
[[VZV]]-positive: ([[valacyclovir|val]])[[acyclovir]]
[[VZV]]-positive: ([[valacyclovir|val]])[[acyclovir]]
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|[[VZV]]-positive: ([[valacyclovir|val]])[[acyclovir]]
|[[VZV]]-positive: ([[valacyclovir|val]])[[acyclovir]]
[[CMV]]-positive: [[valganciclovir]] or preemptive therapy
[[CMV]]-positive: [[valganciclovir]] or preemptive therapy
|[[fluconazole]] (or [[voriconazole]] or [[posaconazole]]) (to day 75)
|[[fluconazole]] (or [[voriconazole]] or [[posaconazole]]) (to day 75-100 and off immunosuppression)
[[TMP-SMX]] for [[PJP]]
[[TMP-SMX]] for [[PJP]]
|-
|-
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|[[posaconazole]], [[TMP-SMX]] for [[PJP]]
|[[posaconazole]], [[TMP-SMX]] for [[PJP]]
|}
|}

=== Autologous HSCT ===

* Bacterial
** Can consider [[levofloxacin]] prophylaxis, which decreases risk of infection but doesn't affect mortality
* Viral
** Suggest [[acyclovir]] as [[HSV]]/[[VZV]] prophylaxis for at least 6 months
** No role for [[CMV]] prophylaxis
** Monitor for [[EBV]] reactivation, which is a concern
** [[Tenofovir]] or [[entecavir]] as [[HBV]] prophylaxis in patients with positive HBsAg or HBcAb, with serial monitoring of HBV DNA
* Fungal
** Can consider [[TMP-SMX]] prophylaxis for [[PJP]] for at least 3-6 months and until CD4 count is about 200
** No role for antifungal, but can consider until ANC over 1 for 3 days


==Further Reading==
==Further Reading==

Latest revision as of 16:42, 28 July 2023

See also:

Timeline of Infections

Time Risk factors Organisms
Bacteria Viruses Fungi Parasites
Pre-engraftment
day 0 to 30
Neutropenia, mucositis, and central lines GPCs and GNBs BK virus, HSV, and resp/enteric viruses Candida and Aspergillus Strongyloides
Early post-engraftment
to day 100
Immunosuppressing meds, acute GVHD, central lines GPCs, encapsulated bacteria, Listeria, Salmonella, Nocardia HSV, CMV, HHV-6, adenovirus, resp/enteric viruses Aspergillus, other molds, PJP Strongyloides, Toxoplasma
Mid post-engraftment
to 1 year
Immunosuppressing meds, chronic GVHD Encapsulated bacteria, Listeria, Salmonella, Nocardia VZV, EBV (and PTLD), CMV, respiratory/enteric viruses Aspergillus, other molds, PJP
Late post-engraftment
after 1 year
Immunosuppresing meds, chronic GVHD Encapsulated bacteria, Listeria, Salmonella, Nocardia VZV, CMV, respiratory/enteric viruses

Prevention

Pre-Transplant Screening

  • For autoHSCT: HBV, HCV, HEV, and HIV screening

By Infection

Infection Preventing exposure Preventing disease
Bacterial infections
Early disease (0-100 days after HCT) Use levofloxacin or other respiratory fluoroquinolone in adult patients with anticipated neutropenia of 7 or more days until recovery of neutropenia. GM-CSF or G-CSF may decrease risk of infection, but unclear if it decreases mortality.
Late disease (100 days after HCT) Antibiotic prophylaxis is indicated for alloHSCT recipients with chronic GVHD to prevent invasive pneumococcal disease until cGVHD resolves.
CLABSI Implement a CLABSI bundle to ensure maximum sterility on insertion. If infection rate is still >1 per 1000 catheter days, can consider prophylactic minocycline plus rifampin.
Streptococcus pneumoniae Routine precautions. Immunization for all HCT recipients. Antibiotic prophylaxis for chronic GVHD and for low IgG levels, regardless of vaccination status, usually with penicillin.
Viridans group streptococci Pre-conditioning dental consults.
Haemophilus influenzae type b Ensuring up-to-date immunizations of close contacts. Immunization of all HCT recipients. Post-exposure prophylaxis if exposed.
Bordetella pertussis Ensuring up-to-date immunizations of close contacts. Immunization of all HCT recipients. Post-exposure prophylaxis if exposed.
Viral infections
Cytomegalovirus Pre-transplant screening of donor and recipient IgG serostatus. All R+ or D+ recipients should have either prophylaxis or close monitoring with preemptive treatment until at least day 100. Monitoring should start on day 10 and continue weekly until at least day 100.
Epstein-Barr virus, especially PTLD Pre-transplant screening of donor and recipient IgG serostatus, especially in children. Monitor high-risk recipients (T-cell depletion, ant-T-cell antibodies, umbilical cord transplants, and haplo-identical transplants), with reduction in immunosuppression if rising viral load.
Herpes simplex virus Pre-transplant screening of donor and recipient IgG serostatus. Counselling of seronegative recipients on protective behaviours. Acyclovir for all seropositive recipients of alloHSCT from conditioning until engraftment (about 30 days). Not necessary if receiving prophylaxis for CMV.
Varicella-zoster virus Pre-transplant screening of donor and recipient IgG serostatus. Close contacts should have up-to-date vaccinations before visiting. Acyclovir or valacyclovir for all seropositive recipients of alloHSCT from conditioning until 1 year and during chronic GVHD. Post-exposure prophylaxis with VariZIG for seronegative recipients.
Influenza Annual immunization of recipient and close contacts. Consider prophylaxis of recipient and possibly also close contacts during outbreaks.
Adenovirus Weekly screening PCR for the first 6 months and during severe immunosuppression.
Hepatitis B virus Pre-transplant screening of donor and recipient serostatus. Immunization of seronegative recipients. Monitoring ALT during prolonged corticosteroid use with HBV DNA viral load if ALT is elevated, and pre-emptive antiviral therapy if the viral load is positive. Consider prophylaxis for anti-HBc-positive recipients from conditioning to 6 months after transplant. Monitor anti-HBs titres every 3 months, with viral load if it is decreasing. Re-immunize if titres become negative. Treatment of choice is lamivudine 100 mg/day.
Hepatitis C virus Pre-transplant screening of donor and recipient serostatus with viral load if positive or if at elevated risk despite negative serology. For those with HCV, consider liver biopsy if iron overloaded, alcohol abuse, HCV for longer than 10 years, or clinical evidence of chronic liver disease. Consider treatment after 2 years post-transplant if without GVHD and no immunosuppressing medications for at least 6 months.
Fungal infections
Yeasts, especially Candida Fluconazole or a mold-active azole from conditioning until engraftment, and possibly to day 75.
Molds, especially Aspergillus Appropriate IPAC practices, including positive-pressure ventilation in recipient rooms. Unclear role for prophylaxis, though can use posaconazole during GVHD.
Pneumocystis jirovecii TMP-SMX in recipients of alloHSCT from engraftment until 6 months after transplant.
Other infections
Mycobacterium tuberculosis Avoid exposure, including certain occupations Screen for and treat LTBI prior to transplant. Consider prophylaxis with INH post-transplant.
Toxoplasma gondii Provide education about decreasing risk. Pretransplant screening of IgG antibody (reactivation in 2 to 6% of those who are positive). Consider preemptive therapy or prophylaxis for high-risk (e.g. allogeneic HSCT) recipients; note that prophylaxis with TMP-SMX may already be indicated for Pneumocystis, above. Not needed for autologous transplants.
Strongyloides stercoralis Avoid contact with outhouses and cutaneous exposure soil or human feces. High-risk patients should be screened for IgG antibodies and treated with ivermectin before transplantation.
Trypanosoma cruzi Pre-transplant screening of donor and recipient serostatus in those who were born in, received a transfusion in, or have ever lived at least 6 months in a Chagas-endemic area. Exclusion of positive donors. Seropositivity is not a contraindication to receiving transplant.
Plasmodium Exclusion of donors who have traveled to malaria-endemic area in past 1 year, or who have lived in an endemic area in past 3 years. If not feasible to wait, consider treating donor empirically before donation. Pre-transplant screening of recipients by blood smear, rapid test, or PCR.

Antimicrobial Prophylaxis in AlloHSCT

Time Organisms
Bacteria Viruses Fungi
Pre-engraftment
day 0 to 30
levofloxacin or other fluoroquinolone starting D+1 until engraftment (ANC>1 x3d) HSV-positive: (val)acyclovir

VZV-positive: (val)acyclovir

CMV-positive: valganciclovir or preemptive therapy (from day 10)

fluconazole (or voriconazole or posaconazole)
Early post-engraftment
to day 100
VZV-positive: (val)acyclovir

CMV-positive: valganciclovir or preemptive therapy

fluconazole (or voriconazole or posaconazole) (to day 75-100 and off immunosuppression)

TMP-SMX for PJP

Mid post-engraftment
to 1 year
VZV-positive: (val)acyclovir TMP-SMX for PJP (to 6 months)
Late post-engraftment
after 1 year
GVHD levofloxacin or other fluoroquinolone for Streptococcus pneumoniae posaconazole, TMP-SMX for PJP

Autologous HSCT

  • Bacterial
    • Can consider levofloxacin prophylaxis, which decreases risk of infection but doesn't affect mortality
  • Viral
    • Suggest acyclovir as HSV/VZV prophylaxis for at least 6 months
    • No role for CMV prophylaxis
    • Monitor for EBV reactivation, which is a concern
    • Tenofovir or entecavir as HBV prophylaxis in patients with positive HBsAg or HBcAb, with serial monitoring of HBV DNA
  • Fungal
    • Can consider TMP-SMX prophylaxis for PJP for at least 3-6 months and until CD4 count is about 200
    • No role for antifungal, but can consider until ANC over 1 for 3 days

Further Reading

  • Life-threatening Infection in Transplant Recipients. Crit Care Clin. 2013 Oct;29(4):953-73. doi: 10.1016/j.ccc.2013.06.012
  • Guidelines for Preventing Infectious Complications among Hematopoietic Cell Transplantation Recipients: A Global Perspective. Biol Blood Marrow Transplant. 2009;15:1143-1238. doi: 10.1016/j.bbmt.2009.06.019