Clonal Dynamics After Allogeneic Haematopoietic Cell Transplantation

Overview

Journal Nature

Specialty Science

Date 2024 Oct 31

PMID 39478227

Authors

Michael Spencer Chapman

C Matthias Wilk

Steffen Boettcher

Emily Mitchell

Kevin Dawson

Nicholas Williams

Jan Muller

Larisa Kovtonyuk

Hyunchul Jung

Francisco Caiado

Kirsty Roberts

Laura ONeill

David G Kent

Anthony R Green

Jyoti Nangalia

Markus G Manz

Peter J Campbell

Affiliations

Soon will be listed here.

Abstract

Allogeneic haematopoietic cell transplantation (HCT) replaces the stem cells responsible for blood production with those from a donor. Here, to quantify dynamics of long-term stem cell engraftment, we sequenced genomes from 2,824 single-cell-derived haematopoietic colonies of ten donor-recipient pairs taken 9-31 years after HLA-matched sibling HCT. With younger donors (18-47 years at transplant), 5,000-30,000 stem cells had engrafted and were still contributing to haematopoiesis at the time of sampling; estimates were tenfold lower with older donors (50-66 years). Engrafted cells made multilineage contributions to myeloid, B lymphoid and T lymphoid populations, although individual clones often showed biases towards one or other mature cell type. Recipients had lower clonal diversity than matched donors, equivalent to around 10-15 years of additional ageing, arising from up to 25-fold greater expansion of stem cell clones. A transplant-related population bottleneck could not explain these differences; instead, phylogenetic trees evinced two distinct modes of HCT-specific selection. In pruning selection, cell divisions underpinning recipient-enriched clonal expansions had occurred in the donor, preceding transplant-their selective advantage derived from preferential mobilization, collection, survival ex vivo or initial homing. In growth selection, cell divisions underpinning clonal expansion occurred in the recipient's marrow after engraftment, most pronounced in clones with multiple driver mutations. Uprooting stem cells from their native environment and transplanting them to foreign soil exaggerates selective pressures, distorting and accelerating the loss of clonal diversity compared to the unperturbed haematopoiesis of donors.

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